Human Physiology

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March 15, 2013

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Contents
1

Homeostasis
1.1 Overview . . . . . . . . . . . . . .
1.2 Pathways That Alter Homeostasis
1.3 Homeostasis Throughout the Body
1.4 Thermoregulation . . . . . . . . .
1.5 Body Composition . . . . . . . . .
1.6 Cell Structure and Function . . . .
1.7 Parts of the Cell . . . . . . . . . .
1.8 Cell Junctions . . . . . . . . . . .
1.9 Cell Metabolism . . . . . . . . . .
1.10 Cell Building Blocks . . . . . . . .
1.11 Review Questions . . . . . . . . .
1.12 Glossary . . . . . . . . . . . . . . .

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3
3
5
6
10
12
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17
26
27
33
35
37

The Integumentary System

2.1 Introduction . . . . . . .
2.2 Skin . . . . . . . . . . . .
2.3 Hair . . . . . . . . . . . .
2.4 Nails . . . . . . . . . . . .
2.5 Glands . . . . . . . . . . .
2.6 Homeostasis . . . . . . . .
2.7 Glossary . . . . . . . . . .
2.8 Review Questions . . . .
2.9 References . . . . . . . . .

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39
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63
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100

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The Nervous System

3.1 Overview of the entire nervous system . . . . . .
3.2 General functions of the CNS . . . . . . . . . . .
3.3 Structure and function of neurons . . . . . . . .
3.4 Function . . . . . . . . . . . . . . . . . . . . . . .
3.5 Excitatory and inhibitory process . . . . . . . . .
3.6 Summation . . . . . . . . . . . . . . . . . . . . .
3.7 Generation & propagation of an action potential
3.8 Brain . . . . . . . . . . . . . . . . . . . . . . . .
3.9 The Peripheral Nervous System . . . . . . . . . .
3.10 The Autonomic System . . . . . . . . . . . . . .
3.11 Nervous Tissue . . . . . . . . . . . . . . . . . . .
3.12 Case Study . . . . . . . . . . . . . . . . . . . . .
3.13 Drugs . . . . . . . . . . . . . . . . . . . . . . . .
3.14 Review Questions . . . . . . . . . . . . . . . . .

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III

Contents
3.15
3.16
4

IV

Glossary . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 102
References . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 103

The Senses
4.1
What are Senses? . . .
4.2
Chemoreception . . .
4.3
The Sense of Vision .
4.4
The Senses Of Hearing
4.5
Touch . . . . . . . . .
4.6
Review Questions . .
4.7 Glossary . . . . . . .
4.8
References . . . . . . .

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105
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137
138

The Muscular System

5.1
Types . . . . . . . . . . . . . . . . . .
5.2
Muscular System Working With Other
5.3
Skeletal Muscle Contractions . . . . .
5.4
Sliding Filament theory . . . . . . . .
5.5
Involuntary Muscle Movement . . . .
5.6
Injury . . . . . . . . . . . . . . . . . .
5.7
Smooth Muscle Contraction . . . . . .
5.8
Cardiac Muscle . . . . . . . . . . . . .
5.9
ATP in the Human Body . . . . . . .
5.10 Lactic Acid . . . . . . . . . . . . . . .
5.11 Muscle Disorders . . . . . . . . . . . .
5.12 Medical Mysteries . . . . . . . . . . .
5.13 Microbiology . . . . . . . . . . . . . .
5.14 Glossary . . . . . . . . . . . . . . . . .
5.15 References . . . . . . . . . . . . . . . .

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Body Systems
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141
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156

Blood Physiology
6.1
Overview of Blood . . . . . . . . . . .
6.2
Blood Composition . . . . . . . . . . .
6.3
Hemostasis (Coagulation or Clotting)
6.4
ABO Group System . . . . . . . . . .
6.5
Diseases of the Blood . . . . . . . . .
6.6
Glossary . . . . . . . . . . . . . . . . .
6.7
Review Questions . . . . . . . . . . .

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157
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176

The Cardiovascular System

7.1
Introduction . . . . . . . . . . . . . . . .
7.2
The Heart . . . . . . . . . . . . . . . . . .
7.3
Passage of Blood Through the Heart . . .
7.4
The Circulatory System . . . . . . . . . .
7.5
The Cardiovascular Pathways . . . . . . .
7.6
Cardiac Cycle . . . . . . . . . . . . . . . .
7.7
The Heart's Electrical Conduction System
7.8
The ECG . . . . . . . . . . . . . . . . . .

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179
180
180
183
184
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190
193
197

Contents
7.9
7.10
7.11
7.12
7.13
7.14
7.15
7.16
7.17
7.18
7.19
7.20
7.21
7.22
7.23
8

Cardiovascular Disease . . . . . . .
Homeostasis . . . . . . . . . . . . .
Interesting Facts . . . . . . . . . .
Ways to a Healthy Heart . . . . .
Aging . . . . . . . . . . . . . . . .
Shock . . . . . . . . . . . . . . . .
Premature ventricular contractions
Intrinsic Control of heartbeat . . .
Electrocardiogram . . . . . . . . .
Extrinsic Control of Heartbeat . .
Case Study . . . . . . . . . . . . .
Summary . . . . . . . . . . . . . .
Review Questions . . . . . . . . .
Glossary . . . . . . . . . . . . . . .
References . . . . . . . . . . . . . .

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(PVC's)
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199
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217
217
218
220
229
230
231
233
234
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235
237
238

The Respiritory System

9.1
Functions . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
9.2
Breathing and Lung Mechanics . . . . . . . . . . . . . . . . . . . . . . .
9.3
Respiratory System: Upper and Lower Respiratory Tracts . . . . . . . .
9.4
Homeostasis and Gas Exchange . . . . . . . . . . . . . . . . . . . . . . .
9.5
Lung Capacity . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
9.6
Stimulation of Breathing . . . . . . . . . . . . . . . . . . . . . . . . . .
9.7
Regulation of Blood pH . . . . . . . . . . . . . . . . . . . . . . . . . . .
9.8
Problems Associated With the Respiratory Tract and Breathing . . . .
9.9
Upper Respiratory Tract Infections . . . . . . . . . . . . . . . . . . . . .
9.10 Lower Respiratory Tract Disorders . . . . . . . . . . . . . . . . . . . . .
9.11 Respiratory Distress Syndrome . . . . . . . . . . . . . . . . . . . . . . .
9.12 Sleep Apnea . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
9.13 Nutrition for COPD (Chronic Obstructive Pulmonary Disease) Patients
9.14 Case Study . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
9.15 Glossary . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
9.16 References . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
9.17 External Resources . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .

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239
240
240
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257

The Urinary System

8.1
Introduction . . . . . . . . . . .
8.2
Functions of the Urinary System
8.3
Organs in the Urinary System .
8.4
Formation of Urine . . . . . . . .
8.5
Maintaining Water-Salt Balance
8.6
Diseases of the Kidney . . . . . .
8.7
Diabetes Insipidus . . . . . . . .
8.8
Urinary tract infections (UTI's) .
8.9
Dialysis and Kidney Transplant .
8.10 Review Questions . . . . . . . .
8.11 Glossary . . . . . . . . . . . . . .
8.12 References . . . . . . . . . . . . .

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Contents
10 The Gastrointestinal System
10.1 Introduction . . . . . . . . . . . . . . . . . . . . .
10.2 Layers of the GI Tract . . . . . . . . . . . . . . . .
10.3 Accessory Organs . . . . . . . . . . . . . . . . . . .
10.4 The Digestive System . . . . . . . . . . . . . . . .
10.5 Esophagus . . . . . . . . . . . . . . . . . . . . . .
10.6 Stomach . . . . . . . . . . . . . . . . . . . . . . . .
10.7 Small Intestine . . . . . . . . . . . . . . . . . . .
10.8 Large Intestine . . . . . . . . . . . . . . . . . . . .
10.9 Pancreas, Liver, and Gallbladder . . . . . . . . . .
10.10 Anus . . . . . . . . . . . . . . . . . . . . . . . . . .
10.11 Conditions Affecting the Esophagus . . . . . . . .
10.12 Conditions Affecting the Stomach and Intestines .
10.13 Disorders of the Pancreas, Liver, and Gallbladder .
10.14 Gastrointestinal Dysfunctions . . . . . . . . . . . .
10.15 Bleeding in the Gastrointestinal tract . . . . . . .
10.16 Colonoscopy . . . . . . . . . . . . . . . . . . . . .
10.17 Case Study . . . . . . . . . . . . . . . . . . . . . .
10.18 Glossary . . . . . . . . . . . . . . . . . . . . . . . .
10.19 External links . . . . . . . . . . . . . . . . . . . . .
10.20 References . . . . . . . . . . . . . . . . . . . . . . .
11 Nutrition
11.1 The Community and Nutrition Programs
11.2 Nutrition and Health in the Community .
11.3 Nutritional Requirements . . . . . . . . .
11.4 Carbohydrates . . . . . . . . . . . . . . .
11.5 Proteins . . . . . . . . . . . . . . . . . . .
11.6 Lipids . . . . . . . . . . . . . . . . . . . .
11.7 Vitamins and Minerals . . . . . . . . . . .
11.8 Nutritional Disorders . . . . . . . . . . .
11.9 Metabolism . . . . . . . . . . . . . . . . .
11.10 Diabetes . . . . . . . . . . . . . . . . . . .
11.11 Calories, Exercise, and Weight . . . . . .
11.12 Glossary . . . . . . . . . . . . . . . . . . .
11.13 Health Information Online . . . . . . . .
11.14 Review Questions . . . . . . . . . . . . .
11.15 References . . . . . . . . . . . . . . . . . .
12 The Endocrine System
12.1 Introduction To The Endocrine
12.2 Types of Glands . . . . . . . .
12.3 Hormones and Types . . . . . .
12.4 Endocrine Glands . . . . . . .
12.5 Antagonistic Hormones . . . .
12.6 Extrathyroidal iodine . . . . .
12.7 Glossary . . . . . . . . . . . . .
12.8 Chapter Review Questions . .

VI

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346
347

Contents
12.9

References . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 349

13 The Male Reproductive System

13.1 Introduction . . . . . . . . . . . .
13.2 Structure . . . . . . . . . . . . . .
13.3 Functions . . . . . . . . . . . . . .
13.4 Puberty . . . . . . . . . . . . . . .
13.5 Sexual Homology . . . . . . . . . .
13.6 Aging . . . . . . . . . . . . . . . .
13.7 Things that can go wrong with the
13.8 Review Questions . . . . . . . . .
13.9 Glossary . . . . . . . . . . . . . . .
13.10 Summary . . . . . . . . . . . . . .
13.11 References . . . . . . . . . . . . . .

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351
351
352
360
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371
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378

14 The Female Reproductive System

14.1 Introduction . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
14.2 External Genitals . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
14.3 Internal Genitals . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
14.4 The Female Reproductive Cycle . . . . . . . . . . . . . . . . . . . .
14.5 Ovarian and Uterine Cycles in the Nonpregnant Woman . . . . . . .
14.6 Sexual Reproduction . . . . . . . . . . . . . . . . . . . . . . . . . . .
14.7 Infertility . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
14.8 Types of Birth Control . . . . . . . . . . . . . . . . . . . . . . . . .
14.9 Sexually Transmitted Diseases . . . . . . . . . . . . . . . . . . . . .
14.10 Diseases and Disorders of the Female Reproductive System
14.11 Check Your Understanding . . . . . . . . . . . . . . . . . . . . . . .
14.12 Glossary . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
14.13 References . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .

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15 Pregnancy and Birth

15.1 Introduction . . . . . . . . . . . . . . . . . . . .
15.2 Fertilization . . . . . . . . . . . . . . . . . . . . .
15.3 Pre-embryonic Period . . . . . . . . . . . . . . .
15.4 Formation of Placenta . . . . . . . . . . . . . . .
15.5 Amniotic Fluid . . . . . . . . . . . . . . . . . . .
15.6 Endocrine Function of the Placenta . . . . . . .
15.7 Developing Baby . . . . . . . . . . . . . . . . . .
15.8 Embryonic Development at Specific Stages . . .
15.9 Pregnancy from the mother's perspective . . . .
15.10 Labor and Birth . . . . . . . . . . . . . . . . . .
15.11 Risks in Pregnancy . . . . . . . . . . . . . . . . .
15.12 Staying Healthy . . . . . . . . . . . . . . . . . .
15.13 In vitro Fertilization and Artificial Implantation
15.14 Embryonic stem cells . . . . . . . . . . . . . . . .
15.15 Pregnancy and Lactation . . . . . . . . . . . . .
15.16 Postpartum Depression . . . . . . . . . . . . . .
15.17 Testing Your Knowledge . . . . . . . . . . . . . .

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413
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VII

Contents
15.18 Glossary . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 448
15.19 Reference . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 451
16 Genetics and Inheritance
16.1 Introduction . . . . . . . . . . . . . . . . . . . . . .
16.2 Transcription and Translation . . . . . . . . . . . . .
16.3 Inheritance . . . . . . . . . . . . . . . . . . . . . . .
16.4 Inherited Genetic Disease . . . . . . . . . . . . . . .
16.5 Non-heritable Genetic Disorders . . . . . . . . . . .
16.6 Mutant Genes . . . . . . . . . . . . . . . . . . . . .
16.7 Genetic Engineering . . . . . . . . . . . . . . . . . .
16.8 Gene Therapy . . . . . . . . . . . . . . . . . . . . .
16.9 Genetic Regulation of Development and Homeostasis
16.10 Glossary . . . . . . . . . . . . . . . . . . . . . . . . .
16.11 Review questions . . . . . . . . . . . . . . . . . . . .

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18 Notes and Resources

18.1 Authors . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
18.2 Content and Contributions . . . . . . . . . . . . . . . . . . . . . . . . . . .
18.3 License . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .

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19 Contributors

525

List of Figures

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17 Human Development
17.1 Overview . . . . . . . . . . . . . . . . . . . .
17.2 Apoptosis . . . . . . . . . . . . . . . . . . . .
17.3 Growth and development . . . . . . . . . . .
17.4 Neonatal . . . . . . . . . . . . . . . . . . . .
17.5 Changes in body Size and Muscle fat makeup
17.6 Infancy . . . . . . . . . . . . . . . . . . . . .
17.7 Adolescence . . . . . . . . . . . . . . . . . . .
17.8 Adulthood . . . . . . . . . . . . . . . . . . .
17.9 Menopause . . . . . . . . . . . . . . . . . . .
17.10 Old Age . . . . . . . . . . . . . . . . . . . . .
17.11 Old Age Diseases . . . . . . . . . . . . . . . .
17.12 The effects of Aging on the Body . . . . . . .
17.13 Life Expectancy . . . . . . . . . . . . . . . .
17.14 Stages of Grief- Death and Dying . . . . . . .
17.15 Sidenotes: Aubrey de Grey . . . . . . . . . .
17.16 Discoveries In Growth And Development . .
17.17 Review Questions . . . . . . . . . . . . . . .
17.18 Glossary . . . . . . . . . . . . . . . . . . . . .
17.19 References . . . . . . . . . . . . . . . . . . . .

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20 Licenses
543
20.1 GNU GENERAL PUBLIC LICENSE . . . . . . . . . . . . . . . . . . . . . 543
20.2 GNU Free Documentation License . . . . . . . . . . . . . . . . . . . . . . . 544

Contents
20.3

GNU Lesser General Public License . . . . . . . . . . . . . . . . . . . . . . 545

1 Homeostasis
1.1 Overview
The human organism consists of trillions of cells all working together for the maintenance
of the entire organism. While cells may perform very different functions, all the cells are
quite similar in their metabolic requirements. Maintaining a constant internal environment
with all that the cells need to survive (oxygen, glucose, mineral ions, waste removal, and so
forth) is necessary for the well-being of individual cells and the well-being of the entire body.
The varied processes by which the body regulates its internal environment are collectively
referred to as homeostasis.

1.1.1 What is Homeostasis?

Homeostasis in a general sense refers to stability, balance or equilibrium. It is the
body's attempt to maintain a constant internal environment. Maintaining a stable internal
environment requires constant monitoring and adjustments as conditions change. This
adjusting of physiological systems within the body is called homeostatic regulation.
Homeostatic regulation involves three parts or mechanisms: 1) the receptor, 2) the control
center and 3) the effector.
The receptor receives information that something in the environment is changing. The
control center or integration center receives and processes information from the receptor. And lastly, the effector responds to the commands of the control center by either
opposing or enhancing the stimulus. This is an ongoing process that continually works to
restore and maintain homeostasis. For example, in regulating body temperature there are
temperature receptors in the skin, which communicate information to the brain, which is
the control center, and the effector is our blood vessels and sweat glands in our skin.
Because the internal and external environment of the body are constantly changing and
adjustments must be made continuously to stay at or near the set point, homeostasis can be
thought of as a synthetic equilibrium.
Since homeostasis is an attempt to maintain the internal conditions of an environment by
limiting fluctuations, it must involve a series of negative feedback loops.

1.1.2 Positive and Negative Feedback

When a change of variable occurs, there are two main types of feedback to which the system
reacts:

Homeostasis
Negative feedback: a reaction in which the system responds in such a way as to reverse
the direction of change. Since this tends to keep things constant, it allows the maintenance
of homeostasis. For instance, when the concentration of carbon dioxide in the human body
increases, the lungs are signaled to increase their activity and expel more carbon dioxide.
Thermoregulation is another example of negative feedback. When body temperature
rises (or falls), receptors in the skin and the hypothalamus sense a change, triggering a
command from the brain. This command, in turn, effects the correct response, in this
case a decrease in body temperature.
Home Heating System Vs. Negative Feedback
When you are at home, you set your thermostat to a desired temperature. Let's say today
you set it at 70 degrees. The thermometer in the thermostat waits to sense a temperature
change either too high above or too far below the 70 degree set point. When this change
happens the thermometer will send a message to the "Control Center", or thermostat,
Which in turn will then send a message to the furnace to either shut off if the temperature
is too high or kick back on if the temperature is too low. In the home-heating example
the air temperature is the "NEGATIVE FEEDBACK." When the Control Center receives
negative feedback it triggers a chain reaction in order to maintain room temperature.
Positive feedback: a response is to amplify the change in the variable. This has a
destabilizing effect, so does not result in homeostasis. Positive feedback is less common
in naturally occurring systems than negative feedback, but it has its applications. For
example, in nerves, a threshold electric potential triggers the generation of a much larger
action potential. Blood clotting in which the platelets process mechanisms to transform
blood liquid to solidify is an example of positive feedback loop. Another example is the
secretion of oxytocin which provides a pathway for the uterus to contract, leading to
child birth.
Harmful Positive Feedback
Although Positive Feedback is needed within Homeostasis it also can be harmful at times.
When you have a high fever it causes a metabolic change that can push the fever higher
and higher. In rare occurrences the body temperature reaches 113 degrees and the cellular
proteins stop working and the metabolism stops, resulting in death.
Summary: Sustainable systems require combinations of both kinds of feedback. Generally
with the recognition of divergence from the homeostatic condition, positive feedbacks are
called into play, whereas once the homeostatic condition is approached, negative feedback
is used for "fine tuning" responses. This creates a situation of "metastability," in which
homeostatic conditions are maintained within fixed limits, but once these limits are exceeded,
the system can shift wildly to a wholly new (and possibly less desirable) situation of
homeostasis.
Homeostatic systems have several properties
They are ultra-stable, meaning the system is capable of testing which way its variables
should be adjusted.
Their whole organization (internal, structural, and functional) contributes to the maintenance of balance.
Physiology is largely a study of processes related to homeostasis. Some of the functions
you will learn about in this book are not specifically about homeostasis (e.g. how muscles

Pathways That Alter Homeostasis

contract), but in order for all bodily processes to function there must be a suitable
internal environment. Homeostasis is, therefore, a fitting framework for the introductory
study of physiology.
Where did the term "Homeostasis" come from?
The concept of homeostasis was first articulated by the French scientist Claude Bernard
(1813-1878) in his studies of the maintenance of stability in the "milieu interior." He said, "All
the vital mechanisms, varied as they are, have only one object, that of preserving constant
the conditions of life in the internal environment" (from Leons sur les Phnonmes de la
Vie Commune aux Animaux et aux Vgtaux, 1879). The term itself was coined by American
physiologist Walter Cannon, author of The Wisdom of the Body (1932). The word comes
from the Greek homoios (same, like, resembling) and stasis (to stand, posture).

1.1.3 Cruise Control on a car as a simple metaphor for homeostasis

When a car is put on cruise control it has a set speed limit that it will travel. At times
this speed may vary by a few miles per hour but in general the system will maintain the
set speed. If the car starts to go up a hill, the systems will automatically increase the
amount of fuel given to maintain the set speed. If the car starts to come down a hill, the
car will automatically decrease the amount of fuel given in order to maintain the set speed.
It is the same with homeostasis- the body has a set limit on each environment. If one of
these limits increases or decreases, the body will sense and automatically try to fix the
problem in order to maintain the pre-set limits. This is a simple metaphor of how the body
operatesconstant monitoring of levels, and automatic small adjustments when those levels
fall below (or rise above) a set point.

1.2 Pathways That Alter Homeostasis

A variety of homeostatic mechanisms maintain the internal environment within tolerable
limits. Either homeostasis is maintained through a series of control mechanisms, or the body
suffers various illnesses or disease. When the cells in the body begin to malfunction, the
homeostatic balance becomes disrupted. Eventually this leads to disease or cell malfunction.
Disease and cellular malfunction can be caused in two basic ways: either, deficiency (cells
not getting all they need) or toxicity (cells being poisoned by things they do not need).
When homeostasis is interrupted in your cells, there are pathways to correct or worsen the
problem. In addition to the internal control mechanisms, there are external influences based
primarily on lifestyle choices and environmental exposures that influence our body's ability
to maintain cellular health.
Nutrition: If your diet is lacking in a specific vitamin or mineral your cells will function
poorly, possibly resulting in a disease condition. For example, a menstruating woman with
inadequate dietary intake of iron will become anemic. Lack of hemoglobin, a molecule that
requires iron, will result in reduced oxygen-carrying capacity. In mild cases symptoms
may be vague (e.g. fatigue), but if the anemia (British English: anaemia) is severe the
body will try to compensate by increasing cardiac output, leading to palpitations and
sweatiness, and possibly to heart failure.

Homeostasis
Toxins: Any substance that interferes with cellular function, causing cellular malfunction.
This is done through a variety of ways; chemical, plant, insecticides, and/or bites. A
commonly seen example of this is drug overdoses. When a person takes too much of a
drug their vital signs begin to waver; either increasing or decreasing, these vital signs can
cause problems including coma, brain damage and even death.
Psychological: Your physical health and mental health are inseparable. Our thoughts
and emotions cause chemical changes to take place either for better as with meditation,
or worse as with stress.
Physical: Physical maintenance is essential for our cells and bodies. Adequate rest,
sunlight, and exercise are examples of physical mechanisms for influencing homeostasis.
Lack of sleep is related to a number of ailments such as irregular cardiac rhythms, fatigue,
anxiety and headaches.
Genetic/Reproductive: Inheriting strengths and weaknesses can be part of our genetic
makeup. Genes are sometimes turned off or on due to external factors which we can have
some control over, but at other times little can be done to correct or improve genetic
diseases. Beginning at the cellular level a variety of diseases come from mutated genes.
For example, cancer can be genetically inherited or can be caused due to a mutation from
an external source such as radiation or genes altered in a fetus when the mother uses
drugs.
Medical: Because of genetic differences some bodies need help in gaining or maintaining
homeostasis. Through modern medicine our bodies can be given different aids, from antibodies to help fight infections, or chemotherapy to kill harmful cancer cells. Traditional
and alternative medical practices have many benefits, but like any medical practice the
potential for harmful effects is present. Whether by nosocomial infections, or wrong
dosage of medication, homeostasis can be altered by that which is trying to fix it. Trial
and error with medications can cause potential harmful reactions and possibly death if
not caught soon enough.
The factors listed above all have their effects at the cellular level, whether harmful or
beneficial. Inadequate beneficial pathways (deficiency) will almost always result in a harmful
waver in homeostasis. Too much toxicity also causes homeostatic imbalance, resulting
in cellular malfunction. By removing negative health influences, and providing adequate
positive health influences, your body is better able to self-regulate and self-repair, thus
maintaining homeostasis.

1.3 Homeostasis Throughout the Body

Each body system contributes to the homeostasis of other systems and of the entire organism.
No system of the body works in isolation, and the well-being of the person depends upon
the well-being of all the interacting body systems. A disruption within one system generally
has consequences for several additional body systems. Here are some brief explanations of
how various body systems contribute to the maintenance of homeostasis:

Homeostasis Throughout the Body

1.3.1 Nervous System

Since the nervous system does not store nutrients, it must receive a continuous supply
from blood. Any interruption to the flow of blood may bring brain damage or death. The
nervous system maintains homeostasis by controlling and regulating the other parts of the
body. A deviation from a normal set point acts as a stimulus to a receptor, which sends
nerve impulses to a regulating center in the brain. The brain directs an effector to act in
such a way that an adaptive response takes place. If, for example, the deviation was a
lowering of body temperature, the effector acts to increase body temperature. The adaptive
response returns the body to a state of normalcy and the receptor, the regulating center,
and the effector temporarily cease their activities. Since the effector is regulated by the very
conditions it produced, this process is called control by negative feedback (fig. 2). This
manner of regulating normalcy results in a fluctuation between two extreme levels. Not
until body temperature drops below normal do receptors stimulate the regulating center
and effectors act to raise body temperature. Regulating centers are located in the central
nervous system, consisting of the brain and spinal cord (fig. 3a, 3b). The hypothalamus is
a portion of the brain particularly concerned with homeostasis; it influences the action of
the medulla oblongata, a lower part of the brain, the autonomic nervous system, and the
pituitary gland.
The nervous system has two major portions: the central nervous system and the peripheral
nervous system (table 3). The peripheral nervous system consists of the cranial and spinal
nerves. The autonomic nervous system is a part of peripheral nervous system and contains
motor neurons that control internal organs. It operates at the subconscious level and has
two divisions, the sympathetic and parasympathetic systems. In general, the sympathetic
system brings about those results we associate with emergency situations, often called fight
or flight reactions, and the parasympathetic system produces those effects necessary to our
everyday existence.

1.3.2 Endocrine System

The endocrine system consists of glands which secrete hormones into the bloodstream. Each
hormone has an effect on one or more target tissues. In this way the endocrine system
regulates the metabolism and development of most body cells and body systems. To be
more specific, the Endocrine system has sex hormones that can activate sebaceous glands,
development of mammary glands, alter dermal blood flow and release lipids from adipocytes
and MSH can stimulate melanocytes on our skin. Our bone growth is regulated by several
hormones, and the endocrine system helps with the mobilization of calcitonin and calcium.
In the muscular system, hormones adjust muscle metabolism, energy production, and growth.
In the nervous system, hormones affect neural metabolism, regulate fluid/electrolyte balance
and help with reproductive hormones that influence CNS development and behaviors. In the
Cardiovascular system, we need hormones that regulate the production of RBC's (red blood
cells), which elevate and lower blood pressure. Hormones also have anti-inflammatory effects
and stimulate the lymphatic system. In summary, the endocrine system has a regulatory
effect on basically every other body system.

Homeostasis

1.3.3 Integumentary System

The integumentary system (the skin) is involved in protecting the body from invading
microbes (mainly by forming a thick impenetrable layer), regulating body temperature
through sweating and vasodilation/vasoconstriction, or shivering and piloerection (goose
bumps), and regulating ion balances in the blood. Stimulation of mast cells also produce
changes in blood flow and capillary permeability which can effect the blood flow in the body
and how it is regulated. It also helps synthesize vitamin D which interacts with calcium
and phosphorus absorption needed for bone growth, maintenance, and repair. Hair on the
skin guards entrance into the nasal cavity or other orifices, preventing invaders from getting
further into our bodies. Our skin also helps maintain balance by excretion of water and
other solutes (i.e.) the keratinized epidermis limits fluid loss through skin. It also provides
mechanical protection against environmental hazards. We need to remember that our skin
is integumentary; it is our first line of defense.

1.3.4 Skeletal System

As the structural framework for the human body, the skeletal system consists mainly of
the 206 or so bones of the skeletal system but also includes cartilages, ligaments, and other
connective tissues that stabilize and interconnect them. Bones work in conjunction with the
muscular system to aid in posture and locomotion. Many bones of the skeleton function
as levers, which change the magnitude and direction of forces generated by skeletal muscle.
Protection is a pivotal role occupied by the skeletal system, as many vital organs are encased
within the skeletal cavities (eg. cranial and spinal), and bones form much of the structural
basis for other body cavities (ex: thoracic and pelvic cavities). The skeletal system also
serves as an important mineral reserve. For example, if blood levels of calcium or magnesium
are low and the minerals are not available in the diet, they will be taken from the bones.
Also, the skeletal system provides calcium needed for all muscular contraction. Finally, red
blood cells, lymphocytes and other cells relating to the immune response are produced and
stored in the bone marrow.

1.3.5 Muscular System

The muscular system is one of the most versatile systems in the body. The muscular system
contains the heart, which constantly pumps blood through the body. The muscular system
is also responsible for involuntary (e.g. goosebumps, digestion, breathing) and voluntary
(e.g. walking, picking up objects) actions. Muscles also help protect organs in the body's
cavities. The muscles in your body contract, which increases your body heat when you're
cold. The act of shivering occurs when internal temperature drops. Muscles around vital
organs contract, breaking down ATP, and thereby expending heat, which is then distributed
to the rest of the body.

1.3.6 Cardiovascular System

The cardiovascular system, in addition to needing to maintain itself within certain levels,
plays a role in maintenance of other body systems by transporting hormones (heart secretes

Homeostasis Throughout the Body

Atrial Natriuretic Peptide and Brain Natriuretic Peptide, or ANP and BNP, respectively)
and nutrients (oxygen, EPO to bones,etc.), taking away waste products, and providing all
living body cells with a fresh supply of oxygen and removing carbon dioxide. Homeostasis
is disturbed if the cardiovascular or lymphatic systems are not functioning correctly. Our
skin, bones, muscles, lungs, digestive tract, and nervous, endocrine, lymphatic, urinary and
reproductive systems use the cardiovascular system as its "road" or "highway" as far as
distribution of things such as nutrients, oxygen, waste products, hormones, drugs, etc. There
are many risk factors for an unhealthy cardiovascular system. Some diseases associated are
typically labeled "uncontrollable" or "controllable." The main uncontrollable risk factors are
age, gender, and a family history of heart disease, especially at an early age.
The cardiovascular system also contains sensors to monitor blood pressure, called baroreceptors, that work by detecting how stretched a blood vessel is. This information is relayed to
the Medulla Oblongata in the brain where action is taken to raise or lower blood pressure
via the autonomic nervous system.

1.3.7 Lymphatic System

The lymphatic system has three principal roles. First is the maintenance of blood and tissue
volume. Excess fluid that leaves the capillaries when under pressure would build up and
cause edema. Secondly, the lymphatic system absorbs fatty acids and triglycerides from fat
digestion so that these components of digestion do not enter directly into the blood stream.
Third, the lymphatic system is involved in defending the body against invading microbes,
and the immune response. This system assists in maintenance, such as bone and muscle
repair after injuries. Another defense is maintaining the acidic pH of urine to fight infections
in the urinary system. The tonsils are our bodies "helpers" to defend us against infections
and toxins absorbed from the digestive tract. The tonsils also protect against infections
entering into our lungs.

1.3.8 Respiratory System

The respiratory system works in conjunction with the cardiovascular system to provide
oxygen to cells within every body system for cellular metabolism. The respiratory system
also removes carbon dioxide. Since CO2 is mainly transported in the plasma as bicarbonate
ions, which act as a chemical buffer, the respiratory system also helps maintain proper blood
pH levels, a fact that is very important for homeostasis. As a result of hyperventilation,
CO2 is decreased in blood levels. This causes the pH of body fluids to increase. If acid levels
rise above 7.45, the result is respiratory alkalosis. On the other hand, too much CO2 causes
pH to fall below 7.35 which results in respiratory acidosis. The respiratory system also helps
the lymphatic system by trapping pathogens and protecting deeper tissues within. Note
that when you have increased thoracic space it can provide abdominal pressure through the
contraction of respiratory muscles. This can assist in defecation. Remember the lungs are
the gateway for our breath of life.
or
The organ of the respiratory system includes the nose, pharynx, larynx, trachea, bronchi
and lungs. Together these organs permit the movement of air into the tiny, thin walled sacs

Homeostasis
of the lungs called alveoli. It is in the alveoli that oxygen from the air is exchanged for
the waste product carbon dioxide, which is carried to lungs by the blood so that it can be
eliminated from the body.

1.3.9 Digestive System

Without a regular supply of energy and nutrients from the digestive system, all body systems
would soon suffer. The digestive system absorbs organic substances, vitamins, ions, and
water that are needed all over the body. In the skin, the digestive tract provides lipids for
storage in the subcutaneous layer. Note that food undergoes three types of processes in the
body: digestion, absorption, and elimination. If one of these is not working, you will have
problems that will be extremely noticeable. Mechanics of digestion can include chemical
digestion, movements, ingestion absorption, and elimination. In order to maintain a healthy
and efficient digestive system, we have to remember the components involved. If these are
disturbed, digestive health may be compromised.

1.3.10 Urinary System

Toxic nitrogenous wastes accumulate as proteins and nucleic acids are broken down and used
for other purposes. The urinary system rids the body of these wastes. The urinary system
is also directly involved in maintaining proper blood volume (and indirectly blood pressure)
and ion concentration within the blood. One other contribution is that the kidneys produce
a hormone (erythropoietin) that stimulates red blood cell production. The kidneys also play
an important role in maintaining the correct water content of the body and the correct salt
composition of extracellular fluid. External changes that lead to excess fluid loss trigger
feedback mechanisms that act to inhibit fluid loss.

1.3.11 Reproductive System

The Reproductive System is unique in that it does little to contribute to the homeostasis of
the organism. Rather than being tied to the maintenance of the organism, the reproductive
system relates to the maintenance of the species. Having said that, the sex hormones do
have an effect on other body systems, and an imbalance can lead to various disorders (e.g. a
woman whose ovaries are removed early in life is at much higher risk of osteoporosis).

1.4 Thermoregulation
The living bodies have been characterized with a number of automated processes, which
make them self-sustainable in the natural environment. Among these many processes are
that of reproduction, adjustment with external environment, and instinct to live, which are
gifted by nature to living beings.
The survival of living beings greatly depends on their capability to maintain a stable body
temperature irrespective of temperature of surrounding environment. This capability of
maintaining body temperature is called thermoregulation. Cold blooded animals, such as

10

Thermoregulation
reptiles, have somewhat different means of temperature regulation than warm blooded (or
homeothermic) animals, such as humans and other mammals. This section is most relevant
when considering warm blooded organisms.
Body temperature depends on the heat produced minus the heat lost. Heat is lost by
radiation, convection, and conduction, but the net loss by all three processes depends on a
gradient between the body and the outside. Thus, when the external temperature is low,
radiation is the most important form of heat loss. When there is a high external temperature,
evaporation is the most important form of heat loss. The balance of heat produced and heat
lost maintains a constant body temperature. However, temperature does vary during the
day, and this set point is controlled by the hypothalamus.
Body temperature is usually about 37.4C, but does vary during the day by about 0.8C.
The lowest daily temperature is when the person is asleep. Temperature receptors are found
in the skin, the great veins, the abdominal organs and the hypothalamus. While the ones
in the skin provide the sensation of coldness, the hypothalamic (central core) temperature
receptors are the most important. The core body temperature is usually about 0.7-1.0C
higher than axillary or oral temperature.
When body temperature drops due to external cold, an important component of protection
is vaso-constriction of skin and limb blood vessels. This drops the surface temperature,
providing an insulating layer (such as the fat cell layer) between the core temperature and
the external environment. Likewise, if the temperature rises, blood flow to the skin increases,
maximizing the potential for loss by radiation and evaporation. Thus, if you dilated the skin
blood vessels by alcohol ingestion this might give a nice warm glow, but it would increase
heat loss (if the external temperature was still low). The major adjustments in cold are to
shiver to increase heat production, and constrict blood vessels in the periphery and skin.
This helps to minimize heat loss through the skin, and directs blood to the vital internal
organs.
Besides the daily variation in body temperature, there are other cyclic variations. In women,
body temperature falls prior to ovulation and rises by about 1C at ovulation, largely due
to progesterone increasing the set point. Thyroid hormone and pyrogens also increase the
set point. The basal metabolic rate (BMR) is about 30 calories/sq m/h. It is higher in
children than in adults, partly as a result of different surface area to body mass ratio. Due to
this relationship, young children are more likely to drop their temperature rapidly; there is
greater temperature variation in children than in adults. It is increased by thyroid hormone
and decreased by thyroid hormone lack. Different foods can affect BMR and the Respiratory
Quotient of foods differ. Carbohydrate 1.0; Protein = 1.0; Fats = 0.7

1.4.1 Excretory System

Excretory System is responsible for removing wastes, excess water and salt in the urine.
Regulates the volume and pH of the internal environment. The human excretory system
maintains homeostasis by removing metabolic waste such as water, salt and metabolite
concentrations in the blood. The kidneys, which are the primary excretory organs, are major
organs of homeostasis because they excrete nitrogenous wastes, and regulate water-salt
balance and acid base balance. This section will examine the kidney in details.

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Homeostasis

1.5 Body Composition

1.6 Cell Structure and Function
1.6.1 What is a Cell?
A cell is a structure as well as functional unit of life-Every living thing has cells: bacteria,
protozoans, fungi, plants, and animals are the main groups (Kingdoms) of living things.
Some organisms are made up of just one cell are called uni cellular. (e.g. bacteria and
protozoans), but animals, including human beings, are multi-cellular. An adult human body
is composed of about 100,000,000,000,000 cells! Each cell has basic requirements to sustain
it, and the body's organ systems are largely built around providing the many trillions of
cells with those basic needs (such as oxygen, food, and waste removal).
There are about 200 different kinds of specialized cells in the human body. When many
identical cells are organized together it is called a tissue (such as muscle tissue, nervous
tissue, etc). Various tissues organized together for a common purpose are called organs (e.g.
the stomach is an organ, and so is the skin, the brain, and the uterus).
Ideas about cell structure have changed considerably over the years. Early biologists saw cells
as simple membranous sacs containing fluid and a few floating particles. Today's biologists
know that cells are inconceivably more complex than this. Therefore, a strong knowledge
of the various cellular organelles and their functions is important to any physiologist. If a
person's cells are healthy, then that person is healthy. All physiological processes, disease,
growth and development can be described at the cellular level.

1.6.2 Specialized Cells of the Human Body

Although there are specialized cells - both in structure and function - within the body,
all cells have similarities in their structural organization and metabolic needs (such as
maintaining energy levels via conversion of carbohydrate to ATP and using genes to create
and maintain proteins).
Here are some of the different types of specialized cells within the human body.
Nerve Cells: Also called Neurons, these cells are in the nervous system and function to
process and transmit information (it is hypothesized). They are the core components of
the brain, spinal cord and peripheral nerves. They use chemical synapses that can evoke
electrical signals, called action potentials, to relay signals throughout the body.
Epithelial cells: Functions of epithelial cells include secretion, absorption, protection,
transcellular transport, sensation detection, and selective permeability. Epithelium lines
both the outside (skin) and the inside cavities and lumen of bodies.
Exocrine cells: These cells secrete products through ducts, such as mucus, sweat, or
digestive enzymes. The products of these cells go directly to the target organ through the
ducts. For example, the bile from the gall bladder is carried directly into the duodenum
via the bile duct.
Endocrine cells: These cells are similar to exocrine cells, but secrete their products
directly into the bloodstream instead of through a duct. Endocrine cells are found

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Cell Structure and Function

throughout the body but are concentrated in hormone-secreting glands such as the
pituitary. The products of the endocrine cells go throughout the body in the blood stream
but act on specific organs by receptors on the cells of the target organs. For example, the
hormone estrogen acts specifically on the uterus and breasts of females because there are
estrogen receptors in the cells of these target organs.
Blood Cells: The most common types of blood cells are:
red blood cells (erythrocytes). The main function of red blood cells is to collect
oxygen in the lungs and deliver it through the blood to the body tissues. Gas exchange
is carried out by simple diffusion.
various types of white blood cells (leukocytes). They are produced in the bone
marrow and help the body to fight infectious disease and foreign objects in the immune
system. White cells are found in the circulatory system, lymphatic system, spleen,
and other body tissues.

1.6.3 Cell Size

Cells are the smallest structural & functional living units within our body, but play a big
role in making our body function properly. Many cells never have a large increase in size like
eggs, after they are first formed from a parental cell. Typical stem cells reproduce, double
in size, then reproduce again. Most Cytosolic contents such as the endomembrane system
and the cytoplasm easily scale to larger sizes in larger cells. If a cell becomes too large, the
normal cellular amount of DNA may not be adequate to keep the cell supplied with RNA.
Large cells often replicate their chromosomes to an abnormally high amount or become
multinucleated. Large cells that are primarily for nutrient storage can have a smooth surface
membrane, but metabolically active large cells often have some sort of folding of the cell
surface membrane in order to increase the surface area available for transport functions.

1.6.4 Cellular Organization

Several different molecules interact to form organelles within our body. Each type of organelle
has a specific function. Organelles perform the vital functions that keep our cells alive.
Cell Membranes
The boundary of the cell, sometimes called the plasma membrane, separates internal
metabolic events from the external environment and controls the movement of materials
into and out of the cell. This membrane is very selective about what it allows to pass
through; this characteristic is referred to as "selective permeability." For example, it allows
oxygen and nutrients to enter the cell while keeping toxins and waste products out. The
plasma membrane is a double phospholipid membrane, or a lipid bilayer, with the nonpolar
hydrophobic tails pointing toward the inside of the membrane and the polar hydrophilic
heads forming the inner and outer surfaces of the membrane.

13

Homeostasis

Figure 1

The molecular structure of the cell membrane.

22
Protein and Cholesterol
Proteins and cholesterol molecules are scattered throughout the flexible phospholipid membrane. Peripheral proteins attach loosely to the inner or outer surface of the plasma
membrane. Integral proteins lie across the membrane, extending from inside to outside. A
variety of proteins are scattered throughout the flexible matrix of phospholipid molecules,
somewhat like icebergs floating in the ocean, and this is termed the fluid mosaic model of
the cell membrane.
The phospholipid bilayer is selectively permeable. Only small, uncharged polar molecules can
pass freely across the membrane. Some of these molecules are H2 O and CO2 , hydrophobic
(nonpolar) molecules like O2 , and lipid soluble molecules such as hydrocarbons. Other
molecules need the help of a membrane protein to get across. There are a variety of
membrane proteins that serve various functions:
Channel proteins: Proteins that provide passageways through the membranes for
certain hydrophilic or water-soluble substances such as polar and charged molecules. No
energy is used during transport, hence this type of movement is called facilitated diffusion.
Transport proteins: Proteins that spend energy (ATP) to transfer materials across
the membrane. When energy is used to provide passageway for materials, the process is
called active transport.
Recognition proteins: Proteins that distinguish the identity of neighboring cells. These
proteins have oligosaccharide or short polysaccharide chains extending out from their cell
surface.
Adhesion proteins: Proteins that attach cells to neighboring cells or provide anchors
for the internal filaments and tubules that give stability to the cell.

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Cell Structure and Function

Receptor proteins: Proteins that initiate specific cell responses once hormones or other
trigger molecules bind to them.
Electron transfer proteins: Proteins that are involved in moving electrons from one
molecule to another during chemical reactions.
Passive Transport Across the Cell Membrane
Passive transport describes the movement of substances down a concentration gradient
and does not require energy use.
Bulk flow is the collective movement of substances in the same direction in response to
a force, such as pressure. Blood moving through a vessel is an example of bulk flow.
Simple diffusion, or diffusion, is the net movement of substances from an area of higher
concentration to an area of lower concentration. This movement occurs as a result of
the random and constant motion characteristic of all molecules, (atoms or ions) and is
independent from the motion of other molecules. Since, at any one time, some molecules
may be moving against the gradient and some molecules may be moving down the
gradient, although the motion is random, the word "net" is used to indicate the overall,
eventual end result of the movement.
Facilitated diffusion is the diffusion of solutes through channel proteins in the plasma
membrane. Water can pass freely through the plasma membrane without the aid of
specialized proteins (though facilitated by aquaporins).
Osmosis is the diffusion of water molecules across a selectively permeable membrane.
When water moves into a body by osmosis, hydrostatic pressure or osmotic pressure may
build up inside the body.
Dialysis is the diffusion of solutes across a selectively permeable membrane.
Active Transport Across the Cell Membrane
Active transport is the movement of solutes against a gradient and requires the expenditure
of energy, usually in the form of ATP. Active transport is achieved through one of these two
mechanisms:
Protein Pumps
Transport proteins in the plasma membrane transfer solutes such as small ions (Na+ , K+ ,
Cl- , H+ ), amino acids, and monosaccharides.
The proteins involved with active transport are also known as ion pumps.
The protein binds to a molecule of the substance to be transported on one side of the
membrane, then it uses the released energy (ATP) to change its shape, and releases it on
the other side.
The protein pumps are specific, there is a different pump for each molecule to be
transported.
Protein pumps are catalysts in the splitting of ATP ADP + phosphate, so they are
called ATPase enzymes.

15

Homeostasis
The sodium-potassium pump (also called the Na+ /K+ -ATPase enzyme) actively moves
sodium out of the cell and potassium into the cell. These pumps are found in the
membrane of virtually every cell, and are essential in transmission of nerve impulses
and in muscular contractions.
Cystic fibrosis is a genetic disorder that results in a mutated chloride ion channel. By not
regulating chloride secretion properly, water flow across the airway surface is reduced and
the mucus becomes dehydrated and thick.
Vesicular Transport
Vesicles or other bodies in the cytoplasm move macromolecules or large particles across
the plasma membrane. Types of vesicular transport include:
1. Exocytosis, which describes the process of vesicles fusing with the plasma membrane
and releasing their contents to the outside of the cell. This process is common when a
cell produces substances for export.
2. Endocytosis, which describes the capture of a substance outside the cell when the
plasma membrane merges to engulf it. The substance subsequently enters the cytoplasm
enclosed in a vesicle.
There are three kinds of endocytosis:
Phagocytosis or cellular eating, occurs when the dissolved materials enter the cell.
The plasma membrane engulfs the solid material, forming a phagocytic vesicle.
Pinocytosis or cellular drinking occurs when the plasma membrane folds inward to
form a channel allowing dissolved substances to enter the cell. When the channel is
closed, the liquid is encircled within a pinocytic vesicle.
Receptor-mediated endocytosis occurs when specific molecules in the fluid surrounding the cell bind to specialized receptors in the plasma membrane. As in pinocytosis,
the plasma membrane folds inward and the formation of a vesicle follows.
Note: Certain hormones are able to target specific cells by receptor-mediated endocytosis.

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Parts of the Cell

1.7 Parts of the Cell

Figure 2

1.7.1 Cytoplasm
The gel-like material within the cell membrane is referred to as the cytoplasm. It is a
fluid matrix, the cytosol, which consists of 80% to 90% water, salts, organic molecules and
many enzymes that catalyze reactions, along with dissolved substances such as proteins and
nutrients. The cytoplasm plays an important role in a cell, serving as a "molecular soup" in
which organelles are suspended and held together by a fatty membrane.
Within the plasma membrane of a cell, the cytoplasm surrounds the nuclear envelope and the
cytoplasmic organelles. It plays a mechanical role by moving around inside the membrane
and pushing against the cell membrane helping to maintain the shape and consistency of
the cell and again, to provide suspension to the organelles. It is also a storage space for
chemical substances indispensable to life, which are involved in vital metabolic reactions,
such as anaerobic glycolysis and protein synthesis.
The cell membrane keeps the cytoplasm from leaking out. It contains many different
organelles which are considered the insoluble constituents of the cytoplasm, such as the
mitochondria, lysosomes, peroxysomes, ribosomes, several vacuoles and cytoskeletons, as
well as complex cell membrane structures such as the endoplasmic reticulum and the Golgi
apparatus that each have specific functions within the cell.

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Homeostasis
Cytoskeleton
Threadlike proteins that make up the cytoskeleton continually reconstruct to adapt to the
cell's constantly changing needs. It helps cells maintain their shape and allows cells and their
contents to move. The cytoskeleton allows certain cells such as neutrophils and macrophages
to make amoeboid movements.
The network is composed of three elements: microtubules, actin filaments, and intermediate
fibers.
Microtubules
Microtubules function as the framework along which organelles and vesicles move within a
cell. They are the thickest of the cytoskeleton structures. They are long hollow cylinders,
composed of protein subunits, called tubulin. Microtubules form mitotic spindles, the
machinery that partitions chromosomes between two cells in the process of cell division.
Without mitotic spindles cells could not reproduce.
Microtubules, intermediate filaments, and microfilaments are three protein fibers of decreasing
diameter, respectively. All are involved in establishing the shape or movements of the
cytoskeleton, the internal structure of the cell.

Figure 3

A photograph of microfilaments.

Microfilaments

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Parts of the Cell

Microfilaments provide mechanical support for the cell, determine the cell shape, and in some
cases enable cell movements. They have an arrow-like appearance, with a fast growing plus
or barbed end and a slow growing minus or pointed end. They are made of the protein actin
and are involved in cell motility. They are found in almost every cell, but are predominant
in muscle cells and in the cells that move by changing shape, such as phagocytes (white
blood cells that scour the body for bacteria and other foreign invaders).

1.7.2 Organelles
Organelles are bodies embedded in the cytoplasm that serve to physically separate the
various metabolic activities that occur within cells. The organelles are each like separate
little factories, each organelle is responsible for producing a certain product that is used
elsewhere in the cell or body.
Cells of all living things are divided into two broad categories: prokaryotes and eukaryotes.
Bacteria (and archea) are prokaryotes, which means they lack a nucleus or other membranebound organelles. Eukaryotes include all protozoans, fungi, plants, and animals (including
humans), and these cells are characterized by a nucleus (which houses the chromosomes) as
well as a variety of other organelles. Human cells vary considerably (consider the differences
between a bone cell, a blood cell, and a nerve cell), but most cells have the features described
below.

Figure 4

A comparison of Eukaryote and Prokaryote cells.

Nucleus
Controls the cell; houses the genetic material (DNA). The nucleus is the largest of the cells
organelles. Cells can have more than one nucleus or lack a nucleus all together. Skeletal
muscle cells contain more than one nucleus whereas red blood cells do not contain a nucleus
at all. The nucleus is bounded by the nuclear envelope, a phospholipid bilayer similar to the
plasma membrane. The space between these two layers is the nucleolemma Cisterna.

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Homeostasis
The nucleus contains the DNA, as mentioned above, the hereditary information in the cell.
Normally the DNA is spread out within the nucleus as a threadlike matrix called chromatin.
When the cell begins to divide, the chromatin condenses into rod-shaped bodies called
chromosomes, each of which, before dividing, is made up of two long DNA molecules and
various histone molecules. The histones serve to organize the lengthy DNA, coiling it into
bundles called nucleosomes. Also visible within the nucleus are one or more nucleoli, each
consisting of DNA in the process of manufacturing the components of ribosomes. Ribosomes
are shipped to the cytoplasm where they assemble amino acids into proteins. The nucleus
also serves as the site for the separation of the chromosomes during cell division.

Figure 5

A cross-sectional diagram of a cell.

Chromosomes

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Parts of the Cell

Figure 6

A rough sketch of a chromosome.

Inside each cell nucleus are chromosomes. Chromosomes are made up of chromatin, which
is made up of protein and deoxyribonucleic acid strands. Deoxyribonucleic acid is DNA,
the genetic material that is in the shape of a twisted ladder, also called the double helix.
Humans have 23 pairs of chromosomes. Down Syndrome and Cri du Chat Syndrome result
from having an abnormal number of chromosomes.

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Homeostasis
Centrioles
Centrioles are rod like structures composed of 9 bundles which contain three microtubules
each. Two perpendicularly placed centrioles surrounded by proteins make up the centrosome.
Centrioles are very important in cellular division, where they arrange the mitotic spindles
that pull the chromosome apart.
Centrioles and basal bodies act as microtubule organizing centers. A pair of centrioles
(enclosed in a centrosome) located outside the nuclear envelope gives rise to the microtubules
that make up the spindle apparatus used during cell division. Basal bodies are at the base
of each flagellum and cilium and appear to organize their development.
Ribosomes

Figure 7

framed

Ribosomes play an active role in the complex process of protein synthesis, where they serve
as the structures that facilitate the joining of amino acids. Each ribosome is composed of
a large and small subunit which are made up of ribosomal proteins and ribosomal RNAs.
They can either be found in groups called polyribosomes within the cytoplasm or found
alone. Occasionally they are attached to the endoplasmic reticulum.

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Parts of the Cell

Figure 8

A cutaway view inside a mitochondria.

Mitochondria
Mitochondria are the organelles that function as the cell "powerhouse", generating ATP, the
universal form of energy used by all cells. It converts food nutrients such as glucose, to a fuel
(ATP) that the cells of the body can use. Mitochondria are tiny sac-like structures found
near the nucleus. Little shelves called cristae are formed from folds in the inner membrane.
Cells that are metabolically active such as muscle, liver and kidney cells have high energy
requirements and therefore have more mitochondria.
Mitochondria are unique in that they have their own mitochondrial DNA (separate from
the DNA that is in the nucleus). It is believed that eukaryotes evolved from one cell living
inside another cell, and mitochondria share many traits with free-living bacteria (similar
chromosome, similar ribosomes, etc).
Endoplasmic Reticulum
Endoplasmic means "within the plasm" and reticulum means "network".
A complex three dimensional internal membrane system of flattened sheets, sacs and tubes,
that play an important role in making proteins and shuttling cellular products; also involved

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Homeostasis
in metabolisms of fats, and the production of various materials. In cross-section, they appear
as a series of maze-like channels, often closely associated with the nucleus. When ribosomes
are present, the rough ER connects polysaccharide groups to the polypeptides as they are
assembled by the ribosomes. Smooth ER, without ribosomes, is responsible for various
activities, including the synthesis of lipids and hormones, especially in cells that produce
these substances for export from the cell.
Rough endoplasmic reticulum has characteristic bumpy appearance due to the multitude
of ribosomes coating it. It is the site where proteins not destined for the cytoplasm are
synthesized.
Smooth endoplasmic reticulum provides a variety of functions, including lipid synthesis
and degradation, and calcium ion storage. In liver cells, the smooth ER is involved in the
breakdown of toxins, drugs, and toxic byproducts from cellular reactions.
Golgi Apparatus
"Packages" cellular products in sacs called vesicles so that the products can cross the cell
membrane and exit the cell. The Golgi apparatus is the central delivery system for the
cell. It is a group of flattened sacs arranged much like a stack of bowls. They function to
modify and package proteins and lipids into vesicles, small spherically shaped sacs that bud
from the ends of a Golgi apparatus. Vesicles often migrate to and merge with the plasma
membrane, releasing their contents outside the cell. The Golgi apparatus also transports
lipids and creates lysosomes and organelles involved in digestion.
Vacuoles
Spaces in the cytoplasm that sometimes serve to carry materials to the cell membrane for
discharge to the outside of the cell. Vacuoles are formed during endocytosis when portions
of the cell membrane are pinched off.
Lysosomes
Lysosomes are sac-like compartments that contain a number of powerful degradative enzymes.
They are built in the Golgi apparatus. They break down harmful cell products and waste
materials, cellular debris, and foreign invaders such as bacteria, and then force them out of
the cell. Tay-Sachs disease and Pompe's disease are just two of the malfunctions of lysosomes
or their digestive proteins.
Peroxisomes
Organelles in which oxygen is used to oxidize substances, breaking down lipids and detoxifying certain chemicals. Peroxisomes self replicate by enlarging and then dividing. They
are common in liver and kidney cells that break down potentially harmful substances.
Peroxisomes can convert hydrogen peroxide, a toxin made of H2 O2 to H2 O.

24

Parts of the Cell

1.7.3 Extracellular structures

Extracellular matrix
Human cells, like other animal cells, do not have a rigid cell wall. Human cells do have
an important and variable structure outside of their cell membrane called the extracellular
matrix. Sometimes this matrix can be extensive and solid (examples = calcified bone
matrix, cartilage matrix), while other times it consists of a layer of extracellular proteins and
carbohydrates. This matrix is responsible for cells binding to each other and is incredibly
important in how cells physically and physiologically interact with each other.
Flagella
Many prokaryotes have flagella, allowing, for example, an E. coli bacteria to propel its way
up the urethra to cause a UTI (Urinary Tract Infection). Human cells, however (and in
fact most eukaryotic cells) lack flagella. This makes sense since humans are multicellular,
and individual cells do not need to swim around. The obvious exception to this is with
sperm, and indeed each sperm is propelled by a single flagellum. The flagellum of sperm is
composed of microtubules.
Cilia
Cilia are especially notable on the single-celled protozoans, where they beat in synchrony
to move the cells nimbly through the water. They are composed of extensions of the cell
membrane that contain microtubules. When present in humans they are typically found in
large numbers on a single surface of the cells, where rather than moving cells, they move
materials. The mucociliary escalator of the respiratory system consists of mucus-secreting
cells lining the trachea and bronchi, and ciliated epithelial cells that move the mucus everupward. In this manner mold spores, bacteria, and debris are caught in the mucus, removed
from the trachea, and pushed into the esophagus (to be swallowed into a pit of acid). In the
oviducts cilia move the ovum from the ovary to the uterus, a journey which takes a few days.

25

Homeostasis

Figure 9

A magnified view of several cells, with visible cilia.

1.8 Cell Junctions

The plasma membranes of adjacent cells are usually separated by extracellular fluids that
allow transport of nutrients and wastes to and from the bloodstream. In certain tissues,
however, the membranes of adjacent cells may join and form a junction. Three kinds of cell
junctions are recognized:
Desmosomes are protein attachments between adjacent cells. Inside the plasma membrane, a desmosome bears a disk shaped structure from which protein fibers extend into
the cytoplasm. Desmosomes act like spot welds to hold together tissues that undergo
considerable stress, such as our skin or heart muscle.
Tight junctions are tightly stitched seams between cells. The junction completely
encircles each cell, preventing the movement of material between the cell. Tight junctions
are characteristic of cells lining the digestive tract, where materials are required to pass
through cells,rather than intercellular spaces, to penetrate the bloodstream.
Gap junctions are narrow tunnels that directly connect the cytoplasm of two neighbouring cells, consisting of proteins called connexons. These proteins allow only the passage
of ions and small molecules. In this manner, gap junctions allow communication between
cells through the exchange of materials or the transmission of electrical impulses.

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Cell Metabolism

1.9 Cell Metabolism

Cell metabolism is the total energy released and consumed by a cell. Metabolism describes
all of the chemical reactions that are happening in the body. Some reactions, called anabolic
reactions, create needed products. Other reactions, called catabolic reactions, break down
products. Your body is performing both anabolic and catabolic reactions at the same time
and around the clock, twenty four hours a day, to keep your body alive and functioning.
Even while you sleep, your cells are busy metabolizing.
Catabolism: The energy releasing process in which a chemical or food is used (broken
down) by degradation or decomposition, into smaller pieces.
Anabolism: Anabolism is just the opposite of catabolism. In this portion of metabolism,
the cell consumes energy to produce larger molecules via smaller ones.

1.9.1 Energy Rich Molecules

Adenosine Triphosphate (ATP)

Figure 10

Chemical diagram of an ATP molecule.

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Homeostasis
ATP is the currency of the cell. When the cell needs to use energy such as when it needs to
move substances across the cell membrane via the active transport system, it "pays" with
molecules of ATP. The total quantity of ATP in the human body at any one time is about
0.1 Mole. The energy used by human cells requires the hydrolysis of 200 to 300 moles of
ATP daily. This means that each ATP molecule is recycled 2000 to 3000 times during a
single day. ATP cannot be stored, hence its consumption must closely follow its synthesis.
On a per-hour basis, 1 kilogram of ATP is created, processed and then recycled in the body.
Looking at it another way, a single cell uses about 10 million ATP molecules per second to
meet its metabolic needs, and recycles all of its ATP molecules about every 20-30 seconds.
Flavin Adenine Dinucleotide (FAD)
When two hydrogen atoms are bonded, FAD is reduced to FADH2 and is turned into
an energy-carrying molecule. FAD accommodates two equivalents of Hydrogen; both the
hydride and the proton ions. This is used by organisms to carry out energy requiring
processes. FAD is reduced in the citric acid cycle during aerobic respiration
Nicotinamide Adenine Dinucleotide (NADH)
Nicotinamide adenine dinucleotide (NAD+ ) and nicotinamide adenine dinucleotide phosphate
(NADP) are two important cofactors found in cells. NADH is the reduced form of NAD+ ,
and NAD+ is the oxidized form of NADH. It forms NADP with the addition of a phosphate
group to the 2' position of the adenosyl nucleotide through an ester linkage.
NAD is used extensively in glycolysis and the citric acid cycle of cellular respiration. The
reducing potential stored in NADH can be converted to ATP through the electron transport
chain or used for anabolic metabolism. ATP "energy" is necessary for an organism to live.
Green plants obtain ATP through photosynthesis, while other organisms obtain it by cellular
respiration.
NADP is used in anabolic reactions, such as fat acid and nucleic acid synthesis, that require
NADPH as a reducing agent. In chloroplasts, NADP is an oxidising agent important in the
preliminary reactions of photosynthesis. The NADPH produced by photosynthesis is then
used as reducing power for the biosynthetic reactions in the Calvin cycle of photosynthesis.

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Cell Metabolism

Figure 11

Chemical diagram of an NADH molecule.

MH2 + NAD+ NADH + H+ + M: + energy, where M is a metabolite. Two hydrogen

ions (a hydride ion and an H+ ion) are transferred from the metabolite. One electron is
transferred to the positively-charged nitrogen, and one hydrogen attaches to the carbon
atom opposite to the nitrogen.
The human body synthesizes NAD from the vitamin niacin in the form of nicotinic acid or
nicotinamide.
Cellular Respiration
Cellular respiration is the energy releasing process by which sugar molecules are broken
down by a series of reactions and the chemical energy gets converted to energy stored in
ATP molecules. The reactions that convert the fuel (glucose) to usable cellular energy
(ATP) are glycolysis, the Krebs cycle (sometimes called the citric acid cycle), and the
electron transport chain. Altogether these reactions are referred to as "cellular respiration"
or "aerobic respiration." Oxygen is needed as the final electron acceptor, and carrying out
cellular respiration is the very reason we breathe and the reason we eat.

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Homeostasis

Figure 12

Flowchart of cellular respiration.

1.9.2 Glycolysis
The glycolytic pathway (glycolysis) is where glucose, the smallest molecule that a carbohydrate can be broken into during digestion, gets oxidized and broken into two 3-carbon
molecules (pyruvates), which are then fed into the Kreb's Cycle. Glycolysis is the beginning of cellular respiration and takes place in the cytoplasm. Two molecules of ATP are
required for glycolysis, but four are produced so there is a net gain of two ATP per glucose
molecule. Two NADH molecules transfer electrons (in the form of hydrogen ions) to the
electron transport chain in the mitochondria, where they will be used to generate additional

30

Cell Metabolism
ATP. During physical exertion when the mitochondria are already producing the maximum
ATP possible with the amount of oxygen available, glycolysis can continue to produce an
additional 2 ATP per glucose molecule without sending the electrons to the mitochondria.
However, during this anaerobic respiration lactic acid is produced, which may accumulate
and lead to temporary muscle cramping.

1.9.3 Krebs Cycle

The Krebs cycle was named after Sir Hans Krebs1 (1900-1981), who proposed the key
elements of this pathway in 1937 and was awarded the Nobel Prize in Medicine for its
discovery in 1953.
Two molecules of pyruvate enter the Krebs cycle, which is called the aerobic pathway because
it requires the presence of oxygen in order to occur. This cycle is a major biological pathway
that occurs in humans and every plant and animal.
After glycolysis takes place in the cell's cytoplasm, the pyruvic acid molecules travel into the
interior of the mitochondrion. Once the pyruvic acid is inside, carbon dioxide is enzymatically
removed from each three-carbon pyruvic acid molecule to form acetic acid. The enzyme
then combines the acetic acid with an enzyme, coenzyme A, to produce acetyl coenzyme A,
also known as acetyl CoA.
Once acetyl CoA is formed, the Krebs cycle begins. The cycle is split into eight steps, each
of which will be explained below.
Step 1: The acetic acid subunit of acetyl CoA is combined with oxaloacetate to form a
molecule of citrate. The acetyl coenzyme A acts only as a transporter of acetic acid from
one enzyme to another. After Step 1, the coenzyme is released by hydrolysis so that it
may combine with another acetic acid molecule to begin the Krebs cycle again.
Step 2: The citric acid molecule undergoes an isomerization. A hydroxyl group and a
hydrogen molecule are removed from the citrate structure in the form of water. The
two carbons form a double bond until the water molecule is added back. Only now, the
hydroxyl group and hydrogen molecule are reversed with respect to the original structure
of the citrate molecule. Thus, isocitrate is formed.
Step 3: In this step, the isocitrate molecule is oxidized by a NAD molecule. The NAD
molecule is reduced by the hydrogen atom and the hydroxyl group. The NAD binds with
a hydrogen atom and carries off the other hydrogen atom leaving a carbonyl group. This
structure is very unstable, so a molecule of CO2 is released creating alpha-ketoglutarate.
Step 4: In this step, our friend, coenzyme A, returns to oxidize the alpha-ketoglutarate
molecule. A molecule of NAD is reduced again to form NADH and leaves with another
hydrogen. This instability causes a carbonyl group to be released as carbon dioxide
and a thioester bond is formed in its place between the former alpha-ketoglutarate and
coenzyme A to create a molecule of succinyl-coenzyme A complex.
Step 5: A water molecule sheds its hydrogen atoms to coenzyme A. Then, a free-floating
phosphate group displaces coenzyme A and forms a bond with the succinyl complex. The
phosphate is then transferred to a molecule of GDP to produce an energy molecule of
GTP. It leaves behind a molecule of succinate.
1

http://en.wikibooks.org/wiki/%3Awikipedia%3AHans_Adolf_Krebs

31

Homeostasis
Step 6: In this step, succinate is oxidized by a molecule of FAD (Flavin adenine dinucleotide). The FAD removes two hydrogen atoms from the succinate and forces a double
bond to form between the two carbon atoms, thus creating fumarate.
Step 7: An enzyme adds water to the fumarate molecule to form malate. The malate
is created by adding one hydrogen atom to a carbon atom and then adding a hydroxyl
group to a carbon next to a terminal carbonyl group.
Step 8: In this final step, the malate molecule is oxidized by a NAD molecule. The
carbon that carried the hydroxyl group is now converted into a carbonyl group. The end
product is oxaloacetate which can then combine with acetyl-coenzyme A and begin the
Krebs cycle all over again.
Summary: In summary, three major events occur during the Krebs cycle. One GTP
(guanosine triphosphate) is produced which eventually donates a phosphate group to
ADP to form one ATP; three molecules of NAD are reduced; and one molecule of FAD
is reduced. Although one molecule of GTP leads to the production of one ATP, the
production of the reduced NAD and FAD are far more significant in the cell's energygenerating process. This is because NADH and FADH2 donate their electrons to an
electron transport system that generates large amounts of energy by forming many
molecules of ATP.
To see a visual summary of "Kreb Cycle" please click here2 .

1.9.4 Electron Transport System

The most complicated system of all. In the respiration chain, oxidation and reduction
reactions occur repeatedly as a way of transporting energy. The respiratory chain is also
called the electron transport chain. At the end of the chain, oxygen accepts the electron
and water is produced.
Redox Reaction
This is a simultaneous oxidation-reduction process whereby cellular metabolism occurs, such
as the oxidation of sugar in the human body, through a series of very complex electron
transfer processes.
The chemical way to look at redox processes is that the substance being oxidized transfers
electrons to the substance being reduced. Thus, in the reaction, the substance being oxidized
(aka. the reducing agent) loses electrons, while the substance being reduced (aka. the
oxidizing agent) gains electrons. Remember: LEO (Losing Electrons is Oxidation) the lion
says GER (Gaining Electrons is Reduction); or alternatively: OIL (Oxidation is Loss) RIG
(Reduction is Gain).
The term redox state is often used to describe the balance of NAD+ /NADH and
NADP+ /NADPH in a biological system such as a cell or organ. The redox state is reflected
in the balance of several sets of metabolites (e.g., lactate and pyruvate, -hydroxybutyrate
and acetoacetate) whose interconversion is dependent on these ratios. An abnormal redox
state can develop in a variety of deleterious situations, such as hypoxia, shock, and sepsis.
2

32

http://homepage.smc.edu/hodson_kent/Energetics/Krebs2.htm

Cell Building Blocks

1.10 Cell Building Blocks

What major classes of molecules are found within cells?

1.10.1 Lipids
The term is more-specifically used to refer to fatty-acids and their derivatives (including tri-,
di-, and mono-glycerides and phospholipids) as well as other fat-soluble sterol-containing
metabolites such as cholesterol. Lipids serve many functions in living organisms including
energy storage, serve as structural components of cell membranes, and constitute important
signaling molecules. Although the term lipid is sometimes used as a synonym for fat, the
latter is in fact a subgroup of lipids called triglycerides and should not be confused with the
term fatty acid.

1.10.2 Carbohydrates
Carbohydrate molecules consist of carbon, hydrogen, and oxygen. They have a general
formula Cn (H2 O)n . There are several sub-families based on molecular size.
Carbohydrates are chemical compounds that contain oxygen, hydrogen, and carbon atoms,
and no other elements. They consist of monosaccharide sugars of varying chain lengths.
Certain carbohydrates are an important storage and transport form of energy in most
organisms, including plants and animals. Carbohydrates are classified by their number of
sugar units: monosaccharides (such as glucose and fructose), disaccharides (such as sucrose
and lactose), oligosaccharides, and polysaccharides (such as starch, glycogen, and cellulose).
The simplest carbohydrates are monosaccharides, which are small straight-chain aldehydes
and ketones with many hydroxyl groups added, usually one on each carbon except the
functional group. Other carbohydrates are composed of monosaccharide units and break
down under hydrolysis. These may be classified as disaccharides, oligosaccharides, or
polysaccharides, depending on whether they have two, several, or many monosaccharide
units.

33

Homeostasis

../images/13.png

Figure 13

1.10.3 Proteins
All proteins contain carbon, hydrogen, oxygen and nitrogen. Some also contain phosphorus
and sulfur. The building blocks of proteins are amino acids. There are 20 different kinds of
amino acids used by the human body. They unite by peptide bonds to form long molecules
called polypeptides. Polypeptides are assembled into proteins. Proteins have four levels of
structure
Primary
Primary structure is the sequence of amino acids bonded in the polypeptide.
Secondary

34

Review Questions
The secondary structure is formed by hydrogen bonds between amino acids. The polypeptide
can coil into a helix or form a pleated sheet.
Tertiary
The tertiary structure refers to the three-dimensional folding of the helix or pleated sheet.
Quaternary
The quaternary structure refers to the spatial relationship among the polypeptide in the
protein.

1.10.4 Enzymes
A biological molecule that catalyzes a chemical reaction. Enzymes are essential for life
because most chemical reactions in living cells would occur too slowly or would lead to
different products without enzymes. Most enzymes are proteins and the word "enzyme" is
often used to mean a protein enzyme. Some RNA molecules also have a catalytic activity,
and to differentiate them from protein enzymes, they are referred to as RNA enzymes or
ribozymes.

1.11 Review Questions

Answers for these questions can be found here3
1. List 2 functions of the cell membrane:
Questions 2 - 6 Match the following organelles with their function: 2. Mitochondria 3.
Vacuoles 4. Cilia 5. Smooth ER 6. Golgi Apparatus
A. Movement of the cell
B. Lipid synthesis and transport
C. "Powerhouse" of the cell, makes ATP
D. Storage areas, mainly found in plant cells
E. Packages and distributes cellular products
7. The diffusion of H2 O across a semi permeable or selectively permeable membrane is
termed
A. Active transport
B. Diffusion
C. Osmosis
D. Endocytosis

http://en.wikibooks.org/wiki/Human_Physiology/Appendix_1:_answers_to_review_
questions#Cell_physiology

35

Homeostasis
8. Oxygen enters a cell via?
a. Diffusion
b. Filtration
c. Osmosis
d. Active transport
9. The term used to describe, "cell eating" is?
a. Exocytosis
b. Phagocytosis
c. Pinocytosis
d. Diffusion
10. Which of the following requires energy?
a. Diffusion
b. Osmosis
c. Active transport
d. Facilitated diffusion
11. Protein synthesis occurs at the
a. Mitochondria
b. Lysosomes
c. Within the nucleus
d. Ribosomes
12. Which of the following is not found in the cell membrane?
a. Cholesterol
b. Phospholipids
c. Proteins
d. Galactose
e. Nucleic acids
13. What is a cell?
a. The largest living units within our bodies.
b. Enzymes that "eat" bacteria
c. Microscopic fundamental units of all living things.
d. All of the above.

36

Glossary

1.12 Glossary
Active Transport: the movement of solutes against a gradient and requires the expenditure
of energy
Adenosine Triphosphate (ATP): a cells source of energy
Bulk Flow: the collective movement of substances in the same direction in response to a
force
Cells: the microscopic fundamental unit that makes up all living things
Cell Membrane: boundary of the cell, sometimes called the plasma membrane
Cytoplasm: a water-like substance that fills cells. The cytoplasm consists of cytosol and
the cellular organelles, except the cell nucleus. The cytosol is made up of water, salts,
organic molecules and many enzymes that catalyze reactions. The cytoplasm holds all of
the cellular organelles outside of the nucleus, maintains the shape and consistency of the
cell, and serves as a storage place for chemical substances.
Cytoskeleton: made of threadlike proteins, helps cells maintain their shape and allows
cells and their contents to move
Dialysis: the diffusion of solutes across a selectively permeable membrane. Most commonly
heard of when a patient has had renal failure. In medicine, dialysis is a type of renal
replacement therapy which is used to provide an artificial replacement for lost kidney
function due to renal failure. It is a life support treatment and does not treat any kidney
diseases.
Endocrine cells: similar to exocrine cells, but secrete their products directly into the
bloodstream instead of through a duct
Endocytosis: the capture of a substance outside the cell when the plasma membrane
merges to engulf it
Endoplasmic Reticulum: organelle that play an important role in making proteins and
shuttling cellular products; also involved in metabolisms of fats, and the production of
various materials
Epithelial Cells: cells that aid in secretion, absorption, protection, trans-cellular transport,
sensation detection, and selective permeability
Exocrine Cells: cells that secrete products through ducts, such as mucus, sweat, or
digestive enzymes
Exocytosis: the process of vesicles fusing with the plasma membrane and releasing their
contents to the outside of the cell
Facilitated Diffusion: the diffusion of solutes through channel proteins in the plasma
membrane
Golgi Apparatus: "packages" cellular products in sacs called vesicles so that the products
can cross the cell membrane and exit the cell
Glycolysis: process in which sugars (glucose) are converted to acid

37

Homeostasis
Lysosomes: sac-like compartments that contain a number of powerful degradative enzymes
Microfilaments: provide mechanical support for the cell, determine the cell shape, and in
some cases enable cell movements
Microtubules: function as the framework along which organelles and vesicles move within
a cell
Mitochondria: the organelles that function as the cell "powerhouse", generating ATP
Nucleus: controls the cell; houses the genetic material
Organelles: bodies embedded in the cytoplasm that serve to physically separate the various
metabolic activities that occur within cells
Osmosis: the diffusion of water molecules across a selectively permeable membrane from
an area of high solute concentration to an area of low solute concentration.
Passive Transport: the movement of substances down a concentration gradient and does
not require energy use
Peroxisomes: organelles in which oxygen is used to oxidize substances, breaking down
lipids and detoxifying certain chemicals
Phagocytosis: a form of endocytosis wherein large particles are enveloped by the cell
membrane of a (usually larger) cell and internalized to form a phagosome, or "food vacuole."
In animals, phagocytosis is performed by specialized cells called phagocytes, which serve
to remove foreign bodies and thus fight infection. In vertebrates, these include larger
macrophages and smaller granulocytes, types of blood cells. Bacteria, dead tissue cells, and
small mineral particles are all examples of objects that may be phagocytosed.
Pinocytosis: also called cellular drinking, is a form of endocytosis, a process in which small
particles are taken in by a cell by splitting into smaller particles. The particles then form
small vesicles which subsequently fuse with lysosomes to hydrolyze, or to break down, the
particles. This process requires adenosine triphosphate (ATP).
Receptor-mediated Endocytosis: occurs when specific molecules in the fluid surrounding
the cell bind to specialized receptors in the plasma membrane
Red Blood Cells (erythrocytes): cells that collect oxygen in the lungs and deliver it
through the blood to the body tissues
Ribosomes: play an active role in the complex process of protein synthesis, where they
serve as the structures that facilitate the joining of amino acids
Simple Diffusion: the net movement of substances from an area of higher concentration
to an area of lower concentration
Vacuoles: spaces in the cytoplasm that sometimes serve to carry materials to the cell
membrane for discharge to the outside of the cell
White Blood Cells (leukocytes): produced in the bone marrow and help the body to
fight infectious disease and foreign objects in the immune system

38

2 The Integumentary System

2.1 Introduction
The integumentary system consists of the skin, hair, nails, the subcutaneous tissue below
the skin,and assorted glands.The most obvious function of the integumentary system is the
protection that the skin gives to underlying tissues. The skin not only keeps most harmful
substances out, but also prevents the loss of fluids.
A major function of the subcutaneous tissue is to connect the skin to underlying tissues
such as muscles. Hair on the scalp provides insulation from cold for the head. The hair of
eyelashes and eyebrows helps keep dust and perspiration out of the eyes, and the hair in our
nostrils helps keep dust out of the nasal cavities. Any other hair on our bodies no longer
serves a function, but is an evolutionary remnant. Nails protect the tips of fingers and toes
from mechanical injury. Fingernails give the fingers greater ability to pick up small objects.
There are four types of glands in the integumentary system: Sudoriferous glands, Sebaceous
glands, Ceruminous glands, and Mammary glands. Sudoriferous glands are sweat producing
glands. These are important to help maintain body temperature. Sebaceous glands are oil
producing glands which help inhibit bacteria, keep us waterproof and prevent our hair and
skin from drying out. Ceruminous glands produce earwax which keeps the outer surface of
the eardrum pliable and prevents drying. Mammary glands produce milk.

2.2 Skin
In zoology and dermatology, skin is an organ of the integumentary system made up of a layer
of tissues that guard underlying muscles and organs. As the interface with the surroundings,
it plays the most important role in protecting against pathogens. Its other main functions
are insulation and temperature regulation, sensation and vitamin D and B synthesis. Skin
is considered one of the most important parts of the body.
Skin has pigmentation, melanin, provided by melanocytes, which absorbs some of the
potentially dangerous radiation in sunlight. It also contains DNA repair enzymes which
reverse UV damage, and people who lack the genes for these enzymes suffer high rates
of skin cancer. One form predominantly produced by UV light, malignant melanoma, is
particularly invasive, causing it to spread quickly, and can often be deadly. Human skin
pigmentation varies among populations in a striking manner. This has sometimes led to the
classification of people(s) on the basis of skin color.
Damaged skin will try to heal by forming scar tissue, often giving rise to discoloration and
depigmentation of the skin.

39

The Integumentary System

The skin is often known as "the largest organ in the human body". This applies to exterior
surface, as it covers the body, appearing to have the largest surface area of all the organs.
Moreover, it applies to weight, as it weighs more than any single internal organ, accounting
for about 15 percent of body weight. For the average adult human, the skin has a surface
area of between 1.5-2.0 square meters, most of it is between 2-3 mm thick. The average
square inch of skin holds 650 sweat glands, 20 blood vessels, 60,000 melanocytes, and more
than a thousand nerve endings.
The use of natural or synthetic cosmetics to treat the appearance of the face and condition
of the skin (such as pore control and black head cleansing) is common among many cultures.

2.2.1 Layers
The skin has two major layers which are made of different tissues and have very different
functions.

40

Skin

Figure 14

Diagram of the layers of human skin

Skin is composed of the epidermis and the dermis. Below these layers lies the hypodermis or
subcutaneous adipose layer, which is not usually classified as a layer of skin.
The outermost epidermis consists of stratified squamous keratinizing epithelium with an
underlying basement membrane. It contains no blood vessels, and is nourished by diffusion
from the dermis. The main type of cells which make up the epidermis are keratinocytes, with
melanocytes and Langerhans cells also present. The epidermis can be further subdivided into
the following strata (beginning with the outermost layer): corneum, lucidum, granulosum,
spinosum, basale. Cells are formed through mitosis at the innermost layers. They move
up the strata changing shape and composition as they differentiate, inducing expression of
new types of keratin genes. They eventually reach the corneum and become sloughed off
(desquamation). This process is called keratinization and takes place within about 30 days.

41

The Integumentary System

This layer of skin is responsible for keeping water in the body and keeping other harmful
chemicals and pathogens out.
Blood capillaries are found beneath the dermis, and are linked to an arteriole and a venule.
Arterial shunt vessels may bypass the network in ears, the nose and fingertips.
The dermis lies below the epidermis and contains a number of structures including blood
vessels, nerves, hair follicles, smooth muscle, glands and lymphatic tissue. It consists of loose
connective tissue otherwise called areolar connective tissue - collagen, elastin and reticular
fibers are present. Erector muscles, attached between the hair papilla and epidermis, can
contract, resulting in the hair fiber pulled upright and consequentially goose bumps. The
main cell types are fibroblasts, adipocytes (fat storage) and macrophages. Sebaceous glands
are exocrine glands which produce, a mixture of lipids and waxy substances: lubrication,
water-proofing, softening and antibactericidal actions are among the many functions of
sebum. Sweat Glands open up via a duct onto the skin by a pore.
The dermis is made of an irregular type of fibrous connective tissue consisting of collagen
and elastin fibers. It can be split into the papillary and reticular layers. The papillary layer
is outermost and extends into the epidermis to supply it with vessels. It is composed of
loosely arranged fibers. Papillary ridges make up the lines of the hands giving us fingerprints.
The reticular layer is more dense and is continuous with the hypodermis. It contains the
bulk of the structures (such as sweat glands). The reticular layer is composed of irregularly
arranged fibers and resists stretching.
The hypodermis is not part of the skin, and lies below the dermis. Its purpose is to attach
the skin to underlying bone and muscle as well as supplying it with blood vessels and
nerves. It consists of loose connective tissue and elastin. The main cell types are fibroblasts,
macrophages and adipocytes (the hypodermis contains 95% of body fat). Fat serves as
padding and insulation for the body.
Clinical Application:
The patch drug delivery system. The transdermal patch is an increasingly popular drug
delivery system. These patches are designed so that the drug molecules diffuse through
the epidermis to the blood vessels in the dermis layer. A typical patch works well for
small lipid-soluble molecules (for example, estrogen, nitroglycerin, and nicotine) that can
make their way between epidermal cells.

42

Skin

2.2.2 Functions

Figure 15

1. Protection: Skin gives an anatomical barrier between the internal and external environment in bodily defense; Langerhans cells in the skin are part of the immune
system
2. Sensation: Skin contains a variety of nerve endings that react to heat, cold, touch,
pressure, vibration, and tissue injury; see somatosensory1 system and touch2 .

1
2

http://en.wikipedia.org/wiki/Somatosensory_system
http://en.wikipedia.org/wiki/Touch

43

The Integumentary System

3. Heat regulation: The skin contains a blood supply far greater than its requirements
which allows precise control of energy loss by radiation, convection and conduction.
Dilated blood vessels increase perfusion and heat loss while constricted vessels greatly
reduce cutaneous blood flow and conserve heat. Erector pili muscles are significant in
animals.
Tumors

Benign tumors of the skin: Squamous cell papilloma

Skin cancer3
Acne4
Keratosis pilaris5
Fungal6 infections such as athlete's foot7
microbial infections8
calcinosis cutis9
ulcer10

2.3 Hair
w:Hair11

2.3.1 Types of hair

Humans have three different types of hair:
Lanugo, the fine, unpigmented hair that covers nearly the entire body of a fetus, although
most has been replaced with vellus by the time of the baby's birth
Vellus hair, the short, downy, "peach fuzz" body hair (also unpigmented) that grows in
most places on the human body. While it occurs in both sexes, and makes up much of
the hair in children, men have a much smaller percentage (around 10%) vellus whereas
2/3 of a female's hair is vellus.
Terminal hair, the fully developed hair, which is generally longer, coarser, thicker, and
darker than vellus hair, and often is found in regions such as the axillary, male beard,
and pubic.

3
4
5
6
7
8
9
10
11

44

http://en.wikipedia.org/wiki/Skin_cancer
http://en.wikipedia.org/wiki/Acne
http://en.wikipedia.org/wiki/Keratosis_pilaris
http://en.wikipedia.org/wiki/Fungus
http://en.wikipedia.org/wiki/Athlete%2527s_foot
http://en.wikipedia.org/wiki/Microbe
http://en.wikipedia.org/wiki/Calcinosis_cutis
http://en.wikipedia.org/wiki/Ulcer
http://en.wikipedia.org/wiki/Hair

Nails

2.3.2 Pathological impacts on hair

Drugs used in cancer chemotherapy frequently cause a temporary loss of hair, noticeable on
the head and eyebrows, because they kill all rapidly dividing cells, not just the cancerous
ones. Other diseases and traumas can cause temporary or permanent loss of hair, either
generally or in patches.
The hair shafts may also store certain poisons for years, even decades, after death. In
the case of Col. Lafayette Baker, who died July 3, 1868, use of an atomic absorption
spectrophotometer showed the man was killed by white arsenic. The prime suspect was
Wallace Pollock, Baker's brother-in-law. According to Dr. Ray A. Neff, Pollack had laced
Baker's beer with it over a period of months, and a century or so later minute traces of
arsenic showed up in the dead man's hair. Mrs. Baker's diary seems to confirm that it was
indeed arsenic, as she writes of how she found some vials of it inside her brother's suit coat
one day.

2.4 Nails
2.4.1 Parts of the fingernail

Figure 16

The parts of a finger nail

The fingernail is an important structure made of keratin. The fingernail generally serve
two purposes. It serves as a protective plate and enhances sensation of the fingertip. The
protection function of the fingernail is commonly known, but the sensation function is
equally important. The fingertip has many nerve endings in it allowing us to receive volumes
of information about objects we touch. The nail acts as a counterforce to the fingertip
providing even more sensory input when an object is touched.

2.4.2 Nail Structure

The structure we know of as the nail is divided into six specific parts - the root, nail bed,
nail plate, eponychium (cuticle), perionychium, and hyponychium.

45

The Integumentary System

Root The root of the fingernail is also known as the germinal matrix. This portion of the
nail is actually beneath the skin behind the fingernail and extends several millimeters into
the finger. The fingernail root produces most of the volume of the nail and the nail bed.
This portion of the nail does not have any melanocytes, or melanin producing cells. The
edge of the germinal matrix is seen as a white, crescent shaped structure called the lunula.
Nail Bed The nail bed is part of the nail matrix called the sterile matrix. It extends from
the edge of the germinal matrix, or lunula, to the hyponychium. The nail bed contains the
blood vessels, nerves, and melanocytes, or melanin-producing cells. As the nail is produced
by the root, it streams down along the nail bed, which adds material to the undersurface of
the nail making it thicker. It is important for normal nail growth that the nail bed be smooth.
If it is not, the nail may split or develop grooves that can be cosmetically unappealing.
Nail Plate The nail plate is the actual fingernail, made of translucent keratin. The pink
appearance of the nail comes from the blood vessels underneath the nail. The underneath
surface of the nail plate has grooves along the length of the nail that help anchor it to the
nail bed.
eponychium The cuticle of the fingernail is also called the eponychium. The cuticle is
situated between the skin of the finger and the nail plate fusing these structures together
and providing a waterproof barrier.
Perionychium The perioncyhium is the skin that overlies the nail plate on its sides. It is
also known as the paronychial edge. The perionychium is the site of hangnails, ingrown
nails, and an infection of the skin called paronychia.
Hyponychium The hyponychium is the area between the nail plate and the fingertip. It is
the junction between the free edge of the nail and the skin of the fingertip, also providing a
waterproof barrier.

Figure 17
male

Nails: left hand, adult human

2.4.3 Nail Diseases

Nail diseases are in a separate category from diseases of the skin. Although nails are a skin
appendage, they have their own signs and symptoms which may relate to other medical
conditions. Nail conditions that show signs of infection or inflammation require medical

46

Nails
assistance and cannot be treated at a beauty parlor. Deformity or disease of the nails may
be referred to as onychosis.
There are many disease that can occur with the fingernails and toenails. The most common
of these diseases are ingrown nails and fungal infections.
Ingrown Nails
Onychocryptosis, commonly known as "ingrown nails" (unguis incarnatus), can affect
either the fingers or the toes. In this condition, the nail cuts into one or both sides of the nail
bed, resulting in inflammation and possibly infection. The relative rarity of this condition in
the fingers suggests that pressure from the ground or shoe against the toe is a prime factor.
The movements involved in walking or other physical disturbances can contribute to the
problem. Mild onychocryptosis, particularly in the absence of infection, can be treated by
trimming and rounding the nail. More advanced cases, which usually include infection, are
treated by surgically excising the ingrowing portion of the nail down to its bony origin and
cauterizing the matrix, or 'root', to prevent recurrence. This surgery is called matricectomy.
The best results are achieved by cauterizing the matrix with phenol. Another method, which
is much less effective, is excision of the matrix, sometimes called a 'cold steel procedure'
Nail Fungus
An infection of nail fungus (onychomycosis) occurs when fungi infect one or more of your
nails. Onychomycosis generally begins as a white or yellow spot under the tip of the
fingernail or toenail. As the nail fungus spreads deeper into the nail, it may cause the nail
to discolor, thicken and develop crumbling edges an unsightly and potentially painful
problem.
Infections of nail fungus account for about half of all nail disorders. These infections usually
develop on nails continually exposed to warm, moist environments, such as sweaty shoes or
shower floors. Nail fungus isn't the same as athlete's foot, which primarily affects the skin
of the feet, but at times the two may coexist and can be caused by the same type of fungus.
An infection with nail fungus may be difficult to treat, and infections may recur. But
medications are available to help clear up nail fungus permanently.

2.4.4 Clinical Application

Nail inspection can give a great deal of information about the internal working of the body as
well, and like tongue or iris inspection, has a long history of diagnostic use in cantraditional
medical practices such as Chinese medicine.
Pliability:
Brittleness is associated with iron deficiency, thyroid problems, impaired kidney function,
circulation problems[2], and biotin deficiency[3] Splitting and fraying are associated with
psoriasis, folic acid, protein and/or Vitamin C deficiency. Unusual thickness is associated
with circulation problems. Thinning nails and itchy skin are associated with lichen planus[4].

47

The Integumentary System

Shape and texture:
Clubbing, or nails that curve down around the fingertips with nail beds that bulge is
associated with oxygen deprivation and lung, heart, or liver disease. Spooning, or nails
that grow upwards is associated with iron or B12 deficiency. Flatness can indicate a B12
vitamin deficiency[5] or Raynaud's disease[6] Pitting of the nails is associated with Psoriasis.
Horizontal ridges indicate stress, and Beau's lines are associated with many serious conditions.
Vertical ridges are associated with arthritis[7]. Vertical grooves are associated with kidney
disorders, aging, and iron deficiency[8]. Beading is associated with rheumatoid arthritis[9].
Nails that resemble hammered brass are associated with (or portend) hair loss[10]. Short
small beds are associated with heart disease[11]. Coloration of the nail bed:
Mee's lines are associated with arsenic or thallium poisoning, and renal failure. White lines
across the nail are associated with heart disease, liver disease, or a history of a recent high
fever[12]. Opaque white nails with a dark band at the fingertip are associated with cancer,
cirrhosis, congestive heart failure, diabetes and aging[13]. Paleness or whitening is associated
with liver or kidney disease and anemia[14]. Yellowing of the nail bed is associated with
chronic bronchitis, lymphatic problems, diabetes, and liver disorders. Brown or copper nail
beds are associated with arsenic or copper poisoning, and local fungal infection. Grey nail
beds are associated with arthritis, edema, malnutrition, post-operative effects, glaucoma
and cardio-pulmonary disease[15]. redness is associated with heart conditions. dark nails
are associated with B12 deficiency. Stains of the nail plate (not the nail bed) are associated
with nail polish[16], smoking, and henna use.
Markings:
Pink and white nails are associated with kidney disease[17]. Parallel white lines in the nails
are associated with hypoalbuminemia. red skin at the base of the nail is associated with
connective tissue disorders[18]. blue lunulae are associated with silver poisoning or lung
disorder[19]. blue nail beds are (much like blue skin) associated with poor oxygenation of the
blood (asthma, emphysema, etc)[20]. small white patches are associated with zinc or calcium
deficiency or malabsorption, parasites, or local injury[21]. receded lunulae (fewer than 8) are
associated with poor circulation[22], shallow breathing habits or thyroid mysfunction[23].
large lunulae (more than 25% of the thumb nail) is associated with high blood pressure.

48

Glands

2.5 Glands
2.5.1 Sweat Glands

Figure 18 A diagrammatic sectional view of the skin (magnified). Sweat

gland labeled as "sudoriferous gland" at center right.

In humans, there are two kinds of sweat glands which differ greatly in both the composition
of the sweat and its purpose: Also "click" here our body Sweats"12 to see a short movie on
sweat glands.

12

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The Integumentary System

Eccrine (a.k.a. merocrine)
Eccrine sweat glands are exocrine glands distributed over the entire body surface but
are particularly abundant on the palms of hands, soles of feet, and on the forehead. These
produce sweat that is composed chiefly of water (99%) with various salts. The primary
function is body temperature regulation.
Eccrine sweat glands are coiled tubular glands derived leading directly to the most superficial
layer of the epidermis (out layer of skin) but extending into the inner layer of the skin
(dermis layer). They are distributed over almost the entire surface of the body in humans
and many other species, but are lacking in some marine and fur-bearing species. The sweat
glands are controlled by sympathetic cholinergic nerves which are controlled by a center in
the hypothalamus. The hypothalamus senses core temperature directly, and also has input
from temperature receptors in the skin and modifies the sweat output, along with other
thermoregulatory processes.
Human eccrine sweat is composed chiefly of water with various salts and organic compounds
in solution. It contains minute amounts of fatty materials, urea, and other wastes. The
concentration of sodium varies from 3565 mmol/l and is lower in people acclimatised to a
hot environment. The sweat of other species generally differ in composition.
Apocrine
Apocrine sweat glands only develop during early- to mid-puberty (approximately age 15)
and release more than normal amounts of sweat for approximately a month and subsequently
regulate and release normal amounts of sweat after a certain period of time. Apocrine
sweat glands produce sweat that contains fatty materials. These glands are mainly present
in the armpits and around the genital area and their activity is the main cause of sweat
odor, due to the bacteria that break down the organic compounds in the sweat from these
glands. Emotional stress increases the production of sweat from the apocrine glands, or
more precisely: the sweat already present in the tubule is squeezed out. Apocrine sweat
glands essentially serve as scent glands.
In some areas of the body, these sweat glands are modified to produce wholly different
secretions, including the cerumen ("wax") of the outer ear. Other glands, such as Mammary
glands, are greatly enlarged and modified to produce milk.

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Glands

2.5.2 Sebaceous Glands

Figure 19 Schematic view of a hair follicle

with sebaceous gland.
The sebaceous glands are glands found in the skin of mammals. They secrete an oily
substance called sebum (Latin, meaning fat or tallow) that is made of fat (lipids) and the
debris of dead fat-producing cells. These glands exist in humans throughout the skin except
in the palms of the hands and soles of the feet. Sebum acts to protect and waterproof hair
and skin, and keep them from becoming dry, brittle, and cracked. It can also inhibit the
growth of microorganisms on skin.
Sebaceous glands can usually be found in hair-covered areas where they are connected to
hair follicles to deposit sebum on the hairs, and bring it to the skin surface along the hair
shaft. The structure consisting of hair, hair follicle and sebaceous gland is also known as
pilosebaceous unit. Sebaceous glands are also found in non haired areas of lips, eyelids,
penis, labia minora and nipples; here the sebum reaches the surface through ducts. In
the glands, sebum is produced within specialized cells and is released as these cells burst;
sebaceous glands are thus classified as holocrine glands.
Sebum is odorless, but its bacterial breakdown can produce odors. Sebum is the cause of
some people experiencing "oily" hair if it is not washed for several days. Earwax is partly
sebum, as is mucopurulent discharge, the dry substance accumulating in the corners of the
eye after sleeping.

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The Integumentary System

Figure 20

A hair follicle with associated structures.

The composition of sebum varies from species to species; in humans, the lipid content consists
of about 25% wax monoesters, 41% triglycerides, 16% free fatty acids, and 12% squalene.
The activity of the sebaceous glands increases during puberty because of heightened levels
of androgens.
Sebaceous glands are involved in skin problems such as acne and keratosis pilaris. A
blocked sebaceous gland can result in a sebaceous cyst. The prescription drug isotretinoin
significantly reduces the amount of sebum produced by the sebaceous glands, and is used to
treat acne. The extreme use (up to 10 times doctor prescribed amounts) of anabolic steroids
by bodybuilders to prevent weight loss tend to stimulate the sebaceous glands which can
cause acne.
The sebaceous glands of a human fetus in utero secrete a substance called Vernix caseosa, a
"waxy" or "cheesy" white substance coating the skin of newborns.
The preputial glands of mice and rats are large modified sebaceous glands that produce
pheromones.

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Glands

2.5.3 Ceruminous glands

Figure 21 Wet-type human earwax on a

cotton swab.
Earwax, also known by the medical term cerumen, is a yellowish, waxy substance secreted
in the ear canal of humans and many other mammals. It plays a vital role in the human ear
canal, assisting in cleaning and lubrication, and also provides some protection from bacteria,
fungus, and insects. A comprehensive review of the physiology and pathophysiology of
cerumen can be found in Roeser and Ballachanda. Excess or impacted cerumen can press
against the eardrum and/or occlude the external auditory canal and impair hearing.
Production, composition, and different types
Cerumen is produced in the outer third of the cartilaginous portion of the human ear
canal. It is a mixture of viscous secretions from sebaceous glands and less-viscous ones from
modified apocrine sweat glands.
Two distinct genetically determined types of earwax are distinguished -- the wet-type which
is dominant, and the dry type which is recessive. Asians and Native Americans are more
likely to have the dry type of cerumen (grey and flaky), whereas Caucasians and Africans

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The Integumentary System

are more likely to have the wet type (honey-brown to dark-brown and moist). Cerumen
type has been used by anthropologists to track human migratory patterns, such as those of
the Inuit.
The difference in cerumen type has been tracked to a single base change (an single nucleotide
polymorphism) in a gene known as "ATP-binding cassette C11 gene". In addition to affecting
cerumen type, this mutation also reduces sweat production. The researchers conjecture that
the reduction in sweat was beneficial to the ancestors of East Asians and Native Americans
who are thought to have lived in cold climates.
Function

Figure 22 Wet-type earwax fluoresces

weakly under ultraviolet light.
Cleaning. Cleaning of the ear canal occurs as a result of the "conveyor belt" process of
epithelial migration, aided by jaw movement. Cells formed in the center of the tympanic
membrane migrate outwards from the umbo (at a rate equivalent to that of fingernail growth)
to the walls of the ear canal, and accelerate towards the entrance of the ear canal. The
cerumen in the canal is also carried outwards, taking with it any dirt, dust, and particulate

54

Glands
matter that may have gathered in the canal. Jaw movement assists this process by dislodging
debris attached to the walls of the ear canal, increasing the likelihood of its extrusion.
Lubrication. Lubrication prevents desiccation and itching of the skin within the ear canal
(known as asteatosis). The lubricative properties arise from the high lipid content of the
sebum produced by the sebaceous glands. In wet-type cerumen at least, these lipids include
cholesterol, squalene, and many long-chain fatty acids and alcohols.
Antibacterial and antifungal roles. While studies conducted up until the 1960s found
little evidence supporting an antibacterial role for cerumen, more recent studies have found
that cerumen provides some bactericidal protection against some strains of bacteria. Cerumen
has been found to be effective in reducing the viability of a wide range of bacteria (sometimes
by up to 99%), including Haemophilus influenzae, Staphylococcus aureus, and many variants
of Escherichia coli. The growth of two fungi commonly present in otomycosis was also
significantly inhibited by human cerumen. These antimicrobial properties are due principally
to the presence of saturated fatty acids, lysozyme and, especially, to the relatively low pH of
cerumen (typically around 6.1 in normal individuals).

2.5.4 Mammary Glands

Figure 23 Cross section of the breast of a

human female.
Mammary glands are the organs that, in the female mammal, produce milk for the
sustenance of the young. These exocrine glands are enlarged and modified sweat glands and
are the characteristic of mammals which gave the class its name.

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The Integumentary System

Structure
The basic components of the mammary gland are the alveoli (hollow cavities, a few millimetres
large) lined with milk-secreting epithelial cells and surrounded by myoepithelial cells. These
alveoli join up to form groups known as lobules, and each lobule has a lactiferous duct that
drains into openings in the nipple. The myoepithelial cells can contract, similar to muscle
cells, and thereby push the milk from the alveoli through the lactiferous ducts towards the
nipple, where it collects in widenings (sinuses) of the ducts. A suckling baby essentially
squeezes the milk out of these sinuses.

Figure 24 Dissection of a lactating breast.

1 - Fat
2 - Lactiferous duct/lobule
3 - Lobule
4 - Connective tissue
5 - Sinus of lactiferous duct
6 - Lactiferous duct
One distinguishes between a simple mammary gland, which consists of all the milk-secreting
tissue leading to a single lactiferous duct, and a complex mammary gland, which consists of
all the simple mammary glands serving one nipple.
Humans normally have two complex mammary glands, one in each breast, and each complex
mammary gland consists of 10-20 simple glands. (The presence of more than two nipples
is known as polythelia and the presence of more than two complex mammary glands as
polymastia.)
Also, "click" this; tissue"13 , to this a movie visual of the breast.

13

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Glands
Development and hormonal control
The development of mammary glands is controlled by hormones. The mammary glands
exist in both sexes, but they are rudimentary until puberty when in response to ovarian
hormones, they begin to develop in the female. Click this http://health.howstuffworks.
com/adam-200042.htmto see what breast tissue does in a female during menustration.
Estrogen promotes formation, while testosterone inhibits it.
At the time of birth, the baby has lactiferous ducts but no alveoli. Little branching occurs
before puberty when ovarian estrogens stimulate branching differentiation of the ducts into
spherical masses of cells that will become alveoli. True secretory alveoli only develop in
pregnancy, where rising levels of estrogen and progesterone cause further branching and
differentiation of the duct cells, together with an increase in adipose tissue and a richer
blood flow.
Colostrum is secreted in late pregnancy and for the first few days after giving birth. True milk
secretion (lactation) begins a few days later due to a reduction in circulating progesterone
and the presence of the hormone prolactin. The suckling of the baby causes the release of
the hormone oxytocin which stimulates contraction of the myoepithelial cells.
Breast cancer
As described above, the cells of mammary glands can easily be induced to grow and multiply
by hormones. If this growth runs out of control, cancer results. Almost all instances of
breast cancer originate in the lobules or ducts of the mammary glands.
Types of breast cancer

14
15
16
17
18
19

DCIS14 : Ductal Carcinoma in Situ

LCIS15 : Lobular Carcinoma in Situ
Invasive ductal carcinoma16
Invasive lobular carcinoma17
Inflammatory breast cancer18
Paget's disease19

http://en.wikibooks.org/wiki/DCIS
http://en.wikibooks.org/wiki/LCIS
http://en.wikibooks.org/wiki/Invasive%20ductal%20carcinoma
http://en.wikibooks.org/wiki/Invasive%20lobular%20carcinoma
http://en.wikibooks.org/wiki/Inflammatory%20breast%20cancer
http://en.wikibooks.org/wiki/Paget%27s%20disease

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The Integumentary System

Figure 25

Early Signs of Breast Cancer

2.6 Homeostasis
As a whole, the integumentary system plays a big part in maintaining homeostasis. The
integumentary system is the outermost organ system of the body and many of its functions
are related to this location. The skin protects the body against pathogens and chemicals,
minimizes loss or entry of water, and blocks the harmful effects of sunlight. Sensory receptors
in the skin provide information about the external environment, helping the skin regulate
body temperature in response to environmental changes and helping the body react to pain

58

Glossary
and other tactile stimuli. The large surface area of the skin makes it ideal for temperature
regulation. The rate of heat loss can be regulated by the amount of blood flowing through
the blood vessels in the dermis close to the surface of the skin. When the body temperature
rises, as for example during exercise, sympathetic tone is reduced and this brings about
dilation of the blood vessels supplying the skin. The increase in skin blood flow allows heat
to be lost more rapidly so that body temperature does not rise above the normal homeostatic
range. The rate of heat loss can also be boosted by the production of sweat, which takes up
additional heat as it evaporates. Conversely, if heat production is less than required, the
dermal vessels constrict, sweating stops, and heat is conserved by the body.

2.7 Glossary
Areolar
Areolar connective tissue is a pliable, mesh-like tissue with a fluid matrix and functions to
cushion and protect body organs. It acts as a packaging tissue holding the internal organs
together and in correct placement.
Basal lamina20
Basal lamina (often erroneously called basement membrane) is a layer on which epithelium
sits. This layer is composed of an electron-dense layer (lamina densa) between two electronlucid layers (lamina lucida), and is approximately 40-50 nm thick (with exceptions such as
the 100-200 nm glomerular basement membrane).
Dermis21
The dermis is the layer of skin beneath the epidermis that consists of connective tissue and
cushions the body from stress and strain. The dermis is tightly connected to the epidermis
by a basement membrane.
Epidermis22
The epidermis is the outermost layer of the skin. It forms the waterproof, protective
wrap over the body's surface and is made up of stratified squamous epithelium with an
underlying basal lamina.
Fibroblasts23
A fibroblast is a cell that makes the structural fibers and ground substance of connective
tissue.
Hair follicle24
A hair follicle is part of the skin that grows hair by packing old cells together.

20
21
22
23
24

http://en.wikipedia.org/wiki/Basement_membrane
http://en.wikipedia.org/wiki/Dermis
http://en.wikipedia.org/wiki/Epidermis_%28skin%29
http://en.wikipedia.org/wiki/Fibroblasts
http://en.wikipedia.org/wiki/Hair_follicle

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The Integumentary System

Hypodermis25
The hypodermis (also called the hypoderm), is the lowermost layer of the integumentary
system in vertebrates. It is derived from the mesoderm, but unlike the dermis, it is not
derived from the dermatome region of the mesoderm.
Impetigo
This is a superficial skin infection most common among children age 26 years. People
who play close contact sports such as rugby, American football and wrestling are also
susceptible, regardless of age. The name derives from the Latin impetere ("assail"). It is
also known as school sores.
Melanocytes26
These are cells located in the bottom layer of the skin's epidermis and in the middle layer
of the eye, the uvea. Through a process called melanogenesis, these cells produce melanin,
a pigment in the skin, eyes, and hair.
Melanoma27
A melanoma is a malignant tumor that originates in melanocytes. It is a highly malignant
form of skin cancer, and, though rare, is responsible for the majority of skin cancer-related
deaths.
Onychosis28
Deformity or disease of the nails
Papillary29
The papillary layer is outermost and extends into the epidermis to supply it with vessels.
It is composed of loosely arranged fibres. Papillary ridges make up the lines of the hands.
Recticular Layer30
The reticular layer is more dense and is continuous with the hypodermis. It contains the
bulk of the structures (such as sweat glands). The reticular layer is composed of irregularly
arranged fibres and resists stretching.
For more fun pictures of other skin diseases and skin problems "click" to this
cool website
Image Database"31 . Note: From this link then click "Clinical Skin Diseases Images".

25
26
27
28
29
30
31

60

http://en.wikipedia.org/wiki/Hypodermis
http://en.wikipedia.org/wiki/Melanocyte
http://en.wikipedia.org/wiki/Melanoma
http://en.wikipedia.org/wiki/Onychosis
http://en.wikipedia.org/wiki/Papillary
http://en.wikipedia.org/wiki/Reticular_layer
http://tray.dermatology.uiowa.edu/Home.html

Review Questions

2.8 Review Questions

Answers for these questions can be found here32
1. Name all of the parts of the integumentary system.
2. Name the cells that produce melanin and describe its function.
3. Name and describe the importance of the cutaneous senses.
4. Explain how sweating helps maintain normal body temperature.
5. Explain where on the body hair has important functions and describe these functions.
6. What is a melanoma?
A) The outermost layer of skin
B) A type of nail disease
C) A malignant tumor that originates in melanocytes
D) The lower most layer of skin

2.9 References
Brannon, Heather (2006). "Nail Anatomy" About, Inc., A part of The New York Times
Company.
American Academy of Dermatology - Nail Health33
Cobb, Judith. Fingernails, Jewels or Tools34 ? Nature's Field - Nail diagnosis
Graaff, Van De (2002). Human Anatomy, Sixth Edition. New York: McGraw-Hill.
Mader, Sylvia S. (2004). Human Biology. New York: McGraw-Hill.
Sorrentino, Sheila A. (2004). Mosby's textbook for Nursing Assistants, 6th Edition. St.
Louis, Missouri: Mosby.

32
33
34

http://en.wikibooks.org/wiki/Human_Physiology/Appendix_1:_answers_to_review_
questions#Integumentary_System
http://www.aad.org/public/Publications/pamphlets/NailHealth.htm
http://www.nspforum.com/faq/index.cgi?read=929

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3 The Nervous System

The central nervous system includes the brain and spinal cord. The brain and spinal
cord are protected by bony structures, membranes, and fluid. The brain is held in the
cranial cavity of the skull and it consists of the cerebrum, cerebellum, and the brain
stem. The nerves involved are cranial nerves and spinal nerves.

Figure 26

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The Nervous System

3.1 Overview of the entire nervous system

The nervous system has three main functions: sensory input, integration of data and motor
output. Sensory input is when the body gathers information or data, by way of neurons,
glia and synapses. The nervous system is composed of excitable nerve cells (neurons) and
synapses that form between the neurons and connect them to centers throughout the body
or to other neurons. These neurons operate on excitation or inhibition, and although nerve
cells can vary in size and location, their communication with one another determines their
function. These nerves conduct impulses from sensory receptors to the brain and spinal
cord. The data is then processed by way of integration of data, which occurs only in the
brain. After the brain has processed the information, impulses are then conducted from the
brain and spinal cord to muscles and glands, which is called motor output. Glia cells are
found within tissues and are not excitable but help with myelination, ionic regulation and
extracellular fluid.
The nervous system is comprised of two major parts, or subdivisions, the central nervous
system (CNS) and the peripheral nervous system (PNS). The CNS includes the brain and
spinal cord. The brain is the body's "control center". The CNS has various centers located
within it that carry out the sensory, motor and integration of data. These centers can be
subdivided to Lower Centers (including the spinal cord and brain stem) and Higher centers
communicating with the brain via effectors. The PNS is a vast network of spinal and cranial
nerves that are linked to the brain and the spinal cord. It contains sensory receptors which
help in processing changes in the internal and external environment. This information is
sent to the CNS via afferent sensory nerves. The PNS is then subdivided into the autonomic
nervous system and the somatic nervous system. The autonomic has involuntary control
of internal organs, blood vessels, smooth and cardiac muscles. The somatic has voluntary
control of skin, bones, joints, and skeletal muscle. The two systems function together, by
way of nerves from the PNS entering and becoming part of the CNS, and vice versa.

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General functions of the CNS

3.2 General functions of the CNS

Figure 27

Brain, brain stem, and spinal cord.

CNS:
The "Central Nervous System", comprised of brain, brain stem, and spinal cord.
The central nervous system (CNS) represents the largest part of the nervous system, including
the brain and the spinal cord. Together, with the peripheral nervous system (PNS), it has a
fundamental role in the control of behavior.

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The Nervous System

The CNS is conceived as a system devoted to information processing, where an appropriate
motor output is computed as a response to a sensory input. Many threads of research
suggest that motor activity exists well before the maturation of the sensory systems, and
senses only influence behavior without dictating it. This has brought the conception of the
CNS as an autonomous system.
w:Central nervous system1

3.3 Structure and function of neurons

3.3.1 Structure
Neurons are highly specialized for the processing and transmission of cellular signals. Given
the diversity of functions performed by neurons in different parts of the nervous system,
there is, as expected, a wide variety in the shape, size, and electrochemical properties of
neurons. For instance, the soma of a neuron can vary in size from 4 to 100 micrometers in
diameter.
The soma (cell body) is the central part of the neuron. It contains the nucleus of the cell,
and therefore is where most protein synthesis occurs. The nucleus ranges from 3 to 18
micrometers in diameter. The dendrites of a neuron are cellular extensions with many
branches, and metaphorically this overall shape and structure is referred to as a dendritic
tree. This is where the majority of input to the neuron occurs. However, information outflow
(i.e. from dendrites to other neurons) can also occur (except in chemical synapse in which
backflow of impulse is inhibited by the fact that axon do not possess chemoreceptors and
dendrites cannot secrete neurotransmitter chemical). This explains one way conduction of
nerve impulse. The axon is a finer, cable-like projection which can extend tens, hundreds,
or even tens of thousands of times the diameter of the soma in length. The axon carries
nerve signals away from the soma (and also carry some types of information back to it).
Many neurons have only one axon, but this axon may - and usually will - undergo extensive
branching, enabling communication with many target cells. The part of the axon where it
emerges from the soma is called the 'axon hillock'. Besides being an anatomical structure, the
axon hillock is also the part of the neuron that has the greatest density of voltage-dependent
sodium channels. This makes it the most easily-excited part of the neuron and the spike
initiation zone for the axon: in neurological terms it has the greatest hyperpolarized action
potential threshold. While the axon and axon hillock are generally involved in information
outflow, this region can also receive input from other neurons as well. The axon terminal
is a specialized structure at the end of the axon that is used to release neurotransmitter
chemicals and communicate with target neurons. Although the canonical view of the neuron
attributes dedicated functions to its various anatomical components, dendrites and axons
often act in ways contrary to their so-called main function.
Axons and dendrites in the central nervous system are typically only about a micrometer
thick, while some in the peripheral nervous system are much thicker. The soma is usually
about 1025 micrometers in diameter and often is not much larger than the cell nucleus it

66

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Function
contains. The longest axon of a human motor neuron can be over a meter long, reaching
from the base of the spine to the toes. Sensory neurons have axons that run from the toes
to the dorsal columns, over 1.5 meters in adults. Giraffes have single axons several meters in
length running along the entire length of their necks. Much of what is known about axonal
function comes from studying the squids giant axon, an ideal experimental preparation
because of its relatively immense size (0.51 millimeters thick, several centimeters long).

3.4 Function
Sensory afferent neurons convey information from tissues and organs into the central nervous
system. Efferent neurons transmit signals from the central nervous system to the effector
cells and are sometimes called motor neurons. Interneurons connect neurons within specific
regions of the central nervous system. Afferent and efferent can also refer generally to
neurons which, respectively, bring information to or send information from brain region.
Classification by action on other neurons
Excitatory neurons excite their target postsynaptic neurons or target cells causing it to
function. Motor neurons and somatic neurons are all excitatory neurons. Excitatory neurons
in the brain are often glutamatergic. Spinal motor neurons, which synapse on muscle cells,
use acetylcholine as their neurotransmitter. Inhibitory neurons inhibit their target neurons.
Inhibitory neurons are also known as short axon neurons, interneurons or microneurons. The
output of some brain structures (neostriatum, globus pallidus, cerebellum) are inhibitory.
The primary inhibitory neurotransmitters are GABA and glycine. Modulatory neurons evoke
more complex effects termed neuromodulation. These neurons use such neurotransmitters
as dopamine, acetylcholine, serotonin and others. Each synapses can receive both excitatory
and inhibitory signals and the outcome is determined by the adding up of summation.

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The Nervous System

3.5 Excitatory and inhibitory process

Figure 28

Nerve Synapse

The release of an excitatory neurotransmitter (e.g. glutamate) at the synapses will cause
an inflow of positively charged sodium ions (Na+) making a localized depolarization of the
membrane. The current then flows to the resting (polarized) segment of the axon.
Inhibitory synapse causes an inflow of Cl- (chlorine) or outflow of K+ (potassium) making
the synaptic membrane hyperpolarized. This increase prevents depolarization, causing a
decrease in the possibility of an axon discharge. If they are both equal to their charges, then
the operation will cancel itself out. This effect is referred to as summation.
There are two types of summation: spatial and temporal. Spatial summation requires several
excitatory synapses (firing several times) to add up, thus causing an axon discharge. It
also occurs within inhibitory synapses, where just the opposite will occur. In temporal
summation, it causes an increase of the frequency at the same synapses until it is large
enough to cause a discharge. Spatial and temporal summation can occur at the same time
as well.
The neurons of the brain release inhibitory neurotransmitters far more than excitatory
neurotransmitters, which helps explain why we are not aware of all memories and all sensory
stimuli simultaneously. The majority of information stored in the brain is inhibited most of
the time.

3.6 Summation
When excitatory synapses exceed the amount of inhibitory synapses there are, then the
excitatory synapses will prevail over the other. The same goes with inhibitory synapses,

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Generation & propagation of an action potential

if there are more inhibitory synapses than excitatory, the synapses will be inhibited. To
determine all of this is called summation.
Classification by discharge patterns:
Neurons can be classified according to their electrophysiological characteristics (note that
a single action potential is not enough to move a large muscle, and instead will cause a
twitch).
Tonic or regular spiking: Some neurons are typically constantly (or tonically) active.
Example: interneurons in neurostriatum.
Phasic or bursting: Neurons that fire in bursts are called phasic.
Fast spiking: Some neurons are notable for their fast firing rates. For example, some types
of cortical inhibitory interneurons, cells in globus pallidus.
Thin-spike: Action potentials of some neurons are more narrow compared to the others.
For example, interneurons in prefrontal cortex are thin-spike neurons.
Classification by neurotransmitter released:
Some examples are cholinergic, GABAergic, glutamatergic and dopaminergic neurons.

3.6.1 Central Nervous System

The central nervous system is the control center for the body. It regulates organ function,
higher thought, and movement of the body. The central nervous system consists of the brain
and spinal cord.

3.7 Generation & propagation of an action potential

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The Nervous System

Figure 29

70

Electrical characteristics of a neurochemical action potential.

Generation & propagation of an action potential

3.7.1 The Nerve Impulse

Figure 30

animated action potential

When a nerve is stimulated the resting potential changes. Examples of such stimuli are pressure, electricity, chemicals, etc. Different neurons are sensitive to different stimuli(although
most can register pain). The stimulus causes sodium ion channels to open. The rapid change
in polarity that moves along the nerve fiber is called the "action potential." This moving
change in polarity has several stages:
Depolarization
The upswing is caused when positively charged sodium ions (Na+) suddenly rush through
open sodium gates into a nerve cell. The membrane potential of the stimulated cell
undergoes a localized change from -65 millivolts to 0 in a limited area. As additional
sodium rushes in, the membrane potential actually reverses its polarity so that the outside
of the membrane is negative relative to the inside. During this change of polarity the
membrane actually develops a positive value for a moment(+40 millivolts). The change in
voltage stimulates the opening of additional sodium channels (called a voltage-gated ion
channel). This is an example of a positive feedback loop.
Repolarization
The downswing is caused by the closing of sodium ion channels and the opening of potassium
ion channels. Release of positively charged potassium ions (K+) from the nerve cell when
potassium gates open. Again, these are opened in response to the positive voltage--they
are voltage gated. This expulsion acts to restore the localized negative membrane potential
of the cell (about -65 or -70 mV is typical for nerves).

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The Nervous System

Figure 31

sodium potassium pump

Refractory phase
is a short period of time after the depolarization stage. Shortly after the sodium gates open
they close and go into an inactive conformation. The sodium gates cannot be opened again
until the membrane is repolarized to its normal resting potential. The sodium-potassium
pump returns sodium ions to the outside and potassium ions to the inside. During the
refractory phase this particular area of the nerve cell membrane cannot be depolarized.
This refractory area explains why action potentials can only move forward from the point
of stimulation.
Increased permeability of the sodium channel occurs when there is a deficit of calcium ions.
when there is a deficit of calcium ions (Ca+2) in the interstitial fluid the sodium channels
are activated (opened) by very little increase of the membrane potential above the normal
resting level. The nerve fiber can therefore fire off action potentials spontaneously, resulting
in tetany. Could be caused by the lack of hormone from parathyroid glands. could be caused
by hyperventilation, which leads to a higher pH, which causes calcium to bind and become
unavailable. Speed of conduction. This area of depolarization/repolarization/recovery moves
along a nerve fiber like a very fast wave. In myelinated fibers, conduction is hundreds of
times faster because the action potential only occurs at the nodes of Ranvier (pictured below
in 'types of neurons') by jumping from node to node. This is called "saltatory" conduction.
Damage to the myelin sheath by the disease can cause severe impairment of nerve cell
function. Some poisons and drugs interfere with nerve impulses by blocking sodium channels
in nerves. See discussion on drug at the end of this outline.

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3.8 Brain

Figure 32

A color-coded image of the brain, showing the main sections.

The brain is found in the cranial cavity. Within it are found the higher nerve centers
responsible for coordinating the sensory and motor systems of the body (forebrain). The
brain stem houses the lower nerve centers (consisting of midbrain, pons, and medulla),

3.8.1 Medulla
The medulla is the control center for respiratory, cardiovascular and digestive functions.

3.8.2 Pons
The pons houses the control centers for respiration and inhibitory functions. Here it will
interact with the cerebellum.

3.8.3 Cerebrum
The cerebrum, or top portion of the brain, is divided by a deep crevice, called the longitudinal
sulcus. The longitudinal sulcus separates the cerebrum in to the right and left hemispheres.
In the hemispheres you will find the cerebral cortex, basal ganglia and the limbic system.
The two hemispheres are connected by a bundle of nerve fibers called the corpus callosum.
The right hemisphere is responsible for the left side of the body while the opposite is true
of the left hemisphere. Each of the two hemispheres are divided into four separated lobes:

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the frontal in control of specialized motor control, learning, planning and speech; parietal
in control of somatic sensory functions; occipital in control of vision; and temporal lobes
which consists of hearing centers and some speech. Located deep to the temporal lobe of
the cerebrum is the insula.

3.8.4 Cerebellum
The cerebellum is the part of the brain that is located posterior to the medulla oblongata and
pons. It coordinates skeletal muscles to produce smooth, graceful motions. The cerebellum
receives information from our eyes, ears, muscles, and joints about what position our body
is currently in (proprioception). It also receives output from the cerebral cortex about
where these parts should be. After processing this information, the cerebellum sends motor
impulses from the brain stem to the skeletal muscles. The main function of the cerebellum
is coordination. The cerebellum is also responsible for balance and posture. It also assists
us when we are learning a new motor skill, such as playing a sport or musical instrument.
Recent research shows that apart from motor functions cerebellum also has some emotional
role.

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3.8.5 The Limbic System and Higher Mental Functions

Figure 33

Image of the brain, showing the Limbic system.

The Limbic System

The Limbic System is a complex set of structures found just beneath the cerebrum and on
both sides of the thalamus. It combines higher mental functions, and primitive emotion, into
one system. It is often referred to as the emotional nervous system. It is not only responsible
for our emotional lives, but also our higher mental functions, such as learning and formation
of memories. The Limbic system explains why some things seem so pleasurable to us, such

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as eating and why some medical conditions are caused by mental stress, such as high blood
pressure. There are two significant structures within the limbic system and several smaller
structures that are important as well. They are:
1.
2.
3.
4.
5.
6.

The
The
The
The
The
The

Hippocampus
Amygdala
Thalamus
Hypothalamus
Fornix and Parahippocampus
Cingulate Gyrus

Structures of the Limbic System

Hippocampus
The Hippocampus is found deep in the temporal lobe, shaped like a seahorse. It consists of
two horns that curve back from the amygdala. It is situated in the brain so as to make the
prefrontal area aware of our past experiences stored in that area. The prefrontal area of the
brain consults this structure to use memories to modify our behavior. The hippocampus is
responsible for memory.
Amygdala
The Amygdala is a little almond shaped structure, deep inside the anteroinferior region of
the temporal lobe, connects with the hippocampus, the septi nuclei, the prefrontal area
and the medial dorsal nucleus of the thalamus. These connections make it possible for the
amygdala to play its important role on the mediation and control of such activities and
feelings as love, friendship, affection, and expression of mood. The amygdala is the center
for identification of danger and is fundamental for self preservation. The amygdala is the
nucleus responsible for fear..
Thalamus
Lesions or stimulation of the medial, dorsal, and anterior nuclei of the thalamus are
associated with changes in emotional reactivity. However, the importance of these nuclei on
the regulation of emotional behavior is not due to the thalamus itself, but to the connections
of these nuclei with other limbic system structures. The medial dorsal nucleus makes
connections with cortical zones of the prefrontal area and with the hypothalamus. The
anterior nuclei connect with the mamillary bodies and through them, via fornix, with the
hippocampus and the cingulated gyrus, thus taking part in what is known as the Papez's
circuit.

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Figure 34

Image of the brain showing the location of the hypothalamus.

Hypothalamus
The Hypothalamus is a small part of the brain located just below the thalamus on both
sides of the third ventricle. Lesions of the hypothalamus interfere with several vegetative
functions and some so called motivated behaviors like sexuality, combativeness, and hunger.
The hypothalamus also plays a role in emotion. Specifically, the lateral parts seem to be
involved with pleasure and rage, while the medial part is linked to aversion, displeasure,
and a tendency to uncontrollable and loud laughing. However, in general the hypothalamus
has more to do with the expression of emotions. When the physical symptoms of emotion

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appear, the threat they pose returns, via the hypothalamus, to the limbic centers and then
the prefrontal nuclei, increasing anxiety.
The Fornix and Parahippocampal
These small structures are important connecting pathways for the limbic system.
The Cingulate Gyrus
The Cingulate Gyrus is located in the medial side of the brain between the cingulated
sulcus and the corpus callosum. There is still much to be learned about this gyrus, but it is
already known that its frontal part coordinates smells and sights, with pleasant memories
of previous emotions. The region participates in the emotional reaction to pain and in the
regulation of aggressive behavior.
Memory and Learning
Memory is defined as : The mental faculty of retaining and recalling past experiences, the
act or instance of remembering recollection. Learning takes place when we retain and utilize
past memories.
Overall, the mechanisms of memory are not completely understood. Brain areas such as
the hippocampus, the amygdala, the striatum, or the mammillary bodies are thought to
be involved in specific types of memory. For example, the hippocampus is believed to be
involved in spatial learning and declarative learning (learning information such as what
you're reading now), while the amygdala is thought to be involved in emotional memory.
Damage to certain areas in patients and animal models and subsequent memory deficits
is a primary source of information. However, rather than implicating a specific area, it
could be that damage to adjacent areas, or to a pathway traveling through the area is
actually responsible for the observed deficit. Further, it is not sufficient to describe memory,
and its counterpart, learning, as solely dependent on specific brain regions. Learning and
memory are attributed to changes in neuronal synapses, thought to be mediated by long-term
potentiation and long-term depression.
There are three basic types of memory:
1. Sensory Memory
2. Short Term Memory
3. Long Term Memory
Sensory Memory
The sensory memories act as a buffer for stimuli through senses. A sensory memory retains
an exact copy of what is seen or heard: iconic memory for visual, echoic memory for aural
and haptic memory for touch. Information is passed from sensory memory into short term

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memory. Some believe it lasts only 300 milliseconds, it has unlimited capacity. Selective
attention determines what information moves from sensory memory to short term memory.
Short Term Memory
Short Term Memory acts as a scratch pad for temporary recall of the information under
process. For instance, in order to understand this sentence you need to hold in your mind
the beginning of the sentence as you read the rest. Short term memory decays rapidly
and also has a limited capacity. Chunking of information can lead to an increase in the
short term memory capacity, this is the reason why a hyphenated phone number is easier
to remember than a single long number. The successful formation of a chunk is known
as closure. Interference often causes disturbance in short term memory retention. This
accounts for the desire to complete a task held in short term memory as soon as possible.
Within short term memory there are three basic operations:
1. Iconic memory - the ability to hold visual images
2. Acoustic memory - the ability to hold sounds. Can be held longer than iconic.
3. Working memory - an active process to keep it until it is put to use. Note that the goal
is not really to move the information from short term memory to long term memory,
but merely to put it to immediate use.
The process of transferring information from short term to long term memory involves the
encoding or consolidation of information. This is not a function of time, that is, the longer
the memory stays in the short term the more likely it is to be placed in the long term
memory. On organizing complex information in short term before it can be encoded into
the long term memory, in this process the meaningfulness or emotional content of an item
may play a greater role in its retention in the long term memory. The limbic system sets up
local reverberating circuits such as the Papez's Circuit.
Long Term Memory
Long Term Memory is used for storage of information over a long time. Information from
short to long term memory is transferred after a short period. Unlike short term memory,
long term memory has little decay. Long term potential is an enhanced response at the
synapse within the hippocampus. It is essential to memory storage. The limbic system
isn't directly involved in long term memory necessarily but it selects them from short term
memory, consolidates these memories by playing them like a continuous tape, and involves
the hippocampus and amygdala.
There are two types of long term memory:
1. Episodic Memory
2. Semantic Memory
Episodic memory represents our memory of events and experiences in a serial form. It is
from this memory that we can reconstruct the actual events that took place at a given point
in our lives. Semantic memory, on the other hand, is a structured record of facts, concepts,

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and skills that we have acquired. The information in the semantic memory is derived from
our own episode memory, such as that we can learn new facts or concepts from experiences.
There are three main activities that are related to long term memory:
1. Storage
2. Deletion
3. Retrieval
Information for short term memory is stored in long term memory by rehearsal. The repeated
exposure to a stimulus or the rehearsal of a piece of information transfers it into long term
memory. Experiments also suggest that learning is most effective if it is distributed over
time. Deletion is mainly caused by decay and interference. Emotional factors also affect
long term memory. However, it is debatable whether we actually ever forget anything or
whether it just sometimes becomes increasingly difficult to retrieve it. Information may not
be recalled sometimes but may be recognized, or may be recalled only with prompting. This
leads us to the third operation of memory, information retrieval.
There are two types of information retrieval:
1. Recall
2. Recognition
In recall, the information is reproduced from memory. In recognition the presentation of the
information provides the knowledge that the information has been seen before. Recognition
is of lesser complexity, as the information is provided as a cue. However, the recall may be
assisted by the provision of retrieval cues which enable the subject to quickly access the
information in memory.
Long-term Potentiation

Warning

Long term potentiation is largely theoretical. Many of the concepts have experimental
backing, but there is still a substantial amount of controversy over other parts. There
are also processes involved in long-term potentiation that go beyond the scope of this
introductory book, and have been simplified. Consider this a starting place.
. Long-term potentiation (LTP) is the lasting enhancement of connections between two
neurons that results from stimulating them simultaneously. Since neurons communicate via
chemical synapses, and because memories are believed to be stored within these synapses,
LTP and it's opposing process, long-term depression, are widely considered the major cellular
mechanisms that underlie learning and memory. This has been proven by lab experiments.
When one of the chemicals involved (PKMzeta, it will be discussed later) is inhibited in
rats, it causes retrograde amnesia with short term memory left intact (meaning they can't
recall events from before the inhibitor was given).
By enhancing synaptic transmission, LTP improves the ability of two neuron, one presynaptic
and the other postsynaptic, to communicate with one another across a synapse. The precise
mechanism for this enhancement isn't known, but it varies based on things like brain region,

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age and species. This will focus on LTP in the CA1 section of the hippocampus, because
that's what is well known.
The end result of LTP is a well established neural circuit that can be called upon later for
memory.
LTP in the CA1 hippocampus is called NMDA receptor-dependent LTP. It has four main
properties.
Rapid induction
LTP can be rapidly induced by applying one or more brief, high-frequency, stimulus to a
presynaptic cell.
Input specificity
Once induced, LTP at one synapse does not spread to other synapses; rather LTP is input
specific. LTP is only propagated to those synapses according to the rules of associativity
and cooperativity.
Associativity
Associativity refers to the observation that when weak stimulation of a single pathway is
insufficient for the induction of LTP, simultaneous strong stimulation of another pathway
will induce LTP at both pathways.
Cooperativity
LTP can be induced either by strong tetanic stimulation of a single pathway to a synapse,
or cooperatively via the weaker stimulation of many. When one pathway into a synapse
is stimulated weakly, it produces insufficient postsynaptic depolarization to induce LTP.
In contrast, when weak stimuli are applied to many pathways that converge on a single
patch of postsynaptic membrane, the individual postsynaptic depolarizations generated
may collectively depolarize the postsynaptic cell enough to induce LTP cooperatively.
Synaptic tagging, discussed later, may be a common mechanism underlying associativity
and cooperativity.
LTP is generally divided into three parts that occur sequentially: Short-term potentiation,
early LTP (E-LTP) and late LTP (L-LTP). Short-term potentiation isn't well understood
and will not be discussed.
E-LTP and L-LTP phases of LTP are each characterized by a series of three events: induction,
maintenance and expression. Induction happens when a short-lived signal triggers that
phase to begin. Maintenance corresponds to the persistent biochemical changes that occur in
response to the induction of that phase. Expression entails the long-lasting cellular changes
that result from activation of the maintenance signal.
Each phase of LTP has a set of mediator molecules that dictate the events of that phase.
These molecules include protein receptors, enzymes, and signaling molecules that allow
progression from one phase to the next. In addition to mediators, there are modulator
molecules that interact with mediators to fine tune the LTP. Modulators are a bit beyond
the scope of this introductory book, and won't be discussed here.

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Early Phase
Induction
E-LTP induction begins when the calcium inside the postsynaptic cell exceeds a threshold.
In many types of LTP, the flow of calcium into the cell requires the NMDA receptor, which
is why these types of LTP are considered NMDA receptor-dependent.
When a stimulus is applied to the presynaptic neuron, it releases a neurotransmitter, typically
glutamate, onto the postsynaptic cell membrane where it binds to AMPA receptors, or
AMPARs. This causes an influx of sodium ions into the postsynaptic cell, this short lived
depolarization is called the excitatory postsynaptic potential (EPSP) and makes it easier for
the neuron to fire an action potential.
A single stimulus doesn't cause a big enough depolarization to trigger an E-LTP, instead it
relies on EPSP summation. If EPSPs are reaching the cell before the others decay, they
will add up. When the depolarization reaches a critical level, NMDA receptors lose the
magnesium molecule they were originally plugged with and let calcium in. The rapid rise
in calcium within the postsynaptic neuron trigger the short lasting activation of several
enzymes that mediate E-LTP induction. Of particular importance are some protein kinase
enzymes, including CaMKII and PKC. To a lesser extent, PKA and MAPK activation also
contribute.
Maintenance
During the maintenance stage of E-LTP, CaMKII and PKC lose their dependence on calcium
and become autonomously active. They then carry out phosphorylation that underlies
E-LTP expression.
Expression
CaMKII and PKC phosphorylate existing AMPA receptors to increase their activity, and
mediate the insertion of additional AMPA receptors onto the postsynaptic cell membrane.
This is achieved by having a pool of nonsynaptic AMPA receptors adjacent to the postsynaptic
membrane. When the appropriate stimulus arrives, the nonsynaptic AMPA receptors are
brought into the postsynaptic membrane under the influence of protein kinases.
AMPA receptors are one of the most common type of receptors in the brain. Their effect is
excitatory. By adding more AMPA receptors, and increasing their activity, future stimuli
will generate larger postsynaptic responses.
Late Phase
Late LTP is the natural extension of E-LTP. L-LTP requires gene transcription and
protein synthesis in the postsynaptic cell, unlike E-LTP. Late LTP is also associated with
the presynaptic synthesis of synaptotagmin and an increase in synaptic vesicle number,
suggesting that L-LTP induces protein synthesis not only in postsynaptic cells, but in
presynaptic cells as well. This is discussed under "retrograde messenger" below.
Induction

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Late LTP is induced by changes in gene expression and protein synthesis brought about
by persistent activation of protein kinases activated during E-LTP, such as MAPK. In fact,
MAPK--Specifically the ERK subfamily of MAPKs--may be the molecular link between
E-LTP and L-LTP, since many signaling cascades involved in E-LTP, including CaMKII
and PKC, can converge on ERK.
Maintenance
Upon activation, ERK may phosphorylate a number of cytoplasmic and nuclear molecules
that ultimately result in the protein synthesis and morphological changes associated with
L-LTP. These chemicals may include transcription factors such as CREB. ERK-mediated
changes in transcription factor activity may trigger the synthesis of proteins that underlie
the maintenance of L-LTP. PKMzeta is one such molecule. When this molecule is inhibited
in rats, they experience retrograde amnesia (where you can't recall previous events but short
term memory works fine).
Expression
Aside from PKMzeta, many of the proteins synthesized during L-LTP are unknown. They
are though to increase postsynaptic dendritic spine number, surface area and sensitivity to
the neurotransmitter associated with L-LTP expression.
Retrograde Signaling
Retrograde signaling is a hypothesis that attempts to explain that, while LTP is induced and
expressed postsynaptically, some evidence suggests that it is expressed presynaptically as well.
The hypothesis gets its name because normal synaptic transmission is directional and proceeds
from the presynaptic to the postsynaptic cell. For induction to occur postsynaptically and
be partially expressed presynaptically, a message must travel from the postsynaptic cell to
the presynaptic cell in a retrograde (reverse) direction. Once there, the message presumably
initiates a cascade of events that leads to a presynaptic component of expression, such as
the increased probability of neurotransmitter vesicle release.
Retrograde signaling is currently a contentious subject as some investigators do not believe
the presynaptic cell contributes at all to the expression of LTP. Even among proponents of
the hypothesis there is controversy over the identity of the messenger.
Language and Speech
Language depends on semantic memory so some of the same areas in the brain are involved
in both memory and language. Articulation, the forming of speech, is represented bilaterally
in the motor areas. However, for most individuals, language analysis and speech formation
take place in regions of the left hemisphere only. The two regions involved are:
1. Broca's Area
2. Wernicke's Area
Broca's area is located just in front of the voice control area of the left motor cortex. This
region assembles the motor of speech and writing. For example, patients with lesions in this
area:

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1. Are unable to understand language perfectly
2. May not be able to write clearly
3. Usually speak spontaneously
Wernicke's area is part of the auditory and visual associations cortex. This region is
responsible for the analysis and formation of language content. For example, patients with
lesions in this area:
1. Are unable to name objects
2. Are unable to understand the meaning of words
3. Articulate speech readily but usually nonsensically
Diseases of the Limbic System
There are several well known diseases that are disorders of the limbic system. Several are
discussed here.
Schizophrenia
An increased dopamine (DA) response in the limbic system results in schizophrenia. DA
may be synthesized or secreted in excess, DA receptors may be supersensitive, and DA
regulatory mechanism may be defective. Symptoms are decreased by drugs which block DA
receptors. Symptoms of schizophrenia are:
1.
2.
3.
4.
5.
6.
7.

Loss of touch with reality

Decreased ability to think and reason
Decreased ability to concentrate
Decreased memory
Regress in child-like behavior
Altered mood and impulsive behavior
Auditory hallucinations

Symptoms may be so severe that the individual cannot function.

Depression
Depression is the most common major mental illness and is characterized by both emotional
and physical symptoms. Symptoms of depression are:
1.
2.
3.
4.
5.
6.
7.
8.

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Intense sadness and despair

Anxiety
Loss of ability to concentrate
Pessimism
Feelings of low self esteem
Insomnia or hypersomnia
Increased or decreased appetite
Changes in body temperature and endocrine gland function

Brain
10 to 15% of depressed individuals display suicidal behavior during their lifetime.
The cause of depression and its symptoms are a mystery but we do understand that it is
an illness associated with biochemical changes in the brain. A lot of research goes on to
explain that it is associated with a lack of amines serotonin and norephinephrine. Therefore
pharmacological treatment strategies often try to increase amine concentrations in the brain.
One class of antidepressants is monoamine oxidase inhibitors. Mono amine oxidase is a
enzyme that breaks down your amines like norephinephrine and serotonin. Because the
antidepressants inhibit their degradation they will remain in the synaptic cleft for a longer
period of time making the effect just as if you had increased theses types of neurotransmitters.
A newer class of antidepressants is selective serotonin reuptake inhibitors (SSRI's). With
SSRI's decreasing the uptake of serotonin back into the cell that will increase the amount
of serotonin present in the synaptic cleft. SSRI's are more specific than the monoamine
oxidase inhibitors because they only affect serotonergic synapses. You might recognize these
SSRI's by name as Prozac and Paxil.
Bipolar Disorder
Another common form of depression is manic depression. Manic is an acute state characterized by:
1.
2.
3.
4.

Excessive elation and impaired judgment

Insomnia and irritability
Hyperactivity
Uncontrolled speech

Manic depression, also known as bipolar disorder, displays mood swings between manic
and depression. The limbic system receptors are unregulated. Drugs used are unique mood
stabilizers.
The hippocampus is particularly vulnerable to several disease processes, including ischemia,
which is any obstruction of blood flow or oxygen deprivation, Alzheimers disease, and epilepsy.
These diseases selectively attack CA1, which effectively cuts through the hippocampal circuit.
An Autism Link
A connection between autism and the limbic system has also been noted as well. URL:
http://www.autism.org/limbic.html
Case Study
Central Pain Syndrome
I was 42 years old when my life changed forever. I had a stroke. As an avid viewer of medical
programs on television I assumed that I would have physical therapy for my paralyzed left
side and get on with my life. No one ever mentioned pain or the possibility of pain, as a

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result of the stroke. I did experience unusual sensitivity to touch while still in the hospital,
but nothing to prepare me for what was to come.
The part of my brain that is damaged is the Thalamus. This turns out to be the pain center
and what I have now is an out of control Thalamus, resulting in Thalamic Pain syndrome,
also called Central Pain Syndrome. This means that 24 hours a day, seven days a week, my
brain sends messages of pain and it never goes away. I am under the care of physicians, who
not only understand chronic pain, but are also willing to treat it with whatever medications
offer some help. None of the medications, not even narcotic medications, take the pain away.
They just allow me to manage it so I can function.

3.9 The Peripheral Nervous System

Figure 35

The Cranial Nerves

The peripheral nervous system includes 12 cranial nerves 31 pairs of spinal nerves. It
can be subdivided into the somatic and autonomic systems. It is a way of communication
from the central nervous system to the rest of the body by nerve impulses that regulate the
functions of the human body.
The twelve cranial nerves are
I Olfactory Nerve for smell
II Optic Nerve for vision
III Oculomotor for looking around

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IV Trochlear for moving eye
V Trigeminal for feeling touch on face
VI Abducens to move eye muscles
VII Facial to smile, wink, and help us taste
VIII Vestibulocochlear to help with balance, equilibrium, and hearing
IX Glossopharengeal for swallowing and gagging
X Vagus for swallowing, talking, and parasympathetic actions of digestion
XI Spinal accessory for shrugging shoulders
XII Hypoglossal for tongue more divided into different regions as muscles
The 10 out of the 12 cranial nerves originate from the brain stem, and mainly control the
functions of the anatomic structures of the head with some exceptions. CN X receives
visceral sensory information from the thorax and abdomen, and CN XI is responsible for
innervating the sternocleidomastoid and trapezius muscles, neither of which is exclusively in
the head.
Spinal nerves take their origins from the spinal cord. They control the functions of the rest
of the body. In humans, there are 31 pairs of spinal nerves: 8 cervical, 12 thoracic, 5 lumbar,
5 sacral and 1 coccygeal. The naming convention for spinal nerves is to name it after the
vertebra immediately above it. Thus the fourth thoracic nerve originates just below the
fourth thoracic vertebra. This convention breaks down in the cervical spine. The first spinal
nerve originates above the first cervical vertebra and is called C1. This continues down to
the last cervical spinal nerve, C8. There are only 7 cervical vertebrae and 8 cervical spinal
nerves.

3.9.1 Lateral cord

The lateral cord gives rise to the following nerves:
The lateral pectoral nerve, C5, C6 and C7 to the pectoralis major muscle, or musculus
pectoralis major.
The musculocutaneous nerve which innervates the biceps muscle
The median nerve, partly. The other part comes from the medial cord. See below for
details.

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3.9.2 Posterior cord

Figure 36 diagram showing human dermatoms, i.e., skin regions

with respect to the routing of their nerve connection of their afferent
nerves through the spinal cord.
The posterior cord gives rise to the following nerves:
The upper subscapular nerve, C7 and C8, to the subscapularis muscle, or musculus supca
of the rotator cuff.
The lower subscapular nerve, C5 and C6, to the teres major muscle, or the musculus
teres major, also of the rotator cuff.

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The thoracodorsal nerve, C6, C7 and C8, to the latissimus dorsi muscle, or musculus
latissimus dorsi.
The axillary nerve, which supplies sensation to the shoulder and motor to the deltoid
muscle or musculus deltoideus, and the teres minor muscle, or musculus teres minor.
The radial nerve, or nervus radialis, which innervates the triceps brachii muscle, the
brachioradialis muscle, or musculus brachioradialis the extensor muscles of the fingers
and wrist (extensor carpi radialis muscle), and the extensor and abductor muscles of the
thumb. See radial nerve injuries.

3.9.3 Medial cord

The medial cord gives rise to the following nerves:

The median pectoral nerve, C8 and T1, to the pectoralis muscle

The medial brachial cutaneous nerve, T1
The medial antebrachial cutaneous nerve, C8 and T1
The median nerve, partly. The other part comes from the lateral cord. C7, C8 and T1
nerve roots. The first branch of the median nerve is to the pronator teres muscle, then
the flexor carpi radialis, the palmaris longus and the flexor digitorum superficialis. The
median nerve provides sensation to the anterior palm, the anterior thumb, index finger
and middle finger. It is the nerve compressed in carpal tunnel syndrome.
The ulnar nerve originates in nerve roots C7, C8 and T1. It provides sensation to the
ring and pinky fingers. It innervates the flexor carpi ulnaris muscle, the flexor digitorum
profundus muscle to the ring and pinky fingers, and the intrinsic muscles of the hand
(the interosseous muscle, the lumbrical muscles and the flexor pollicus brevis muscle).
This nerve traverses a groove on the elbow called the cubital tunnel, also known as the
funny bone. Striking the nerve at this point produces an unpleasant sensation in the ring
and little fingers.

3.9.4 Other thoracic spinal nerves (T3-T12)

The remainder of the thoracic spinal nerves, T3 through T12, do little recombining. They
form the intercostal nerves, so named because they run between the ribs. For points of
reference, the 7th intercostal nerve terminates at the lower end of the sternum, also known
as the xyphoid process. The 10th intercostal nerve terminates at the umbilicus, or the belly
button.
The somatic nervous system is that part of the peripheral nervous system associated
with the voluntary control of body movements through the action of skeletal muscles, and
also reception of external stimuli. The somatic nervous system consists of afferent fibers
that receive information from external sources, and efferent fibers that are responsible for
muscle contraction. The somatic system includes the pathways from the skin and skeletal
muscles to the Central Nervous System. It is also described as involved with activities that
involve consciousness.
The basic route of the efferent somatic nervous system includes a two neuron sequence. The
first is the upper motor neuron, whose cell body is located in the precentral gyrus (Brodman
Area 4) of the brain. It receives stimuli from this area to control skeletal (voluntary) muscle.

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The upper motor neuron carries this stimulus down the corticospinal tract and synapses
in the ventral horn of the spinal cord with the alpha motor neuron, a lower motor neuron.
The upper motor neuron releases acetylcholine from its axon terminal knobs and these are
received by nicotinic receptors on the alpha motor neuron. The alpha motor neurons cell
body sends the stimulus down its axon via the ventral root of the spinal cord and proceeds
to its neuromuscular junction of its skeletal muscle. There, it releases acetylcholine from its
axon terminal knobs to the muscles nicotinic receptors, resulting in stimulus to contract the
muscle.
The somatic system includes all the neurons connected with the muscles, sense organs and
skin. It deals with sensory information and controls the movement of the body.

3.10 The Autonomic System

The Autonomic system deals with the visceral organs, like the heart, stomach, gland,
and the intestines. It regulates systems that are unconsciously carried out to keep our body
alive and well, such as breathing, digestion (peristalsis), and regulation of the heartbeat.
The Autonomic system consists of the sympathetic and the parasympathetic divisions.
Both divisions work without conscious effort, and they have similar nerve pathways, but
the sympathetic and parasympathetic systems generally have opposite effects on target
tissues (they are antagonistic). By controlling the relative input from each division, the
autonomic system regulates many aspects of homeostasis. One of the main nerves for the
parasympathetic autonomic system is Cranial Nerve X, the Vagus nerve.

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Figure 37 Figure 1: The right sympathetic chain and its connections with the thoracic,
abdominal, and pelvic plexuses. (After Schwalbe.)

3.10.1 The Sympathetic and Parasympathetic Systems

The sympathetic nervous system activates what is often termed the fight or flight response,
as it is most active under sudden stressful circumstances (such as being attacked). This
response is also known as sympathetico-adrenal response of the body, as the pre-ganglionic
sympathetic fibers that end in the adrenal medulla (but also all other sympathetic fibers)
secrete acetylcholine, which activates the secretion of adrenaline (epinephrine) and to a lesser
extent noradrenaline (norepinephrine) from it. Therefore, this response that acts primarily

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on the cardiovascular system is mediated directly via impulses transmitted through the
sympathetic nervous system and indirectly via catecholamines secreted from the adrenal
medulla.
Western science typically looks at the SNS as an automatic regulation system, that is, one
that operates without the intervention of conscious thought. Some evolutionary theorists
suggest that the sympathetic nervous system operated in early organisms to maintain survival
(Origins of Consciousness, Robert Ornstein; et al.), as the sympathetic nervous system is
responsible for priming the body for action. One example of this priming is in the moments
before waking, in which sympathetic outflow spontaneously increases in preparation for
action.
The parasympathetic nervous system is part of the autonomic nervous system. Sometimes
called the rest and digest system or feed and breed. The parasympathetic system conserves
energy as it slows the heart rate, increases intestinal and gland activity, and relaxes sphincter
muscles in the gastrointestinal tract.
After high stress situations (ie: fighting for your life) the parasympathetic nervous system
has a backlash reaction that balances out the reaction of the sympathetic nervous system.
For example, the increase in heart rate that comes along with a sympathetic reaction will
result in an abnormally slow heart rate during a parasympathetic reaction.

3.10.2 Organization
Sympathetic nerves originate inside the vertebral column, toward the middle of the spinal
cord in the intermediolateral cell column (or lateral horn), beginning at the first thoracic
segment of the spinal cord and extending into the second or third lumbar segments. Because
its cells begin in the thoracic and lumbar regions of the spinal cord, the SNS is said to have
a thoracolumbar outflow. Axons of these nerves leave the spinal cord in the ventral branches
(rami) of the spinal nerves, and then separate out as 'white rami' (so called from the shiny
white sheaths of myelin around each axon) which connect to two chain ganglia extending
alongside the vertebral column on the left and right. These elongated ganglia are also known
as paravertebral ganglia or sympathetic trunks. In these hubs, connections (synapses) are
made which then distribute the nerves to major organs, glands, and other parts of the body.
[1]
In order to reach the target organs and glands, the axons must travel long distances in the
body, and, to accomplish this, many axons link up with the axon of a second cell. The ends
of the axons do not make direct contact, but rather link across a space, the synapse.
In the SNS and other components of the peripheral nervous system, these synapses are made
at sites called ganglia. The cell that sends its fiber is called a preganglionic cell, while the
cell whose fiber leaves the ganglion is called a postganglionic cell. As mentioned previously,
the preganglionic cells of the SNS are located between the first thoracic segment and the
second or third lumbar segments of the spinal cord. Postganglionic cells have their cell
bodies in the ganglia and send their axons to target organs or glands.
The ganglia include not just the sympathetic trunks but also the superior cervical ganglion
(which sends sympathetic nerve fibers to the head), and the celiac and mesenteric ganglia
(which send sympathetic fibers to the gut).

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3.10.3 Information transmission

Messages travel through the SNS in a bidirectional flow. Efferent messages can trigger
changes in different parts of the body simultaneously. For example, the sympathetic nervous
system can accelerate heart rate; widen bronchial passages; decrease motility (movement) of
the large intestine; constrict blood vessels; increase peristalsis in the esophagus; cause pupil
dilation, piloerection (goose bumps) and perspiration (sweating); and raise blood pressure.
Afferent messages carry sensations such as heat, cold, or pain.
The first synapse (in the sympathetic chain) is mediated by nicotinic receptors physiologically
activated by acetylcholine, and the target synapse is mediated by adrenergic receptors
physiologically activated by either noradrenaline or adrenaline. An exception is with sweat
glands which receive sympathetic innervation but have muscarinic acetylcholine receptors
which are normally characteristic of PNS. Another exception is with certain deep muscle
blood vessels, which have acetylcholine receptors and which dilate (rather than constrict)
with an increase in sympathetic tone. The sympathetic system cell bodies are located on
the spinal cord excluding the cranial and sacral regions. The preganglonic neurons exit from
the vertebral column and synapse with the postganglonic nerouns in the sympathetic trunk.
The parasympathetic nervous system is one of three divisions of the autonomic nervous
system. Sometimes called the rest and digest system, the parasympathetic system conserves
energy as it slows the heart rate, increases intestinal and gland activity, and relaxes sphincter
muscles in the gastrointestinal tract.

3.10.4 Relationship to sympathetic

While an oversimplification, it is said that the parasympathetic system acts in a reciprocal
manner to the effects of the sympathetic nervous system; in fact, in some tissues innervated
by both systems, the effects are synergistic.

3.10.5 Receptors
The parasympathetic nervous system uses only acetylcholine (ACh) as its neurotransmitter.
The ACh acts on two types of receptors, the muscarinic and nicotinic cholinergic receptors.
Most transmissions occur in two stages: When stimulated, the preganglionic nerve releases
ACh at the ganglion, which acts on nicotinic receptors of the postganglionic nerve. The
postganglionic nerve then releases ACh to stimulate the muscarinic receptors of the target
organ.
The three main types of muscarinic receptors that are well characterised are:
The M1 muscarinic receptors are located in the neural system.
The M2 muscarinic receptors are located in the heart, and act to bring the heart back to
normal after the actions of the sympathetic nervous system: slowing down the heart rate,
reducing contractile forces of the atrial cardiac muscle, and reducing conduction velocity
of the atrioventricular node (AV node). Note, they have no effect on the contractile forces
of the ventricular muscle.

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The M3 muscarinic receptors are located at many places in the body, such as the
smooth muscles of the blood vessels, as well as the lungs, which means that they cause
vasoconstriction and bronchoconstriction. They are also in the smooth muscles of the
gastrointestinal tract (GIT), which help in increasing intestinal motility and dilating
sphincters. The M3 receptors are also located in many glands that help to stimulate
secretion in salivary glands and other glands of the body.

3.11 Nervous Tissue

The nervous system coordinates the activity of the muscles, monitors the organs, constructs
and also stops input from the senses, and initiates actions. Prominent participants in a
nervous system include neurons and nerves, which play roles in such coordination.Our
nervous tissue only consists of two types of cells. These cells are neurons and neuroglia cells.
The neurons are responsible for transmitting nerve impulses. Neuroglia cells are responsible
for supporting and nourishing the neuron cells.

3.11.1 Types of Neurons

Figure 38

There are three types of neurons in the body. We have sensory neurons, interneurons, and
motor neurons. Neurons are a major class of cells in the nervous system. Neurons are
sometimes called nerve cells, though this term is technically imprecise, as many neurons
do not form nerves. In vertebrates, neurons are found in the brain, the spinal cord and in
the nerves and ganglia of the peripheral nervous system. Their main role is to process and
transmit information. Neurons have excitable membranes, which allow them to generate
and propagate electrical impulses. Sensory neuron takes nerve impulses or messages right

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Case Study
from the sensory receptor and delivers it to the central nervous system. A sensory receptor
is a structure that can find any kind of change in it's surroundings or environment.

3.11.2 Structure of a neuron

Neurons have three different parts to them. They all have an axon, a cell body and dendrites.
The axon is the part of the neuron that conducts nerve impulses. Axons can get to be
quite long. When an axon is present in nerves, it is called a nerve fiber. A cell body has a
nucleous and it also has other organelles. The dendrites are the short pieces that come off
of the cell body that receive the signals from sensory receptors and other neurons.

3.11.3 Myelin Sheath

Schwann cells contain a lipid substance called myelin in their plasma membranes. When
schwann cells wrap around axons, a myelin sheath forms. There are gaps that have no
myelin sheath around them; these gaps are called nodes of Ranvier. Myelin sheathes make
excellent insulators. Axons that are longer have a myelin sheath, while shorter axons do not.
The disease multiple sclerosis is an autoimmune disease where the body attacks the myelin
sheath of the central nervous system.

3.12 Case Study

A 35-year-old male in 1986 had been admitted to a hospital in Florida three weeks previous
to being diagnosed, with complaints of weakness and spasticity in the right leg, difficulties
with balance, and fatigue and malaise. Tests performed at the Florida hospital had revealed
abnormalities in spinal fluid and MRI brain scan. The patient complained of being severely
depressed and anxious. He had anger at his circumstances and frequent crying spells. One
month previously he had noticed aching and loss of vision in the left eye that had since
improved.
This man was diagnosed with Multiple Sclerosis (MS). MS is a chronic, degenerative, and
progressive disorder that affects the nerve fibers in the brain and spinal cord. Myelin is a
fatty substance that surrounds and insulates the nerve fibers and facilitates the conduction
of the nerve impulse transmissions. MS is characterized by intermittent damage to myelin
(called demyelination) caused by the destruction of specialized cells (oligodendrocytes) that
form the substance. Demyelination causes scarring and hardening (sclerosis) of nerve fibers
usually in the spinal cord, brain stem, and optic nerves, which slows nerve impulses and
results in weakness, numbness, pain, and vision loss. Because different nerves are affected at
different times, MS symptoms often worsen (exacerbate), improve, and develop in different
areas of the body. Early symptoms of the disorder may include vision changes (blurred
vision, blind spots) and muscle weakness. MS can progress steadily or cause acute attacks
(exacerbations) followed by partial or complete reduction in symptoms (remission). Most
patients with the disease have a normal lifespan.
There are different types of MS

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Multiple sclerosis is classified according to frequency and severity of neurological symptoms,
the ability of the CNS to recover, and the accumulation of damage.

Figure 39

3.12.1 Treating Depression

Every now and then we all feel a little blue, these feelings can be caused by losing a loved
one. Clinical depression goes much further than just feeling down. Depression has many
symptoms, including lack of energy, abnormal eating habits (either too much or too little)
and sleeping problems (also too much or too little). Often a person can feel worthless
and have thoughts of committing suicide. The cause of depression and its symptoms are a
mystery but we do understand that it is an illness associated with biochemical changes in
the brain. A lot of research goes on to explain that it is associated with a lack of amines
serotonin and norephinephrine. Therefore pharmacological treatment strategies often try to
increase amine concentrations in the brain.
One class of antidepressants is monoamine oxidase inhibitors. Mono amine oxidase is a
enzyme that breaks down your amines like norephinephrine and serotonin. Because the
antidepressants inhibit their degradation they will remain in the synaptic cleft for a longer
period of time making the effect just as if you had increased theses types of neurotransmitters.
A newer class of antidepressants is selective serotonin reuptake inhibitors (SSRI's). With
SSRI's decreasing the uptake of serotonin back into the cell that will increase the amount

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Drugs
of serotonin present in the synaptic cleft. SSRI's are more specific than the monoamine
oxidase inhibitors because they only affect serotonergic synapses. You might recognize these
SSRI's by name as Prozac and Paxil.

3.13 Drugs
A drug is, generally speaking, any substance that changes the way your body works. Some
drugs have a medicinal effect, and some are used recreationally. They have diverse effects,
depending on the drug. Drugs can do anything from diminish pain, to preventing blood
clots, to helping a depressed person.
Different drugs work in different ways, called the mechanism of action, the drugs covered
here will all act on the nervous system via receptors on different neurons. There are also
drugs that change how enzymes work, but that's not part of the nervous system (at least
directly) and will not be discussed here.
You've probably heard the terms stimulant (excitatory) and depressant (inhibitory). This
is a broad way of classifying drugs that work on the CNS. Depressants slow down neural
function, and stimulants speed it up.
Most of the common depressants (including alcohol, benzodiazepines, barbiturates and GHB)
work on GABA receptors, although there are others. Opiates, for example, work on mu
opioid receptors and also produce inhibitory effects, and some antipsychotics block serotonin.
See the alcohol section below to see one way this can work.
Stimulants work mostly with epinephrine, dopamine or serotonin (or a combination of them).
Many of them either mimic one, or stop them from leaving the synapse, causing more action
potentials to be fired. Methamphetamine, discussed below, is a fairly typical stimulant drug.

3.13.1 Drug Abuse

Scientists have long accepted that there is a biological basis for drug addiction, though the
exact mechanisms responsible are only now being identified. It is believed that addictive
substances create dependence in the user by changing the brain's reward functions, located
in the mesolimbic dopamine systemthe part of the brain that reinforces certain behaviors
such as eating, sexual intercourse, exercise, and social interaction. Addictive substances,
through various means and to different degrees, cause the synapses of this system to flood
with excessive amounts of dopamine, creating a brief rush of euphoria more commonly
called a "high. Some say that abuse begins when the user begins shirking responsibility
in order to afford drugs or to have enough time to use them. Some say it begins when
a person uses "excessive" amounts, while others draw the line at the point of legality,
and others believe it amounts to chronic use despite degenerating mental and physical

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health in the user. Some think that any intoxicant consumption is an inappropriate
activity. Here are some drugs that are abused frequently: Acid/LSD, Alcohol, various
tryptamines and phenethylamines, Cocaine, Ecstasy/MDMA, Heroin, Inhalants, Marijuana,
Methamphetamine, PCP/Phencyclidine, Prescription Medications, Smoking/Nicotine and
Steroids.

3.13.2 Alcohol
Alcohol is, and has been for thousands of years, one of the most commonly used drugs in the
world. It is legal, with some restrictions and exceptions, nearly everywhere. It is a common
misconception that somehow alcohol is 'better' or 'safer' than other recreational drugs. This
is simply NOT the case. Alcohol is a depressant, and as such it has the potential to cause
coma, respiratory depression/arrest and possibly death. Compared with some other (illegal
in most places) drugs of recreational value (such as marijuana, serotonin based hallucinogens
like LSD or psilocybin) alcohol is far more toxic and has more risk of overdose. That doesn't
mean that moderate drinking will probably hurt you, though, either.
Short term effects from drinking (listed roughly as they appear, and as dosage goes up)
are: decreased inhibitions and thusly judgment, flushing of the face, drowsiness, memory
problems begin, severe motor impairment, blurry vision, dizziness, confusion, nausea, possible
unconsciousness, coma, death (due to respiratory arrest or possibly aspiration on vomit).
Alcohol produces these effects mainly via the GABA receptors in the brain. When GABA
(or in this case alcohol) binds to it's receptor, it lets either Cl- ions in, or K+ out. This is
called hyperpolarization, or an inhibitory postsynaptic potential (IPSP). It makes it harder
for the neuron to depolarize and hence harder for it to fire an action potential, slowing
neural function. At higher doses alcohol will start to block NMDA. NMDA is involved in
memory (see the long-term potentiation section) so this is thought to account for memory
blackouts.

3.13.3 Methamphetamine
In the US, medically prescribed methamphetamine is distributed in tablet form under
the brand name Desoxyn, generally for Attention Deficit Hyperactivity Disorder (ADHD)
but also for narcolepsy or obesity.
Illicit methamphetamine comes in a variety of forms. Most commonly it is found as a
colorless crystalline solid, sold on the street under a variety of names, such as: crystal meth
or crystal. Methamphetamine may also be referred to as shards, rock, pony, crissie, crystal,
glass, ice, Jib, critter, Tina, tweak or crank. Dope may refer to methamphetamine or other
drugs, especially heroin or marijuana. The term "speed" can denote any stimulant including
other amphetamines (e.g. adderall), cocaine and methylphenidate (Ritalin).
Methamphetamine can be injected (either subcutaneous, intramuscular or intravenous),
smoked, snorted, swallowed, or used rectally or sublingually. The latter two being fairly
uncommon. After administration, methamphetamine takes from a few seconds (smoked
or injected IV) to around 30 minutes (oral) for effects to arise, lasting around eight hours
depending on the route of administration. Effects/side effects include euphoria, anorexia,

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increased energy, clenching of the jaw/grinding of teeth (bruxism), weight loss, insomnia,
tooth decay and psychosis among others.
Methamphetamine is neurotoxic to at least some areas of the brain, and owes most of it's
effects to the neurotransmitters dopamine, norepinephrine and serotonin it releases. It also
blocks the reuptake of those neurotransmitters, causing them to stay in the synaptic cleft
longer than normal.

3.13.4 Marijuana

Figure 41

Cannabis sativa.

Marijuana contains a myriad of chemicals, called cannabinoids, that have psychoactive and
medicinal effects when consumed, the major one being tetrahydrocannabinol (THC). THC
serves to mimic the endogenous neurotransmitter anandamide (also found in chocolate) at
the CB1 receptors in the brain. Other cannabinoids include Cannabidiol (CBD), cannabinol

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(CBN) and tetrahydrocannabivarin (THCV). Although THC is found in all parts of the
plant, the flower of the female plant has the highest concentration, commonly around eight
percent. The flowers can be used, or they can be refined. Trichomes contain most of the THC
on the flowers and can be removed by a few different methods. These removed trichomes
are called kief. Kief can, in turn, be pressed into hashish. By far the most common way to
consume any of these products is by smoking, but it can be taken orally as well.
Cannabis has a very long, very good safety record. Nobody on record has ever died because
of marijuana, directly at least. It is estimated that it would take 1-1.8 kilograms of average
potency marijuana, taken orally, to have a fifty percent chance of killing a 68kg human.
Despite this, the possession, use, or sale of psychoactive cannabis products became illegal
in many parts of the world in the early 20th century. Since then, while some countries
have intensified the enforcement of cannabis prohibition, others have reduced the priority of
enforcement to the point of de facto legality. Cannabis remains illegal in the vast majority
of the world's countries.
The nature and intensity of the immediate effects of cannabis consumption vary according
to the dose, the species or hybridization of the source plant, the method of consumption, the
user's mental and physical characteristics (such as possible tolerance), and the environment
of consumption. This is sometimes referred to as set and setting. Smoking the same cannabis
either in a different frame of mind (set) or in a different location (setting) can alter the
effects or perception of the effects by the individual. Effects of cannabis consumption may be
loosely classified as cognitive and physical. Anecdotal evidence suggests that the Cannabis
sativa species tends to produce more of the cognitive or perceptual effects, while Cannabis
indica tends to produce more of the physical effects.

3.14 Review Questions

Answers for these questions can be found here2
1. The junction between one neuron and the next, or between a neuron and an effector is
called:
A ) A synapse
B ) A dendrite
C ) A neuotransmitter
D ) A ventricle
E ) None of the above
2. A fast excitatory synapses follows this order:
A ) (1) neurotransmitter released (2) diffused across the synaptic cleft to a receptor protein
(3) binding of the transmitter opens pores in the ion channels and positive ions move in.

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http://en.wikibooks.org/wiki/Human_Physiology/Appendix_1:_answers_to_review_
questions#The_Nervous_System

Review Questions
B ) (1) neurotransmitter released (2) diffused across the synaptic cleft to a receptor protein
(3) binding of the transmitter opens pores in the ion channels and negative ions move in.
C ) (1) neurotransmitter released (2) diffused across the synaptic cleft to a receptor amino
acid (3) binding of the transmitter opens pores in the ion channels and positive ions move
in.
D ) (1) diffused across the synaptic cleft to a receptor protein (2) neurotransmitter released
(3) binding of the transmitter opens pores in the ion channels and positive ions move in.
E ) None of the above
3. Resting potential is
A ) excess positive ions accumulate inside the plasma membrane
B ) excess negative ions accumulate inside the plasma membrane
C ) excess positive ions accumulate outside the plasma membrane
D ) both b & c
E ) both a & c
4. Sensory neurons have:
A ) A short dendrite and a long axon
B ) A short dendrite and a short axon
C ) A long dendrite and a short axon
D ) A long dendrite and a long axon
E ) Their axons and dendrites may be either long or short
5. ________blocks Acetylcholine receptor sites causing muscle relaxation.
A ) Novocain
B ) curare
C ) Nicotine
D ) Nerve gases
6. Transmission across a synapse is dependent on the release of _______?
A ) neurotransmitters
B ) synaptic vesicle
C ) neuromuscular tisssue
D ) receptor proteins
7. Motor neurons take messages
A ) from the muscle fiber to the central nervous system
B ) away from the central nervous system to the central nervous system

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C ) that are classified
D ) away from the central nervous system to muscle fiber
8. The medulla oblongata helps to regulate which of the following:
A ) Breathing
B ) Heartbeat
C ) Sneezing
D ) Vomiting
E ) All of the above
9. The nervous systems main components are what?
A) The Synapses and Sprinal cord
B) The neurons and the synapses
C) The bain and the neurons
D)The brain and the spinal cord
10. Explain what LTP does to enhance communication between two neurons, on the
postsynaptic end.
11. Explain what LTP does to enhance communication between two neurons, on the
presynaptic end.

3.15 Glossary
Afferent Messages: carry sensations such as heat, cold, or pain
Autonomic System: deals with the visceral organs, like the heart, stomach, gland, and
the intestines
Axon: the part of the neuron that conducts nerve impulses
Cannabis: a psychoactive drug produced from parts of the cannabis plant
Central Nervous System (CNS): the system that includes the brain and the spinal cord
Cerebellum: part of the brain that is located posterior to the medulla oblongata and pons,
coordinates skeletal muscles to produce smooth, graceful motions
Cerebrospinal Fluid (CSF): acts a shock absorber for the central nervous system, protecting the brain and spinal cord from injury; it also has a high glucose content which serves
as a nutritional factor
Cerebrum motor control, learning, speech, somatic sensory functions, vision,hearing and
more.
Dendrites: short pieces that come off of the cell body that receive the signals from sensory
receptors and other neurons

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References
Episodic Memory: represents our memory of events and experiences in a serial form
Excitatory Neurotransmitter: a neurotransmitter that acts to elicit an action potential
by opening sodium ion channels
Longitudinal Sulcus: separates the cerebrum in to the right and left hemispheres
Long Term Memory: used for storage of information over a long time
Long-Term Potentiation (LTP) long term communication enhancement between two
neurons. Results in neural pathways that store memoris.
Medulla control center for respiratory, cardiovascular and digestive functions.
Myelin: a fatty substance that surrounds and insulates the nerve fibers and facilitates the
conduction of the nerve impulse transmissions
Multiple Sclerosis (MS): disease that affects the CNS by causing hardening and scaring
of the myelin
Nodes of Ranvier: unmyelinated gaps between sections of myelin
Peripheral Nervous System (PNS): a way of communication from the central nervous
system to the rest of the body by nerve impulses that regulate the functions of the human
body
Pons control centers for respiration and inhibitory functions.
Postganglionic Cells: have their cell bodies in the ganglia and send their axons to target
organs or glands
Postsynaptic Cells the cell on the receiving (second) end of the synapse.
Presynaptic Cell The cell on the sending (first) end of the synapse.
Proprioception the sense that indicates whether the body is moving with required effort,
as well as where various parts of the body are located in relation to each other.
Sensory Receptor: structure that can find any kind of change in it's surroundings or
environment
Somatic Nervous System (SNS): the part of the peripheral nervous system associated
with the voluntary control of body movements through the action of skeletal muscles, and
also reception of external stimuli
Synapses: the gap between two neurons; new synapses lead to learning

3.16 References
http://action.painfoundation.org/site/News2?page=NewsArticle&id=
5135&security=1&news_iv_ctrl=1061 Esther Wednesday, October 19, 2005
http://www.neurologychannel.com/multiplesclerosis/
http://www.theraj.com/ms/casestudy.html

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4 The Senses
4.1 What are Senses?
We experience reality through our senses. Senses are the physiological methods of perception,
so a sense is a faculty by which outside stimuli are perceived. The senses and their
operation, classification, and theory are overlapping topics studied by a variety of fields.
Many neurologists disagree about how many senses there actually are due to a broad
interpretation of the definition of a sense. Our senses are split into two different groups.
Our exteroceptors detect stimulation from the outsides of our body. For example smell,
taste, and equilibrium. The interoceptors receive stimulation from the inside of our bodies.
For instance, blood pressure dropping, changes in the gluclose and pH levels. Children are
generally taught that there are five senses (sight, hearing, touch, smell, taste). However, it
is generally agreed that there are at least seven different senses in humans, and a minimum
of two more observed in other organisms. Sense can also differ from one person to the next.
Take taste for an example: what may taste great to one person will taste awful to someone
else. This has to do with how the brain interprets the stimuli that are received.

4.2 Chemoreception
The senses of gustation (taste) and olfaction (smell) fall under the category of chemoreception. Specialized cells act as receptors for certain chemical compounds. As these
compounds react with the receptors, an impulse is sent to the brain and is registered as a
certain taste or smell. Gustation and olfaction are chemical senses because the receptors
they contain are sensitive to the molecules in the food we eat, along with the air we breathe.

4.2.1 Gustatory System

In humans, the sense of taste is transduced by taste buds and is conveyed via three of the
twelve cranial nerves. Cranial nerve VII, the facial nerve, carries taste sensations from the
anterior two thirds of the tongue (excluding the circumvallate papillae, see lingual papilla)
and soft palate. Cranial nerve IX the glossopharyngeal nerve carries taste sensations from
the posterior one third of the tongue (including the circumvallate papillae). Also a branch of
the vagus nerve carries some taste sensations from the back of the oral cavity (i.e. pharynx
and epiglottis). Information from these cranial nerves is processed by the gustatory system.
Though there are small differences in sensation, which can be measured with highly specific
instruments, all taste buds can respond to all types of taste. Sensitivity to all tastes is
distributed across the whole tongue and indeed to other regions of the mouth where there
are taste buds (epiglottis, soft palate).

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The Senses
Papilla
Papilla are specialized epithelial cells. There are four types of papillae: filiform (threadshape), fungiform (mushroom-shape), foliate (leaf-shape), and circumvallate (ringedcircle). All papillae except the filiform have taste buds on their surface. Some act directly
by ion channels, others act indirectly.
Fungiform papillae - as the name suggests, are slightly mushroom shaped if looked at
in section. These are present mostly at the apex (tip) of the tongue.
Filiform papillae - these are thin, longer papillae that don't contain taste buds but are
the most numerous. These papillae are mechanical and not involved in gustation.
Foliate papillae - these are ridges and grooves towards the posterior part of the tongue.
Circumvallate papillae - there are only about 3-14 of these papillae on most people
and they are present at the back of the oral part of the tongue. They are arranged in a
circular-shaped row just in front of the sulcus terminalis of the tongue.

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Structure of Taste Buds

Figure 42 The mouth cavity. The cheeks have been slit transversely and the tongue
pulled forward.

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The Senses

Figure 43 Semidiagrammatic view of a portion of the mucous membrane of the tongue.

Two fungiform papill are shown. On some of the filiform papill the epithelial
prolongations stand erect, in one they are spread out, and in three they are folded in.

Each taste bud is flask-like in shape, its broad base resting on the corium, and its neck
opening by an orifice, the gustatory pore, between the cells of the epithelium.
The bud is formed by two kinds of cells: supporting cells and gustatory cells.
The supporting cells are mostly arranged like the staves of a cask, and form an outer envelope
for the bud. Some, however, are found in the interior of the bud between the gustatory cells.
The gustatory cells occupy the central portion of the bud; they are spindle-shaped, and each
possesses a large spherical nucleus near the middle of the cell. The peripheral end of the cell
terminates at the gustatory pore in a fine hair-like filament, the gustatory hair.

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The central process passes toward the deep extremity of the bud, and there ends in single or
bifurcated varicosities.
The nerve fibrils after losing their medullary sheaths enter the taste bud, and end in fine
extremities between the gustatory cells; other nerve fibrils ramify between the supporting
cells and terminate in fine extremities; these, however, are believed to be nerves of ordinary
sensation and not gustatory.
Types of Taste
Salt
Arguably the simplest receptor found in the mouth is the salt (NaCl) receptor. An ion
channel in the taste cell wall allows Na+ ions to enter the cell. This on its own depolarizes
the cell, and opens voltage-regulated Ca2+ gates, flooding the cell with ions and leading to
neurotransmitter release. This sodium channel is known as EnAC and is composed of three
subunits. EnAC can be blocked by the drug amiloride in many mammals, especially rats.
The sensitivity of the salt taste to amiloride in humans, however, is much less pronounced,
leading to conjecture that there may be additional receptor proteins besides EnAC that
may not have been discovered yet.
Sour
Sour taste signals the presence of acidic compounds (H+ ions in solution). There are three
different receptor proteins at work in sour taste. The first is a simple ion channel which
allows hydrogen ions to flow directly into the cell. The protein for this is EnAC, the same
protein involved in the distinction of salt taste (this implies a relationship between salt and
sour receptors and could explain why salty taste is reduced when a sour taste is present).
There are also H+ gated channels present. The first is a K+ channel, which ordinarily
allows K+ ions to escape from the cell. H+ ions block these, trapping the potassium ions
inside the cell (this receptor is classified as MDEG1 of the EnAC/Deg Family). A third
protein opens to Na+ ions when a hydrogen ion attaches to it, allowing the sodium ions to
flow down the concentration gradient into the cell. The influx of ions leads to the opening
of a voltage regulated Ca2+ gate. These receptors work together and lead to depolarization
of the cell and neurotransmitter release.
Bitter
There are many classes of bitter compounds which can be chemically very different. It
is interesting that the human body has evolved a very sophisticated sense for bitter
substances: we can distinguish between the many radically different compounds which
produce a generally bitter response. This may be because the sense of bitter taste is so
important to survival, as ingesting a bitter compound may lead to injury or death. Bitter
compounds act through structures in the taste cell walls called G-protein coupled receptors
(GPCRs). Recently, a new group of GPCRs was discovered, known as the T2Rs, which
is thought to only respond to bitter stimuli. When the bitter compound activates the
GPCR, it in turn releases gustducin, the G-protein it was coupled to. Gustducin is made
of three subunits. When it is activated by the GPCR, its subunits break apart and activate
phosphodiesterase, a nearby enzyme. It then converts a precursor within the cell into a
secondary messenger, which closes potassium ion channels. This secondary messenger can

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stimulate the endoplasmic reticulum to release Ca2+, which contributes to depolarization.
This leads to a build-up of potassium ions in the cell, depolarization, and neurotransmitter
release. It is also possible for some bitter tastants to interact directly with the G-protein,
because of a structural similarity to the relevant GPCR.
Sweet
Like bitter tastes, sweet taste transduction involves GPCRs. The specific mechanism
depends on the specific molecule. Natural sweeteners such as saccharides activate the
GPCR, which releases gustducin. The gustducin then activates the molecule adenylate
cyclase, which is already inside the cell. This molecule increases concentration of the
molecule cAMP, or adenosine 3', 5'-cyclic monophosphate. This protein will either directly
or indirectly close potassium ion channels, leading to depolarization and neurotransmitter
release. Synthetic sweeteners such as saccharin activate different GPCRs, initiating a
similar process of protein transitions, starting with the protein phospholipase A, which
ultimately leads to the blocking of potassium ion channels.
Umami
Umami is a Japanese word meaning "savory" or "meaty". It is thought that umami receptors
act much the same way as bitter and sweet receptors (they involve GPCRs), but not much
is known about their specific function. We do know that umami detects glutamates that are
common in meats, cheese and other protein-heavy foods. Umami receptors react to foods
treated with monosodium glutamate (MSG). This explains why eating foods that have
MSG in them often give a sense of fullness. It is thought that the amino acid L-glutamate
bonds to a type of GPCR known as a metabotropic glutamate receptor (mGluR4). This
causes the G-protein complex to activate a secondary receptor, which ultimately leads to
neurotransmitter release. The intermediate steps are not known.
Disorders of the Tongue
Loss of taste
You may lose your sense of taste if the facial nerve is damaged. Then there is also Sjogren's
Syndrome where the saliva production is reduced. In most cases the loss of taste is typically
a symptom of anosmia - a loss of the sense of smell.
Sore tongue
It is usually caused by some form of trauma, such as biting your tongue, or eating piping-hot
or highly acidic food or drink.
If your top and bottom teeth dont fit neatly together, tongue trauma is more likely.
Some people may experience a sore tongue from grinding their teeth (bruxism).
Disorders such as diabetes, anemia, some types of vitamin deficiency and certain skin
diseases can include a sore tongue among the range of symptoms.
Glossodynia
A condition characterized by a burning sensation on the tongue.

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Benign migratory glossitis
This condition is characterized by irregular and inflamed patches on the tongue surface
that often have white borders. The tongue may be generally swollen, red and sore. Another
name for this condition is geographic tongue. The cause of benign migratory glossitis is
unknown.
Risk factors are thought to include:

Mineral or vitamin deficiencies

Local irritants, such as strong mouthwashes, cigarettes or alcohol
Certain forms of anemia
Infection
Certain medications
Stress

4.2.2 Olfactory System

Olfaction is the sense of smell. In humans the sence of Smell is received in nasopharynx.
Airborne molecules go into solution on moist epithelial surface of nasal passage. An olfactory
receptors neuron sends an impulse via Cranial nerve I the olfactory nerve. Although 80-90%
of what we think is "taste" actually is due to smell. This is why when we have a head cold
or stuffed up nose we have a harder time tasting our foods.
Receptors
Humans have 347 functional odor receptor genes; the other genes have nonsense mutations.
This number was determined by analyzing the genome in the Human Genome Project; the
number may vary among ethnic groups, and does vary among individuals. For example, not
all people can smell androstenone, a component of male sweat.
Each olfactory receptor neuron in the nose expresses only one functional odor receptor.
Odor receptor nerve cells may function like a key-lock system: if the odor molecules can fit
into the lock the nerve cell will respond. According to shape theory, each receptor detects
a feature of the odor molecule. Weak-shape theory, known as odotope theory, suggests
that different receptors detect only small pieces of molecules, and these minimal inputs are
combined to create a larger olfactory perception (similar to the way visual perception is built
up of smaller, information-poor sensations, combined and refined to create a detailed overall
perception). An alternative theory, the vibration theory proposed by Luca Turin (1996,
2002), posits that odor receptors detect the frequencies of vibrations of odor molecules in
the infrared range by electron tunneling. However, the behavioral predictions of this theory
have been found lacking (Keller and Vosshall, 2004).
An olfactory receptor neuron, also called an olfactory sensory neuron, is the primary
transduction cell in the olfactory system. Humans have about 40 million olfactory receptor
neurons. In vertebrates, olfactory receptor neurons reside on the olfactory epithelium in the
nasal cavity. These cells are bipolar neurons with a dendrite facing the interior space of the
nasal cavity and an axon that travels along the olfactory nerve to the olfactory bulb.

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Many tiny hair-like cilia protrude from the olfactory receptor cell's dendrite and into the
mucus covering the surface of the olfactory epithelium. These cilia contain olfactory receptors,
a type of G protein-coupled receptor. Each olfactory receptor cell contains only one type
of olfactory receptor, but many separate olfactory receptor cells contain the same type of
olfactory receptor. The axons of olfactory receptor cells of the same type converge to form
glomeruli in the olfactory bulb.
Olfactory receptors can bind to a variety of odor molecules. The activated olfactory receptor
in turn activates the intracellular G-protein GOLF, and adenylate cyclase and production
of Cyclic AMP opens ion channels in the cell membrane, resulting in an influx of sodium
and calcium ions into the cell. This influx of positive ions causes the neuron to depolarize,
generating an action potential.
Individual olfactory receptor neurons are replaced approximately every 40 days by neural
stem cells residing in the olfactory epithelium. The regeneration of olfactory receptor cells, as
one of the only few instances of adult neurogenesis in the central nervous system, has raised
considerable interest in dissecting the pathways for neural development and differentiation
in adult organisms.
In the brain
The axons from all the thousands of cells expressing the same odor receptor converge in the
olfactory bulb. Mitral cells in the olfactory bulb send the information about the individual
features to other parts of the olfactory system in the brain, which puts together the features
into a representation of the odor. Since most odor molecules have many individual features,
the combination of features gives the olfactory system a broad range of odors that it can
detect.
Odor information is easily stored in long term memory and has strong connections to
emotional memory. This is possibly due to the olfactory system's close anatomical ties to
the limbic system and hippocampus, areas of the brain that have long been known to be
involved in emotion and place memory, respectively.

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Figure 44

The Olfactory Nerve leading to the brain.

Pheromonal olfaction
Some pheromones are detected by the olfactory system, although in many vertebrates
pheromones are also detected by the vomeronasal organ, located in the vomer, between the
nose and the mouth. Snakes use it to smell prey, sticking their tongue out and touching
it to the organ. Some mammals make a face called flehmen to direct air to this organ. In
humans, it is unknown whether or not pheromones exist.
Olfaction and Gustation
Olfaction, taste and trigeminal receptors together contribute to flavor. It should be emphasized that there are no more than 5 distinctive tastes: salty, sour, sweet, bitter, and
umami. The 10,000 different scents which humans usually recognize as 'tastes' are often
lost or severely diminished with the loss of olfaction. This is the reason why food has little
flavor when your nose is blocked, as from a cold.
The key nutrition players in our taste is the olfactory function, 80-90% of what we consider
taste is dependent on our senses of smell. With aging our olfactory function declines. In the
elderly careful monitoring of appetite is necessary due to the alterations in the olfactory
function. Nutritionist suggest giving a dual approach of supplementation of the trace
minerals zinc and iron to enhance the smell and taste senses.

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Disorders of Olfaction
Anosmia
Anosmia is the lack of olfaction, or a loss of the sense of smell. It can be either temporary
or permanent. A related term, hyposmia refers to a decrease in the ability to smell. Some
people may be anosmic for one particular odor. This is called "specific anosmia" and may
be genetically based. Anosmia can have a number of detrimental effects. Patients with
anosmia may find food less appetizing. Loss of smell can also be dangerous because it
hinders the detection of gas leaks, fire, body odor, and spoiled food. The common view
of anosmia as trivial can make it more difficult for a patient to receive the same types of
medical aid as someone who has lost other senses, such as hearing or sight. A temporary
loss of smell can be caused by a stuffy nose or infection. In contrast, a permanent loss of
smell may be caused by death of olfactory receptor neurons in the nose, or by brain injury
in which there is damage to the olfactory nerve or damage to brain areas that process
smell. The lack of the sense of smell at birth, usually due to genetic factors, is referred
as congenital anosmia. Anosmia may be an early sign of degenerative brain diseases such
as Parkinson's disease and Alzheimer's disease. Another specific cause of permanent loss
could be from damage to olfactory receptor neurons due to use of nasal sprays. To avoid
loss of smell from nasal sprays, use them for only a short amount of time. Nasal sprays
that are used to treat allergy related congestion are the only nasal sprays that are safe to
use for extended periods of time.
Phantosmia
Phantosmia is the phenomenon of smelling odors that aren't really present. (AKA Phantom
odors) The most common odors are unpleasant smells such as rotting flesh, vomit, feces,
smoke etc. Phantosmia often results from damage to the nervous tissue in the olfactory
system. The damage can be caused by viral infection, trauma, surgery, and possibly
exposure to toxins or drugs. It can also be induced by epilepsy affecting the olfactory
cortex. It is also thought the condition can have psychiatric origins.
Dysosmia
When things smell differently than they should.

4.3 The Sense of Vision

Vision needs to have the work of both the eyes and the brain to process any information.
The majority of the stimuli is done in the eyes and then the information is sent to the brain
by the way of nerve impulses. At least one-third of the information of what the eye sees is
processed in the cerebral cortex of the brain.

4.3.1 Anatomy of the Eye

The human eye is a elongated ball about 1-inch (2.5 cm) in diameter and is protected by a
bony socket in the skull. The eye has three layers or coats that make up the exterior wall of
the eyeball, which are the sclera, choroid, and retina.

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Sclera
The outer layer of the eye is the sclera, which is a tough white fibrous layer that maintains,
protects and supports the shape of the eye. The front of the sclera is transparent and is
called the cornea. The cornea refracts light rays and acts like the outer window of the eye.
Choroid
The middle thin layer of the eye is the choroid, also known as the choroidea or choroid
coat, it is the vascular layer of the eye lying between the retina and the sclera. The choroid
provides oxygen and nourishment to the outer layers of the retina. It also contains a
nonreflective pigment that acts as a light shield and prevents light from scattering. Light
enters the front of the eye through a hole in the choroid coat called the pupil. The iris
contracts and dilates to compensate for the changes in light intensity. If the light is bright
the iris then contracts making the pupil smaller, and if the light is dim, the iris dilates
making the pupil bigger. Just posterior to the iris is the lens, which is composed mainly
of proteins called crystallins. The lens is attached by the zonules to the ciliary body that
contains the ciliary muscles that control the shape of the lens for accommodation. Along
with the ciliary body and iris, the choroid forms the uveal tract. The uvea is the middle
of the three concentric layers that make up an eye. The name is possibly a reference to
its almost black color, wrinkled appearance and grape-like size and shape when stripped
intact from a cadaveric eye.
Retina

Figure 45 Illustration of the "blind spot." Situate your head about one foot from the
monitor. Close your right eye and look at the dot on the right with your left eye. Move
your head slowly closer. When you get to the correct spot, the dot on the left will
disappear.

The third or the innermost layer of the eye is call the retina. In adult humans the entire
retina is 72% of a sphere about 22 mm in diameter. The retina lays over the back two thirds
of the choroid coat, which is located in the posterior compartment. The compartment is
filled with vitreous humor which is a clear, gelatinous material. Within the retina there
are cells called rod cells and cone cells also known as photoreceptors. The rod cells are
very sensitive to light and do not see color, that is why when we are in a darkened room
we see only shades of gray. The cone cells are sensitive to different wavelengths of light,
and that is how we are able to tell different colors. It is a lack of cones sensitive to red,
blue, or green light that causes individuals to have deficiencies in color vision or various
kinds of color blindness. At the center of the retina is the optic disc, sometimes known as
"the blind spot" because it lacks photoreceptors. It is where the optic nerve leaves the eye
and takes the nerve impulses to the brain. The cornea and the lens of the eye focuses the
light onto a small area of the retina called the fovea centralis where the cone cells are

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densely packed. The fovea is a pit that has the highest visual acuity and is responsible for
our sharp central vision - there are no rods in the fovea.
framed1
Retina's simplified axial organization. The retina is a stack of several neuronal layers. Light
is concentrated from the eye and passes across these layers (from left to right) to hit the
photoreceptors (right layer). This elicits chemical transformation mediating a propagation of
signal to the bipolar and horizontal cells (middle yellow layer). The signal is then propagated
to the amacrine and ganglion cells. These neurons ultimately may produce action potentials
on their axons. This spatiotemporal pattern of spikes determines the raw input from the eyes
to the brain.
Photoreceptors
A photoreceptor, or photoreceptor cell, is a specialized type of neuron found in the
eye's retina that is capable of phototransduction. More specifically, the photoreceptor
sends signals to other neurons by a change in its membrane potential when it absorbs
photons. Eventually, this information will be used by the visual system to form a complete
representation of the visual world. There are 2 types of photoreceptors: rods are responsible
for scotopic, or night vision, whereas cones are responsible for photopic, or daytime vision
as well as color perception.
Extraocular muscles
Each eye has six muscles that control its movements: the lateral rectus, the medial rectus,
the inferior rectus, the superior rectus, the inferior oblique, and the superior oblique. When
the muscles exert different tensions, a torque is exerted on the globe that causes it to turn.
This is an almost pure rotation, with only about one millimeter of translation, thus, the
eye can be considered as undergoing rotations about a single point in the center of the
eye. Five of the extraocular muscles have their origin in the back of the orbit in a fibrous
ring called the annulus of Zinn. Four of these then course forward through the orbit
and insert onto the globe on its anterior half (i.e., in front of the eye's equator). These
muscles are named after their straight paths, and are called the four rectus muscles, or
four recti. They insert on the globe at 12, 3, 6, and 9 o'clock, and are called the superior,
lateral, inferior and medial rectus muscles. (Note that lateral and medial are relative to
the subject, with lateral toward the side and medial toward the midline, thus the medial
rectus is the muscle closest to the nose).

4.3.2 Eye Movement

The visual system in the brain is too slow to process that information if the images are
slipping across the retina at more than a few degrees per second, thus, for humans to
be able to see while moving, the brain must compensate for the motion of the head by
turning the eyes. To get a clear view of the world, the brain must turn the eyes so that the
image of the object of regard falls on the fovea. Eye movements are thus very important
for visual perception, and any failure to make them correctly can lead to serious visual
disabilities. Having two eyes is an added complication, because the brain must point both
1

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of them accurately enough that the object of regard falls on corresponding points of the
two retinas; otherwise, double vision would occur. The movements of different body parts
are controlled by striated muscles acting around joints. The movements of the eye are no
exception, but they have special advantages not shared by skeletal muscles and joints, and
so are considerably different.
Try This Experiment
Hold your hand up, about one foot (30 cm) in front of your nose. Keep your head still,
and shake your hand from side to side, slowly at first, and then faster and faster. At first
you will be able to see your fingers quite clearly. But as the frequency of shaking passes
about one hertz, the fingers will become a blur. Now, keep your hand still, and shake your
head (up and down or left and right). No matter how fast you shake your head, the image
of your fingers remains clear. This demonstrates that the brain can move the eyes opposite
to head motion much better than it can follow, or pursue, a hand movement. When your
pursuit system fails to keep up with the moving hand, images slip on the retina and you
see a blurred hand.

4.3.3 How we see an object

The light rays enter the eye through the cornea (transparent front portion of eye to focus
the light rays)
Then, light rays move through the pupil, which is surrounded by Iris to keep out extra
light
Then, light rays move through the crystalline lens (Clear lens to further focus the light
rays )
Then, light rays move through the vitreous humor (clear jelly like substance)
Then, light rays fall on the retina, which processes and converts incident light to neuron
signals using special pigments in rod and cone cells.
These neuron signals are transmitted through the optic nerve,
Then, the neuron signals move through the visual pathway - Optic nerve > Optic Chiasm
> Optic Tract > Optic Radiations > Cortex
Then, the neuron signals reach the occipital (visual) cortex and its radiations for the
brain's processing.
The visual cortex interprets the signals as images and along with other parts of the brain,
interpret the images to extract form, meaning, memory and context of the images.

4.3.4 Depth Perception

Depth perception is the visual ability to perceive the world in three dimensions. It is a trait
common to many higher animals. Depth perception allows the beholder to accurately gauge
the distance to an object.
Depth perception is often confused with binocular vision, also known as Stereopsis. Depth
perception does rely on binocular vision, but it also uses many other monocular cues.

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4.3.5 Diseases, disorders, and age-related changes

There are many diseases, disorders, and age-related changes that may affect the eyes and
surrounding structures. As the eye ages certain changes occur that can be attributed solely to
the aging process. Most of these anatomic and physiologic processes follow a gradual decline.
With aging, the quality of vision worsens due to reasons independent of aging eye diseases.
While there are many changes of significance in the non-diseased eye, the most functionally
important changes seem to be a reduction in pupil size and the loss of accommodation or
focusing capability (presbyopia). The area of the pupil governs the amount of light that can
reach the retina. The extent to which the pupil dilates also decreases with age. Because
of the smaller pupil size, older eyes receive much less light at the retina. In comparison to
younger people, it is as though older persons wear medium-density sunglasses in bright light
and extremely dark glasses in dim light. Therefore, for any detailed visually guided tasks on
which performance varies with illumination, older persons require extra lighting.

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Figure 46 This image contains a two digit number similar to the sample above. Someone
who is protanopic might not see this number.
Color Blindness
Color Blindness or color vision deficiency, in humans is the inability to perceive differences
between some or all colors that other people can distinguish. It is most often of genetic
nature, but may also occur because of eye, nerve, or brain damage, or due to exposure to
certain chemicals. There are many types of color blindness. The most common variety are
hereditary (genetic) photoreceptor disorders, but it is also possible to acquire color blindness
through damage to the retina, optic nerve, or higher brain areas. There is generally no
treatment to cure color deficiencies, however, certain types of tinted filters and contact
lenses may help an individual to distinguish different colors better.
Night Blindness

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Also known as Nyctalopia, is a condition making it difficult or impossible to see in the dark.
It is a symptom of several eye diseases. Night blindness may exist from birth, or be caused
by injury or malnutrition (for example, a lack of vitamin A). The most common cause of
nyctalopia is retinitis pigmentosa, a disorder in which the rod cells in the retina gradually
lose their ability to respond to the light. Patients suffering from this genetic condition
have progressive nyctalopia and eventually their day-time vision may also be affected. In
congenital stationary night blindness the rods do not work from birth, but as the name
implies, sufferers do not get worse. Another cause of night blindness is a deficiency of
retinol, or vitamin A, found in fish oils, liver and dairy products.
Day Blindness
Also known as Hemeralopia is the inability to see clearly in bright light. The daytime
vision gets worse and worse. Nighttime vision remains unchanged due to the use of rods as
opposed to cones (during the day), which get affected by hemeralopia and in turn degrade
the daytime optical response.

Figure 47 Impression
of floaters, as seen
against a blue sky.
Floater
Also known as "Muscae Volitantes" are deposits of various size, shape, consistency, refractive
index, and motility within the eye's normally transparent vitreous humour. Floaters are
suspended in the vitreous humour, the thick fluid or gel that fills the eye. Thus, they
generally follow the rapid motions of the eye, while drifting slowly within the fluid. Floaters
are visible only because they do not remain perfectly fixed within the eye. The shapes
are shadows projected onto the retina by tiny structures of protein or other cell debris
discarded over the years and trapped in the vitreous humour. They are also common after
cataract operations or after trauma. In some cases, floaters are congenital.

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Figure 48

Picture of children holding a ball as seen by someone with glaucoma.

Glaucoma
A group of diseases of the optic nerve involving loss of retinal ganglion cells in a characteristic
pattern of optic neuropathy. Although raised intraocular pressure is a significant risk factor
for developing glaucoma, there is no set threshold for intraocular pressure that causes
glaucoma. One person may develop nerve damage at a relatively low pressure, while another
person may have high eye pressures for years and yet never develop damage. Untreated
glaucoma leads to permanent damage of the optic nerve and resultant visual field loss,
which can progress to blindness.
Visual Agnosia
Visual agnosia is the inability of the brain to make sense of or make use of some part
of otherwise normal visual stimulus, and is typified by the inability to recognize familiar
objects or faces. This is distinct from blindness, which is a lack of sensory input to the
brain due to damage to the eye or optic nerve. Visual agnosia is often due to damage, such
as stroke, in posterior parietal lobe in the right hemisphere of the brain. Careful analysis
of the nature of visual agnosia has led to improved understanding of the brain's role in
normal vision.
Deadly Nightshade

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Deadly Nightshade is a plant oil that can potentially kill you. Atrophine taken from this
plant causes your eyes to dilate. This was used in the middle ages by women who wanted
to look more attractive for men. To this day, it is still used by opthamologists. How this
works is that the atrophine is a competitor with acetylcholine. The Nightshadow goes into
your receptors on the postsynaptic membrane of an action potential. This makes it so that
the acetylcholine doesnt have any receptor site so the Na ion is not able to be released.

4.3.6 Critical Thinking

The answers for these critical thinking questions is right here2
1. Explain why you are normally unaware of your blind spot.
2. Stare at a bright light for 10 seconds and then stare at a white sheet of paper. What
do you observe and why?
3. What is it that makes things "disappear" when you are staring at them at night, and
how do you make them reappear?
4. Name what rods are sensitive to and also what cones are sensitive to.
5. Explain how Deadly Nightshade works.

4.4 The Senses Of Hearing

The ear is the sense organ that collects and detects sound waves and plays a major role
in the sense of balance and body position. The sensory receptors for both hearing and
equilibrium are mechanoreceptors found in the inner ear; these receptors are hair cells that
have stereocilia (long microvilli) that are extremely sensitive to mechanical stimulations.

4.4.1 Anatomy of the Ear

The ear has three divisions: the outer ear, the middle ear, and the inner ear.

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Figure 49

Anatomy of the human ear.

Outer Ear (Auricle, Ear Canal, Surface of Ear Drum)

The outer ear is the most external portion of the ear. The outer ear includes the pinna
(also called auricle), the ear canal, and the very most superficial layer of the ear drum (also
called the tympanic membrane). Although the word "ear" may properly refer to the pinna
(the flesh covered cartilage appendage on either side of the head), this portion of the ear is
not vital for hearing. The complicated design of the human outer ear does help capture
sound, but the most important functional aspect of the human outer ear is the ear canal
itself. This outer ear canal skin is applied to cartilage; the thinner skin of the deep canal
lies on the bone of the skull. If the ear canal is not open, hearing will be dampened. Ear
wax (medical name - cerumen) is produced by glands in the skin of the outer portion of
the ear canal. Only the thicker cerumen-producing ear canal skin has hairs. The outer ear
ends at the most superficial layer of the tympanic membrane. The tympanic membrane is
commonly called the ear drum.
Middle Ear (Air Filled Cavity behind the Ear Drum, includes most of the Ear
Drum, and Ear Bones)
The middle ear includes most of the ear drum (tympanic membrane) and the 3 ear bones
ossicles: malleus (or hammer), incus (or anvil), and stapes (or stirrup). The opening of the
Eustachian tube is also within the middle ear. The malleus has a long process (the handle)
that is attached to the mobile portion of the ear drum. The incus is the bridge between
the malleus and stapes. The stapes is the smallest named bone in the human body. The
stapes transfers the vibrations of the incus to the oval window, a portion of the inner ear
to which it is connected. It is the final bone in the chain to transfer vibrations from the
eardrum to the inner ear. The arrangement of these 3 bones is a sort of Rube Goldberg
device: movement of the tympanic membrane causes movement of the first bone, which
causes movement of the second, which causes movement of the third. When this third
bone pushes down, it causes movement of fluid within the cochlea (a portion of the inner
ear). This particular fluid only moves when the stapes footplate is depressed into the inner
ear. Unlike the open ear canal, however, the air of the middle ear is not in direct contact

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with the atmosphere outside the body. The Eustachian tube connects from the chamber of
the middle ear to the back of the pharynx. The middle ear in humans is very much like a
specialized paranasal sinus, called the tympanic cavity, it, like the paranasal sinuses, is a
hollow mucosa lined cavity in the skull that is ventilated through the nose. The mastoid
portion of the temporal bone, which can be felt as a bump in the skull behind the pinna,
also contains air, which ventilates through the middle ear.
Inner Ear (Cochlea, Vestibule, and Semi-Circular Canals)
The inner ear includes both the organ of hearing (the cochlea) and a sense organ (the
labyrinth or vestibular apparatus) that is attuned to the effects of both gravity and motion.
The balance portion of the inner ear consists of three semi-circular canals and the vestibule.
The inner ear is encased in the hardest bone of the body. Within this ivory hard bone,
there are fluid-filled hollows. Within the cochlea are three fluid filled spaces: the tympanic
canal, the vestibular canal, and the middle canal. The eighth cranial nerve comes from
the brain stem to enter the inner ear. When sound strikes the ear drum, the movement is
transferred to the footplate of the stapes, which attaches to the oval window and presses
into one of the fluid-filled ducts of the cochlea. The hair cells in the organ of Corti are
stimulated by particular frequencies of sound, based on their location within the cochlea.
High pitch sounds are at a higher frequency and, due to the shorter wavelength they "hit"
the membrane "faster" (ie. close to the oval window). In contrast, low frequency sounds
have large wavelengths, and will travel further through the scala vestibuli before "hitting"
the tectorial membrane near the apex of the cochlea. The fluid inside the cochlea is moved,
flowing against the receptor (hair) cells of the organ of Corti, which fire in a graded response
based on the volume of the sound. The hair cells then stimulate the nerve cells in the
Spiral Ganglion, which sends information through the auditory portion of the eighth cranial
nerve to the brain. Humans are able to hear sounds between about 20 Hz and 20,000
Hz. Mammals that can hear lower frequency sounds, such as whales and elephants, have
a longer cochlea. Humans tend to lose high-frequency hearing first, which has led some
teenagers to using high-frequency ring tones (above 17,000 Hz) that may go undetected by
their middle-aged teachers.

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Figure 50

Cross section of the cochlea

Hair Cell
Hair cells are columnar cells, each with a bundle of 100-200 specialized cilia at the top,
for which they are named. These cilia are the mechanosensors for hearing. Lightly resting
atop the longest cilia is the tectorial membrane, which moves back and forth with each
cycle of sound, tilting the cilia and allowing electric current into the hair cell. Hair cells,
like the photoreceptors of the eye, show a graded response, instead of the spikes typical
of other neurons. Immediately over the hair cells of the organ of Corti is an overhanging
tectorial membrane. When the Bones of the Middle Ear vibrate the oval window, these
vibrations are transmitted to the fluid within the cochlea and eventually cause the round
window on the cochlea to bulge outward. These vibrations deflect the membrane on which
the Organ of Corti is located, causing the three rows of outer hair cells to rub against
the overhanging tectorial membrane. By their muscle-like activity they ampify the weakest
vibrations for the inner hair cells. The louder sounds are not amplified. The disturbed
inner hair cells will then activate the cochlear nerve fibers. The current model is that cilia
are attached to one another by tip links, structures which link the tips of one cilium to
another. Stretching and compressing the tip links may open an ion channel and produce
the receptor potential in the hair cell. These graded potentials are not bound by the all
or none properties of an action potential. There are far fewer hair cells than afferent
(leading to the brain) nerve fibers in the cochlea. The nerve that innervates the cochlea is
the cochlear nerve, and forms cranial nerve number VIII with the vestibular nerve from the
balance organ. Neuronal dendrites innervate cochlear hair cells. The neurotransmitter itself
is thought to be glutamate. At the presynaptic juncture, there is a distinct presynaptic
dense body or ribbon. This dense body is surrounded by synaptic vesicles and is thought
to aid in the fast release of neurotransmitter. Efferent projections from the brain to the
cochlea also play a role in the perception of sound. Efferent synapses occur on outer hair
cells and on afferent dendrites under inner hair cells.

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4.4.2 Process of Hearing

Detection of sound motion is associated with the right posterior superior temporal gyrus.
The superior temporal gyrus contains several important structures of the brain, including:
(1)marking the location of the primary auditory cortex, the cortical region responsible for
the sensation of sound. Sections 41 and 42 are called the primary auditory area of the
cerebrum, and processes the basic characteristics of sound such as pitch and rhythm. The
auditory association area is located within the temporal lobe of the brain, in an area called
the Wernicke's area, or area 22. This area, near the lateral cerebral sulcus, is an important
region for the processing of acoustic energy so that it can be distinguished as speech, music,
or noise. It also interprets words that are heard into an associated thought pattern of
understanding. The gnostic area of the cerebrum, (areas 5, 7, 39 and 40) helps to integrate
all incoming sense patterns so that a common thought can be formed (correlated) using all
arriving sensory information.

4.4.3 Hearing Under Water

Hearing threshold and the ability to localize sound sources are reduced underwater. in
which the speed of sound is faster than in air. Underwater, hearing is by bone conduction
and localization of sound appears to depend on differences in amplitude detected by bone
conduction.

4.4.4 Localization of Sound by Humans

Humans are normally able to hear a variety of sound frequencies, from about 20Hz to 20kHz.
Our ability to estimate just where the sound is coming from, sound localization, is dependent
on both hearing ability of each of the two ears, and the exact quality of the sound. Since
each ear lies on an opposite side of the head, a sound will reach the closest ear first, and its
amplitide will be loudest in that ear. Much of the brain's ability to localize sound depends on
interaural (between ears) intensity differences and interaural temporal or phase differences.
Two mechanisms are known to be used.
Bushy neurons can resolve time differences as small as the time it takes sound to pass one ear
and reach the other (10 milliseconds). For high frequencies, frequencies with a wavelength
shorter than the listener's head, more sound reaches the nearer ear. Human echolocation
is a technique involving echolocation used by some blind humans to navigate within their
environment.

4.4.5 Process of Equilibrium

Equilibrioception or sense of balance is one of the physiological senses. It allows humans and
animals to walk without falling. Some animals are better in this than humans, for example
allowing a cat (as a quadruped using its inner ear and tail) to walk on a thin fence. All
forms of equilibrioception can be described as the detection of acceleration.

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The Senses Of Hearing

It is determined by the level of fluid properly called endolymph in the labyrinth - a complex
set of tubing in the inner ear.
When the sense of balance is interrupted it causes dizziness, disorientation and nausea.
You can temporarily disturb your sense of balance by closing your eyes and turning rapidly
in circles five or six times. This starts the fluid swirling in circles inside your ear canal.
When you stop turning it takes a few seconds for the fluid to lose momentum, and until
then the sense from your inner ear conflicts with the information coming from your vision,
causing dizziness and disorientation. Most astronauts find that their sense of balance is
impaired when in orbit, because there is not enough gravity to keep the ear's fluid in balance.
This causes a form of motion sickness called space sickness.

4.4.6 Disorders with the Ear

Case Study A 45-year-old woman wakes up not feeling well. She believes that she may
be coming down with the flu due to nausea that she is feeling, so she continues with her
day. As the day progresses so does the feeling of nausea. While watching a movie with
members of her family, the sick feeling seems to intensify and so they leave the movie.
In the lobby of the movie theater she becomes very unbalanced and collapses. The fear
is that she is experiencing a stroke. After being taken to the hospital via ambulance,
the ER doctors also feel that it may be a stroke and do CAT scans to verify. Nothing
shows up on the scans but the feeling of nausea and vertigo are intense. The woman is
later diagnosed with an inner ear infection. The next 6-9 months of her life are filled
with antibiotics, balance therapy and continued nausea and vertigo. Nothing seems to
help so the doctors go into her inner ear surgically through her skull. They cut the
vestibular nerve that is linked to the balance center on the left side. The right inner ear
will eventually compensate for this loss of balance however it will take months of balance
therapy. After a year from the onset on the inner ear infection, the woman has had three
inner ear surgeries, loss of hearing in the left ear and problems with her balance. Doctors
have told her they have done everything that they can and that she will now have to live
with these conditions on a daily basis.
Deafness
The word deaf can have at least two different meanings. The first term is used to indicate
the presence of enough hearing loss such that an individual is not sensitive to sound.
Someone with a partial loss of hearing is more likely to be referred to as hearing impaired
or the qualified partially deaf by professionals. The second term is used to indicate someone
who considers themselves 'culturally deaf', and they often use a capital D to distinguish
this. Deaf people often are signers and consider that their Deafness is not something that
needs to be medically fixed.
Cochlear Implants A cochlear implant is a device which has been used to restore
hearing function to some deaf and hearing impaired people. It consists of an internal
device; which extends electrodes into the cochlea and indirectly stimulates the auditory
nerve, and an external device; which works much like a hearing aid, except it transmits

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The Senses

information to the internal device rather than to the ear. The cochlear implant basically
bypasses the middle ear and the cochlea hair cells, and allows some people with damage
to these structures to hear 'electronically'.

Figure 51

An inflamed Otitis Media.

Otitis Media
An inflammation of the middle ear segment. It is usually associated with a buildup of
fluid and frequently causes an earache. The fluid may or may not be infected. The typical
progress of otitis media is: the tissues surrounding the Eustachian tube swell due to an
infection and/or severe congestion. The Eustachian tube remains blocked most of the
time. The air present in the middle ear is slowly absorbed into the surrounding tissues. A
strong negative pressure creates a vacuum in the middle ear. The vacuum reaches a point
where fluid from the surrounding tissues accumulates in the middle ear. Streptococcus
pneumoniae and Haemophilus influenzae are the most common bacterial causes of otitis
media. As well as being caused by Streptococcus pneumoniae and Haemophilus influenzae
it can also be caused by the common cold.
Vertigo (dizziness)
Vertigo, sometimes called a headrush, is a major symptom of a balance disorder. It is the
sensation of spinning while the body is stationary with respect to the earth or surroundings.
With the eyes shut, there will be a sensation that the body is in movement, called subjective
vertigo; if the eyes are open, the surroundings will appear to move past the field of vision,
called objective vertigo. The effects may be slight. It may cause nausea or, if severe,
may give rise to difficulty with standing and walking. Vertigo is usually associated with a
problem in the inner ear balance mechanisms (vestibular system), in the brain, or with the
nerve connections between these two organs. The most common cause is benign paroxysmal
positional vertigo, or BPPV. Vertigo can be a symptom of an underlying harmless cause,

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such as in BPPV or it can suggest more serious problems. These include drug toxicities,
strokes or tumors (though these are much less common than BPPV).
Motion sickness
Motion sickness is a condition in which the endolymph (the fluid found in the semicircular
canals of the inner ears) becomes 'stirred up', causing confusion between the difference between apparent perceived movement (none or very little), and actual movement. Depending
on the cause, it is also referred to as seasickness, carsickness, airsickness, or spacesickness.
Nausea is the most common symptom of motion sickness. If the motion causing nausea
is not resolved, the sufferer will frequently vomit within twenty minutes. Unlike ordinary
sickness, vomiting in motion sickness tends not to relieve the nausea. If you don't want to
consult a doctor, one common form of relief is to eat mints.
Dysacusis
Dysacusis is a hearing impairment characterized by difficulty in processing details of sound,
but not primarily a loss of the ability to perceive sound. May also refer to pain or discomfort
due to sound.

4.4.7 Critical Thinking

The answers for these critical thinking questions can be found here3 .
1. Explain how the pitch of sound is coded. How is the loudness of sound coded?
2. What do the three semicircular canals in the inner ear enable us to do? How do they
accomplish this?
3. What does the eustachian tube do? What does the eustachian tube have to do with a
middle ear infection?
4. What is the advantage of having a oval window?

4.5 Touch
Touch is the first sense developed in the womb and the last sense used before death. With
50 touch receptors for every square centimeter and about 5 million sensory cells overall,
the skin is very sensitive and is the largest and one of the most complex organs in our
bodies. These touch receptors are grouped by type and include Mechanoreceptors (sensitive
to pressure, vibration and slip), Thermoreceptors (sensitive to changes in temperature), and
Nocioreceptors (responsible for pain).

4.5.1 Pacinian Corpuscles

Pacinian corpuscles detect gross pressure changes and vibrations. They are the largest of
the receptors. Any deformation in the corpuscle causes action potentials to be generated, by
opening pressure-sensitive sodium ion channels in the axon membrane. This allows sodium

http://en.wikibooks.org/wiki/Human_Physiology/Appendix_1:_answers_to_review_
questions#Critical_Thinking:_Hearing

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The Senses
ions to influx in, creating a receptor potential. Pacinian corpuscles cause action potentials
when the skin is rapidly indented but not when the pressure is steady, due to the layers of
connective tissue that cover the nerve ending (Kandel et al., 2000). It is thought that they
respond to high velocity changes in joint position.

4.5.2 Meissner's Corpuscle

Meissner's corpuscles are distributed throughout the skin, but concentrated in areas especially
sensitive to light touch, such as the fingertips, palms, soles, lips, tongue, face, nipples and the
external skin of the male and female genitals. They are primarily located just beneath the
epidermis within the dermal papillae. Any physical deformation in the Meissners corpuscle
will cause an action potential in the nerve. Since they are rapidly adapting or phasic, the
action potentials generated quickly decrease and eventually cease. If the stimulus is removed,
the corpuscle regains its shape and while doing so (ie: while physically reforming) causes
another volley of action potentials to be generated. (This is the reason one stops "feeling"
one's clothes.) This process is called sensory adaption. Because of their superficial location
in the dermis, these corpuscles are particularly sensitive to touch and vibrations, but for the
same reasons, they are limited in their detection because they can only signal that something
is touching the skin. Meissner's corpuscles do not detect pain; this is signaled exclusively by
free nerve endings.

Figure 52

Layers of the skin, showing the Merkel's Cell.

4.5.3 Merkels Discs

Merkels Discs are Mechanoreceptors, making them sensitive to pressure and vibration. In
humans, Merkel cells occur in the superficial skin layers, and are found clustered beneath the

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Touch
ridges of the fingertips that make up fingerprints. Theyre somewhat rigid in structure, and
the fact that they are not encapsulated, causes them to have a sustained response (in the form
of action potentials or spikes) to mechanical deflection of the tissue. Merkel nerve endings
are extremely sensitive to tissue displacement, and may respond to displacements of less
than 1 um. Several studies indicate that they mediate high-resolution tactile discrimination,
and are responsible for the ability of our fingertips to feel fine detailed surface patterns (e.g.
for reading Braille).

4.5.4 Ruffini corpuscles

Ruffini corpuscles are Thermoreceptors, aiding in the detection of temperature changes.
Named after Angelo Ruffini, the Ruffini ending is a class of slowly adapting mechanoreceptor
thought to exist only in the glabrous dermis and subcutaneous tissue of humans. This
spindle-shaped receptor is sensitive to skin stretch, and contributes to the kinesthetic sense
of and control of finger position and movement.

4.5.5 Disorders of Touch

Sensory Processing Disorder
In most people sensory integration occurs naturally without a thought process. But in some
people the sensory integration does not develop properly and becomes distorted. In these
people, the brain and central nervous system misinterprets everyday sensory information
such as touch, sound and movement. Research is still being done on this disorder but they
are finding direct links to SPD with other disorders like ADD/ADHD, premature birth,
Autism, Downs Syndrome and Fragile X.
Tactile defensiveness
Considered a category of SPD, tactile defensiveness is an overreaction to the sense of touch.
Identified by Dr. Jean Ayers in the 1960s. A person with tactile defensiveness will react
with a flight or fight reaction to touch stimuli that a normal person would interpret as
harmless. Most cases are noticed in children or babies due to the fact that they do not
want to be touched or cuddled as a normal child would. A child with this disorder will
probably have these sign or symptoms:

Does not like to go barefoot or have feet touched

Does not enjoy baths, haircuts, nail clipping
Requires tags to be removed from all clothing
Does not want their face touched
Hard time eating because of textures, temperatures of the food
Does not want to touch anything that is messy or has a sticky texture

Congenital insensitivity to pain with anhidrosis or CIPA

Exceedingly rare disease. There are only about 35 known cases in the United States. CIPA
is a severe autosomal recessive condition in which the peripheral nerves demonstrate a loss
of unmyelinated and small myelinated fibers. The actual physiopathological mechanism
is still unknown and being studied- this is an extremely hard disease to study due to the

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The Senses
rarity of cases. Most people with the disease will not live long due to injuries received that
go untreated because they are unknown and severe

4.5.6 Case Study

Insensitivity to pain
Wouldn't it wonderful if you could no longer feel pain. Is that not something we all would
like to have? Or do we have pain for a good reason? Although it is rare there is a disease
known as congenital insensitivity to pain. This genetic abnormality cause some people to
lack certain components of the sensory system to receive pain. The exact reason for the
problem is unknown and varies between people. Sadly people who have the disease often die
in childhood. Injuries are very common with people who have congenital insensitivity to
pain. They often will lose digits, may suffer from burns and their knees often have sores
from kneeling to long. Clearly pain has a purpose, it is our warning signal when things are
awry.

4.5.7 The newborn's senses

Newborns can feel all different sensations, but respond most enthusiastically to soft stroking,
cuddling and caressing. Gentle rocking back and forth will oftentimes calm a crying infant,
as will massages and warm baths. Newborns may comfort themselves by sucking their
thumbs, or a pacifier. The need to suckle is instinctive and allows newborns to feed.
Vision
Newborn infants have unremarkable vision, being able to focus on objects only about
18 inches (45 cm) directly in front of their face. While this may not be much, it is all
that is needed for the infant to look at the mothers face when breastfeeding. When a
newborn is not sleeping, or feeding, or crying, he or she may spend a lot of time staring
at random objects. Usually anything that is shiny, has sharp contrasting colors, or has
complex patterns will catch an infant's eye. However, the newborn has a preference for
looking at other human faces above all else.
Hearing
While still inside the mother, the infant can hear many internal noises, such as the mother's
heartbeat, as well as many external noises including human voices, music and most other
sounds. Therefore, although a newborn's ears may have some fluid present, he or she can
hear sound from birth. Newborns usually respond to a female's voice over a male's. This
may explain why people will unknowingly raise the pitch of their voice when talking to
newborns. The sound of other human voices, especially the mother's, can have a calming
or soothing effect on the newborn. Conversely, loud or sudden noises will startle and scare
a newborn.
Taste
Newborns can respond to different tastes, including sweet, sour, bitter, and salty substances,
with preference toward sweets.

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Touch
Smell
A newborn has a developed sense of smell at birth, and within the first week of life can
already distinguish the differences between the mother's own breast milk and the breast
milk of another female.
Reflex

Stimulation

Response

Eye blink

Bright light
shinning in
eyes or clap
hands by
eyes.

Closes eyelids
quickly.

Withdrawal

Stick sole of
foot with a
stimulus like a
pin.

Rooting

Touch cheek
near the corner of the
mouth.

This causes
the foot to
withdraw.
Flexing of
the knee to
hip occurs.
The infant's
head will turn
towards the
site of stimulation.

Sucking

Place fingers
in infant's
mouth.

Swimming

Place the
baby in pool
of water face
down.

Age of disappearance
Permanent

Decreases
after the 10th
day of birth

Function
This reflex
protects the
infant from
an excessive
amount of
stimulation.
This protects
the infant
from excessive
unpleasant
tactile stimulation.
This reflex
helps baby to
find the mothers' nipple.

3 weeks (due
to the voluntary response
that is now
capable for infant to do at
this time)
The infant
4 months
This helps
will suck fin(voluntary
with feeding.
ger rhythmisucking will
cally.
come about)
The baby
4 to 6 month
This helps
paddles and
baby to
kicks in swimsurvive if
ming movedropped into
ments.
the water.

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The Senses
Reflex

Stimulation

Response

Moro

Hold infant
in a cradling
horizontal
position and
slightly lower
the baby in
a fast motion
toward the
ground while
making a loud
sound.

Palmar grasp

Place the finger in baby's

palm and
press against
the palm.
Turn the
baby's head
to one side
while the
baby is
awake.

The baby
will make
a embracing motion
and arch its
back extending it's legs
and throwing
it's arms outward. Finally
it will bring
the arms in
toward its
body
The baby
will immediately grasp
the finger.

Tonic neck

134

Stepping

Hold the
baby under
the arm and
permit the
bare feet of
the baby to
touch a flat
surface.

Babinski

Touch the
foot in a
stroking manner form the
toe toward
the heel.

This will
cause the
baby to extend one arm
in front of its
eye or to the
side to which
the head has
been turned.
The baby
will lift one
foot after the
other in a
stepping fashion.

The baby's
toes will fan
out and curl
as the foot
twists inward.

Age of disappearance
6 months

3 to 4
months

4 months

2 months
(this applies
to a baby who
has gained
weight. For
baby who is
not as heavy,
this reflex
may be submissive.)
8 to 12
months

Function
In the evolutionary past
this may have
helped the
baby cling to
the mother.

This prepares
infant for voluntary grasping.
This may
prepare for
voluntary
reaching.

This prepares
the baby for
voluntary
walking.

Unknown

Review Questions

4.6 Review Questions

Answers for these questions can be found here4
1. Located under the hardest bone in the body, these control not only hearing but also a
sense of gravity and motion:
A) The incus and the stapes
B) The pinna and the ear drum
C) the vestibular nerve and the semi circular canals
D) The eustachian tube and the stapes
2. The retina does the following;
A) allows vision in light and dark, using cones and rods
B) Gives depth perception using binocular vision
C) Contains the ciliary muscles that control the shape of the lens
D) Protects and supports the shape of the eye
3. This is the reason that we stop feeling the clothes that we are wearing
A) Merkels Discs are somewhat rigid in structure, and the fact that they are not encapsulated,
causes them to have a sustained response
B) Meissners corpuscle are rapidly adapting or phasic, the action potentials generated
quickly decrease and eventually cease
C) Ruffini corpuscles is a class of slowly adapting mechanoreceptor
D) Pacinian corpuscles allow sodium ions to influx in, creating a receptor potential
4. When eating a piece of candy, I will use the following to sense that it is sweet
A) Fungiform papillae
B) Filiform papillae
C) Foliate papillae
D) Circumvallate papillae
E) All of the above
5. If I have a cold, food may not taste as good to me because
A) The nerve fibrils are not functioning properly
B) My food will taste the same; taste and smell have nothing in common
C) Papilla become blocked by mucus and are unable to function

http://en.wikibooks.org/wiki/Human_Physiology/Appendix_1:_answers_to_review_
questions#Senses

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The Senses
D) Olfaction, taste and trigeminal receptors together contribute to the flavor of my food
6. Walking from a well lit room into a dark room would cause the following to occur
A) The sclera in the eye to open and eventually allow me to see in the dark
B) The extraocular muscles in the eye to open and eventually allow me to see in the dark
C) The cones in the eye to open and eventually allow me to see in the dark
D) the rods in the eye to open and eventually allow me to see in the dark
7. Hair cells in the ear
A) Are the actual sensory receptors that will fire off action potentials when they are disturbed
B) Show a graded response, instead of the spikes typical of other neurons
C) Rub against the overhanging tectorial membrane
D) All of the above
8. Eyesight decreases with age because
A) Older eyes receive much less light at the retina
B) There are numerous eye diseases that can affect an older eye
C) The extent to which the pupil dilates decreases with age
D) all of the above
9. Teens walking off of a roller coaster in Magic Mountain seem to have vertigo because
A) The fluid in the auricle has not stopped moving causing conflicts with the information
coming from your vision
B) the fluid in the cochlea has not stopped moving causing conflicts with the information
coming from your vision
C) The fluid in the tympanic membrane has not stopped moving causing conflicts with the
information coming from your vision
D) The fluid in the stirrup has not stopped moving causing conflicts with the information
coming from your vision
10. These receptors react to foods treated with monosodium glutamate
A) Salt
B) Sour
C) Bitter
D) Sweet
E) Umami
11. What senses fall under the catagory of chemoreception?
A) Hearing and smell

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Glossary
B) Touch and hearing
C) Vision and taste
D) Taste and smell

4.7 Glossary
Anosmia: Lack of olfaction, or a loss of the sense of smell
Auditory Canal: Tube from the auditory meatus or opening of the ear to the tympanic
membrane
Auditory Tube: Either of the paired tubes connecting the middle ears to the nasopharynx;
equalizes air pressure on the two sides of the eardrum
Chemoreception: Physiological response of a sense organ to a chemical stimulus
Choroid: Vascular layer of the eye lying between the retina and the sclera
Circumvallate papillae: Papillae that are present on the back of the oral part of the
tongue
Cochlea: Is concerned with hearing, resembling a shell of a snail
Dysosmia: When things smell differently than they should
Equilibrium: Sense of balance
Extraocular muscles: Six muscles that control eye movements: lateral rectus, medial
rectus, inferior rectus, superior rectus, inferior oblique and superior oblique
Filiform papillae: Thin, longer papillae that don't contain taste buds but are the most
numerous
Foliate papillae: Ridges and grooves towards the posterior part of the tongue
Fungiform papillae: These are present mostly at the apex (tip) of the tongue- slightly
mushroom shaped
Gustation: The sense of taste
Hair Cell: Mechanosensors for hearing, columnar cells each with a bundle of 100-200
specialized cilia at the top
Haptic: From the Greek Haphe, means pertaining to the sense of touch
Hyposmia: Decreased ability to smell
Inner Ear: Innermost part of the ear, contains the cochlea, westibule and semi-circular
canals
Mechanoreceptor: Sensory receptor that responds to mechanical pressure or distortion
Meissner's Corpuscle: Encapsulated unmyelinated nerve endings, usually found in areas
sensitive to light touch

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The Senses
Middle Ear: Air Filled Cavity behind the Ear Drum, includes most of the ear Drum and
ear Bones
Nasopharynx: Nasal part of the pharynx that lies behind the nose and above the level of
the soft palate
Nociception: The perception of pain
Olfaction: The sense of smell
Otitis Media: An inflammation of the middle ear
Outer Ear: External portion of the ear, includes the auricle, ear canal and surface of the
ear drum
Oval Window: Fenestra that has the base of the stapes attached to it
Pacinian Corpuscles; Detect gross pressure changes and vibrations
Papilla: Specialized epithelial cells that are small projections on the top of the tongue
Perception: The brains interpretation of a sensation
Phantosmia: Phenomenon of smelling odors that aren't really present (AKA Phantom
odors)
Photoreceptors: Specialized type of neuron found in the eye's retina that is capable of
phototransduction
Pinna: Auricle of the ear
Retina: Thin layer of neural cells that lines the back of the eyeball of vertebrates and some
cephalopods
Round Window: Fenestra leading into the cochlea
Sclera: White outer coating of the eye- gives the eye its shape and helps to protect the
delicate inner parts
Semicircular Canals: Certain canals of the inner ear
Sensation: Occurs when nerve impulses arrive in the brain
Sensory adaptation: A decrease in response to stimuli
Stapes: One of the small bones in the tympanum of the ear; the stirrups bone
Tactition: The sense of pressure perception, generally in the skin
Tympanic Membrane: The membrane in the ear that vibrates to produce sound
Umami: Japanese word meaning savory or meaty- type of taste signal

4.8 References
Hnig, D.P., 1901. Zur Psychophysik des Geschmackssinnes. Philosophische Studien, 17:
576-623.

138

References
Collings, V.B., 1974. Human Taste Response as a Function of Locus of Stimulation on
the Tongue and Soft Palate. Perception & Psychophysics, 16: 169-174.
Buck, Linda and Richard Axel. (1991). A Novel Multigene Family May Encode Odorant
Receptors: A Molecular Basis for Odor Recognition. Cell 65:175-183.

139

5 The Muscular System

Figure 53

Head and Neck Muscles

The muscular system is the biological system of humans that produces movement. The
muscular system, in vertebrates, is controlled through the nervous system, although some

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The Muscular System

muscles, like cardiac muscle, can be completely autonomous. Muscle is contractile tissue
and is derived from the mesodermal layer of embryonic germ cells. Its function is to produce
force and cause motion, either locomotion or movement within internal organs. Much of
muscle contraction occurs without conscious thought and is necessary for survival, like the
contraction of the heart or peristalsis, which pushes food through the digestive system.
Voluntary muscle contraction is used to move the body and can be finely controlled, such as
movements of the finger or gross movements that of the biceps and triceps.

Figure 54

Muscle structure

Muscle is composed of muscle cells (sometimes known as "muscle fibers"). Within the
cells are myofibrils; myofibrils contain sarcomeres which are composed of actin and myosin.
Individual muscle cells are lined with endomysium. Muscle cells are bound together by
perimysium into bundles called fascicles. These bundles are then grouped together to form
muscle, and is lined by epimysium. Muscle spindles are distributed throughout the muscles,
and provide sensory feedback information to the central nervous system. Skeletal muscle,
which involves muscles from the skeletal tissue, is arranged in discrete groups. An example
is the biceps brachii. It is connected by tendons to processes of the skeleton. In contrast,
smooth muscle occurs at various scales in almost every organ, from the skin (in which it
controls erection of body hair) to the blood vessels and digestive tract (in which it controls
the caliber of a lumen and peristalsis, respectively).

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Types

Figure 55

A top-down view of skeletal muscle

There are approximately 640 skeletal muscles in the human body (see list of muscles of the
human body). Contrary to popular belief, the number of muscle fibers cannot be increased
through exercise; instead the muscle cells simply get bigger. It is however believed that
myofibrils have a limited capacity for growth through hypertrophy and will split if subject
to increased demand. There are three basic types of muscles in the body (smooth, cardiac,
and skeletal). While they differ in many regards, they all use actin sliding against myosin
to create muscle contraction and relaxation. In skeletal muscle, contraction is stimulated
at each cell by nervous impulses that releases acetylcholine at the neuromuscular junction,
createing action potentials along the cell membrane. All skeletal muscle and many smooth
muscle contractions are stimulated by the binding of the neurotransmitter acetylcholine.
Muscular activity accounts for most of the body's energy consumption. Muscles store energy
for their own use in the form of glycogen, which represents about 1% of their mass. Glycogen
can be rapidly converted to glucose when more energy is necessary.

5.1 Types
There are three types of muscle:

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Figure 56
Smooth muscle or "involuntary muscle" consists of spindle shaped muscle cells found
within the walls of organs and structures such as the esophagus, stomach, intestines,
bronchi, uterus, ureters, bladder, and blood vessels. Smooth muscle cells contain only
one nucleus and no striations.
Cardiac muscle is also an "involuntary muscle" but it is striated in structure and
appearance. Like smooth muscle, cardiac muscle cells contain only one nucleus. Cardiac
muscle is found only within the heart.
Skeletal muscle or "voluntary muscle" is anchored by tendons to the bone and is used
to effect skeletal movement such as locomotion. Skeletal muscle cells are multinucleated
with the nuclei peripherally located. Skeletal muscle is called 'striated' because of the
longitudinally striped appearance under light microscopy. Functions of the skeletal muscle
include:
Support of the body
Aids in bone movement
Helps maintain a constant temperature throughout the body
Assists with the movement of cardiovascular and lymphatic vessels through contractions
Protection of internal organs and contributing to joint stability
Cardiac and skeletal muscle are striated in that they contain sarcomere and are packed into
highly-regular arrangements of bundles; smooth muscle has neither. Striated muscle is often
used in short, intense bursts, whereas smooth muscle sustains longer or even near-permanent
contractions.
Skeletal muscle is further divided into several subtypes:
Type I, slow oxidative, slow twitch, or "red" muscle is dense with capillaries and is rich in
mitochondria and myoglobin, giving the muscle tissue its characteristic red color. It can
carry more oxygen and sustain aerobic activity.
Type II, fast twitch, muscle has three major kinds that are, in order of increasing
contractile speed:
a) Type IIa, which, like slow muscle, is aerobic, rich in mitochondria and capillaries
and appears red.
b) Type IIx (also known as type IId), which is less dense in mitochondria and myoglobin.
This is the fastest muscle type in humans. It can contract more quickly and with a
greater amount of force than oxidative muscle, but can sustain only short, anaerobic
bursts of activity before muscle contraction becomes painful (often attributed to a

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build-up of lactic acid). N.B. in some books and articles this muscle in humans was,
confusingly, called type IIB
c) Type IIb, which is anaerobic, glycolytic, "white" muscle that is even less dense in
mitochondria and myoglobin. In small animals like rodents or rabbits this is the major
fast muscle type, explaining the pale color of their meat.
For most muscles, contraction occurs as a result of conscious effort originating in the brain.
The brain sends signals, in the form of action potentials, through the nervous system to the
motor neuron that innervates the muscle fiber. However, some muscles (such as the heart)
do not contract as a result of conscious effort. These are said to be autonomic. Also, it is not
always necessary for the signals to originate from the brain. Reflexes are fast, unconscious
muscular reactions that occur due to unexpected physical stimuli. The action potentials for
reflexes originate in the spinal cord instead of the brain.
There are three general types of muscle contractions, skeletal muscle contractions, heart
muscle contractions, and smooth muscle contractions.

5.2 Muscular System Working With Other Body Systems

1.
2.
3.
4.

Homeostasis
Protection
Calcium Metabolism
Maintaining Body Temperature

5.3 Skeletal Muscle Contractions

Steps of a skeletal muscle contraction:
An action potential reaches the axon of the motor neuron.
The action potential activates voltage gated calcium ion channels on the axon, and
calcium rushes in.
The calcium causes acetylcholine vesicles in the axon to fuse with the membrane, releasing
the acetylcholine into the cleft between the axon and the motor end plate of the muscle
fiber.
The skeletal muscle fiber is excited by large mylenated nerve fibers which attach to the
neuromuscular junction. There is one neuromuscular junction for each fiber.
The acetylcholine diffuses across the cleft and binds to nicotinic receptors on the motor
end plate, opening channels in the membrane for sodium and potassium. Sodium rushes
in, and potassium rushes out. However, because sodium is more permeable, the muscle
fiber membrane becomes more positively charged, triggering an action potential.
The action potential on the muscle fiber causes the sarcoplasmic reticulum to release
calcium ions(Ca++).
The calcium binds to the troponin present on the thin filaments of the myofibrils. The
troponin then allosterically modulates the tropomyosin. Normally the tropomyosin
physically obstructs binding sites for cross-bridge; once calcium binds to the troponin,
the troponin forces the tropomyosin to move out of the way, unblocking the binding sites.

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The cross-bridge (which is already in a ready-state) binds to the newly uncovered binding
sites. It then delivers a power stroke.
ATP binds the cross-bridge, forcing it to conform in such a way as to break the actinmyosin bond. Another ATP is split to energize the cross bridge again.
Steps 7 and 8 repeat as long as calcium is present on thin filament.
Throughout this process, the calcium is actively pumped back into the sarcoplasmic
reticulum. When no longer present on the thin filament, the tropomyosin changes back
to its previous state, so as to block the binding sites again. The cross-bridge then ceases
binding to the thin filament, and the contractions cease as well.
Muscle contraction remains as long as Ca++ is abundant in sarcoplasm.
Types of Contractions:
Isometric contraction--muscle does not shorten during contraction and does not require
the sliding of myofibrils but muscles are stiff.
Isotonic contraction--inertia is used to move or work. More energy is used by the muscle
and contraction lasts longer than isometric contraction. Isotonic muscle contraction is
divided into two categories: concentric, where the muscle fibers shorten as the muscle
contracts (ie. biceps brachialis on the up phase of a biceps curl); and eccentric, where
the muscle fibers lengthen as they contract (ie. biceps brachialis on the down phase of a
biceps curl).
Twitch--exciting the nerve to a muscle or by passing electrical stimulus through muscle
itself. Some fibers contract quickly while others contract slowly.
Tonic -maintaining postural tone against the force of gravity.
The Efficiency of Muscle Contraction:
Only about 20% of input energy converts into muscular work. The rest of the energy is
heat.
50% of energy from food is used in ATP formation.
If a muscle contraction is slow or without movement, energy is lost as maintenance heat.
If muscle contraction is rapid, energy is used to overcome friction.
Summation of Muscle Contraction: It is the adding together of individual muscle twitches
to make strong muscle movements.
Multiple motor unit summation--increasing number of motor units contracting simultaneously.
Wave summation--increasing rapidity of contraction of individual motor units.
Tetanization--higher frequency successive contractions fuse together and cannot be distinguished from one another.

5.4 Sliding Filament theory

When a muscle contracts, the actin is pulled along myosin toward the center of the sarcomere
until the actin and myosin filaments are completely overlapped. The H zone becomes smaller
and smaller due to the increasing overlap of actin and myosin filaments, and the muscle
shortens. Thus when the muscle is fully contracted, the H zone is no longer visible (as in the

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Sliding Filament theory

bottom diagram, left). Note that the actin and myosin filaments themselves do not change
length, but instead slide past each other.

5.4.1 Cellular Action of Skeletal Muscles

During cellular respiration the mitochondria, within skeletal muscle cells, convert glucose
from the blood to carbon dioxide and water in the process of producing ATP (see cell
physiology1 ). ATP is needed for all muscular movement. When the need of ATP in the muscle
is higher than the cells can produce with aerobic respiration, the cells will produce extra
ATP in a process called anaerobic respiration. The first step of aerobic respiration(glycolysis)
produces two ATP per glucose molecule. When the rest of the aerobic respiration pathway
is occupied the pyruvate molecule can be converted to lactic acid. This method produces
much less ATP than the aerobic method, but it does it faster and allows the muscles to
do a bit more than if they relied solely on ATP production from aerobic respiration. The
drawback to this method is that lactic acid accumulates and causes the muscles to fatigue.
They will eventually stop contracting until the breakdown of lactic acid is sufficient to allow
for movement once again. People experience this most noticeably when they repeatedly lift
heavy things such as weights or sprint for a long distance. Muscle soreness sometimes occurs
after vigorous activity, and is often misunderstood by the general public to be the result of
lactic acid buildup. This is a misconception because the muscle does fatigue from lactic acid
buildup, but it does not stay in the muscle tissue long enough to cause tissue breakdown or
soreness. During heavy breathing, following exercise, the cells are converting the lactic acid
either back into glucose or converting it to pyruvate and sending it through the additional
steps of aerobic respiration. By the time a person is breathing normally again the lactic acid
has been removed. The soreness is actually from small tears in the fibers themselves. After
the fibers heal they will increase in size. The number of mitochondria will also increase if
there is continued demand for additional ATP. Hence, through exercise the muscles can
increase in both strength and endurance.
Another misconception is that as the muscle increases in size it also gains more fibers. This
is not true. The fibers themselves increase in size rather than in quantity. The same holds
true for adipose tissue--fat cells do not increase in number, but rather the amount of lipids
(oil) in the cells increase.
Muscle fibers are also genetically programmed to reach a certain size and stop growing from
there, so after awhile even the hardest working weightlifter will only reach a certain level of
strength and endurance. Some people will get around this by taking steroids. The artificial
steroids cause all sorts of trouble for the person. They can cause the adrenal glands to
stop producing corticosteroids and glucosteroids. This leads to the atrophy of the gland's
medulla and causes permanent loss of the production of these hormones. The testicles may
also atrophy in response to steroids. Eventually the testes will stop making testosterone and
sperm, rendering the male infertile.
One of the more serious problems associated with abnormal gain of muscle mass is heart
failure. While for most people gaining muscle and losing fat is desirable, a body builder
is at risk of producing more muscle mass than the heart can handle. One pound of fat

Chapter 1.5 on page 12

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The Muscular System

contains about 3.5 miles of blood vessels, but one pound of muscle has about 6.5 miles.
Hence, additional muscle causes the heart to pump more blood. Some people that have
too much muscle will be very strong but will not have a healthy aerobic endurance, in part
because of the difficulty of providing oxygenated blood to so much tissue.
Sliding filament theory2
This link shows the animation of the sliding filament theory.
explanation and image of sliding filament theory3
this link gives a better demonstration of the theory with the explanation.

5.5 Involuntary Muscle Movement

Spasms
When Smooth and skeletal muscles go through multiple spasms it is referred either as seizure
or convulsion.
Cramps
Strenuous activities can cause painful spasms that are long, this is referred to as cramps.

5.6 Injury
Sprain
An injury to a joint that involves a stretched or torn ligament.
Muscle Strain
A strain occurs when a muscle or the tendon that attaches it to the bone is overstretched or
torn. Muscle strains are also called pulled muscles. Who gets it?
Anyone can strain a muscle. However, people involved in sports or other forms of strenuous
exercise are more likely to strain a muscle. What causes it?
Muscles are bunches of fibers that can contract. Muscle strains usually occur during activities
that require the muscle to tighten forcefully. The muscle is strained either because it is not
properly stretched, or warmed up, before the activity; it is too weak; or because the muscle
is already injured and not allowed time to recover. So, many muscle strains occur during
exercise or sports activities. They can also occur when lifting heavy objects. What are the
symptoms?
When a muscle is strained, it hurts and is difficult to move. You may also feel a burning
sensation in the area of the injured muscle, or feel as though something has "popped."
Sometimes the area of the strained muscle looks bruised or swells. A strained muscle might

2
3

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http://3dotstudio.com/zz.html
http://www.ucl.ac.uk/~sjjgsca/muscleSlidingFilament.html

Injury
spasm, which means it contracts suddenly and involuntarily, causing severe pain. How is it
diagnosed?
To diagnose a muscle strain, your doctor will examine the painful area, and ask how and
when the injury happened. He or she may order other diagnostic tests, such as x-rays, to
rule out any injury to the bone.
What is the treatment?
Muscle strains are treated with rest, ice, compression, and elevation, or RICE. You will be
told to rest the injured area to reduce pain and swelling. If the strain is in the leg or foot
area, you may need to use crutches. Ice packs are recommended at regular intervals (as
recommended by your doctor) over the first few days after the injury. Ice causes the blood
vessels to constrict, which reduces inflammation and pain. Anti-inflammatory medications
might also be used to relieve pain. Compression and elevation help to reduce swelling. Your
doctor may also recommend physical therapy to speed your recovery. You should avoid the
type of activity that caused the injury until the muscle is completely healed. Self-care tips
You can prevent muscle strains by warming up for at least 10 minutes before participating
in any strenuous exercise or heavy lifting. When you warm up, you increase the blood
circulation to the muscle and prepare it for exercise. When starting any new exercise
program or sport, it's important to begin gradually so your muscles are conditioned for the
activity.

5.6.1 Steroids
Anabolic steroids, which are synthetic versions of the primary male sex hormone testosterone,
can be injected, taken orally, or used transdermally. These drugs are Controlled Substances
that can be prescribed to treat conditions such as body wasting in patients with AIDS, and
other diseases that occur when the body produces abnormally low amounts of testosterone.
However, the doses prescribed to treat these medical conditions are 10 to 100 times lower
than the doses that are used for performance enhancement.
Let me be clear:- while anabolic steroids can enhance certain types of performance or
appearance,they are dangerous drugs, and when used inappropriately, they can cause a host
of severe, long-lasting, and often irreversible negative health consequences. These drugs can
stunt the height of growing adolescents, masculinize women, and alter sex characteristics of
men. Anabolic steroids can lead to premature heart attacks, strokes, liver tumors, kidney
failure and serious psychiatric problems. In addition, because steroids are often injected,
users risk contracting or transmitting HIV or hepatitis.
Abuse of anabolic steroids differs from the abuse of other illicit substances because the initial
use of anabolic steroids is not driven by the immediate euphoria that accompanies most
drugs of abuse, such as cocaine, heroin, and marijuana, but by the desire of the user to
change their appearance and performance, characteristics of great importance to adolescents.
These effects of steroids can boost confidence and strength leading the user to overlook the
potential serious long-term damage that these substances can cause.
Government agencies such as NIDA support research that increases our understanding of
the impact of steroid use and improves our ability to prevent abuse of these drugs. For

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example, NIDA funding led to the development of two highly effective programs that not
only prevent anabolic steroid abuse among male and female high school athletes, but also
promote other healthy behaviors and attitudes. The ATLAS (targeting male athletes) and
ATHENA (targeting female athletes) programs have been adopted by schools in 29 states
and Puerto Rico. Both Congress and the Substance Abuse and Mental Health Services
Administration have endorsed ATLAS and ATHENA as model prevention programs, which
could and should be implemented in more communities throughout the country.
In addition to these prevention programs and other research efforts, also has invested in
public education efforts to increase awareness about the dangers of steroid abuse. We have
material on our website about steroid abuse at www.steroidabuse.gov and in April 2005 we
again will distribute a "Game Plan" public service announcement designed to bring attention
to abuse of anabolic steroids.
Research has shown that the inappropriate use of anabolic steroids can have catastrophic
medical, psychiatric and behavioral consequences.
I hope that students, parents, teachers, coaches and others will take advantage of the
information on our website about anabolic steroids abuse and join us in our prevention and
education efforts. Participating in sports offers many benefits, but young people and adults
shouldn't take unnecessary health risks in an effort to win.(Nora D. Volkow, M.D.)
-Human-made substances related to male sex hormones. Some athletes abuse anabolic
steroids to enhance performance. Abuse of anabolic steroids can lead to serious health
problems, some of which are irreversible.
Major side effects can include liver tumors and cancer, jaundice, high blood pressure, kidney
tumors, severe acne, and trembling. In males, side effects may include shrinking of the
testicles and breast development. In females, side effects may include growth of facial hair,
menstrual changes, and deepened voice. In teenagers, growth may be halted prematurely
and permanently.
The therapeutic use of steroids can be realized by patients and their doctors by using them
in a manner that is beneficial to the person.

5.6.2 MyoD and other muscular factors

MyoD is a protein and a transcription factor that activates muscle cell differentiation by
turning on transcription of specific regulatory genes. It turns stem cells into myoblasts, a
cell that can turn into many muscle cell, also called "muscle stem cell". MyoD belongs to a
family of proteins knowns as myogenic regulatory factor(MRFs). MyoD can also turn on
transcription of it's own regulatory genes (MyoD protein coding genes), and this means that
it can produce more of itself. The positive feedback turns on transcription of other muscle
proteins, cell cycle blockers, and microRNA-206. One of the main actions of MyoD is to
remove cells from the cell cycle by enhancing the transcription of p21The function of MyoD
is to commit mesoderm cells to a skeletal lineage. MyoD can also regulate muscle repair.
One of the main actions of MyoD is to remove cells from the cell cycle by enhancing the
transcription of p21. Bidirectional Signalling- muscle cells and nerves cells send signals back
and forth to each other. Amyotrophic Lateral Sclerosis(ALS) is a loss of motor neuron and

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this blocks the formation of neuromuscular junctions. Therefore, no muscle growth which
means a potential of leading to paralysis. Stephen Hawking suffers from this disease.

5.6.3 Muscle Homeostasis

MicroRNA-206 indirectly forms neuromuscular junctions with motor neurons. Neuromuscular
junction sends synaptic signals to MyoD and this blcoks MyoD and stops or limits muscle
development. Myostatin is a protein that also blocks MyoD. Without myostatin, muscle
development increases.
Myostatin Mutations In Sheep: they can have a mutant myostatin that causes microRNA-206
to block myostatin translation
Myostatin Mutations In Humans: humans with mutant myostatin will develop lots of muscle
(like a body builder) is possible to create a drug that blocks myostatin production.

5.7 Smooth Muscle Contraction

Contractions are initiated by an influx of calcium which binds to calmodulin.
The calcium-calmodulin complex binds to and activates myosin light-chain kinase.
Myosin light-chain kinase phosphorylates myosin light-chains using ATP, causing them
to interact with actin filaments.
Powerstroke.
Calcium is actively pumped out of the cell by receptor regulated channels. A second
messanger, IP3, causes the release.
As calcium is removed the calcium-calmodulin complex breaks away from the myosin
light-chain kinase, stopping phosphorylation.
Myosin phophatase dephosphorylates the myosin. If the myosin was bound to an actin
molecule, the release is slow, this is called a latch state. In this manner, smooth muscle
is able to stay contracted for some time without the use of much ATP. If the myosin was
not bound to an actin chain it loses its affinity for actin.

It should be noted that ATP is still needed for crossbridge cycling, and that there is no
reserve, such as creatine phosphate, available. Most ATP is created from aerobic metabolism,
however anaerobic production may take place in times of low oxygen concentrations.

5.8 Cardiac Muscle

Cardiac muscle is found in the heart and lungs of humans

5.9 ATP in the Human Body

Muscles cells, like all cells, use ATP as an energy source. The total quantity of ATP in the
human body at any one time is about 0.1 Mole. The energy used by human cells requires the

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hydrolysis of 200 to 300 moles of ATP daily. This means that each ATP molecule is recycled
2000 to 3000 times during a single day. ATP cannot be stored, hence its consumption must
closely follow its synthesis. On a per-hour basis, 1 kilogram of ATP is created, processed
and then recycled in the body. Looking at it another way, a single cell uses about 10 million
ATP molecules per second to meet its metabolic needs, and recycles all of its ATP molecules
about every 20-30 seconds.

5.10 Lactic Acid

Catabolized carbohydrates is known as glycolysis. The end product of glycolysis, pyruvate
can go into different directions depending on aerobic or anaerobic conditions. In aerobic
it goes through the Krebs cycle and in anaerobic it goes through the Cori cycle. In the
Cori cycle pyruvate is converted to lactate, this forms lactic acid, lactic acid causes muscle
fatigue. In the aerobic conditions pyruvate goes through the Krebs cycle. For more about
Krebs cycle refer to chapter 2 Cell Physiology.

5.11 Muscle Disorders

5.11.1 Dermatomyositis and Polymyositis
Dermatomyositis and polymyositis cause inflammation of the muscles. They are rare
disorders, affecting only about one in 100,000 people per year. More women than men are
affected. Although the peak age of onset is in the 50s, the disorders can occur at any age.
Signs and symptoms Patients complain of muscle weakness that usually worsens over
several months, though in some cases symptoms come on suddenly. The affected muscles
are close to the trunk (as opposed to in the wrists or feet), involving for example the hip,
shoulder, or neck muscles. Muscles on both sides of the body are equally affected. In
some cases, muscles are sore or tender. Some patients have involvement of the muscles of
the pharynx (throat) or the esophagus (the tube leading from the throat to the stomach),
causing problems with swallowing. In some cases, this leads to food being misdirected from
the esophagus to the lungs, causing severe pneumonia.
In dermatomyositis, there is a rash, though sometimes the rash resolves before muscle
problems occur. A number of different types of rash can occur, including rashes on the
fingers, the chest and shoulders, or on the upper eyelids (show picture 1-3). In rare cases,
the rash of dermatomyositis appears but myopathy never develops.
Other problems sometimes associated with these diseases include fever, weight loss, arthritis,
cold-induced color changes in the fingers or toes (Raynaud phenomenon), and heart or lung
problems.

5.11.2 Muscle Atrophy

Alternative names : Atrophy of the muscles, Muscle wasting, Wasting

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The majority of muscle atrophy in the general population results from disuse. People with
sedentary jobs and senior citizens with decreased activity can lose muscle tone and develop
significant atrophy. This type of atrophy is reversible with vigorous exercise. Bed-ridden
people can undergo significant muscle wasting. Astronauts, free of the gravitational pull of
Earth, can develop decreased muscle tone and loss of calcium from their bones following
just a few days of weightlessness.
Muscle atrophy resulting from disease rather than disuse is generally one of two types, that
resulting from damage to the nerves that supply the muscles, and disease of the muscle
itself. Examples of diseases affecting the nerves that control muscles would be poliomyelitis,
amyotrophic lateral sclerosis (ALS or Lou Gehrig's disease), and Guillain-Barre syndrome.
Examples of diseases affecting primarily the muscles would include muscular dystrophy,
myotonia congenita, and myotonic dystrophy as well as other congenital, inflammatory or
metabolic myopathies.
Even minor muscle atrophy usually results in some loss of mobility or power.
Common Causes

some atrophy that occurs normally with ageing

cerebrovascular accident (stroke)
spinal cord injury
peripheral nerve injury (peripheral neuropathy)
other injury
prolonged immobilization
osteoarthritis
rheumatoid arthritis
prolonged corticosteroid therapy
diabetes (diabetic neuropathy)
burns
poliomyelitis
amyotrophic lateral sclerosis (ALS or Lou Gehrig's disease)
Guillain-Barre syndrome
muscular dystrophy
myotonia congenita
myotonic dystrophy
myopathy

5.11.3 Muscular Dystrophy

Muscular dystrophy (MD) is a group of rare inherited muscle diseases in which muscle
fibers are unusually susceptible to damage. Muscles, primarily voluntary muscles, become
progressively weaker. In the late stages of muscular dystrophy, muscle fibers are often
replaced by fat and connective tissue. In some types of muscular dystrophy, heart muscles,
other involuntary muscles and other organs are affected.
The most common types of muscular dystrophy appear to be due to a genetic deficiency of
the muscle protein dystrophin. There's no cure for muscular dystrophy, but medications
and therapy can slow the course of the disease.

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5.12 Medical Mysteries

Sleep Twitches
The twitching phenomenon that happens in the early stage of sleep is called a hypnagogic
massive jerk, or simply a hypnic jerk. It has also been referred to as a sleep start. There has
been little research on this topic, but there have been some theories put forth. When the
body drifts off into sleep, it undergoes physiological changes related to body temperature,
breathing rate and muscular tone. Hypnic jerks may be the result of muscle changes. Another
theory suggests that the transition from the waking to the sleeping state signals the body to
relax. But the brain may interpret the relaxation as a sign of falling and then signal the arms
and legs to wake up. Electroencephalogram studies have shown sleep starts affect almost 10
percent of the population regularly, 80 percent occasionally, and another 10 percent rarely.
Muscle movement or twitching also may take place during the Rapid Eye Movement, or
REM, phase of sleep. This also is the time when dreams occur. During the REM phase, all
voluntary muscular activity stops with a drop in muscle tone, but some individuals may
experience slight eyelid or ear twitching or slight jerks. Some people with REM behavioral
disorder, or RBD, may experience more violent muscular twitching and full-fledged activity
during sleep. This is because they do not achieve muscle paralysis, and as a result, act out
their dreams. Researchers think that people with RBD lack neurological barriers that define
the different stages of sleep. New research done by the Mayo Clinic and published in the
July 2003 issue of Sleep Medicine shows that melatonin can help lessen RBD symptoms.
Resources:
Sleep twitches, or myoclonic jerks, as they are sometimes called, are explained in easily
understood language on this website.
Learn more about REM Behavior Disorder, or RBD, and treatment for sufferers.
View information about various sleep disorders such as insomnia, apnea, and narcolepsy.

5.13 Microbiology
Clostridium tetani
Tetanus
Normally a nerve impulse initiates contraction of a muscle. At the same time, an opposing
muscle receives the signal to relax so as not to oppose the contraction. Tetanus toxin blocks
the relaxation, so both sets of muscle contract. The usual cause of tetany is lack of calcium,
but excess of phosphate (high phosphate-to-calcium ratio) can also trigger the spasms.
Clostridium botulinum
Infant botulism (floppy baby syndrome) the most common form of botulism in the U.S. of
the four forms of botulism.
If ingested, the toxin is absorbed in the intestine, goes to the blood, and on to the nervous
system. It acts on the peripheral nervous system by blocking the impulse that is normally

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Glossary
passes along to the nervous system. By clocking the impulse that is normally passed along
to motor end plates so the muscle contraction can be released, resulting in paralysis.

5.14 Glossary
Actin
A protien that forms a long polymer rods called microfilaments; Interacts with myosin to
cause movement in muscles.
ATP
"Adenosine Triphosphate" is a nucleotide that comes from adenosine that takes place in
muscle tissue: This provides a large source of energy for cellular reactions.
Cardiac muscle
is also an "involuntary muscle" but it's a specialized kind of muscle found only within the
heart.
Clostridium botulinum
A pathogen that causes botulism, gram stain positive, morphology is rod shaped, grows in
anaerobic conditions, and produces spores.
Clostridium tetani
A pathogen that causes lock jaw, gram stain positive, morphology is tennis racket shaped
rod, grows in anaerobic conditions, and produces spores.
Cori cycle
In anaerobic conditions produces lactic acid.
Cramp
A localized muscle spasm that happens after strenuous activity.
Glycogen
Glucose that has been converted for energy storage. Muscles store energy for their own use
in this form.
Lactic acid
Causes muscle fatigue.
Muscle
Contractile tissue that is derived from the mesodermal layer of embryonic germ cells.
Muscular Dystrophy
A hereditary disease characterized by progressive atrophy of muscle fibers
Myosin
The fibrous motor protein that uses ATP to drive movements along actin filaments.

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Sarcoplasmic Reticulum
Smooth-surfaced tubules forming a plexus around each myofibril that function as a storage
and release area for calcium ions (CA+2).
Skeletal muscle
this "voluntary muscle" is anchored by tendons to the bone and is used to affect skeletal
movement such as locomotion.
Smooth muscle
this "involuntary muscle" is found within the walls of organs and structures such as the
esophagus, stomach, intestines, bronchi, uterus, ureters, bladder, and blood vessels.
Sprain
Injuries that involves a stretched or torn ligament.
Strain
A injury to the muscle or tendon attachment

5.15 References
Van De Graaff (2002) Human Anatomy 6th ed. McGraw-Hill Higher Education
Windmaier, P.W. Raff, H. Strang, T.S. (2004) Vander, Sherman, & Luciano's Human
Physiology, the Mechanisms of Body Function 9th ed. Mcgraw-Hill
Neil A. Campbell , Jane B. Reece "Biology 8th edition"

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6 Blood Physiology
6.1 Overview of Blood
The primary function of blood is to supply oxygen and nutrients as well as constitutional
elements to tissues and to remove waste products. Blood also enables hormones and other
substances to be transported between tissues and organs. Problems with blood composition or
circulation can lead to downstream tissue malfunction. Blood is also involved in maintaining
homeostasis by acting as a medium for transferring heat to the skin and by acting as a
buffer system for bodily pH.
The blood is circulated through the lungs and body by the pumping action of the heart. The
right ventricle pressurizes the blood to send it through the capillaries of the lungs, while the
left ventricle re-pressurizes the blood to send it throughout the body. Pressure is essentially
lost in the capillaries, hence gravity and especially the actions of skeletal muscles are needed
to return the blood to the heart.

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Blood Physiology

Figure 57

Blood circulation from the heart to the lungs.

6.1.1 Gas Exchange

Oxygen (O2 ) is the most immediate need of every cell and is carried throughout the
body by the blood circulation. Oxygen is used at the cellular level as the final electron
acceptor in the electron transport chain (the primary method of generating ATP for cellular
reactions). Oxygen is carried in the blood bound to hemoglobin molecules within red blood
cells. Hemoglobin binds oxygen when passing through the alveoli of the lungs and releases
oxygen in the warmer, more acidic environment of bodily tissues, via simple diffusion.
Carbon dioxide (CO2 ) is removed from tissues by blood and released into the air via
the lungs. Carbon dioxide is produced by cells as they undergo the processes of cellular
respiration (particularly the Kreb's Cycle). The molecules are produced from carbons that
were originally part of glucose. Most of the carbon dioxide combines with water and is

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Blood Composition
carried in the plasma as bicarbonate ions. An excess of carbon dioxide (through exercise,
or from holding ones breath) quickly shifts the blood pH to being more acidic (acidosis).
Chemoreceptors in the brain and major blood vessels detect this shift and stimulate the
breathing center of the brain (the medulla oblongata). Hence, as CO2 levels build up and
the blood becomes more acidic, we involuntarily breathe faster, thus lowering CO2 levels
and stabilizing blood pH. In contrast, a person who is hyperventilating (such as during a
panic attack) will expire more CO2 than being produced in the body and the blood will
become too alkaline (alkalosis).

6.2 Blood Composition

Blood is a circulating tissue composed of fluid plasma and cells (red blood cells, white blood
cells, platelets). Anatomically, blood is considered a connective tissue, due to its origin in
the bones and its function. Blood is the means and transport system of the body used in
carrying elements (e.g. nutrition, waste, heat) from one location in the body to another, by
way of blood vessels.
Blood is made of two parts:
1. Plasma which makes up 55% of blood volume.
2. Formed cellular elements (red and white blood cells, and platelets) which combine to
make the remaining 45% of blood volume.

6.2.1 Plasma makeup

Plasma is made up of 90% water, 7-8% soluble proteins (albumin maintains bloods osmotic
integrity, others clot, etc), 1% electrolytes, and 1% elements in transit. One percent of
the plasma is salt, which helps with the pH of the blood. The largest group of solutes in
plasma contains three important proteins to be discussed. There are: albumins, globulins,
and clotting proteins.
Albumins are the most common group of proteins in plasma and consist of nearly two-thirds
of them (60-80%). They are produced in the liver. The main function of albumins is to
maintain the osmotic balance between the blood and tissue fluids and is called colloid
osmotic pressure. In addition, albumins assist in transport of different materials, such as
vitamins and certain molecules and drugs (e.g. bilirubin, fatty acids, and penicillin).
Globulins are a diverse group of proteins, designated into three groups: gamma, alpha, and
beta. Their main function is to transport various substances in the blood. Gamma globulins
assist the body's immune system in defense against infections and illness.
Clotting proteins are mainly produced in the liver as well. There are at least 12 substances,
known as "clotting factors" that participate in the clotting process. One important clotting
protein that is part of this group is fibrinogen, one of the main components in the formation
of blood clots. In response to tissue damage, fibrinogen makes fibrin threads, which serve
as adhesive in binding platelets, red blood cells, and other molecules together, to stop the
blood flow. (This will be discussed in more detail later on in the chapter.)

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Plasma also carries Respiratory gases; CO2 in large amounts(about 97%) and O2 in small
amounts(about 3%), various nutrients(glucose, fats), wastes of metabolic exchange(urea,
ammonia), hormones, and vitamins.

Figure 58

160

Picture of red blood cells.

Blood Composition

6.2.2 Red Blood Cells

Overview
Red blood cell (erythrocyte) also known as "RBC's". RBCs are formed in the myeloid
tissue or most commonly known as red bone marrow, although when the body is under
severe conditions the yellow bone marrow, which is also in the fatty places of the marrow in
the body will also make RBCs. The formation of RBCs is called erythropoiesis ( erythro
/ red; poiesis / formation). Red blood cells lose nuclei upon maturation, and take on a
biconcave, dimpled, shape. They are about 7-8 micrometers in diameter. There are about
1000x more red blood cells than white blood cells. RBC's live about 120 days and do not
self repair. RBC's contain hemoglobin which transports oxygen from the lungs to the rest of
the body, such as to the muscles, where it releases the oxygen load.The hemoglobin gets it's
red color from their respiratory pigments.
Shape
RBC'S have a shape of a disk that appears to be caved in or almost flattened in the
middle; this is called bi-concave. This bi-concave shape allows the RBC to carry oxygen
and pass through even the smallest capillaries in the lungs. This shape also allows RBCs to
stack like dinner plates and bend as they flow smoothly through the narrow blood vessels
in the body. RBC's lack a nucleus (no DNA) and no organelles, meaning that these cells
cannot divide or replicate themselves like the cells in our skin and muscles. RBCs have a
short life span of about 120 days, however, as long as our myeloid tissue is working correctly,
we will produce about 2-3 million RBC's per second. That is about 200 billion a day! This
allows us to have more to replace the ones we lose.
Main Component
The main component of the RBC is hemoglobin protein which is about 250 million per cell.
The word hemoglobin comes from hemo meaning blood and globin meaning protein. This
is the protein substance of four different proteins: polypeptide globin chains that contain
anywhere from 141 to 146 amino acids. Hemoglobin also is responsible for the cells ability
to transport oxygen and carbon dioxide. This hemoglobin + iron + oxygen interact with
each other forming the RBC's bright red color. You can call this interaction by product
oxyhemoglobin. Carbon Monoxide forms with hemoglobin faster that oxygen, and stays
formed for several hours making hemoglobin unavailable for oxygen transport right away.
Also a red blood cell contains about 200 million hemoglobin molecules. If all this hemoglobin
was in the plasma rather than inside the cells, your blood would be so "thick" that the heart
would have a difficult time pumping it through. The thickness of blood is called viscosity.
The greater the viscosity of blood, the more friction there is and more pressure is needed to
force blood through.
Functions
The main function is the transportation of oxygen throughout the body and the ability of the
blood to carry out carbon dioxide which is called carbamino hemoglobin. Maintaining
the balance of blood is important. The balance can be measured by the acid and base levels
in the blood. This is called pH. Normal pH of blood ranges between 7.35-7.45; this normal

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Blood Physiology
blood is called Alkaline (less acidic then water). A drop in pH is called Acidic. This
condition is also called Acidosis. A jump in pH higher then 7.45 is called "Alkalosis". To
maintain the homeostasis (or balance,) the blood has tiny molecules within the RBC that
help prevent drops or increases from happening.

Figure 59 From left to right diagram of Erythrocyte, Thrombocyte, and

Leukocyte
Destruction
Red blood cells are broken down and hemoglobin is released. The globin part of the
hemoglobin is broken down into amino acid components, which in turn are recycled by the
body. The iron is recovered and returned to the bone marrow to be reused. The heme
portion of the molecule experiences a chemical change and then gets excreted as bile pigment
(bilirubin) by the liver. Heme portion after being broken down contributes to the color of
feces and your skin color changing after being bruised.

6.2.3 White Blood Cells

Shape
White blood cells are different from red cells in the fact that they are usually larger in
size 10-14 micrometers in diameter. White blood cells do not contain hemoglobin which
in turn makes them translucent. Many times in diagrams or pictures white blood cells are
represented in a blue color, mainly because blue is the color of the stain used to see the cells.

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White blood cells also have nucleii, that are some what segmented and are surrounded by
electrons inside the membrane.
Functions
White blood cells (leukocytes) are also known as "WBC's". White blood cells are made
in the bone marrow but they also divide in the blood and lymphatic systems. They are
commonly amoeboid (cells that move or feed by means of temporary projections, called
pseudopods (false feet), and escape the circulatory system through the capillary beds. The
different types of WBC's are Basophils, Eosinophils, Neutrophils, Monocytes, B- and
T-cell lymphocytes. Neutrophils, Eosinophils, and Basophils are all granular leukocytes.
Lymphocytes and Monocytes are agranular leukocytes. Basophils store and synthesize
histamine which is important in allergic reactions. They enter the tissues and become "mast
cells" which help blood flow to injured tissues by the release of histamine. Eosinophils are
chemotoxic and kill parasites. Neutrophils are the first to act when there is an infection
and are also the most abundant white blood cells. Neutrophils fight bacteria and viruses by
phagocytosis which mean they engulf pathogens that may cause infection. The life span of
a of Neutrophil is only about 12-48 hours. Monocytes are the biggest of the white blood
cells and are responsible for rallying the cells to defend the body. Monocytes carry out
phagocytosis and are also called macrophages. Lymphocytes help with our immune response.
There are two Lymphocytes: the B- and T- cell. B-Lymphocytes produce antibodies that
find and mark pathogens for destruction. T-Lymphocytes kill anything that they deem
abnormal to the body.
WBCs are classified by phenotype which can be identified by looking at the WBCs under a
microscope. The Granular phenotype are able to stain blue. The Agranular phenotype are
able to stain red. Neutrophils make up 50-70% of Granular cells Eosinophils make up 2-4%,
and Basophils 0-1%. Monocytes make up 2-8% of Agranular cells. B and T Lymphocytes
make up 20-30%. As you can see, there is a great deal of differentiation between WBCs.
These special cells help our bodies defend themselves against pathogens. Not only do they
help our immune system but they remove toxins, wastes, and abnormal or damaged cells.
Thus, we can say that WBCs' main function is being Phagocytic which means to engulf or
swallow cells.

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6.2.4 Platelets

Figure 60 A 250 ml bag of

newly collected platelets.

Platelets, also called thrombocytes, are membrane-bound cell fragments. Platelets have
no nucleus,they are between one to two micrometers in diameter, and are about 1/10th to
1/20th as abundant as white blood cells. Less than 1% of whole blood consists of platelets.
They result from fragmentation of large cells called Megakaryocytes - which are cells derived
from stem cells in the bone marrow. Platelets are produced at a rate of 200 billion per day.
Their production is regulated by the hormone called Thrombopoietin. The circulating life
of a platelet is 810 days. The sticky surface of the platelets allow them to accumulate
at the site of broken blood vessels to form a clot. This aids in the process of hemostasis
("blood stopping"). Platelets secrete factors that increase local platelet aggregation (e.g.,
Thromboxane A), enhance vasoconstriction (e.g., Serotonin), and promote blood coagulation
(e.g., Thromboplastin).

6.3 Hemostasis (Coagulation or Clotting)

Hemostasis is the natural process of stopping blood flow or loss of blood following an injury.
(hemo = blood; stasis = standing). It has three stages: (1) vascular spasm, vasoconstriction,
or intense contraction of blood vessels, (2) formation of a platelet plug and (3) blood clotting
or coagulation. Once the flow of blood has been stopped, tissue repair can begin.
Vascular spasm or Vasoconsriction: In a normal individual, immediately after a blood
vessel has been cut and endothelial cells are damaged, vasoconstriction occurs, thus slowing
blood flow to the area. Smooth muscle in the vessel wall goes through spasms or intense
contractions that constrict the vessel. If the vessels are small, spasms compress the inner
walls together and may be able to stop the bleeding completely. If the vessels are medium
to large-sized, the spasms slow down immediate outflow of blood, lessening the damage but

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still preparing the vessel for the later steps of hemostasis. These vascular spasms usually
last for about 30 minutes, long enough for the next two stages of hemostasis to take place.
Formation of a Platelet Plug: Within 20 seconds of an injury, coagulation is initiated.
Contrary to popular belief, clotting of a cut on the skin is not initiated by air or drying out,
but by platelets adhering to and activated by collagen in the blood vessels endothelium.
The activated platelets then release the contents of their granules, which contain a variety
of substances that stimulate further platelet activation and enhance the hemostatic process.
When the lining of a blood vessel breaks and endothelial cells are damaged, revealing collagen
proteins in the vessel wall, platelets swell, grow spiky extensions, and start clumping together.
They start to stick to each other and the walls of the vessel. This continues as more platelets
congregate and undergo these same transformations. This process results in a platelet plug
that seals the injured area. If the injury is small, a platelet plug may be able to form and
close it within several seconds. If the damage is more serious, the next step of blood clotting
will take place. Platelets contain secretory granules. When they stick to the proteins in the
vessel walls, they degranulate, thus releasing their products, which include ADP (adenosine
diphosphate), serotonin, and thromboxane A2.
A Blood Clot Forms: If the platelet plug is not enough to stop the bleeding, the third
stage of hemostasis begins: the formation of a blood clot. First, blood changes from a liquid
to a gel. At least 12 substances called clotting factors take part in a series of chemical
reactions that eventually create a mesh of protein fibers within the blood. Each of the
clotting factors has a very specific function. We will discuss just three of the substances
here: prothrombin, thrombin, and fibrin. Prothrombin and fibrinogen are proteins that are
produced and deposited in the blood by the liver.
Prothrombin: When blood vessels are damaged, vessels and nearby platelets are stimulated
to release a substance called prothrombin activator, which in turn activates the conversion
of prothrombin, a plasma protein, into an enzyme called thrombin. This reaction requires
calcium ions.
Thrombin: Thrombin facilitates the conversion of a soluble plasma protein called fibrinogen
into long insoluble fibers or threads of the protein fibrin.
Fibrin: Fibrinogen is cleaved by thrombin to form its active form, "fibrin." Fibrin threads
wind around the platelet plug at the damaged area of the blood vessel, forming an
interlocking network of fibers and a framework for the clot. This net of fibers traps and
helps hold platelets, blood cells and other molecules tight to the site of injury, functioning
as the initial clot. This temporary fibrin clot can form in less than a minute, and usually
does a good job of reducing the blood flow. Next, platelets in the clot begin to shrink,
tightening the clot and drawing together the vessel walls. Usually, this whole process of
clot formation and tightening takes less than a half hour.
The use of adsorbent chemicals, such as zeolites, and other hemostatic agents, are also being
explored for use in sealing severe injuries quickly.

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6.4 ABO Group System

The ABO blood group is represented by substances on the surface of red blood cells
(RBCs). These substances are important because they contain specific sequences of amino
acid and carbohydrates which are antigenic. As well as being on the surface of RBCs, some
of these antigens are also present on the cells of other tissues. A complete blood type
describes the set of 29 substances on the surface of RBCs, and an individual's blood type
is one of the many possible combinations of blood group antigens. Usually only the ABO
blood group system and the presence or absence of the Rhesus D antigen (also known as
the Rhesus factor or RH factor) are determined and used to describe the blood type. Over
400 different blood group antigens have been found, many of these being very rare. If an
individual is exposed to a blood group antigen that is not recognized as self, the individual
can become sensitized to that antigen; the immune system makes specific antibodies which
binds specifically to a particular blood group antigen and an immunological memory against
that particular antigen is formed. These antibodies can bind to antigens on the surface
of transfused red blood cells (or other tissue cells) often leading to destruction of the cells
by recruitment of other components of the immune system. Knowledge of a individual's
blood type is important to identify appropriate blood for transfusion or tissue for organ
transplantation.

6.4.1 Surface Antigens

Several different RBC surface antigens stemming from one allele (or very closely linked genes)
are collectively labeled as a blood group system (or blood group). The two most important
blood group systems were discovered during early experiments with blood transfusion, the
ABO group in 1901 and the Rhesus group in 1937 . These two blood groups are reflected in
the common nomenclature A positive, O negative, etc. with letters referring to the ABO
group and positive/negative to the presence/absence of the RhD antigen of the Rhesus
group. Development of the Coombs test in 1945 and the advent of transfusion medicine led
to discovery of more blood groups.

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ABO Group System

Figure 61

Compatibility of blood types.

Blood Group AB individuals have both A and B antigens on the surface of their RBCs,
and their blood serum does not contain any antibodies against either A or B antigen.
Therefore, a individual with type AB blood can receive blood from any group (with AB
being preferable), but can only donate blood to another group AB individual. AB blood is
also known as "Universal receiver."
Blood Group A individuals have the A antigen on the surface of their RBCs, and blood
serum containing IgM antibodies against the B antigen. Therefore, a group A individual
can only receive blood from individuals of groups A or O (with A being preferable), and can
donate blood to individuals of groups A or AB.
Blood Group B individuals have the B antigen on their surface of their RBCs, and blood
serum containing IgM antibodies against the A antigen. Therefore, a group B individual
can only receive blood from individuals of groups B or O (with B being preferabe), and can
donate blood to individuals of groups B or AB.

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Blood Physiology
Blood group O individuals do not have either A or B antigens on the surface of their RBCs,
but their blood serum contains IgM antibodies against both A and B antigens. Therefore, a
group O individual can only receive blood from a group O individual, but they can donate
blood to individuals of any ABO blood group (ie A, B, O or AB). O blood is also know as
"Universal donor."

6.4.2 Inheritance
Blood types are inherited and represent contributions from both parents. The ABO blood
type is controlled by a single gene with three alleles: i, IA, and IB. The gene encodes an
enzyme that modifies the carbohydrate content of the red blood cell antigens.
IA gives type A, IB gives type B, i give types O
Blood group inheritance
Mother/Father
O
O
O
A
O, A
B
O, B
AB
A, B

A
O,
O,
O,
A,

A
A
A, B, AB
B, AB

B
O,
O,
O,
A,

B
A, B, AB
B
B, AB

AB
A, B
A, B, AB
A, B, AB
A, B, AB

IA and IB are dominant over i, so ii people have type O, IAIA or IAi have A, and IBIB or
IBi have type B. IAIB people have both phenotypes because A and B are codominant, which
means that type A and B parents can have an AB child. Thus, it is extremely unlikely for a
type AB parent to have a type O child (it is not, however, direct proof of illegitimacy): the
cis-AB phenotype has a single enzyme that creates both A and B antigens. The resulting red
blood cells do not usually express A or B antigen at the same level that would be expected
on common group A or B red blood cells, which can help solve the problem of an apparently
genetically impossible blood group.
Rh Factor
Many people have the Rh Factor on the red blood cell. Rh carriers do not have the antibodies
for the Rh Factor, but can make them if exposed to Rh. Most commonly Rh is seen when
anti-Rh antibodies cross from the mothers placenta into the child before birth. The Rh
Factor enters the child destroying the child's red blood cells. This is called Hemolytic
Disease.

6.4.3 Compatibility in Blood/Plasma Transfusions

Blood transfusions between donor and recipient of incompatible blood types can cause
severe acute immunological reactions, hemolysis (RBCT destruction), renal failure, shock,
and sometimes death. Antibodies can be highly active and can attack RBCs and bind
components of the complement system to cause massive hemolysis of the transfused blood.
A patient should ideally receive their own blood or type-specific blood products to minimize
the chance of a transfusion reaction. If time allows, the risk will further be reduced by
cross-matching blood, in addition to blood typing both recipient and donor. Cross-matching

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ABO Group System

involves mixing a sample of the recipient's blood with a sample of the donor's blood and
checking to see if the mixture agglutinates, or forms clumps. Blood bank technicians usually
check for agglutination with a microscope, and if it occurs, that particular donor's blood
cannot be transfused to that particular recipient. Blood transfusion is a potentially risky
medical procedure and it is vital that all blood specimens are correctly identified, so in
cross-matching labeling is standardized using a barcode system known as ISBT 128.
Plasma compatibility table
Donor
Recipient
O
O
OK
A
B
AB

A
OK
OK

B
OK
OK

AB
OK
OK
OK
OK

When considering a plasma transfusion, keep in mind that plasma carries antibodies and
no antigens. For example you can't give type O plasma to a type A, B or AB, because a
person with type O blood has A and B antibodies and the recipient would have an immune
response. On the other hand an AB donor could give plasma to anyone, since they have no
antibodies.
The table to the right is for plasma transfusions, and it's just the opposite for RBC
transfusions. It doesn't take the Rh factor into effect, though, because most people don't
have antibodies for the Rhesus factor (it only happens upon exposure).
Hemolytic Disease of the Newborn
Often a pregnant woman carries a fetus with a different blood type to herself, and sometimes
the mother forms antibodies against the red blood cells of the fetus, leading to low fetal
blood counts, a condition known as hemolytic disease of the newborn.
Hemolytic disease of the newborn, (also known as HDN) is an alloimmune condition that
develops in a fetus when the IgG antibodies produced by the mother and passing through
the placenta include ones which attack the red blood cells in the fetal circulation. The
red cells are broken down and the fetus can develop reticulocytosis and anemia. The fetal
disease ranges from mild to very severe and fetal death from heart failure - hydrops fetalis can occur. When the disease is moderate or severe many erythroblasts are present in the
fetal blood and so these forms of the disease can be called erythroblastosis fetalis.
Before birth, options for treatment include intrauterine transfusion or early induction of
labor when pulmonary maturity has been attained, fetal distress is present, or 35 to 37
weeks of gestation have passed. The mother may also undergo plasma exchange to reduce
the circulating levels of antibody by as much as 75%.
After birth, treatment depends on the severity of the condition, but could include temperature
stabilization and monitoring, phototherapy, transfusion with compatible packed red blood,
exchange transfusion with a blood type compatible with both the infant and the mother,
sodium bicarbonate for correction of acidosis and/or assisted ventilation.

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Blood Physiology
Rh negative mothers who have had a pregnancy with or are pregnant with a Rh positive
infant, are given Rh immune globulin (RhIG) also known as Rhogam, during pregnancy and
after delivery to prevent sensitization to the D antigen. It works by binding any fetal red
cells with the D antigen before the mother is able to produce an immune response and form
anti-D IgG. A drawback to pre-partum administration of RhIG is that it causes a positive
antibody screen when the mother is tested which is indistinguishable from immune reasons
for antibody production.

6.5 Diseases of the Blood

6.5.1 Von Willebrand Disease
The most common inherited bleeding disorder, von Willebrand disease affects both men
and women equally. Von Willebrand disease is similar to hemophilia in that it involves a
definciency in the ability of blood to clot properly. Those affect by von Willebrand disease
will have one or more of the following- low levels of von Willebrand factor (a protein that
helps the blood to clot), and/or their von Willebrand factor doesn't work properly. While it
is mostly an inherited disease (with factors contributed by both parents), von Willebrand
disease may be an aquired syndrome in rare cases.
There are three types of von Willebrand disease: Type 1, which is the mildest and most
common form of the disease; Type 2, which has four subtypes (2A, 2B, 2M, and 2N) and
ranges from mild to moderate in severity; and finally, Type 3, which is very rare and is the
most severe form.
Type 1
In type 1 von Willebrand disease, there is a low level of von Willebrand factor. The level of
factor VIII may also be lower than normal. This is the mildest and most common form of
the disease. About 3 out of 4 people diagnosed with von Willebrand disease have type 1.
Type 2
In type 2 von Willebrand disease, a defect in von Willebrand factor causes it to not work
properly. Type 2 is divided into 2A, 2B, 2M, and 2N. Each is treated differently, so knowing
the exact type is important.
People with type 1 and type 2 von Willebrand disease may have the following mild-tomoderate bleeding symptoms: easy bruising, nosebleeds, bleeding from the gums after a
dental procedure, heavy menstrual bleeding in women, blood in their stools or urine (from
bleeding in the intestines, stomach, kidneys or bladder), excessive bleeding after a cut or
other accident or surgery.
Type 3
People with type 3 von Willebrand disease usually have no von Willebrand factor and very
low factor VIII. Type 3 is severe and very rare.
Symptoms of type 3 von Willebrand disease might include any of the symptoms of types 1
and 2, and also include severe bleeding episodes for no reason, which can be life threatening

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if not treated immediately. Bleeding into soft tissues or joints (hemarthrosis), causing severe
pain and swelling, is another symptom.
Treatment
Many people with von Willebrand disease do not require treatment to manage the disease.
However, if treatment is ncessary, it may include a range of different interventions depending
on the severity. These involve medicine to increase the level of von Willebrand factor in
the blood (DDAVP), medicine to prevent the breakdown of clots (called antifibrinolytic
drugs), medicine to control heavy menstrual bleeding in women (often birth control pills), or
injection of clotting factor concentrates (containing von Willebrand factor and factor VIII).

6.5.2 Disseminated Intravascular Coagulation

Disseminated intravascular coagulation (DIC), also called consumptive coagulopathy, is
a pathological process in the body where the blood starts to coagulate throughout the
whole body. This depletes the body of its platelets and coagulation factors, and there is
a paradoxically increased risk of hemorrhage. It occurs in critically ill patients, especially
those with Gram-negative sepsis (particularly meningococcal sepsis) and acute promyelocytic
leukemia.

6.5.3 Hemophilia
Hemophilia is a disease where there is low or no blood protein, causing an inability to
produce blood clots. There are two types of Hemophilia: Type A, which is a deficiency in
factor VIII and Type B, (Christmas disease) a deficiency on factor IX. Because people with
hemophilia do not have the ability to make blood clots, even a little cut may kill them, or
the smallest bump or jar to the body could cause severe bruising that doesn't get better for
months.
Hemophilia is passed down from mothers to their sons. Hemophilia is sometimes known as
the "Royal Disease". This is because Queen Victoria, Queen of England (1837-1901), was
a carrier of hemophilia. The hemophilia disease was passed down to her son Leopold who
ended up dying at age 31. Queen Victoria also had two daughters who were carriers. These
daughters passed hemophilia into the Spanish, German, and Russian royal families. One of
the most famous stories is that of the Russian royal family. Alexandra, granddaughter to
Queen Victoria, married Nicholas (Tsar of Russia in the 1900s). Alexandra was a carrier
of the disease and passed the disease to their first son, Tsarevich Alexi, who was heir to
the throne of Russia. The family tried to keep their son's secret from the people, but Alexi
suffered with serious bruises and extreme pain. The family found help from a monk named
Rasputin. He kept their secret and gained a great deal of power over the family, making
them think he was their only hope. During this time of great turmoil in Russia, Nicholas
and Alexandra spent most of their attentions on their son, and not on the people. It wasn't
long before the Bolshevik Revolution of 1917 began.

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6.5.4 Factor V Leiden

The opposite of Hemophilia, Factor V Leiden is the name given to a variant of human factor
V that causes a hypercoagulability disorder. In this disorder the Leiden variant of factor
V, cannot be inactivated by activated protein C. Factor V Leiden is the most common
hereditary hypercoagulability disorder amongst Eurasians. It is named after the city Leiden
(The Netherlands), where it was first identified in 1994 by Prof R. Bertina et al. Those that
have it are at a slightly higher risk of developing blood clots than those without. Those that
test positive for factor V should avoid (oral contraceptives, obesity, smoking, and high blood
pressure.)

6.5.5 Anemia
Anemia (AmE) or anaemia (BrE), from the Greek () meaning "without blood", refers
to a deficiency of red blood cells (RBCs) and/or hemoglobin. This results in a reduced
ability of blood to transfer oxygen to the tissues, causing hypoxia. Since all human cells
depend on oxygen for survival, varying degrees of anemia can have a wide range of clinical
consequences. Hemoglobin (the oxygen-carrying protein in the red blood cells) has to be
present to ensure adequate oxygenation of all body tissues and organs.
The three main classes of anemia include excessive blood loss (acutely such as a hemorrhage
or chronically through low-volume loss), excessive blood cell destruction (hemolysis) or
deficient red blood cell production (ineffective hematopoiesis). In menstruating women,
dietary iron deficiency is a common cause of deficient red blood cell production.

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Diseases of the Blood

6.5.6 Sickle cell

Figure 62

Image of RBC's with Sickle Cell mutations.

Sickle-cell disease is a general term for a group of genetic disorders caused by sickle hemoglobin
(Hgb S or Hb S). In many forms of the disease, the red blood cells change shape upon
deoxygenation because of polymerization of the abnormal sickle hemoglobin. This process
damages the red blood cell membrane, and can cause the cells to become stuck in blood
vessels. This deprives the downstream tissues of oxygen and causes ischemia and infarction.
The disease is chronic and lifelong. Individuals are most often well, but their lives are
punctuated by periodic painful attacks. In addition to periodic pain, there may be damage
of internal organs, and/or stroke. Lifespan is often shortened with sufferers living to an

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average of 40 years. It is common in people from parts of the world where malaria is or was
common, especially in sub-Saharan Africa or in descendants of those peoples.
Genetics: Sickle-cell disease is inherited in the autosomal recessive pattern, depicted above.
The allele responsible for sickle cell anemia is autosomal recessive. A person who receives
the defective gene from both father and mother develops the disease; a person who receives
one defective and one healthy allele remains healthy, but can pass on the disease and is
known as a carrier. If two parents who are carriers have a child, there is a 1-in-4 chance of
their child developing the illness and a 1-in-2 chance of their child just being a carrier.

6.5.7 Polycythemia
Polycythemia is a condition in which there is a net increase in the total circulating erythrocyte
(red blood cell) mass of the body. There are several types of polycythemia.
Primary Polycythemia
In primary polycythemia, there may be 8 to 9 million and occasionally 11 million erythrocytes
per cubic millimeter of blood (a normal range for adults is 4-5 million), and the hematocrit
may be as high as 70 to 80%. In addition, the total blood volume can increase to as much
as twice as normal. The entire vascular system can become markedly engorged with blood,
and circulation times for blood throughout the body can increase up to twice the normal
value. The increased numbers of erythrocytes can increase of the viscosity of the blood to as
much as five times normal. Capillaries can become plugged by the very viscous blood, and
the flow of blood through the vessels tends to be extremely sluggish.
As a consequence of the above, people with untreated Polycythemia are at a risk of various
thrombotic events (deep venous thrombosis, pulmonary embolism), heart attack and stroke,
and have a substantial risk of Budd-Chiari syndrome (hepatic vein thrombosis). The
condition is considered chronic; no cure exists. Symptomatic treatment (see below) can
normalize the blood count and most patients can live a normal life for years.
Secondary polycythemia
Secondary polycythemia is caused by either appropriate or inappropriate increases in the
production of erythropoietin that result in an increased production of erythrocytes. In
secondary polycythemia, there may be 6 to 8 million and occasionally 9 million erythrocytes
per cubic millimeter of blood. A type of secondary polycythemia in which the production
of erythropoietin increases appropriately is called physiologic polycythemia. Physiologic
polycythemia occurs in individuals living at high altitudes (4275 to 5200 meters), where
oxygen availability is less than at sea level. Many athletes train at higher altitudes to take
advantage of this effect a legal form of blood doping. Actual polychthemia sufferers have
been known to use their condition as an athletic advantage for greater stamina.
Other causes of secondary polycythemia include smoking, renal or liver tumors, or heart
or lung diseases that result in hypoxia. Endocrine abnormalities, prominently including
pheochromocytoma and adrenal adenoma with Cushing's Syndrome, are also secondary
causes. Athletes and bodybuilders who abuse anabolic steroids or erythropoietin may develop
secondary polycythemia.
Relative polycythemia

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Glossary
Relative polycythemia is an apparent rise of the erythrocyte level in the blood; however, the
underlying cause is reduced blood plasma. Relative polycythemia is often caused by fluid
loss i.e. burns, dehydration and stress polycythemia.

6.5.8 Leukemia
Leukemia is a cancer of the blood or bone marrow characterized by an abnormal proliferation
of blood cells, usually white blood cells (leukocytes). It is part of the broad group of
diseases called hematological neoplasms. Damage to the bone marrow, by way of displacing
the normal marrow cells with increasing numbers of malignant cells, results in a lack of
blood platelets, which are important in the blood clotting process. This means people with
leukemia may become bruised, bleed excessively, or develop pin-prick bleeds (petechiae).
White blood cells, which are involved in fighting pathogens, may be suppressed or dysfunctional, putting the patient at the risk of developing infections. The red blood cell deficiency
leads to anaemia, which may cause dyspnea. All symptoms may also be attributable to
other diseases; for diagnosis, blood tests and a bone marrow biopsy are required.

6.6 Glossary
Albumin: a major blood protein responsible for the maintenance of osmotic (water) pressure
in the blood
Anemia: a deficiency of red blood cells or hemoglobin caused by lack of iron, folic acid or
vitamin B12 in the diet, or by red blood cell destruction; associated with decreased ability
of blood to carry oxygen
B-Cell: cell responsible for the distribution of antibodies
Basophil: this white blood cell enters damaged tissues and releases a histamine and other
chemicals that promote inflammation in the body to fight pathogens
Blood: the means and transport system of the body used in carrying elements - nutrition,
waste, heat - from one location in the body to another by way of blood vessels
Eosinophil: white blood cell that is involved in the immune response against parasitic
worms (such as tapeworms and roundworms). Named because it stains with the red dye
"eosin."
Factor V Leiden most common genetic hypercoagulability disorder.
Formed Elements: the red blood cells, white blood cells and platelets found in blood
Hematocrit: measurement of the % of red blood cells found in blood
Hemoglobin (Hb): iron-containing pigment in red blood cells that combines with and
transports oxygen
Hemophilia: genetic disorder in which the affected individual may have uncontrollable
bleeding; blood does not clot

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Hemostasis: the process by which blood flow is stopped; also describes the clotting of
blood
Lymphocytes: cells of the Lymphatic system, provide defense against specific pathogen or
toxins
Monocytes: The largest white blood cell. Becomes a macrophage when activated. Engulfs
pathogens and debris through phagocytosis, also involved in presenting antigens to B and T
lymphocytes.
Neutrophils: the most common white blood cell; they are phagocytic and engulf pathogens
or debris in the tissues; also release cytotoxic enzymes and chemicals to kill pathogens
NK-Cells: also known as "Natural Killer Cells", these T lymphocytes are responsible for
surveillance and detection of abnormal tissue cells; important in preventing cancer
Phagocytosis: process by which amoeboid-like cells engulf and ingest, and thereby destroy,
foreign matter or material
T-Cell: cells that mediate by coordinating the immune system and enter the peripheral
tissues. They can attack foreign cells directly and control the activities of other lymphocytes
,

6.7 Review Questions

Answers for these questions can be found here1
1.Taking aspirin every day can reduce the risk of heart disease because:
A) it is a powerful vasodilator
B) it blocks pain receptors in heart tissue
C) it stops ventricular fibrillation
D) it loosens plaque on arterial walls
E) it prevents platelet clumping
2. A hematocrit measures percentage of:
A) White blood cells
B) Plasma
C) Platelets
D) Red blood cells
3. Fred's blood type is O- and Ginger's is B+. Fred and Ginger have a son who is AB+.
What do you conclude?
A) If they have a second child Ginger needs to have RhoGam shot

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http://en.wikibooks.org/wiki/Human_Physiology/Appendix_1:_answers_to_review_
questions#Blood_Physiology

Review Questions
B) There is no risk to a second child, unless it has a negative blood type
C) If the child needs a blood transfusion Fred could provide it safely, but not Ginger
D) Fred is not the boys father
4. Which blood component plays the largest role in maintaining the osmotic pressure of
blood?
A) albumin
B) carbon dioxide
C) white blood cells
D) fibrinogen
E) globulins
5. If you hold your breath for one minute
A) The kidneys will increase sodium ion reabsorption
B) Hydrogen-ion concentration in the blood will increase
C) Your heart rate will greatly slow
D) Hemoglobin will bind to oxygen more strongly
6. Most of the carbon dioxide produced by tissues is transported to the lungs as:
A) Small gas bubbles in the plasma
B) Gas bound to hemoglobin in the red blood cells
C) Bicarbonate ions in the plasma
D) Gas bound to white blood cells and albumin
E) Gas transported through the lymphatic system
7. To prevent blood loss after a tissue injury, blood vessels first
A) Form a platelet plug
B) Form a clot
C) Initiate the coagulation cascade
D) Constrict and form barriers
8. You take a blood sample from a male cyclist at the end of a long race. The hematocrit is
60%. The most likely conclusion is:
A) This is within normal range for most adult males
B) This cyclist is anemic
C) This low of a hematocrit could indicate liver damage or leukemia
D) The cyclist is dehydrated
E) The cyclist has been taking pharmaceutical erythropoietin

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9. In a normal blood sample, which of the following cells will be the most abundant?
A) Neutrophils
B) Basophils
C) Eosinophils
D) Monocytes
E) Lymphocytes
10. A bag of donated blood does not clot because
A) There is not enough oxygen
B) It cannot dry out
C) It is kept refrigerated
D) There is no free calcium
E) All of the above
11. What is the primary function of bood?
A) Supply nutrients to tissues
B) Remove waste products
C) To keep your body at one consistent temperature
D) A and B
E) B and C
12. What is the main component of the Red blood cell?
A) Albumin
B) Globulins
C) Hemoglobin
D) Nucleus

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7 The Cardiovascular System

Figure 63

Model of a human heart

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The Cardiovascular System

7.1 Introduction
The heart is the life-giving, ever-beating muscle in your chest. From inside the womb until
death, the thump goes on. The heart for the average human will contract about 3 billion
times; never resting, never stopping to take a break except for a fraction of a second between
beats. At 80 years of age, a person's heart will continue to beat an average of 100,000 times
a day. Many believe that the heart is the first organ to become functional. Within weeks of
conception the heart starts its mission of supplying the body with nutrients even though the
embryo is no bigger than a capital letter on this page. The primary function of the heart is
to pump blood through the arteries, capillaries, and veins. There are an estimated 60,000
miles of vessels throughout an adult body. Blood transports oxygen, nutrients, disease
causing viruses, bacteria, hormones and has other important functions as well. The heart is
the pump that keeps blood circulating properly. Americans today have many options to
take care of their heart and circulatory system. Expanding medical technology has made it
much easier to do so. This chapter is dedicated to the heart and its many parts.

7.2 The Heart

The heart is a hollow, muscular organ about the size of a fist. It is responsible for pumping
blood through the blood vessels by repeated, rhythmic contractions. The heart is composed
of cardiac muscle, an involuntary muscle tissue that is found only within this organ. The
term "cardiac" (as in cardiology) means "related to the heart and comes from the Greek
word kardia, for "heart." It has a four-chambered, double pump and is located in the thoracic
cavity between the lungs. The cardiac muscle is self-exciting, meaning it has its own
conduction system. This is in contrast with skeletal muscle, which requires either conscious
or reflex nervous stimuli. The heart's rhythmic contractions occur spontaneously, although
the frequency or heart rate can be changed by nervous or hormonal influence such as exercise
or the perception of danger.

7.2.1 Endocardium
The endocardium is the innermost lining of the heart which consists of the endothelial cells
forming a smooth membrane in places, and a pocked and tribeculated surface in others
(mainly the ventricles, or lower pumping chambers).

7.2.2 Myocardium
The myocardium is the muscular tissue of the heart. The myocardium is composed of
specialized cardiac muscle cells with an ability not possessed by muscle tissue elsewhere in
the body. Cardiac muscle, like other muscles, can contract, but it can also conduct electricity,
like nerves. The blood to the myocardium is supplied by the coronary arteries. If these
arteries are occluded by atherosclerosis and/or thrombosis, this can lead to angina pectoris
or myocardial infarction due to ischemia (lack of oxygen). Failure of the heart to contract
properly (for various reasons) is termed heart failure, generally leading to fluid retention,

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edema, pulmonary edema, renal insufficiency, hepatomegaly, a shortened life expectancy and
decreased quality of life.

7.2.3 Epicardium
The outer most layer next to the myocardium is known as the Epicardium. This is the outer
layer after endocardium and myocardium that consists of a thin layer of connective tissue
and fat.

7.2.4 Pericardium
The pericardium is the thick, membranous sac that surrounds the heart. It protects and
lubricates the heart. There are two layers to the pericardium: the fibrous pericardium and
the serous pericardium. The serous pericardium is divided into two layers; in between these
two layers there is a space called the pericardial cavity.

7.2.5 Heart Chambers

The heart has four chambers, two atria and two ventricles. The atria are smaller with thin
walls, while the ventricles are larger and much stronger.
Atrium
There are two atria on either side of the heart. On the right side is the atrium that contains
blood which is poor in oxygen. The left atrium contains blood which has been oxygenated
and is ready to be sent to the body. The right atrium receives de-oxygenated blood from
the superior vena cava and inferior vena cava. The left atrium receives oxygenated blood
from the left and right pulmonary veins. Atria facilitate circulation primarily by allowing
uninterrupted venous flow to the heart, preventing the inertia of interrupted venous flow
that would otherwise occur at each ventricular systole.
Ventricles
The ventricle is a heart chamber which collects blood from an atrium and pumps it out of
the heart. There are two ventricles: the right ventricle pumps blood into the pulmonary
circulation for the lungs, and the left ventricle pumps blood into the systemic circulation
for the rest of the body. Ventricles have thicker walls than the atria, and thus can create
the higher blood pressure. Comparing the left and right ventricle, the left ventricle has
thicker walls because it needs to pump blood to the whole body. This leads to the common
misconception that the heart lies on the left side of the body.

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7.2.6 Septum
The interventricular septum (ventricular septum, or during development septum inferius) is
the thick wall separating the lower chambers (the ventricles) of the heart from one another.
The ventricular septum is directed backward and to the right, and is curved toward the
right ventricle. The greater portion of it is thick and muscular and constitutes the muscular
ventricular septum. Its upper and posterior part, which separates the aortic vestibule from
the lower part of the right atrium and upper part of the right ventricle, is thin and fibrous,
and is termed the membranous ventricular septum.

7.2.7 Valves
The two atrioventricular (AV) valves are one-way valves that ensure that blood flows from
the atria to the ventricles, and not the other way. The two semilunar (SL) valves are present
in the arteries leaving the heart; they prevent blood from flowing back into the ventricles.
The sound heard in a heart beat is the heart valves shutting. The right AV valve is also called
the tricuspid valve because it has three flaps. It is located between the right atrium and the
right ventricle. The tricuspid valve allows blood to flow from the right atrium into the right
ventricle when the heart is relaxed during diastole. When the heart begins to contract, the
heart enters a phase called systole, and the atrium pushes blood into the ventricle. Then, the
ventricle begins to contract and blood pressure inside the heart rises. When the ventricular
pressure exceeds the pressure in the atrium, the tricuspid valve snaps shut. The left AV
valve is also called the bicuspid valve because it has two flaps. It is also known as the mitral
valve due to the resemblance to a bishop's mitre (liturgical headdress). This valve prevents
blood in the left ventricle from flowing into the left atrium. As it is on the left side of the
heart, it must withstand a great deal of strain and pressure; this is why it is made of only
two cusps, as a simpler mechanism entails a reduced risk of malfunction. There are two
remaining valves called the Semilunar Valves. They have flaps that resemble half moons.
The pulmonary semilunar valve lies between the right ventricle and the pulmonary trunk.
The aortic semilunar valve is located between the ventricle and the aorta.

7.2.8 Subvalvular Apparatus

The chordae tendinae are attached to papillary muscles that cause tension to better hold
the valve. Together, the papillary muscles and the chordae tendinae are known as the
subvalvular apparatus. The function of the subvalvular apparatus is to keep the valves from
prolapsing into the atria when they close. The subvalvular apparatus have no effect on the
opening and closing of the valves. This is caused entirely by the pressure gradient across
the valve.

7.2.9 Complications with the Heart

The most common congenital abnormality of the heart is the bicuspid aortic valve. In this
condition, instead of three cusps, the aortic valve has two cusps. This condition is often
undiagnosed until the person develops calcific aortic stenosis. Aortic stenosis occurs in this
condition usually in patients in their 40s or 50s, an average of 10 years earlier than in people

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with normal aortic valves. Another common complication of rheumatic fever is thickening
and stenosis (partial blocking) of the mitral valve. For patients who have had rheumatic
fever dentists are advised to prophylactally administer antibiotics prior to dental work to
prevent bacterial endocarditis that occurs when bacteria from the teeth enter the circulation
and attach to damaged heart valves.
The aortic valve is a semilunar valve, but its called bicuspid because of its regular three
"cusps" or "semilunar" valves, and is not to be confused with the left atrioventricular valve,
which is more commonly called the mitral valve, and is one of the two cuspidal valves.

7.3 Passage of Blood Through the Heart

Figure 64

Diagram of the human heart

While it is convenient to describe the flow of the blood through the right side of the heart
and then through the left side, it is important to realize that both atria contract at the same
time and that both ventricles contract at the same time. The heart works as two pumps,
one on the right and one on the left that works simultaneously. The right pump pumps
the blood to the lungs or the pulmonary circulation at the same time that the left pump
pumps blood to the rest of the body or the systemic circulation. Venous blood from systemic
circulation (deoxygenated) enters the right atrium through the superior and inferior vena
cava. The right atrium contracts and forces the blood through the tricuspid valve (right

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The Cardiovascular System

atrioventricular valve) and into the right ventricles. The right ventricles contract and force
the blood through the pulmonary semilunar valve into the pulmonary trunk and out the
pulmonary artery. This takes the blood to the lungs where the blood releases carbon dioxide
and receives a new supply of oxygen. The new blood is carried in the pulmonary veins that
take it to the left atrium. The left atrium then contracts and forces blood through the left
atrioventricular, bicuspid, or mitral, valve into the left ventricle. The left ventricle contracts
forcing blood through the aortic semilunar valve into the ascending aorta. It then branches
to arteries carrying oxygen rich blood to all parts of the body.

7.3.1 Blood Flow After the Heart

Aorta-Arteries-Arterioles-Capillaries-Venules-Veins-Vena Cava

7.3.2 Blood Flow Through Capillaries

From the arterioles, the blood then enters one or more capillaries. The walls of capillaries
are so thin and fragile that blood cells can only pass in single file. Inside the capillaries,
exchange of oxygen and carbon dioxide takes place. Red blood cells inside the capillary
releases their oxygen which passes through the wall and into the surrounding tissue. The
tissue then releases waste, such as carbon dioxide, which then passes through the wall and
into the red blood cells.

7.4 The Circulatory System

The circulatory system is extremely important in sustaining life. Its proper functioning
is responsible for the delivery of oxygen and nutrients to all cells, as well as the removal
of carbon dioxide, waste products, maintenance of optimum pH, and the mobility of the
elements, proteins and cells, of the immune system. In developed countries, the two leading
causes of death, myocardial infarction and stroke are each direct results of an arterial system
that has been slowly and progressively compromised by years of deterioration.

7.4.1 Arteries
Arteries are muscular blood vessels that carry blood away from the heart, oxygenated and
deoxygenated blood . The pulmonary arteries will carry deoxygenated blood to the lungs
and the sytemic arteries will carry oxygenated blood to the rest of the body. Arteries have
a thick wall that consists of three layers. The inside layer is called the endothelium, the
middle layer is mostly smooth muscle and the outside layer is connective tissue. The artery
walls are thick so that when blood enters under pressure the walls can expand.
Arterioles
An arteriole is a small artery that extends and leads to capillaries. Arterioles have thick
smooth muscular walls. These smooth muscles are able to contract (causing vessel con-

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The Circulatory System

striction) and relax (causing vessel dilation). This contracting and relaxing affects blood
pressure; the higher number of vessels dilated, the lower blood pressure will be. Arterioles
are just visible to the naked eye.

7.4.2 Capillaries

Figure 65

Capillaries are the smallest of a bodys vessels; they connect arteries and veins, and most
closely interact with tissues. They are very prevalent in the body; total surface area is about
6,300 square meters. Because of this, no cell is very far from a capillary, no more than
50 micrometers away. The walls of capillaries are composed of a single layer of cells, the
endothelium, which is the inner lining of all the vessels. This layer is so thin that molecules
such as oxygen, water and lipids can pass through them by diffusion and enter the tissues.
Waste products such as carbon dioxide and urea can diffuse back into the blood to be carried
away for removal from the body.
The "capillary bed" is the network of capillaries present throughout the body. These beds
are able to be opened and closed at any given time, according to need. This process is
called autoregulation and capillary beds usually carry no more than 25% of the amount of
blood it could hold at any time. The more metabolically active the cells, the more capillaries
it will require to supply nutrients.

7.4.3 Veins
Veins carry blood to the heart. The pulmonary veins will carry oxygenated blood to the
heart awhile the systemic veins will carry deoxygenated to the heart. Most of the blood
volume is found in the venous system; about 70% at any given time. The veins outer walls
have the same three layers as the arteries, differing only because there is a lack of smooth
muscle in the inner layer and less connective tissue on the outer layer. Veins have low blood

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The Cardiovascular System

pressure compared to arteries and need the help of skeletal muscles to bring blood back to
the heart. Most veins have one-way valves called venous valves to prevent backflow caused
by gravity. They also have a thick collagen outer layer, which helps maintain blood pressure
and stop blood pooling. If a person is standing still for long periods or is bedridden, blood
can accumulates in veins and can cause varicose veins. The hollow internal cavity in which
the blood flows is called the lumen. A muscular layer allows veins to contract, which puts
more blood into circulation. Veins are used medically as points of access to the blood stream,
permitting the withdrawal of blood specimens (venipuncture) for testing purposes, and
enabling the infusion of fluid, electrolytes, nutrition, and medications (intravenous delivery).

7.4.4 Venules
A venule is a small vein that allows deoxygenated blood to return from the capillary beds
to the larger blood veins, except in the pulmonary circuit were the blood is oxygenated.
Venules have three layers; they have the same makeup as arteries with less smooth muscle,
making them thinner.

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The Cardiovascular Pathways

7.5 The Cardiovascular Pathways

Figure 66

Human circulatory system. Arteries are shown in red, veins blue.

The double circulatory system of blood flow refers to the separate systems of pulmonary
circulation and the systemic circulation in amphibians, birds and mammals (including
humans.) In contrast, fishes have a single circulation system. For instance, the adult human
heart consists of two separated pumps, the right side with the right atrium and ventricle
(which pumps deoxygenated blood into the pulmonary circulation), and the left side with
the left atrium and ventricle (which pumps oxygenated blood into the systemic circulation).
Blood in one circuit has to go through the heart to enter the other circuit. Blood circulates

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The Cardiovascular System

through the body two to three times every minute. In one day, the blood travels a total of
19,000 km (12,000 miles), or four times the distance across the U.S. from coast to coast.

7.5.1 The Pulmonary Circuit

In the pulmonary circuit, blood is pumped to the lungs from the right ventricle of the heart.
It is carried to the lungs via pulmonary arteries. At lungs, oxygen in the alveolae diffuses to
the capillaries surrounding the alveolae and carbon dioxide inside the blood diffuses to the
alveolae. As a result, blood is oxygenated which is then carried to the heart's left half -to
the left atrium via pulmonary veins. Oxygen rich blood is prepared for the whole organs
and tissues of the body. This is important because mitochondria inside the cells should use
oxygen to produce energy from the organic compounds.

7.5.2 The Systemic Circuit

The systemic circuit supplies oxygenated blood to the organ system. Oxygenated blood from
the lungs is returned to the left atrium, then the ventricle contracts and pumps blood into
the aorta. Systemic arteries split from the aorta and direct blood into the capillaries. Cells
consume the oxygen and nutrients and add carbon dioxide, wastes, enzymes and hormones.
The veins drain the deoxygenated blood from the capillaries and return the blood to the
right atrium.

7.5.3 Aorta
The aorta is the largest of the arteries in the systemic circuit. The blood is pumped from
the left ventricle into the aorta and from there it branches to all parts of the body. The
aorta is an elastic artery, and as such is able to distend. When the left ventricle contracts to
force blood into the aorta, the aorta expands. This stretching gives the potential energy that
will help maintain blood pressure during diastole, as during this time the aorta contracts
passively.

7.5.4 Superior Venae Cavae

The superior vena cava (SVC) is a large but short vein that carries de-oxygenated blood
from the upper half of the body to the heart's right atrium. It is formed by the left and
right brachiocephalic veins (also referred to as the innominate veins) which receive blood
from the upper limbs and the head and neck. The azygous vein (which receives blood from
the ribcage) joins it just before it enters the right atrium.

7.5.5 Inferior Venae Cavae

The inferior vena cava (or IVC) is a large vein that carries de-oxygenated blood from the
lower half of the body into the heart. It is formed by the left and right common iliac veins

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The Cardiovascular Pathways

and transports blood to the right atrium of the heart. It is posterior to the abdominal cavity,
and runs along side of the vertebral column on its right side.

7.5.6 Coronary Arteries

Figure 67

Heart showing the Coronary Arteries

Heart showing the Coronary Arteries The coronary circulation consists of the blood vessels
that supply blood to, and remove blood from, the heart muscle itself. Although blood fills
the chambers of the heart, the muscle tissue of the heart, or myocardium, is so thick that it
requires coronary blood vessels to deliver blood deep into the myocardium. The vessels that
supply blood high in oxygen to the myocardium are known as coronary arteries. The vessels
that remove the deoxygenated blood from the heart muscle are known as cardiac veins. The
coronary arteries that run on the surface of the heart are called epicardial coronary arteries.
These arteries, when healthy, are capable of auto regulation to maintain coronary blood flow
at levels appropriate to the needs of the heart muscle. These relatively narrow vessels are
commonly affected by atherosclerosis and can become blocked, causing angina or a heart
attack. The coronary arteries are classified as "end circulation", since they represent the
only source of blood supply to the myocardium: there is very little redundant blood supply,

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The Cardiovascular System

which is why blockage of these vessels can be so critical. In general there are two main
coronary arteries, the left and right. Right coronary artery Left coronary artery Both
of these arteries originate from the beginning (root) of the aorta, immediately above the
aortic valve. As discussed below, the left coronary artery originates from the left aortic
sinus, while the right coronary artery originates from the right aortic sinus. Four percent of
people have a third, the posterior coronary artery. In rare cases, a patient will have one
coronary artery that runs around the root of the aorta.

7.5.7 Hepatic Veins

In human anatomy, the hepatic veins are the blood vessels that drain de-oxygenated blood
from the liver and blood cleaned by the liver (from the stomach, pancreas, small intestine
and colon) into the inferior vena cava. They arise from the substance of the liver, more
specifically the central vein of the liver lobule. They can be differentiated into two groups,
the upper group and lower group. The upper group of three typically arises from the
posterior aspect of the liver and drain the quadrate lobe and left lobe. The lower group rise
from the right lobe and caudate lobe, are variable in number, and are typically smaller than
those in the upper group. None of the hepatic veins have valves.

7.6 Cardiac Cycle

Cardiac cycle is the term used to describe the relaxation and contraction that occur, as
a heart works to pump blood through the body. Heart rate is a term used to describe
the frequency of the cardiac cycle. It is considered one of the four vital signs. Usually it
is calculated as the number of contractions (heart beats) of the heart in one minute and
expressed as "beats per minute" (bpm). When resting, the adult human heart beats at about
70 bpm (males) and 75 bpm (females), but this rate varies between people. However, the
reference range is nominally between 60 bpm (if less termed bradycardia) and 100 bpm (if
greater, termed tachycardia). Resting heart rates can be significantly lower in athletes, and
significantly higher in the obese. The body can increase the heart rate in response to a wide
variety of conditions in order to increase the cardiac output (the amount of blood ejected by
the heart per unit time). Exercise, environmental stressors or psychological stress can cause
the heart rate to increase above the resting rate. The pulse is the most straightforward way
of measuring the heart rate, but it can be deceptive when some strokes do not lead to much
cardiac output. In these cases (as happens in some arrhythmias), the heart rate may be
considerably higher than the pulse. Every single 'beat' of the heart involves three major
stages: atrial systole, ventricular systole and complete cardiac diastole. Throughout the
cardiac cycle, the blood pressure increases and decreases. As ventricles contract the pressure
rise, causing the AV valves to slam shut.

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Cardiac Cycle

7.6.1 Systole

Figure 68

The heart in the systole phase.

The heart in the systole phase. Systole, or contraction, of the heart is initiated by the
electrical cells of the sinoatrial node, which is the heart's natural pacemaker. These cells are
activated spontaneously by depolarization of their membranes beyond a certain threshold
for excitation. At this point, voltage-gated calcium channels on the cell membrane open
and allow calcium ions to pass through, into the sarcoplasm, or interior, of the muscle
cell. Some calcium ions bind to receptors on the sarcoplasmic reticulum causing an influx
of calcium ions into the sarcoplasm. The calcium ions bind to the troponin, causing a
conformation change, breaking the bond between the protein tropomyosin, to which the
troponin is attached, and the myosin binding sites. This allows the myosin heads to bind
to the myosin binding sites on the actin protein filament and contraction results as the
myosin heads draw the actin filaments along, are bound by ATP, causing them to release
the actin, and return to their original position, breaking down the ATP into ADP and a
phosphate group. The action potential spreads via the passage of sodium ions through the
gap junctions that connect the sarcoplasm of adjacent myocardial cells. Norepinephrine
(noradrenaline) is released by the terminal boutons of depolarized sympathetic fibers, at the
sinoatrial and atrioventricular nodes. Norepinephrine diffuses across the synaptic cleft binds
to the 1-adrenoreceptors G-protein linked receptors, consisting of seven transmembrane
domains shifting their equilibrium towards the active state. The receptor changes its
conformation and mechanically activates the G-protein which is released. The G-protein is
involved in the production of adenosine 3',5'-cyclic monophosphate (cAMP) from adenosine
triphosphate (ATP) and this in turn activates the protein kinase (-adrenoreceptor kinase).
-adrenoreceptor kinase phosphorylates the calcium ion channels in the sarcolemma, so that

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calcium ion influx is increased when they are activated by the appropriate transmembrane
voltage. This will of course, cause more of the calcium receptors in the sarcoplasmic reticulum
to be activated, creating a larger flow of calcium ions into the sarcoplasm. More troponin
will be bound and more myosin binding sites cleared [of tropomyosin] so that more myosin
heads can be recruited for the contraction and a greater force and speed of contraction
results. [Phosphodiesterase catalyses the decomposition of cAMP to AMP so that it is no
longer able to activate the protein kinase. AMP will of course, go on to be phosphorylated
to ATP and may be recycled.] Noradrenaline also affects the atrioventricular node, reducing
the delay before continuing conduction of the action potential via the bundle of HIS.

7.6.2 Diastole

Figure 69

The heart in the diastole phase.

The heart in the diastole phase. Cardiac Diastole is the period of time when the heart relaxes
after contraction in preparation for refilling with circulating blood. Ventricular diastole is
when the ventricles are relaxing, while atrial diastole is when the atria are relaxing. Together
they are known as complete cardiac diastole. It should be noted that even this relaxation
is an active, energy-spending process. During ventricular diastole, the pressure in the (left
and right) ventricles drops from the peak that it reaches in systole. When the pressure in
the left ventricle drops to below the pressure in the left atrium, the mitral valve opens, and
the left ventricle fills with blood that was accumulating in the left atrium. Likewise, when
the pressure in the right ventricle drops below that in the right atrium, the tricuspid valve
opens and the right ventricle fills with blood that was in the right atrium

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The Heart's Electrical Conduction System

7.6.3 "Lub-Dub"
The first heart tone, or S1, "Lub" is caused by the closure of the atrioventricular valves,
mitral and tricuspid, at the beginning of ventricular contraction, or systole. When the
pressure in the ventricles rises above the pressure in the atria, these valves close to prevent
regurgitation of blood from the ventricles into the atria. The second heart tone, or S2 (A2
and P2), "Dub" is caused by the closure of the aortic valve and pulmonic valve at the end
of ventricular systole. As the left ventricle empties, its pressure falls below the pressure in
the aorta, and the aortic valve closes. Similarly, as the pressure in the right ventricle falls
below the pressure in the pulmonary artery, the pulmonic valve closes. During inspiration,
negative intrathoracic pressure causes increased blood return into the right side of the heart.
The increased blood volume in the right ventricle causes the pulmonic valve to stay open
longer during ventricular systole. This causes an increased delay in the P2 component of S2.
During expiration, the positive intrathoracic pressure causes decreased blood return to the
right side of the heart. The reduced volume in the right ventricle allows the pulmonic valve
to close earlier at the end of ventricular systole, causing P2 to occur earlier, and "closer" to
A2. It is physiological to hear the splitting of the second heart tone by younger people and
during inspiration. During expiration normally the interval between the two components
shortens and the tone becomes merged.

7.7 The Heart's Electrical Conduction System

The heart is primarily made up of muscle tissue. A network of nerve fibers coordinates
the contraction and relaxation of the cardiac muscle tissue to obtain an efficient, wave-like
pumping action of the heart
How Stuff Works (The Heart)1
Control of Heartbeat
The heart contains two cardiac pacemakers that spontaneously cause the heart to beat.
These can be controlled by the autonomic nervous system and circulating adrenaline. If the
cardiac muscles just contracted and relaxed randomly at a natural rhythm the cycle would
become disordered and the heart would become unable to carry on its function of being
a pump. Sometimes when the heart undergoes great damage to one part of the cardiac
muscle or the person incurs an electric shock, the cardiac cycle can become uncoordinated
and chaotic. Some parts of the heart will contract whilst others will relax so that instead
of contracting and relaxing as a whole, the heart will flutter abnormally. This is called
fibrillation and can be fatal if not treated within 60 seconds.

http://health.howstuffworks.com/adam-200080.htm

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Figure 70 Schematic representation of the sinoatrial node and the

atrioventricular bundle of His. The location of the SA node is shown
in blue. The bundle, represented in red, originates near the orifice of
the coronary sinus, undergoes slight enlargement to form the AV
node. The AV node tapers down into the bundle of HIS, which
passes into the ventricular septum and divides into two bundle
branches, the left and right bundles. The ultimate distribution
cannot be completely shown in this diagram.
SA Node
The sinoatrial node (abbreviated SA node or SAN, also called the sinus node) is the impulse
generating (pacemaker) tissue located in the right atrium of the heart. Although all of the
heart's cells possess the ability to generate the electrical impulses (or action potentials) that
trigger cardiac contraction, the sinoatrial node is what normally initiates it, simply because
it generates impulses slightly faster than the other areas with pacemaker potential. Because
cardiac myocytes, like all nerve cells, have refractory periods following contraction during

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which additional contractions cannot be triggered, their pacemaker potential is overridden
by the sinoatrial node. The SA node emits a new impulse before either the AV or purkinje
fibers reach threshold. The sinoatrial node (SA node) is a group of cells positioned on
the wall of the right atrium, near the entrance of the superior vena cava. These cells are
modified cardiac myocytes. They possess some contractile filaments, though they do not
contract. Cells in the SA node will naturally discharge (create action potentials) at about
70-80 times/minute. Because the sinoatrial node is responsible for the rest of the heart's
electrical activity, it is sometimes called the primary pacemaker. If the SA node doesn't
function, or the impulse generated in the SA node is blocked before it travels down the
electrical conduction system, a group of cells further down the heart will become the heart's
pacemaker. These cells form the atrioventricular node (AV node), which is an area between
the right atrium and ventricle, within the atrial septum. The impulses from the AV node will
maintain a slower heart rate (about 40-60 beats per a minute). When there is a pathology in
the AV node or purkinje fibers, an ectopic pacemaker can occur in different parts of the heart.
The ectopic pacemaker typically discharges faster than the SA node and causes an abnormal
sequence of contraction. The SA node is richly innervated by vagal and sympathetic fibers.
This makes the SA node susceptible to autonomic influences. Stimulation of the vagus
nerve causes decrease in the SA node rate (thereby causing decrease in the heart rate).
Stimulation via sympathetic fibers causes increase in the SA node rate (thereby increasing
the heart rate). The sympathetic nerves are distributed to all parts of the heart, especially
in ventricular muscles. The parasympathetic nerves mainly control SA and AV nodes, some
atrial muscle and ventricular muscle. Parasympathetic stimulation from the vagal nerves
decreases the rate of the AV node by causing the release of acetylcholine at vagal endings
which in turn increases the K+ permeability of the cardiac muscle fiber. Vagal stimulation
can block transmission through AV junction or stop SA node contraction which is called
"ventricular escape." When this happens, the purkinje fibers in the AV bundle develops a
rhythm of their own. In the majority of patients, the SA node receives blood from the right
coronary artery, meaning that a myocardial infarction occluding it will cause ischemia in
the SA node unless there is a sufficiently good anastomosis from the left coronary artery. If
not, death of the affected cells will stop the SA node from triggering the heartbeat
AV Node
The atrioventricular node (abbreviated AV node) is the tissue between the atria and the
ventricles of the heart, which conducts the normal electrical impulse from the atria to
the ventricles. The AV node receives two inputs from the atria: posteriorly via the crista
terminalis, and anteriorly via the interatrial septum. [1] An important property that is
unique to the AV node is decremental conduction. This is the property of the AV node that
prevents rapid conduction to the ventricle in cases of rapid atrial rhythms, such as atrial
fibrillation or atrial flutter. The atrioventricular node delays impulses for 0.1 second before
spreading to the ventricle walls. The reason it is so important to delay the cardiac impulse
is to ensure that the atria are empty completely before the ventricles contract (Campbell et
al., 2002). The blood supply of the AV node is from a branch of the right coronary artery in
85% to 90% of individuals, and from a branch of the left circumflex artery in 10% to 15% of
individuals. In certain types of supraventricular tachycardia, a person could have two AV
Nodes; this will cause a loop in electrical current and uncontrollably-rapid heart beat. When
this electricity catches up with itself, it will dissipate and return to normal heart-beat speed.

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AV Bundle
The bundle of HIS is a collection of heart muscle cells specialized for electrical conduction
that transmits the electrical impulses from the AV node (located between the atria and the
ventricles) to the point of the apex of the fascicular branches. The fascicular branches then
lead to the Purkinje fibers which innervate the ventricles, causing the cardiac muscle of the
ventricles to contract at a paced interval. These specialized muscle fibers in the heart were
named after the Swiss cardiologist Wilhelm His, Jr., who discovered them in 1893. Cardiac
muscle is very specialized, as it is the only type of muscle that has an internal rhythm;
i.e., it is myogenic which means that it can naturally contract and relax without receiving
electrical impulses from nerves. When a cell of cardiac muscle is placed next to another,
they will beat in unison. The fibers of the Bundle of HIS allow electrical conduction to
occur more easily and quickly than typical cardiac muscle. They are an important part of
the electrical conduction system of the heart as they transmit the impulse from the AV
node (the ventricular pacemaker) to the rest of the heart. The bundle of HIS branches into
the three bundle branches: the right left anterior and left posterior bundle branches that
run along the intraventricular septum. The bundles give rise to thin filaments known as
Purkinje fibers. These fibers distribute the impulse to the ventricular muscle. Together,
the bundle branches and purkinje network comprise the ventricular conduction system. It
takes about 0.03-0.04s for the impulse to travel from the bundle of HIS to the ventricular
muscle. It is extremely important for these nodes to exist as they ensure the correct control
and co-ordination of the heart and cardiac cycle and make sure all the contractions remain
within the correct sequence and in sync.
Purkinje Fibers
Purkinje fibers (or Purkyne tissue) are located in the inner ventricular walls of the heart,
just beneath the endocardium. These fibers are specialized myocardial fibers that conduct
an electrical stimulus or impulse that enables the heart to contract in a coordinated fashion.
Purkinje fibers work with the sinoatrial node (SA node) and the atrioventricular node (AV
node) to control the heart rate. During the ventricular contraction portion of the cardiac
cycle, the Purkinje fibers carry the contraction impulse from the left and right bundle
branches to the myocardium of the ventricles. This causes the muscle tissue of the ventricles
to contract and force blood out of the heart either to the pulmonary circulation (from the
right ventricle) or to the systemic circulation (from the left ventricle). They were discovered
in 1839 by Jan Evangelista Purkinje, who gave them his name.
Pacemaker
The contractions of the heart are controlled by electrical impulses, these fire at a rate which
controls the beat of the heart. The cells that create these rhythmical impulses are called
pacemaker cells, and they directly control the heart rate. Artificial devices also called
pacemakers can be used after damage to the body's intrinsic conduction system to produce
these impulses synthetically.

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The ECG
Fibrillation
Fibrillation is when the heart flutters abnormally. This can be detected by an electrocardiogram which measures the waves of excitation passing through the heart and plotting
a graph of potential difference (voltage) against time. If the heart and cardiac cycle is
functioning properly the electrocardiogram shows a regular, repeating pattern. However
if there is fibrillation there will be no apparent pattern, either in the much more common
'Atrial Fibrillation', or the less likely but much more dangerous 'Ventricular Fibrillation'. In
a hospital during VF the monitor would make a sound and alert the doctors to treat the
fibrillation by passing a huge current through the chest wall and shocking the heart out of
its fibrillation. This causes the cardiac muscle to stop completely for 5 seconds and when it
begins to beat again the cardiac cycle would have resumed to normal and the heart will be
beating in a controlled manner again. Fibrillation is an example of "circus movement" of
impulses through the heart muscle.
Circus movement occurs when an impulse begins in one part of the heart muscle and spreads
in a circuitous pathway through the heart then returns to the originally excited muscle and
"re-enters" it to stimulate it once more. The signal never stops. A cause of circus movement
is long length pathway in which the muscle is no longer in a refractatory state when the
stimulus returns to it. A "flutter" is a circus movement in coordinated, low frequency waves
that cause rapid heart rate. If the Bundle of HIS is blocked, it will result in dissociation
between the activity of the atria and that of the ventricles, otherwise called a third degree
heart block. The other cause of a third degree block would be a block of the right, left
anterior, and left posterior bundle branches. A third degree block is very serious medical
condition that will most likely require an artificial pacemaker.

7.8 The ECG

E.C.G stands for Electrocardiogram and represents the electrophysiology of the heart.
Cardiac electrophysiology is the science of the mechanisms, functions, and performance of
the electrical activities of specific regions of the heart. The ECG is the recording of the
heart's electrical activity as a graph. The graph can show the heart's rate and rhythm, it
can detect enlargement of the heart, decreased blood flow, or the presence of current or past
heart attacks. ECG's are inexpensive, Non-invasive, quick, and painless. Depending on the
results, the patients medical history, and a physical exam; further tests or a combination of
medications and lifestyle changes may be ordered.
How To Read An ECG
ECG Waveform

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Figure 71

P
P wave- indicates that the atria are
electrically stimulated (depolarized) to
pump blood into the ventricles.
QRS
QRS complex- indicates that the ventricles are electrically stimulated (depolarized) to pump blood out.
ST
ST segment- indicates the amount of
time from the end of the contraction of
the ventricles to the beginning of the T
wave.
T
T wave- indicates the recovery period
(repolarization) of the ventricles.
U
U wave- rarely seen, and thought to
possibly be the repolarization of the
papillary muscles

7.8.1 Cardiac Muscle Contraction

After an action potential excites the plasma membrane of the cardiac muscle cell the
contraction is due to an increase in the cytoplasmic concentration of Calcium ions. Similar
to skeletal muscle, the release of Ca+ ions from the sarcoplasmic reticulum binds to troponin
which allows actin to bind with myosin. The difference between skeletal muscle and cardiac
muscle is that when the action potential opens voltage gated calcium ion channels in the
T-tubules. The increase in cytosolic calcium causes calcium ions to bind to receptors on the
surface of the sarcoplasmic reticulum. The binding of calcium ions to these receptors causes
the opening of more calcium ion channels in the SR membrane. Calcium ions then rush
out of the SR and bind to troponin and allow the myosin and actin to bind together which
causes contraction. This sequence is called calcium-induced calcium release. Contraction
ends when the level of cytosolic calcium returns to normal resting levels.

7.8.2 Blood Pressure

Blood pressure is the pressure exerted by the blood on the walls of the blood vessels. Unless
indicated otherwise, blood pressure refers to systemic arterial blood pressure, i.e., the

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pressure in the large arteries delivering blood to body parts other than the lungs, such
as the brachial artery (in the arm). The pressure of the blood in other vessels is lower
than the arterial pressure. Blood pressure values are universally stated in millimeters of
mercury (mmHg). The systolic pressure is defined as the peak pressure in the arteries during
the cardiac cycle; the diastolic pressure is the lowest pressure (at the resting phase of the
cardiac cycle). The mean arterial pressure and pulse pressure are other important quantities.
Typical values for a resting, healthy adult are approximately 120 mmHg systolic and 80mm
Hg diastolic (written as 120/80 mmHg), with individual variations. These measures of
blood pressure are not static, but undergo natural variations from one heartbeat to another,
and throughout the day (in a circadian rhythm); they also change in response to stress,
nutritional factors, drugs, or disease.
Systolic Pressure
Systolic Pressure is the highest when the blood is being pumped out of the left ventricle
into the aorta during ventricular systole. The average high during systole is 120 mmHg.
Diastolic Pressure
Diastolic blood pressure lowers steadily to an average low of 80 mmHg during ventricular
diastole.

7.9 Cardiovascular Disease

Cardiovascular disease refers to the class of diseases that involve the heart and/or blood
vessels (arteries and veins). While the term technically refers to any disease that affects the
cardiovascular system, it is usually used to refer to those related to atherosclerosis (arterial
disease). These conditions have similar causes, mechanisms, and treatments. Over 50 million
Americans have cardiovascular problems, and most other Western countries face high and
increasing rates of cardiovascular disease. It is the number 1 cause of death and disability
in the United States and most European countries. By the time that heart problems are
detected, the underlying cause (atherosclerosis) is usually quite advanced, having progressed
for decades. There is therefore increased emphasis on preventing atherosclerosis by modifying
risk factors, such as healthy eating, exercise and avoidance of smoking.
Hypertension
Hypertension or high blood pressure is a medical condition wherein the blood pressure is
chronically elevated. Hypertension is defined by some authors as systolic pressure over 130
and diastolic over 85 mmHg. 2 Hypertension often has an insidious or un-noticed onset and
is sometimes called the silent killer because strecthing of the arteries causes microscopic

Tortora, G. & Grabowski, S. (2000)Principles of anatomy and physiology. Ninth Edition. Wiley page
733.

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tears in the arterial wall and accelerates degenrative changes. Persistent hypertension is one
of the risk factors for strokes, heart attacks, heart failure and arterial aneurysm, and is a
leading cause of chronic renal failure
Atherosclerosis

Figure 72 Severe atherosclerosis of the aortaa .

Autopsyb specimen.
a
b

http://en.wikibooks.org/wiki/aorta
http://en.wikibooks.org/wiki/Autopsy

Atherosclerosis is a disease affecting the arterial blood vessel. It is commonly referred to as

a "hardening" or "furring" of the arteries. It is caused by the formation of multiple plaques
within the arteries. Arteriosclerosis ("hardening of the artery") results from a deposition
of tough, rigid collagen inside the vessel wall and around the atheroma. This increases
the stiffness, decreases the elasticity of the artery wall. Atherosclerosis typically begins in
early adolescence, is usually found in most major arteries, and yet is asymptomatic and

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not detected by most diagnostic methods during life. It most commonly becomes seriously
symptomatic when interfering with the coronary circulation supplying the heart or cerebral
circulation supplying the brain, and is considered the most important underlying cause of
strokes, heart attacks, various heart diseases including congestive heart failure and most
cardiovascular diseases in general.
Plaque
Plaque Atheroma or commonly known as plaque is an abnormal inflammatory accumulation
of macrophage white blood cells within the walls of arteries.
Circulatory Shock
Circulatory Shock is a severe condition that results from reduced blood circulation.
Thrombus
A thrombus, or blood clot, is the final product of the blood coagulation step in hemostasis.
It is achieved via the aggregation of platelets that form a platelet plug, and the activation
of the humoral coagulation system (i.e. clotting factors). A thrombus is physiologic in cases
of injury, but pathologic in case of thrombosis.
Preventing blood clots reduces the risk of stroke, heart attack and pulmonary embolism.
Heparin and warfarin are often used to inhibit the formation and growth of existing blood
clots, thereby allowing the body to shrink and dissolve the blood clots through normal
methods.
Embolism
An embolism occurs when an object (the embolus) migrates from one part of the body
(through circulation) and causes a blockage (occlusion) of a blood vessel in another part
of the body. Blood clots form the most common embolic material by far: other possible
embolic materials include fat globules (a fat embolism), air bubbles (an air embolism), septic
emboli (containing pus and bacteria), or amniotic fluid.
Stroke
A stroke, also known as cerebrovascular accident (CVA), is an acute neurological injury
whereby the blood supply to a part of the brain is interrupted. Strokes can be classified into
two major categories: ischemic and hemorrhagic. 80% of strokes are due to ischemia.
Ischemic Stroke: In ischemic stroke, which occurs in approximately 85-90% of strokes,
a blood vessel becomes occluded and the blood supply to part of the brain is totally or
partially blocked. Ischemic stroke is commonly divided into thrombotic stroke, embolic
stroke, systemic hypoperfusion (Watershed or Border Zone stroke), or venous thrombosis

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Hemorrhagic Stroke: A hemorrhagic stroke, or cerebral hemorrhage, is a form of stroke
that occurs when a blood vessel in the brain ruptures or bleeds. Like ischemic strokes,
hemorrhagic strokes interrupt the brain's blood supply because the bleeding vessel can
no longer carry the blood to its target tissue. In addition, blood irritates brain tissue,
disrupting the delicate chemical balance, and, if the bleeding continues, it can cause
increased intracranial pressure which physically impinges on brain tissue and restricts
blood flow into the brain. In this respect, hemorrhagic strokes are more dangerous than
their more common counterpart, ischemic strokes. There are two types of hemorrhagic
stroke: intracerebral hemorrhage, and subarachnoid hemorrhage.
The term "brain attack" is starting to come into use in the United States for stroke, just
as the term "heart attack" is used for myocardial infarction, where a cutoff of blood causes
necrosis to the tissue of the heart. Many hospitals have "brain attack" teams within their
neurology departments specifically for swift treatment of stroke. If symptoms of stroke
are detected at early on-set, special "clot busting" drugs may be administered. These clot
busters will dissolve clots before they can cause tissue death and restore normal circulation.
One of the initial drugs used to dissolve clots was streptokinase, although its use creates
a possibility of clot destruction throughout the entire body, leading to serious hemorrhage.
There are newer, third generation thrombolytics that are safer.
Heart Attack
w:Heart Attack3
Acute myocardial infarction (AMI or MI), commonly known as a heart attack, A heart
attack occurs when the supply of blood and oxygen to an area of heart muscle is blocked,
usually by a clot in a coronary artery. Often, this blockage leads to arrhythmias (irregular
heartbeat or rhythm) that cause a severe decrease in the pumping function of the heart
and may bring about sudden death. If the blockage is not treated within a few hours, the
affected heart muscle will die and be replaced by scar tissue. It is the leading cause of death
for both men and women all over the world
Angina Pectoris
Angina Pectoris is chest pain due to ischemia (a lack of blood and hence oxygen supply) of
the heart muscle, generally due to obstruction or spasm of the coronary arteries (the heart's
blood vessels).
Coronary Bypass
Coronary artery bypass surgery, coronary artery bypass graft surgery and heart bypass
are surgical procedures performed on patients with coronary artery disease for the relief of
angina and possible improved heart muscle function. Veins or arteries from elsewhere in the
patient's body are grafted from the aorta to the coronary arteries, bypassing coronary artery

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http://en.wikipedia.org/wiki/Heart%20Attack

Cardiovascular Disease
narrowing caused by atherosclerosis and improves the blood supply to the myocardium
(heart muscle).
Congestive Heart Failure
Congestive heart failure (CHF), also called congestive cardiac failure (CCF) or just heart
failure, is a condition that can result from any structural or functional cardiac disorder that
impairs the ability of the heart to fill with or pump a sufficient amount of blood throughout
the body. It is not to be confused with "cessation of heartbeat", which is known as asystole,
or with cardiac arrest, which is the cessation of normal cardiac function in the face of heart
disease. Because not all patients have volume overload at the time of initial or subsequent
evaluation, the term "heart failure" is preferred over the older term "congestive heart failure".
Congestive heart failure is often undiagnosed due to a lack of a universally agreed definition
and difficulties in diagnosis, particularly when the condition is considered "mild".
Aneurysm
An aneurysm (or aneurism) is a localized dilation or ballooning of a blood vessel by more
than 50% of the diameter of the vessel and can lead to instant death at anytime. Aneurysms
most commonly occur in arteries at the base of the brain (the circle of Willis) and in the
aorta (the main artery coming out of the heart) - this is an aortic aneurysm. This bulge
in a blood vessel, much like a bulge on an over-inflated inner tube, can lead to death at
anytime. The larger an aneurysm becomes, the more likely it is to burst. Aneurysms are also
described according to their shape: Saccular or fusiform. A saccular aneurysm resembles a
small sack; a fusiform aneurysm is shaped like a spindle.
Dissolving Blood Clots
To dissolve blood clots you would use a drug that converts plasminogen (molecule found in
blood), to plasmin, (enzyme that dissolves blood clots).
Clearing Clogged Arteries
One way to unblock a coronary artery (or other blood vessel) is percutaneous transluminal
coronary angioplasty (PTCA), which was first performed in 1977. A wire is passed from the
femoral artery in the leg or the radial artery in the arm up to the diseased coronary artery,
to beyond the area of the coronary artery that is being worked upon. Over this wire, a
balloon catheter is passed into the segment that is to be opened up. The end of the catheter
contains a small folded balloon. When the balloon is hydraulically inflated, it compresses
the atheromatous plaque and stretches the artery wall to expand. At the same time, if an
expandable wire mesh tube (stent) was on the balloon, then the stent will be implanted (left
behind) to support the new stretched open position of the artery from the inside.

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The Cardiovascular System

7.9.1 Dilated and Inflamed Veins

Varicose Veins
Varicose veins are veins on the leg which are large, twisted, and ropelike, and can cause pain,
swelling, or itching. They are an extreme form of telangiectasia, or spider veins. Varicose
veins result due to insufficiency of the valves in the communicating veins. These are veins
which link the superficial and deep veins of the lower limb. Normally, blood flows from the
superficial to the deep veins, facilitating return of blood to the heart. However, when the
valve becomes defective, blood is forced into the superficial veins by the action of the muscle
pump (which normally aids return of blood to the heart by compressing the deep veins).
People who have varicose veins are more at risk of getting a Deep Vein Thrombosis (DVT)
and pulmonary embolisms.
Phlebitis
Phlebitis is an inflammation of a vein, usually in the legs. This is usually the most serious if
found in a deep vein. However, most people with the condition, perhaps 80 to 90 percent, are
women. The disease may also have a genetic component, as it is known to run in families.

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7.9.2 Congenital Heart Defects

Figure 73

Illustration of VSD

Heart defects present at birth are called congenital heart defects. Slightly less than 1% of
all newborn infants have congenital heart disease. Eight defects are more common than all
others and make up 80% of all congenital heart diseases, whereas the remaining 20% consist
of many independently infrequent conditions or combinations of several defects.

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Acyanotic Defects
Acyanotic heart defects are those in which there is a normal amount of oxygen in the
bloodstream. The most common congenital heart defect is a ventral septal defect, which
occurs in about 20% of all children with congenital heart disease. In VSD blood from the
left ventricle is shunted to the right ventricle, resulting in oxygenated blood returning into
pulmonic circulation. One of the potential problems of VSD is pulmonary hypertension.
Cyanotic Defects
Cyanotic heart defects refer to defects that result in decreased amounts of oxygen in the
blood. In cyanotic heart defects deoxygenated blood from the right ventricle flows into the
systemic circulation. Cyanotic defects include tetrogy of fallot and transposition of the great
arteries.

7.10 Homeostasis
Homeostasis in the body is only possible if the cardiovascular system is working properly.
This means that the system needs to deliver oxygen and nutrients to the tissue fluid that
surrounds the cells and also take away the metabolic waste. The heart is composed of
arteries that take blood from the heart, and vessels that return blood to the heart. Blood is
pumped by the heart into two circuits: the pulmonary and systemic circuits. The pulmonary
circuit carries blood through the lungs where gas exchange occurs and the systemic system
transports blood to all parts of the body where exchange with tissue fluid takes place. The
cardiovascular system works together with all other systems to maintain homeostasis.

7.10.1 The Lymphatic System

The lymphatic system is closely related to the cardiovascular system. There are three main
ways that they work together to maintain homeostasis: the lymphatic system receives the
excess tissue fluid and returns it to the bloodstream, lacteal take fat molecules from the
intestinal villi and transport them to the bloodstream and both systems work together to
defend the body against disease.The lymphatic system can create white blood cells that
fight off disease and infections.

7.11 Interesting Facts

Heart Disease is the number one killer in American women.
16.7 million deaths are result forms of cardiovascular disease, heart disease and stroke.

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Ways to a Healthy Heart

Stress, eating high fat foods, obesity, tobacco and alcohol use are just some risk factors of
developing heart disease.
Recent research suggests that taking a small dose of aspirin daily may help prevent a
heart attack (because aspirin inhibits platelet clumping).
The length of all your blood vessels lined up is about 60,000 miles long! To put this in
perspective, the Earth's circumference is 40,075.02 kilometres and 60,000 miles is around
96,000 km - so your blood vessels would go twice around the world and still have some to
spare!

7.12 Ways to a Healthy Heart

Eating healthy, good nutrition.
Fitness and Exercise.
Having a healthy lifestyle; don't drink, smoke, or do drugs.
Lowering LDL cholesterol and high blood pressure.
Reduce the fat, sodium, and calories in your diet.
The total length of capillaries in an average adult human is approximately 25,000 mi
(42,000 km).

7.13 Aging
The heart muscle becomes less efficient with age, and there is a decrease in both maximum
cardiac output and heart rate, although resting levels may be more than adequate. The
health of the myocardium depends on its blood supply, and with age there is greater likelihood
that arthrosclerosis will narrow the coronary arteries. Atherosclerosis is the deposition of
cholesterol on and in the walls of the arteries, which decreases blood flow and forms rough
surfaces that may cause intravascular clot formation High blood pressure (hypertension)
causes the left ventricle to work harder. It may enlarge and outgrow its blood supply, thus
becoming weaker. A weak ventricle is not an efficient pump, and may progress to congestive
heart failure. This process may be slow or rapid. The heart valves may become thickened
by fibrosis, leading to heart murmurs and less efficient pumping. Arrhythmias are also more
common with age, as the cells of the conduction pathway become less efficient.

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7.14 Shock
Physiological Stress
Physiological stress can be any kind of injury from burns, to broken bones; the body's
response to stress is categorized in two phases the ebb phase (early phase) begins immediately
after the injury. And the second phase is about 36 to 48 hours after injury is called the flow
phase. In the ebb (shock) phase there is Inadequate circulation, decreased insulin level, decreased oxygen consumption, hypothermia (low body temperature), hypovolemia (low blood
volume), and hypotension (low blood pressure). In the flow phase there is increased levels of
catecholamine, glucocorticoids, and glucagons, normal or elevated insulin levels, catabolic
(breakdown), hyperglycemic (high blood sugar), increased oxygen consumption/respiratory
rate, hyperthermia (high body temperature) fever sets in, hypermetabolism, increased insulin
resistance, increased cardiac output.

7.15 Premature ventricular contractions (PVC's)

Excitation occurs through the SA node to the AV node if there are abnormalities or drug
interference that malfunctions the AV node the ventricles will not receive the initiating
stimuli and the autorhythmic cells in the bundle branches begin to initiate actions on their
own rate becoming the pacemakers for the ventricles. This in turn will cause conduction
disorder. With conduction that causes problems with the bundle branches there is the
right and the left premature ventricular contractions. Right is most common and may go
untreated. Left is always a serious problem and must be treated.

7.16 Intrinsic Control of heartbeat

SA node (located in the right atrium near the entrance of the superior vena cava)
AV node (located at the base of right atrium)
AV bundle (located in the intraventricular septum between the two ventricles that go in
two directions right and left bundle branches that leave the septum to enter the walls of
both ventricle)
Bundle Branches (the branching off the septum to the walls of the ventricles that run
into the purkinje fibers that then make contact with ventricular myocardial cells to spread
the impulse to the rest of the ventricles)

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Electrocardiogram

Figure 74

Animation of a normal ECG wave.

7.17 Electrocardiogram
The P is the atrial depolarization
QRS is the ventricular depolarization, as well as atrial repolarization.
T is the ventricular repolarization

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Figure 75

Schematic representation of normal ECG

7.18 Extrinsic Control of Heartbeat

Autonomic system with two subdivisions: the sympathetic division and the parasympathetic
division. Hormonal control of blood pressure

Epinephrine
Norepinephrine
ANP : Atrial natriuretic peptide
ADH: Antidiuretic hormone
Renin-Angiotension system

7.19 Case Study

An example of the ever expanding technology for the heart is best described in this story:
In 1955, when I was five years old, I first learned by my family physician that I had a heart
murmur and that it would eventually need attention. By the time I was 15 in 1965, I had
two cardiac catherizations at Rhode Island Hospital. The tests were inconclusive and I was
told to go on with my life and wait and see if I had a problem. It wasn't until 1975 that I was

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Summary
told by my family physician that I should have my heart checked again. Dr. David Kitzes of
Mariam Hospital performed another catherization. This time, unlike the others, I was told
that because of new machine technology, Dr. Kitzes found that I had aortic stenosis, which
is a narrowing of the valve passage by build-up of plaque due to the valve being malformed
at birth. Dr. Kitzes informed me that I could lead a normal life until I was in my fifties
or sixties before I would need corrective surgery. In 1996, I had an echocardiogram and it
was determined that my heart was enlarged. My family physician said that I should see a
cardiologist. I down played the visit as not being serious after hearing the same thing many
times. This time I entered the office of Jon Lambrecht, I had never met him before. Within
a few minutes my whole life was turned around. After asking me about my symptoms,
which were fatigue, weakness, asthmatic symptoms, as well as ashen skin color and dizziness,
he informed me of how serious my condition was and the only salvation was immediate
open-heart surgery to replace the aortic valve. I began to cry as I thought my life was over.
Dr. Lambrecht studied my reaction and told me that this condition is repairable and that
I don't have a terminal illness. I didn't have a lot of time to think about it. Within 10
days from that visit, I was the recipient of a Meditronic Hall Prosthetic heart valve. The
operation was performed by Dr. Robert Indeglia at Miriam Hospital in Providence, R.I.
on March 20th, 1996. It has been almost 3 years since the surgery and I am doing better
than I could have expected. In 1977 my son Kevin was born with Hypoplastic Left-heart
Syndrome and only lived for 2 days because heart surgery wasn't performed like today. I am
thankful that I lived at a time when medical technology paved the way for a second chance
because of my new aortic heart valve. Our goal in this chapter is to take you by the hand
and lead you through each part of the cardiovascular system, so that you too may learn and
come to respect the greatness of this blood pumping machine we all call the heart.
Stroke
Cerebrovascular disease are those that affect blood vessels in the brain and happen to be the
third cause of death in the United States only behind heart disease and cancer. Stroke (also
called cerebrovascular accident or CVR) is a cerebrovascular disorder caused by a sudden
decrease or stoppage of blood flow to a part of the brain. Decreased blood flow also known
as ischemia is dangerous to any tissue but brain tissue is even more vulnerable, mainly due
to the high rate of its metabolic reactions. In fact if you stopped blood flow for no more
than three minutes it may be sufficient enough to cause death of most brain cells. For this
reason a stroke can kill people within minutes or leave them with severe brain damage.
Strokes may be classified as either occlusive or hemorrhagic and may happen either in the
interior of the brain or on its surface. In a occlusive stroke blood flow through a vessel is
blocked. In a hemorrhagic stroke a blood vessel ruptures causing a hemorrhage.

7.20 Summary
As with all of the body systems, the cardiovascular system plays a part in maintaining
homeostasis. The nervous system regulates the functioning of the heart based on what the
heart is supposed to do. The pumping of the heart maintains normal blood pressure and
proper oxygenation of tissues. The vascular system forms passageways for the blood, but

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they aren't simply just a pipeline system. The vessels are not passive tubes, but rather
active contributors to homeostasis. The arteries and veins help maintain blood pressure,
and the capillaries provide sites for the necessary exchanges of materials between the blood
and the tissues.

7.21 Review Questions

Answers for these questions can be found here4
1. This conducts electricity like nerves
A) Epicardium
B) Pericardium
C) Myocardium
D) Subvalaular Apparatus
E) None of these, only nerves conduct electricity
2. This carries the most blood at any given time in the body
A) Veins
B) Capillary Beds
C) Veins
D) Aorta
E) Vena Cava
3. The following contract together to pump blood
A) Right atrium with the right ventricle and left atrium with the left ventricle
B) Right atrium with left atrium and right ventricles with left ventricle
C) Tricuspid valve and mitral valve
D) Aorta and pulmonary artery
E) Aorta, pulmonary artery and pulmonary vein
4. This is the pacemaker of the heart
A) AV node
B) Purkinje fibers
C) AV Bundle
D) SA node

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http://en.wikibooks.org/wiki/Human_Physiology/Appendix_1:_answers_to_review_
questions#The_cardiovascular_system

Review Questions
E) None of these, a pacemaker is surgically inserted
5. When reading an EKG, this letter shows the depolarization from the AV node down to
the AV bundle
A) S
B) P
C) U
D) T
E) Q
6. The T wave in an EKG shows
A) Resting potential
B) Atrial depolarization
C) SA node excitation
D) Ventricle repolarization
E) Purkinje Excitation
7. Blood pressure is the measure of
A) Pressure exerted by the blood on the walls of the blood vessels
B) Pressure exerted by the blood on the arteries
C) Pressure exerted by the blood on the veins
D) Pressure exerted by the blood on the aorta
E) Pressure exerted by the blood on the capillaries
8. Systolic Pressure is
A) An average of 120 mm Hg
B) Lowers steadily during ventricle systole
C) The highest when blood is being pumped out of the left ventricle into the aorta
D) An average of 80 mm Hg
E) Both A and C
F) Both B and D
9. The heart has how many chambers?
A) One
B) Two
C) Three
D) Four

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E) Five

7.22 Glossary
Acute myocardial infarction (AMI or MI) commonly known as a heart attack, is a
disease state that occurs when the blood supply to a part of the heart is interrupted. The
resulting ischemia or oxygen shortage causes damage and potential death of heart tissue.
Aorta: the largest of the arteries in the systemic circuit Aortic Valve: lies between the left
ventricle and the aorta Antidiuretic hormone: Produced in the posterior pituitary ADH
(vasopressin), major function is to regulate blood pressure by water retention by the kidneys.
Arteriole: a small diameter blood vessel that extends and branches out from an artery
and leads to capillaries Atrial natriuretic peptide: Produced in the atria of the heart, it
increases urinary excretion of sodium which causes water loss which in turn the viscosity
of the blood is lowered and in turn lowers the blood pressure. Atrioventricular Node
(abbreviated AV node): the tissue between the atria and the ventricles of the heart, which
conducts the normal electrical impulse from the atria to the ventricles Atrioventricular
valves: large, multi-cusped valves that prevent backflow from the ventricles into the
atria during systole AV Bundle: collection of heart muscle cells specialized for electrical
conduction that transmits the electrical impulses from the AV node Barbiturates: CNS
depressants, sedative-hypnotics Blood Pressure: the pressure exerted by the blood on
the walls of the blood vessels Capillaries: the smallest of a bodys vessels, they connect
arteries and veins Cardiac Cycle: term used to describe the sequence of events that occur
as a heart works to pump blood through the body Cerebral Vascular Accident (CVA):
Also known as a stroke, is a rapidly developing loss of a part of brain function or loss of
consciousness due to an interruption in the blood supply to all or part of the brain. That is, a
stroke involves the sudden loss of neuronal function due to a disturbance in cerebral perfusion.
There are many different causes for the interruption of blood supply, and different parts of
the brain can be affected. Because of this, a stroke can be quite heterogeneous. Patients with
the same cause of stroke can have widely differing handicaps. Similarly, patients with the
same clinical handicap can in fact have different causes of their stroke. Chordae Tendinae:
cord-like tendons that connect the papillary muscles to the tricuspid valve and the mitral
valve in the heart Coronary Arteries: blood vessels that supply blood to, and remove
blood from, the heart muscle itself Continuous Capillaries: have a sealed epithelium and
only allow small molecules, water and ions to diffuse Deep-vein thrombosis (DVT): is
the formation of a blood clot ("thrombus") in a deep vein. It commonly affects the leg veins,
such as the femoral vein or the popliteal vein or the deep veins of the pelvis. Occasionally
the veins of the arm are affected Diastole: period of time when the heart relaxes after
contraction in preparation for refilling with circulating blood Diastolic Pressure: lowest
point in blood pressure where the heart relaxes Edema: The swelling that forms when too
much tissue fluid forms or not enough taken away Electrocardiogram: the recording of
the heart's electrical activity as a graph Epinephrine: Produced in the adrenal medulla of
the adrenal glands, major function is vasoconstriction that will in turn increase respiratory
rate and increase cardiac out put. Fenestrated Capillaries: have openings that allow
larger molecules to diffuse Fibrous Pericardium: a dense connective tissue that protects
the heart, anchoring it to the surrounding walls, and preventing it from overfilling with
blood Heart Rate: term used to describe the frequency of the cardiac cycle Hepatic

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References
Veins: blood vessels that drain de-oxygenated blood from the liver and blood cleaned by
the liver (from the stomach, pancreas, small intestine and colon) into the inferior vena
cava Hypertension or High Blood Pressure: medical condition wherein the blood
pressure is chronically elevated Inferior Vena Cava (or IVC): a large vein that carries
de-oxygenated blood from the lower half of the body into the heart Intraventricular
Septum: the stout wall separating the lower chambers (the ventricles) of the heart from one
another Left Atrium:receives oxygenated blood from the left and right pulmonary veins
Lub: first heart tone, or S1; caused by the closure of the atrioventricular valves, mitral and
tricuspid, at the beginning of ventricular contraction, or systole Lumen: hollow internal
cavity in which the blood flows Lymph: originates as blood plasma that leaks from the
capillaries of the circulatory system, becoming interstitial fluid, filling the space between
individual cells of tissue Mitral valve: also known as the bicuspid valve; prevents blood
flowing from the left ventricle into the left atrium Myocardium: the muscular tissue of the
heart. Norepinephrine: Produced in the adrenal medulla of the adrenal glands, major
function is a strong vasoconstrictor that will in turn increase respiratory rate. Pacemaker
Cells: cells that create these rhythmical impulses of the heart Plaque: an abnormal
inflammatory accumulation of macrophage white blood cells within the walls of
arteries Pulmonary Valve: lies between the right ventricle and the pulmonary artery;
prevents back-flow of blood into the ventricle Pulse: the number of heartbeats per
minute Purkinje Fibers (or Purkinje tissue): located in the inner ventricular walls
of the heart, just beneath the endocardium; specialized myocardial fibers that conduct an
electrical stimulus or impulse that enables the heart to contract in a coordinated fashion
Renin-Angiotension system: Right Atrium: receives de-oxygenated blood from the
superior vena cava and inferior vena cava Serous Pericardium: functions in lubricating
the heart to prevent friction from occurring during heart activity Semilunar Valves:
positioned on the pulmonary artery and the aorta Sinoatrial Node: (abbreviated SA node
or SAN, also called the sinus node): the impulse generating (pacemaker) tissue located in the
right atrium of the heart Sinusoidal Capillaries: special forms of fenestrated capillaries
that have larger opening allowing RBCs and serum proteins to enter Systole: contraction
of the heart Systolic Pressure:the highest point in blood pressure when the blood is
being pumped out of the left ventricle into the aorta during ventricular systole
Superior Vena Cava (SVC): a large but short vein that carries de-oxygenated blood
from the upper half of the body to the heart's right atrium Thrombus: a blood clot in
an intact blood vessel Tricuspid Valve: on the right side of the heart, between the right
atrium and the right ventricle; allows blood to flow from the right atrium into the right
ventricle when the heart is relaxed during diastole Vasoconstriction: the constriction of
blood vessels Vasodilation: the dilation of blood vessels Veins:carry de-oxygenated
blood from the capillary blood vessels to the right part of the heart Ventricle: a heart
chamber which collects blood from an atrium Venule: a small blood vessel that allows
deoxygenated blood to return from the capillary beds to the larger blood vessels called

7.23 References
1. Van De Graaff, Kent M. Human Anatomy. McGraw Hill Publishing, Burr Ridge, IL.
2002.
2. Essentials of Anatomy and Physiology, Valerie C. Scanlon and Tina Sanders

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3. Tortora, G. & Grabowski, S. (2000) Principles of Anatomy & Physiology. Wiley &
Sons. Brisbane, Singapore & Chichester.
4. Anderson, RM. The Gross Physiology of the Cardiovascular System (1993) <http:
//cardiac-output.info>.

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8 The Urinary System

Figure 76

8.1 Introduction
The Urinary System is a group of organs in the body concerned with filtering out excess
fluid and other substances from the bloodstream. The substances are filtered out from
the body in the form of urine. Urine is a liquid produced by the kidneys, collected in
the bladder and excreted through the urethra. Urine is used to extract excess minerals or
vitamins as well as blood corpuscles from the body. The Urinary organs include the kidneys,
ureters, bladder, and urethra. The Urinary system works with the other systems of the body

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The Urinary System

to help maintain homeostasis. The kidneys are the main organs of homeostasis because they
maintain the acid base balance and the water salt balance of the blood.

8.2 Functions of the Urinary System

One of the major functions of the Urinary system is the process of excretion. Excretion is the
process of eliminating, from an organism, waste products of metabolism and other materials
that are of no use. The urinary system maintains an appropriate fluid volume by regulating
the amount of water that is excreted in the urine. Other aspects of its function include
regulating the concentrations of various electrolytes in the body fluids and maintaining
normal pH of the blood. Several body organs carry out excretion, but the kidneys are the
most important excretory organ. The primary function of the kidneys is to maintain a stable
internal environment (homeostasis) for optimal cell and tissue metabolism. They do this by
separating urea, mineral salts, toxins, and other waste products from the blood. They also
do the job of conserving water, salts, and electrolytes. At least one kidney must function
properly for life to be maintained. Six important roles of the kidneys are:
Regulation of plasma ionic composition. Ions such as sodium, potassium, calcium,
magnesium, chloride, bicarbonate, and phosphates are regulated by the amount that the
kidney excretes.
Regulation of plasma osmolarity. The kidneys regulate osmolarity because they have
direct control over how many ions and how much water a person excretes.
Regulation of plasma volume. Your kidneys are so important they even have an effect
on your blood pressure. The kidneys control plasma volume by controlling how much water
a person excretes. The plasma volume has a direct effect on the total blood volume, which
has a direct effect on your blood pressure. Salt(NaCl)will cause osmosis to happen; the
diffusion of water into the blood.
Regulation of plasma hydrogen ion concentration (pH). The kidneys partner up
with the lungs and they together control the pH. The kidneys have a major role because they
control the amount of bicarbonate excreted or held onto. The kidneys help maintain the
blood Ph mainly by excreting hydrogen ions and reabsorbing bicarbonate ions as needed.
Removal of metabolic waste products and foreign substances from the plasma.
One of the most important things the kidneys excrete is nitrogenous waste. As the liver
breaks down amino acids it also releases ammonia. The liver then quickly combines that
ammonia with carbon dioxide, creating urea which is the primary nitrogenous end product
of metabolism in humans. The liver turns the ammonia into urea because it is much less
toxic. We can also excrete some ammonia, creatinine and uric acid. The creatinine comes
from the metabolic breakdown of creatine phospate (a high-energy phosphate in muscles).
Uric acid comes from the break down of nucleotides. Uric acid is insoluble and too much
uric acid in the blood will build up and form crystals that can collect in the joints and cause
gout.
Secretion of Hormones The endocrine system has assistance from the kidney's when
releasing hormones. Renin is released by the kidneys. Renin leads to the secretion of
aldosterone which is released from the adrenal cortex. Aldosterone promotes the kidneys

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Functions of the Urinary System

to reabsorb the sodium (Na+) ions. The kidneys also secrete erythropoietin when the
blood doesn't have the capacity to carry oxygen. Erythropoietin stimulates red blood cell
production. The Vitamin D from the skin is also activated with help from the kidneys.
Calcium (Ca+) absorption from the digestive tract is promoted by vitamin D.
CC: Chapter Check: Name the role of the kidneys and how they work?

Figure 77

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The Urinary System

8.3 Organs in the Urinary System

8.3.1 Kidneys And Their Structure

Figure 78 1. Renal pyramid 2. Interlobar artery 3.

Renal artery 4. Renal vein 5. Renal hylum 6. Renal
pelvis 7. Ureter 8. Minor calyx 9. Renal capsule 10.
Inferior renal capsule 11. Superior renal capsule 12.
Interlobar vein 13. Nephron 14. Minor calyx 15. Major
calyx 16. Renal papilla 17. Renal column
The kidneys are a pair of bean shaped, brown organs about the size of your fist.It measures
10-12 cm long. They are covered by the renal capsule, which is a tough capsule of fibrous
connective tissue. Adhering to the surface of each kidney is two layers of fat to help cushion
them. There is a concaved side of the kidney that has a depression where a renal artery
enters, and a renal vein and a ureter exit the kidney. The kidneys are located at the rear
wall of the abdominal cavity just above the waistline, and are protected by the ribcage.
They are considered retroperitoneal, which means they lie behind the peritoneum. There
are three major regions of the kidney, renal cortex, renal medulla and the renal pelvis.
The outer, granulated layer is the renal cortex. The cortex stretches down in between a
radially striated inner layer. The inner radially striated layer is the renal medulla. This
contains pyramid shaped tissue called the renal pyramids, separated by renal columns. The
ureters are continuous with the renal pelvis and is the very center of the kidney.

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Organs in the Urinary System

Renal Vein
The renal veins are veins that drain the kidney. They connect the kidney to the inferior
vena cava. Because the inferior vena cava is on the right half of the body, the left renal
vein is generally the longer of the two. Unlike the right renal vein, the left renal vein often
receives the left gonadal vein (left testicular vein in males, left ovarian vein in females). It
frequently receives the left suprarenal vein as well.
Renal Artery
The renal arteries normally arise off the abdominal aorta and supply the kidneys with
blood. The arterial supply of the kidneys are variable and there may be one or more renal
arteries supplying each kidney. Due to the position of the aorta, the inferior vena cava and
the kidneys in the body, the right renal artery is normally longer than the left renal artery.
The right renal artery normally crosses posteriorly to the inferior vena cava. The renal
arteries carry a large portion of the total blood flow to the kidneys. Up to a third of the
total cardiac output can pass through the renal arteries to be filtered by the kidneys.

8.3.2 Ureters
The ureters are two tubes that drain urine from the kidneys to the bladder. Each ureter is
a muscular tube about 10 inches (25 cm) long. Muscles in the walls of the ureters send the
urine in small spurts into the bladder, (a collapsible sac found on the forward part of the
cavity of the bony pelvis that allows temporary storage of urine). After the urine enters
the bladder from the ureters, small folds in the bladder mucosa act like valves preventing
backward flow of the urine. The outlet of the bladder is controlled by a sphincter muscle. A
full bladder stimulates sensory nerves in the bladder wall that relax the sphincter and allow
release of the urine. However, relaxation of the sphincter is also in part a learned response
under voluntary control. The released urine enters the urethra.

8.3.3 Urinary Bladder

The urinary bladder is a hollow, muscular and distendible or elastic organ that sits on
the pelvic floor (superior to the prostate in males). On its anterior border lies the pubic
symphysis and, on its posterior border, the vagina (in females) and rectum (in males). The
urinary bladder can hold approximately 17 to 18 ounces (500 to 530 ml) of urine, however
the desire to micturate is usually experienced when it contains about 150 to 200 ml. When
the bladder fills with urine (about half full), stretch receptors send nerve impulses to the
spinal cord, which then sends a reflex nerve impulse back to the sphincter (muscular valve)
at the neck of the bladder, causing it to relax and allow the flow of urine into the urethra.
The Internal urethral sphincter is involuntary. The ureters enter the bladder diagonally
from its dorsolateral floor in an area called the trigone. The trigone is a triangular shaped
area on the postero-inferior wall of the bladder. The urethra exits at the lowest point of the
triangle of the trigone. The urine in the bladder also helps regulate body temperature. A
bladder when operating normally empties completely upon a complete discharge, otherwise

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it is a sign that its elasticity is compromised, when it becomes completely void of fluid, it
may cause a chilling sensation due to the rapid change of body temperature.

8.3.4 Urethra

Figure 79

222

Female urethra (labeled at bottom right.)

Organs in the Urinary System

Figure 80 Male Sphincter urethrae muscle

- The male urethra laid open on its anterior
(upper) surface. (Region visible, but muscle
not labeled.)
The urethra is a muscular tube that connects the bladder with the outside of the body.
The function of the urethra is to remove urine from the body. It measures about 1.5 inches
(3.8 cm) in a woman but up to 8 inches (20 cm) in a man. Because the urethra is so much
shorter in a woman it makes it much easier for a woman to get harmful bacteria in her
bladder this is commonly called a bladder infection or a UTI. The most common bacteria of
a UTI is E-coli from the large intestines that have been excreted in fecal matter. Female
urethra
In the human female, the urethra is about 1-2 inches long and opens in the vulva between
the clitoris and the vaginal opening.
Men have a longer urethra than women. This means that women tend to be more susceptible
to infections of the bladder (cystitis) and the urinary tract.
Male urethra

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In the human male, the urethra is about 8 inches long and opens at the end of the head of
the penis.
The length of a male's urethra, and the fact it contains a number of bends, makes catheterisation more difficult.
The urethral sphincter is a collective name for the muscles used to control the flow of
urine from the urinary bladder. These muscles surround the urethra, so that when they
contract, the urethra is closed.
There are two distinct areas of muscle: the internal sphincter, at the bladder neck and
the external, or distal, sphincter.
Human males have much stronger sphincter muscles than females, meaning that they can
retain a large amount of urine for twice as long, as much as 800mL, i.e. "hold it".

8.3.5 Nephrons
A nephron is the basic structural and functional unit of the kidney. The name nephron
comes from the Greek word (nephros) meaning kidney. Its chief function is to regulate water
and soluble substances by filtering the blood, reabsorbing what is needed and excreting the
rest as urine. Nephrons eliminate wastes from the body, regulate blood volume and pressure,
control levels of electrolytes and metabolites, and regulate blood pH. Its functions are vital
to life and are regulated by the endocrine system by hormones such as antidiuretic hormone,
aldosterone, and parathyroid hormone.
Each nephron has its own supply of blood from two capillary regions from the renal artery.
Each nephron is composed of an initial filtering component (the renal corpuscle) and a
tubule specialized for reabsorption and secretion (the renal tubule). The renal corpuscle
filters out large solutes from the blood, delivering water and small solutes to the renal tubule
for modification.
Glomerulus
The glomerulus is a capillary tuft that receives its blood supply from an afferent arteriole
of the renal circulation. The glomerular blood pressure provides the driving force for fluid
and solutes to be filtered out of the blood and into the space made by Bowman's capsule.
The remainder of the blood not filtered into the glomerulus passes into the narrower efferent
arteriole. It then moves into the vasa recta, which are collecting capillaries intertwined with
the convoluted tubules through the interstitial space, where the reabsorbed substances will
also enter. This then combines with efferent venules from other nephrons into the renal vein,
and rejoins with the main bloodstream.
Afferent/Efferent Arterioles
The afferent arteriole supplies blood to the glomerulus. A group of specialized cells known as
juxtaglomerular cells are located around the afferent arteriole where it enters the renal
corpuscle. The efferent arteriole drains the glomerulus. Between the two arterioles lies
specialized cells called the macula densa. The juxtaglomerular cells and the macula densa
collectively form the juxtaglomerular apparatus. It is in the juxtaglomerular apparatus

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cells that the enzyme renin is formed and stored. Renin is released in response to decreased
blood pressure in the afferent arterioles, decreased sodium chloride in the distal convoluted
tubule and sympathetic nerve stimulation of receptors (beta-adrenic) on the juxtaglomerular
cells. Renin is needed to form Angiotensin I and Angiotensin II which stimulate the secretion
of aldosterone by the adrenal cortex.
Glomerular Capsule or Bowman's Capsule
Bowman's capsule (also called the glomerular capsule) surrounds the glomerulus and is
composed of visceral (simple squamous epithelial cells) (inner) and parietal (simple squamous
epithelial cells) (outer) layers. The visceral layer lies just beneath the thickened glomerular
basement membrane and is made of podocytes which send foot processes over the length of
the glomerulus. Foot processes interdigitate with one another forming filtration slits that, in
contrast to those in the glomeruluar endothelium, are spanned by diaphragms. The size
of the filtration slits restricts the passage of large molecules (eg, albumin) and cells (eg,
red blood cells and platelets). In addition, foot processes have a negatively-charged coat
(glycocalyx) that limits the filtration of negatively-charged molecules, such as albumin. This
action is called electrostatic repulsion.
The parietal layer of Bowman's capsule is lined by a single layer of squamous epithelium.
Between the visceral and parietal layers is Bowman's space, into which the filtrate enters
after passing through the podocytes' filtration slits. It is here that smooth muscle cells and
macrophages lie between the capillaries and provide support for them. Unlike the visceral
layer, the parietal layer does not function in filtration. Rather, the filtration barrier is
formed by three components: the diaphragms of the filtration slits, the thick glomerular
basement membrane, and the glycocalyx secreted by podocytes. 99% of glomerular filtrate
will ultimately be reabsorbed.
The process of filtration of the blood in the Bowman's capsule is ultrafiltration (or glomerular
filtration), and the normal rate of filtration is 125 ml/min, equivalent to ten times the
blood volume daily. Measuring the glomerular filtration rate (GFR) is a diagnostic test of
kidney function. A decreased GFR may be a sign of renal failure. Conditions that can affect
GFR include: arterial pressure, afferent arteriole constriction, efferent arteriole constriction,
plasma protein concentration and colloid osmotic pressure.
Any proteins that are roughly 30 kilodaltons or under can pass freely through the membrane.
Although, there is some extra hindrance for negatively charged molecules due to the negative
charge of the basement membrane and the podocytes. Any small molecules such as water,
glucose, salt (NaCl), amino acids, and urea pass freely into Bowman's space, but cells,
platelets and large proteins do not. As a result, the filtrate leaving the Bowman's capsule is
very similar to blood plasma in composition as it passes into the proximal convoluted tubule.
Together, the glomerulus and Bowman's capsule are called the renal corpuscle.
Proximal Convoluted Tubule (PCT)
The proximal tubule can be anatomically divided into two segments: the proximal convoluted
tubule and the proximal straight tubule. The proximal convoluted tubule can be divided
further into S1 and S2 segments based on the histological appearance of it's cells. Following

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this naming convention, the proximal straight tubule is commonly called the S3 segment.
The proximal convoluted tubule has one layer of cuboidal cells in the lumen. This is the
only place in the nephron that contains cuboidal cells. These cells are covered with millions
of microvilli. The microvilli serve to increase surface area for reabsorption.
Fluid in the filtrate entering the proximal convoluted tubule is reabsorbed into the peritubular
capillaries, including approximately two-thirds of the filtered salt and water and all filtered
organic solutes (primarily glucose and amino acids). This is driven by sodium transport
from the lumen into the blood by the Na+/K+ ATPase in the basolateral membrane of the
epithelial cells. Much of the mass movement of water and solutes occurs in between the cells
through the tight junctions, which in this case are not selective.
The solutes are absorbed isotonically, in that the osmotic potential of the fluid leaving the
proximal tubule is the same as that of the initial glomerular filtrate. However, glucose,
amino acids, inorganic phosphate, and some other solutes are reabsorbed via secondary
active transport through cotransport channels driven by the sodium gradient out of the
nephron.

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Loop of the Nephron or Loop of Henle

Figure 81

The Nephron Loop or Loop of Henle.

The loop of Henle (sometimes known as the nephron loop) is a U-shaped tube that consists
of a descending limb and ascending limb. It begins in the cortex, receiving filtrate from the
proximal convoluted tubule, extends into the medulla, and then returns to the cortex to
empty into the distal convoluted tubule. Its primary role is to concentrate the salt in the
interstitium, the tissue surrounding the loop.
Descending limb
Its descending limb is permeable to water but completely impermeable to salt, and thus
only indirectly contributes to the concentration of the interstitium. As the filtrate descends
deeper into the hypertonic interstitium of the renal medulla, water flows freely out of the
descending limb by osmosis until the tonicity of the filtrate and interstitium equilibrate.

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Longer descending limbs allow more time for water to flow out of the filtrate, so longer
limbs make the filtrate more hypertonic than shorter limbs.
Ascending limb
Unlike the descending limb, the ascending limb of Henle's loop is impermeable to water,
a critical feature of the countercurrent exchange mechanism employed by the loop. The
ascending limb actively pumps sodium out of the filtrate, generating the hypertonic
interstitium that drives countercurrent exchange. In passing through the ascending limb,
the filtrate grows hypotonic since it has lost much of its sodium content. This hypotonic
filtrate is passed to the distal convoluted tubule in the renal cortex.
Distal Convoluted Tubule (DCT)
The distal convoluted tubule is similar to the proximal convoluted tubule in structure and
function. Cells lining the tubule have numerous mitochondria, enabling active transport to
take place by the energy supplied by ATP. Much of the ion transport taking place in the
distal convoluted tubule is regulated by the endocrine system. In the presence of parathyroid
hormone, the distal convoluted tubule reabsorbs more calcium and excretes more phosphate.
When aldosterone is present, more sodium is reabsorbed and more potassium excreted.
Atrial natriuretic peptide causes the distal convoluted tubule to excrete more sodium. In
addition, the tubule also secretes hydrogen and ammonium to regulate pH. After traveling
the length of the distal convoluted tubule, only 3% of water remains, and the remaining salt
content is negligible. 97.9% of the water in the glomerular filtrate enters the convoluted
tubules and collecting ducts by osmosis.
Collecting ducts
Each distal convoluted tubule delivers its filtrate to a system of collecting ducts, the first
segment of which is the connecting tubule. The collecting duct system begins in the renal
cortex and extends deep into the medulla. As the urine travels down the collecting duct
system, it passes by the medullary interstitium which has a high sodium concentration as a
result of the loop of Henle's countercurrent multiplier system. Though the collecting duct
is normally impermeable to water, it becomes permeable in the presence of antidiuretic
hormone (ADH). As much as three-fourths of the water from urine can be reabsorbed as
it leaves the collecting duct by osmosis. Thus the levels of ADH determine whether urine
will be concentrated or dilute. Dehydration results in an increase in ADH, while water
sufficiency results in low ADH allowing for diluted urine. Lower portions of the collecting
duct are also permeable to urea, allowing some of it to enter the medulla of the kidney, thus
maintaining its high ion concentration (which is very important for the nephron).
Urine leaves the medullary collecting ducts through the renal papilla, emptying into the
renal calyces, the renal pelvis, and finally into the bladder via the ureter. Because it has a
different embryonic origin than the rest of the nephron (the collecting duct is from endoderm
whereas the nephron is from mesoderm), the collecting duct is usually not considered a part
of the nephron proper.
Renal Hormones

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Formation of Urine
1. Vitamin D- Becomes metabolically active in the kidney. Patients with renal disease have
symptoms of disturbed calcium and phosphate balance.
2. Erythropoietin- Released by the kidneys in response to decreased tissue oxygen levels
(hypoxia).
3. Natriuretic Hormone- Released from cardiocyte granules located in the right atria of the
heart in response to increased atrial stretch. It inhibits ADH secretions which can contribute
to the loss of sodium and water.

8.4 Formation of Urine

Urine is formed in three steps: Filtration, Reabsorption, and Secretion.

8.4.1 Filtration
Blood enters the afferent arteriole and flows into the glomerulus. Blood in the glomerulus
has both filterable blood components and non-filterable blood components. Filterable blood
components move toward the inside of the glomerulus while non-filterable blood components
bypass the filtration process by exiting through the efferent arteriole. Filterable Blood
components will then take a plasma like form called glomerular filtrate. A few of the filterable
blood components are water, nitrogenous waste, nutrients and salts (ions). Nonfilterable
blood components include formed elements such as blood cells and platelets along with
plasma proteins. The glomerular filtrate is not the same consistency as urine, as much of it
is reabsorbed into the blood as the filtrate passes through the tubules of the nephron.

8.4.2 Reabsorption
Within the peritubular capillary network, molecules and ions are reabsorbed back into the
blood. Sodium Chloride reabsorbed into the system increases the osmolarity of blood in
comparison to the glomerular filtrate. This reabsorption process allows water (H2O) to pass
from the glomerular filtrate back into the circulatory system.
Glucose and various amino acids also are reabsorbed into the circulatory system. These
nutrients have carrier molecules that claim the glomerular molecule and release it back into
the circulatory system. If all of the carrier molecules are used up, excess glucose or amino
acids are set free into the urine. A complication of diabetes is the inability of the body to
reabsorb glucose. If too much glucose appears in the glomerular filtrate it increases the
osmolarity of the filtrate, causing water to be released into the urine rather than reabsorbed
by the circulatory system. Frequent urination and unexplained thirst are warning signs of
diabetes, due to water not being reabsorbed.
Glomerular filtrate has now been separated into two forms: Reabsorbed Filtrate and Nonreabsorbed Filtrate. Non-reabsorbed filtrate is now known as tubular fluid as it passes
through the collecting duct to be processed into urine.

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8.4.3 Secretion
Some substances are removed from blood through the peritubular capillary network into the
distal convoluted tubule or collecting duct. These substances are Hydrogen ions, creatinine,
and drugs. Urine is a collection of substances that have not been reabsorbed during
glomerular filtration or tubular reabsorbtion.

8.5 Maintaining Water-Salt Balance

It is the job of the kidneys to maintain the water-salt balance of the blood. They also
maintain blood volume as well as blood pressure. Simple examples of ways that this balance
can be changed include ingestion of water, dehydration, blood loss and salt ingestion.

8.5.1 Reabsorption of water

Direct control of water excretion in the kidneys is exercised by the anti-diuretic hormone
(ADH), released by the posterior lobe of the pituitary gland. ADH causes the insertion
of water channels into the membranes of cells lining the collecting ducts, allowing water
reabsorption to occur. Without ADH, little water is reabsorbed in the collecting ducts and
dilute urine is excreted. There are several factors that influence the secretion of ADH. The
first of these happen when the blood plasma gets too concentrated. When this occurs, special
receptors in the hypothalamus release ADH. When blood pressure falls, stretch receptors in
the aorta and carotid arteries stimulate ADH secretion to increase volume of the blood.

8.5.2 Reabsorption of Salt

The Kidneys also regulate the salt balance in the blood by controlling the excretion and
the reabsorption of various ions. As noted above, ADH plays a role in increasing water
reabsorption in the kidneys, thus helping to dilute bodily fluids. The kidneys also have
a regulated mechanism for reabsorbing sodium in the distal nephron. This mechanism is
controlled by aldosterone, a steroid hormone produced by the adrenal cortex. Aldosterone
promotes the excretion of potassium ions and the reabsorption of sodium ions. The release of
Aldosterone is initiated by the kidneys. The juxtaglomerular apparatus is a renal structure
consisting of the macula densa, mesangial cells, and juxtaglomerular cells. Juxtaglomerular
cells (JG cells, also known as granular cells) are the site of renin secretion. Renin is an
enzyme that converts angiotensinogen (a large plasma protein produced by the liver) into
Angiotensin I and eventually into Angiotensin II which stimulates the adrenal cortex to
produce aldosterone. The reabsorption of sodium ions is followed by the reapsorption of
water. This causes blood pressure as well as blood volume to increase.
Atrial natriuretic hormone (ANH) is released by the atria of the heart when cardiac
cells are streatched due to increased blood volume. ANH inhibits the secretion of renin by
the juxtaglomerular apparatus and the secretion of the aldosterone by the adrenal cortex.
This promotes the excretion of sodium. When sodium is excreted so is water. This causes
blood pressure and volume to decrease.

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Hypernatremia
An increase in plasma sodium levels above normal is hypernatremia. Sodium is the primary
solute in the extracellular fluid. Sodium levels have a major role in osmolarity regulation.
For excitable cells the electrochemical gradient for sodium across the plasma membrane
is critical for life. Water retention and an increased blood pressure usually are signs of
hypernatremia. If the plasma sodium levels are below normal it is called hyponatremia.
Signs of this are low plasma volume and hypotension.
Diuretics
A diuretic (colloquially called a water pill) is any drug that elevates the rate of bodily urine
excretion (diuresis). Diuretics also decrease the extracellular fluid (ECF) volume, and are
primarily used to produce a negative extracellular fluid balance. Caffeine, cranberry juice
and alcohol are all weak diuretics. In medicine, diuretics are used to treat heart failure,
liver cirrhosis, hypertension and certain kidney diseases. Diuretics alleviate the symptoms of
these diseases by causing sodium and water loss through the urine. As urine is produced by
the kidney, sodium and water which cause edema related to the disease move into the
blood to replace the volume lost as urine, thereby reducing the pathological edema. Some
diuretics, such as acetazolamide, help to make the urine more alkaline and are helpful in
increasing excretion of substances such as aspirin in cases of overdose or poisoning. The
antihypertensive actions of some diuretics (thiazides and loop diuretics in particular) are
independent of their diuretic effect. That is, the reduction in blood pressure is not due to
decreased blood volume resulting from increased urine production, but occurs through other
mechanisms and at lower doses than that required to produce diuresis. Indapamide was
specifically designed with this is mind, and has a larger therapeutic window for hypertension
(without pronounced diuresis) than most other diuretics. Chemically, diuretics are a diverse
group of compounds that either stimulate or inhibit various hormones that naturally occur
in the body to regulate urine production by the kidneys. Alcohol produces diuresis through
modulation of the vasopressin system.

8.6 Diseases of the Kidney

Diabetic nephropathy (nephropatia diabetica), also known as Kimmelstiel-Wilson syndrome and intercapillary glomerulonephritis, is a progressive kidney disease caused by
angiopathy of capillaries in the kidney glomeruli. It is characterized by nodular glomerulosclerosis. It is due to longstanding diabetes mellitus, and is a prime cause for dialysis in
many Western countries.

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Figure 82

An image of a kidney stone.

In medicine, hematuria (or "haematuria") is the presence of blood in the urine. It is a sign
of a large number of diseases of the kidneys and the urinary tract, ranging from trivial to
lethal.
Kidney stones, also known as nephrolithiases, urolithiases or renal calculi, are solid
accretions (crystals) of dissolved minerals in urine found inside the kidneys or ureters. They
vary in size from as small as a grain of sand to as large as a golf ball. Kidney stones typically
leave the body in the urine stream; if they grow relatively large before passing (on the order
of millimeters), obstruction of a ureter and distention with urine can cause severe pain

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Diabetes Insipidus
most commonly felt in the flank, lower abdomen and groin. Kidney stones are unrelated to
gallstones.
Case Study I was 34 weeks pregnant when I noticed blood in my urine. I immediately
went to my OBGYN where I was told that I had a bladder infection and given an antibiotic.
The next morning I experienced the most intense pain. I was rushed to the ER where I was
told that I had kidney stones. The doctors explained that there was nothing they could do
as long as I was pregnant. The next 3 weeks of my life were filled with intense pain and
multiple painkillers. After I delivered my baby, CAT scans were done and I was informed
that I had 6 kidney stones. It took three more weeks for me to pass all of the stones the
largest measuring 5 mm. The stones were tested and I was informed that my body had been
building up calcium due to my pregnancy and this was the cause of the kidney stones. I
continued to have kidney pain for 6 months after passing the stones. I now live my life on a
low calcium diet and the hope that my body will not develop more kidney stones.
Pyelonephritis When an infection of the renal pelvis and calices, called pyelitis, spreads
to involve the rest of the kidney as well, the result is pyelonephritis. It usually results from
the spread of fecal bacterium Escherichia coli from the anal region superiorly through the
urinary tract. In severe cases, the kidney swells and scars, abscesses form, and the renal
pelvis fills with pus. Left untreated, the infected kidney may be severely damaged, but
administration of antibiotics usually achieve a total cure.
glomerulonephritis Inflammation of the glomerular can be caused by immunologic abnormalities, drugs or toxins, vascular disorders, and systemic diseases. Glomerulonephritis
can be acute, chronic or progressive. Two major changes in the urine are distinctive of
glomerulonephritis: hematuria and proteinuria with albumin as the major protein. There is
also a decrease in urine as there is a decrease in GFR (glomerular filtration rate). Renal
failure is associated with oliguria (less than 400 ml of urine output per day).
Renal Failure Uremia is a syndrome of renal failure and includes elevated blood urea and
creatinine levels. Acute renal failure can be reversed if diagnosed early. Acute renal failure
can be caused by severe hypotension or severe glomerular disease. Diagnostic tests include
BUN and plasma creatinine level tests. It is considered to be chronic renal failure if the
decline of renal function to less than 25%.

8.7 Diabetes Insipidus

This is caused by the deficiency of or decrease of ADH. The person with (DI) has the inability
to concentrate their urine in water restriction, in turn they will void up 3 to 20 liters/day.
There are two forms of (DI), neurogenic, and nephrogenic. In nephrogenic (DI) the kidneys
do not respond to ADH. Usually the nephrogenic (DI) is characterized by the impairment
of the urine concentrating capability of the kidney along with concentration of water. The
cause may be a genetic trait, electrolyte disorder, or side effect of drugs such as lithium. In
the neurogenic (DI), it is usually caused by head injury near the hypophysisal tract.

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8.8 Urinary tract infections (UTI's)

The second most common type of bacterial infections seen by health care providers is UTI's.
Out of all the bacterias that colonize and cause urinary tract infections the big gun is
Escherichia coli. In the hospital indwelling catheters and straight catheterizing predispose
the opportunity for urinary tract infections. In females there are three stages in life that
predispose urinary tract infections, that is menarche, manipulation between intercourse,
and menopause. However, a small percentage of men and children will get urinary tract
infections. In men it is usually due to the prostate gland growth which usually occurs in
older age men. In children it can occur 3% to 5% in girls and 1% in boys, uncircumcised
boys it is more common than circumcised ones to have a urinary tract infection, in girls
it may be the result of onset of toilet training, some predispositions for getting urinary
tract infection include family history and urinary tract anomalies. In neonates urinary tract
infections is most common when bacteremia is present.

8.9 Dialysis and Kidney Transplant

Figure 83

Plugged into dialysis

Generally, humans can live normally with just one kidney. Only when the amount of
functioning kidney tissue is greatly diminished will renal failure develop. If renal function is
impaired, various forms of medications are used, while others are contraindicated. Provided
that treatment is begun early, it may be possible to reverse chronic kidney failure due
to diabetes or high blood pressure. If creatinine clearance (a measure of renal function)
has fallen very low ("end-stage renal failure"), or if the renal dysfunction leads to severe
symptoms, dialysis is commenced. Dialysis is a medical procedure, performed in various
different forms, where the blood is filtered outside of the body.
Kidney transplantation is the only cure for end stage renal failure; dialysis, is a supportive
treatment; a form of "buying time" to bridge the inevitable wait for a suitable organ.
The first successful kidney transplant was announced on March 4, 1954 at Peter Bent
Brigham Hospital in Boston. The surgery was performed by Dr. Joseph E. Murray, who
was awarded the Nobel Prize in Medicine in 1990 for this feat.

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Review Questions
There are two types of kidney transplants: living donor transplant and a cadaveric (dead
donor) transplant. When a kidney from a living donor, usually a blood relative, is transplanted into the patient's body, the donor's blood group and tissue type must be judged
compatible with the patient's, and extensive medical tests are done to determine the health
of the donor. Before a cadaveric donor's organs can be transplanted, a series of medical tests
have to be done to determine if the organs are healthy. Also, in some countries, the family
of the donor must give its consent for the organ donation. In both cases, the recipient of the
new organ needs to take drugs to suppress their immune system to help prevent their body
from rejecting the new kidney.

8.10 Review Questions

Answers for these questions can be found here1
1.While reading a blood test I notice a high level of creatinine, I could assume from this that
A) There is a possibility of a UTI
B) There is a possibility of diabetes
C) There is a possibility of kidney failure
D) There is nothing wrong, this is normal
2.Direct control of water excretion in the kidneys is controlled by
A) Anti-diuretic hormone
B) The medulla oblongata
C) Blood plasma
D) Sodium amounts in the blood
3. Nephrons
A) Eliminate wastes from the body
B) Regulate blood volume and pressure
C) Control levels of electrolytes and metabolites
D) Regulate blood pH
E) All of the above
4. If I am dehydrated, my body will increase
A) ATP
B) ADP
C) Diluted urine

http://en.wikibooks.org/wiki/Human_Physiology/Appendix_1:_answers_to_review_
questions#The_Urinary_System

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D) ADH
5.Which part of the nephron removes water, ions and nutrients from the blood?
A ) vasa recta
B ) loop of henle
C ) proximal convuluted tubule
D ) peritubular capillaries
E ) glomerulus
6.Kidneys have a direct effect on which of the following
A ) Blood pressure
B ) How much water a person excretes
C ) Total blood volume
D ) pH
E ) all of the above
7. Why do substances in the glomerulus enter the Bowman's capsule?
A ) the magnetic charge of the Bowman's capsule attracts the substances
B ) the substances are actively transported into the Bowman's capsule
C ) blood pressure of the glomerulus is so great that most substances in blood move into
capsule
D ) little green men force it in with their ray guns
8. What happens in tubular excretion?
A ) urine bonds are formed between the wastes
B ) wastes are diffused from the tubule
C ) wastes move into the distal convoluted tubule from the blood
D ) blood pressure forces wastes away from the kidney
9. The countercurrent exchange system includes_________and_________.
A ) glomerulus and macula densa
B ) proximal convoluted tubule and distal convoluted tubule
C ) loop of Henle and collecting tubule
D ) afferent arteriole and efferent arteriole
E ) ureters and bladder
10. The function of the loop of the nephron in the process of urine formation is:
A ) reabsorption of water

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Glossary
B ) production of filtrate
C ) reabsorption of solutes
D ) secretion of solutes
11. Name the six important roles of the kidneys.

8.11 Glossary
Antidiuretic: lessening or decreasing of urine production or an agent that decreases the
release of urine.
Catheterisation: a catheter is a tube that can be inserted into a body cavity, duct or vessel.
Catheters thereby allow drainage or injection of fluids or access by surgical instruments. The
process of inserting a catheter is catheterisation. In most uses a catheter is a thin, flexible
tube: a "soft" catheter; in some uses, it is a larger, solid tube: a "hard" catheter.
Dehydration: condition resulting from excessive loss of body fluid.
Diabetes: a general term for a disease characterized by the begining stages and onset of
renal failure. It is derived from the Greek word diabanein, that literally means "passing
through," or "siphon", a reference to one of diabetes' major symptomsexcessive urine
production.
Diuresis: secretion and passage of large amounts of urine.
Diuretic: increasing of urine production, or an agent that increases the production of urine.
Erythropoietin: hormone that stimulates stem cells in the bone marrow to produce red
blood cells
Fibrous Capsule: the kidney's loose connective tissue
Glomerulus: capillary tuft that receives its blood supply from an afferent arteriole of the
renal circulation.
Gluconeogenesis: the cycle of producing a glucose form fat or protein; preformed by the
kidney in times of long fasting, initially gluconeogenesis is preformed by the liver
Juxtaglomerular (JG) cells: Renin-secreting cells that are in contact with the macula
densa and the afferent arterioles of the renal nephron.
Juxtaglomerular apparatus (JGA): A site of juxtaglomerular cells connecting with
the macula densa where renin is secreted and sensor for control of secretion of golmerular
filtration rate.
Loop of Henle/ Nephron Loop: u-shaped tube that consists of a descending limb
and ascending limb; primary role is to concentrate the salt in the interstitium, the tissue
surrounding the loop
Medullary Pyramids or Renal Pyramids: the cone shaped masses in the kidney
Micturition: another name for excretions

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Nephron: basic structural and functional unit of the kidney; chief function is to regulate
water and soluble substances by filtering the blood, reabsorbing what is needed and excreting
the rest as urine
Podocytes: filtration membrane, in the visceral layer of the bowman's capsule
Renal Calculi: kidney stones, solid crystals of dissolved minerals in urine found inside the
kidneys
Renal Cortex: outer portion of the kidney
Renal Lobe: each pyramid together with the associated overlying cortex
Renal Pelvis: a central space, or cavity that transmits urine to the urinary bladder via
the ureter
Renin: hormone released by the Juxtaglomerular (JG) cells of the kidneys when blood
pressure falls
TURP: transurethral resection of the prostate. During TURP, an instrument is inserted
up the urethra to remove the section of the prostate that is blocking urine flow. This is
most commonly caused by benign prostatic hyperplasia (BPH). A TURP usually requires
hospitalization and is done using a general or spinal anesthetic. It is now the most common
surgery used to remove part of an enlarged prostate.
Urethra: a muscular tube that connects the bladder with the outside of the body
Ureters: two tubes that drain urine from the kidneys to the bladder
Urine: liquid produced by the kidneys, collected in the bladder and excreted through the
urethra
Urinary Bladder: a hollow, muscular and distensible or elastic organ that sits on the
pelvic floor
Urinary System: a group of organs in the body concerned with filtering out excess fluid
and other substances from the bloodstream

8.12 References
Graaff, Van De (2002). "Human Anatomy, Sixth Edition". New York: McGraw-Hill.
Mader, Sylvia S. (2004). Human Biology. New York: McGraw-Hill.
Smith, Peter (1998). Internet reference, http://www.liv.ac.uk/~petesmif/teaching/
1bds_mb/notes/homeo/kidney.htm. Department of Clinical Dental Sciences,The University of Liverpool.
McCance, Katherine L., Heuther, Sue E. (1994). "Pathophysiology: The Biological Basis
for Disease In Adults and Children, Second Edition". Mosby-Year Book, Inc.

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9 The Respiritory System

The Respiratory System is crucial to every human being. Without it, we would cease to
live outside of the womb. Let us begin by taking a look at the structure of the respiratory
system and how vital it is to life. During inhalation or exhalation air is pulled towards or
away from the lungs, by several cavities, tubes, and openings.
The organs of the respiratory system make sure that oxygen enters our bodies and carbon
dioxide leaves our bodies.
The respiratory tract is the path of air from the nose to the lungs. It is divided into two
sections: Upper Respiratory Tract and the Lower Respiratory Tract. Included in
the upper respiratory tract are the Nostrils, Nasal Cavities, Pharynx, Epiglottis, and
the Larynx. The lower respiratory tract consists of the Trachea, Bronchi, Bronchioles,
and the Lungs.
As air moves along the respiratory tract it is warmed, moistened and filtered.

Figure 84 The lungs flank the heart and great

vessels in the chest cavity. (Source: Gray's Anatomy of
the Human Body, 20th ed. 1918.)

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9.1 Functions
In this chapter we will discuss the four processes of respiration. They are:
1. BREATHING or ventilation
2. EXTERNAL RESPIRATION, which is the exchange of gases (oxygen and carbon
dioxide) between inhaled air and the blood.
3. INTERNAL RESPIRATION, which is the exchange of gases between the blood
and tissue fluids.
4. CELLULAR RESPIRATION
In addition to these main processes, the respiratory system serves for:
REGULATION OF BLOOD pH, which occurs in coordination with the kidneys,
and as a
DEFENSE AGAINST MICROBES
Control of body temperature due to loss of evaporate during expiration

9.2 Breathing and Lung Mechanics

Ventilation is the exchange of air between the external environment and the alveoli. Air
moves by bulk flow from an area of high pressure to low pressure. All pressures in the
respiratory system are relative to atmospheric pressure (760mmHg at sea level). Air will
move in or out of the lungs depending on the pressure in the alveoli. The body changes the
pressure in the alveoli by changing the volume of the lungs. As volume increases pressure
decreases and as volume decreases pressure increases. There are two phases of ventilation;
inspiration and expiration. During each phase the body changes the lung dimensions to
produce a flow of air either in or out of the lungs.
The body is able to stay at the dimensions of the lungs because of the relationship of the
lungs to the thoracic wall. Each lung is completely enclosed in a sac called the pleural sac.
Two structures contribute to the formation of this sac. The parietal pleura is attached to the
thoracic wall where as the visceral pleura is attached to the lung itself. In-between these two
membranes is a thin layer of intrapleural fluid. The intrapleural fluid completely surrounds
the lungs and lubricates the two surfaces so that they can slide across each other. Changing
the pressure of this fluid also allows the lungs and the thoracic wall to move together during
normal breathing. Much the way two glass slides with water in-between them are difficult
to pull apart, such is the relationship of the lungs to the thoracic wall.
The rhythm of ventilation is also controlled by the "Respiratory Center" which is located
largely in the medulla oblongata of the brain stem. This is part of the autonomic system and
as such is not controlled voluntarily (one can increase or decrease breathing rate voluntarily,
but that involves a different part of the brain). While resting, the respiratory center sends
out action potentials that travel along the phrenic nerves into the diaphragm and the external
intercostal muscles of the rib cage, causing inhalation. Relaxed exhalation occurs between
impulses when the muscles relax. Normal adults have a breathing rate of 12-20 respirations
per minute.

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9.2.1 The Pathway of Air

When one breathes air in at sea level, the inhalation is composed of different gases. These
gases and their quantities are Oxygen which makes up 21%, Nitrogen which is 78%, Carbon
Dioxide with 0.04% and others with significantly smaller portions.

Figure 85

Diagram of the Pharynx.

In the process of breathing, air enters into the nasal cavity through the nostrils and is
filtered by coarse hairs (vibrissae) and mucous that are found there. The vibrissae filter
macroparticles, which are particles of large size. Dust, pollen, smoke, and fine particles are
trapped in the mucous that lines the nasal cavities (hollow spaces within the bones of the
skull that warm, moisten, and filter the air). There are three bony projections inside the
nasal cavity. The superior, middle, and inferior nasal conchae. Air passes between
these conchae via the nasal meatuses.
Air then travels past the nasopharynx, oropharynx, and laryngopharynx, which are the three
portions that make up the pharynx. The pharynx1 is a funnel-shaped tube that connects
our nasal and oral cavities to the larynx. The tonsils which are part of the lymphatic
system, form a ring at the connection of the oral cavity and the pharynx. Here, they protect
against foreign invasion of antigens. Therefore the respiratory tract aids the immune system
through this protection. Then the air travels through the larynx. The larynx closes at the
epiglottis to prevent the passage of food or drink as a protection to our trachea and lungs.

http://en.wikipedia.org/wiki/pharynx

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The larynx is also our voicebox; it contains vocal cords, in which it produces sound. Sound
is produced from the vibration of the vocal cords when air passes through them.
The trachea, which is also known as our windpipe, has ciliated cells and mucous secreting
cells lining it, and is held open by C-shaped cartilage rings. One of its functions is similar
to the larynx and nasal cavity, by way of protection from dust and other particles. The dust
will adhere to the sticky mucous and the cilia helps propel it back up the trachea, to where
it is either swallowed or coughed up. The mucociliary escalator extends from the top of
the trachea all the way down to the bronchioles, which we will discuss later. Through the
trachea, the air is now able to pass into the bronchi.

9.2.2 Inspiration
Inspiration is initiated by contraction of the diaphragm and in some cases the
intercostals muscles when they receive nervous impulses. During normal quiet breathing,
the phrenic nerves stimulate the diaphragm to contract and move downward
into the abdomen. This downward movement of the diaphragm enlarges the thorax.
When necessary, the intercostal muscles also increase the thorax by contacting and drawing
the ribs upward and outward.
As the diaphragm contracts inferiorly and thoracic muscles pull the chest wall outwardly, the
volume of the thoracic cavity increases. The lungs are held to the thoracic wall by negative
pressure in the pleural cavity, a very thin space filled with a few milliliters of lubricating
pleural fluid. The negative pressure in the pleural cavity is enough to hold the lungs open
in spite of the inherent elasticity of the tissue. Hence, as the thoracic cavity increases in
volume the lungs are pulled from all sides to expand, causing a drop in the pressure (a
partial vacuum) within the lung itself (but note that this negative pressure is still not as
great as the negative pressure within the pleural cavity--otherwise the lungs would pull away
from the chest wall). Assuming the airway is open, air from the external environment then
follows its pressure gradient down and expands the alveoli of the lungs, where gas exchange
with the blood takes place. As long as pressure within the alveoli is lower than atmospheric
pressure air will continue to move inwardly, but as soon as the pressure is stabilized air
movement stops.

9.2.3 Expiration
During quiet breathing, expiration is normally a passive process and does not require muscles
to work (rather it is the result of the muscles relaxing). When the lungs are stretched and
expanded, stretch receptors within the alveoli send inhibitory nerve impulses to the medulla
oblongata, causing it to stop sending signals to the rib cage and diaphragm to contract.
The muscles of respiration and the lungs themselves are elastic, so when the diaphragm and
intercostal muscles relax there is an elastic recoil, which creates a positive pressure (pressure
in the lungs becomes greater than atmospheric pressure), and air moves out of the lungs by
flowing down its pressure gradient.
Although the respiratory system is primarily under involuntary control, and regulated by the
medulla oblongata, we have some voluntary control over it also. This is due to the higher
brain function of the cerebral cortex.

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When under physical or emotional stress, more frequent and deep breathing is needed, and
both inspiration and expiration will work as active processes. Additional muscles in the
rib cage forcefully contract and push air quickly out of the lungs. In addition to deeper
breathing, when coughing or sneezing we exhale forcibly. Our abdominal muscles will
contract suddenly (when there is an urge to cough or sneeze), raising the abdominal pressure.
The rapid increase in pressure pushes the relaxed diaphragm up against the pleural cavity.
This causes air to be forced out of the lungs.
Another function of the respiratory system is to sing and to speak. By exerting conscious
control over our breathing and regulating flow of air across the vocal cords we are able to
create and modify sounds.

9.2.4 Lung Compliance

Lung Compliance is the magnitude of the change in lung volume produced by a change
in pulmonary pressure. Compliance can be considered the opposite of stiffness. A low
lung compliance would mean that the lungs would need a greater than average change in
intrapleural pressure to change the volume of the lungs. A high lung compliance would
indicate that little pressure difference in intrapleural pressure is needed to change the
volume of the lungs. More energy is required to breathe normally in a person with low lung
compliance. Persons with low lung compliance due to disease therefore tend to take shallow
breaths and breathe more frequently.
Determination of Lung Compliance Two major things determine lung compliance. The
first is the elasticity of the lung tissue. Any thickening of lung tissues due to disease will
decrease lung compliance. The second is surface tensions at air water interfaces in the alveoli.
The surface of the alveoli cells is moist. The attractive force, between the water cells on the
alveoli, is called surface tension. Thus, energy is required not only to expand the tissues of
the lung but also to overcome the surface tension of the water that lines the alveoli.
To overcome the forces of surface tension, certain alveoli cells (Type II pneumocytes) secrete
a protein and lipid complex called ""Surfactant, which acts like a detergent by disrupting
the hydrogen bonding of water that lines the alveoli, hence decreasing surface tension.

9.2.5 Control of respiration

central control
Peripheral control
CO2 is converted to HCO3 ; most CO2 produced at the tissue cells is carried to lungs in the
form of HCO3
CO2 & H2 O form carbonic acid (H2 CO3 )
changes to H CO3 & H+ ions
result is H+ ions are buffered by plasma proteins

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9.3 Respiratory System: Upper and Lower Respiratory

Tracts
For the sake of convenience, we will divide the respiratory system in to the upper and lower
respiratory tracts:

9.3.1 Upper Respiratory Tract

The upper respiratory tract consists of the nose and the pharynx. Its primary function is to
receive the air from the external environment and filter, warm, and humidify it before it
reaches the delicate lungs where gas exchange will occur.
Air enters through the nostrils of the nose and is partially filtered by the nose hairs, then
flows into the nasal cavity. The nasal cavity is lined with epithelial tissue, containing blood
vessels, which help warm the air; and secrete mucous, which further filters the air. The
endothelial lining of the nasal cavity also contains tiny hairlike projections, called cilia. The
cilia serve to transport dust and other foreign particles, trapped in mucous, to the back of
the nasal cavity and to the pharynx. There the mucus is either coughed out, or swallowed
and digested by powerful stomach acids. After passing through the nasal cavity, the air
flows down the pharynx to the larynx.

9.3.2 Lower Respiratory Tract

The lower respiratory tract starts with the larynx, and includes the trachea, the two bronchi
that branch from the trachea, and the lungs themselves. This is where gas exchange actually
takes place.
1. Larynx
The larynx (plural larynges), colloquially known as the voice box, is an organ in our neck
involved in protection of the trachea and sound production. The larynx houses the vocal
cords, and is situated just below where the tract of the pharynx splits into the trachea and
the esophagus. The larynx contains two important structures: the epiglottis and the vocal
cords.
The epiglottis is a flap of cartilage located at the opening to the larynx. During swallowing,
the larynx (at the epiglottis and at the glottis) closes to prevent swallowed material from
entering the lungs; the larynx is also pulled upwards to assist this process. Stimulation of
the larynx by ingested matter produces a strong cough reflex to protect the lungs. Note:
choking occurs when the epiglottis fails to cover the trachea, and food becomes lodged in
our windpipe.
The vocal cords consist of two folds of connective tissue that stretch and vibrate when
air passes through them, causing vocalization. The length the vocal cords are stretched
determines what pitch the sound will have. The strength of expiration from the lungs also
contributes to the loudness of the sound. Our ability to have some voluntary control over
the respiratory system enables us to sing and to speak. In order for the larynx to function
and produce sound, we need air. That is why we can't talk when we're swallowing.

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1. Trachea
2. Bronchi
3. Lungs

9.4 Homeostasis and Gas Exchange

Figure 86

Gas exchange

Homeostasis is maintained by the respiratory system in two ways: gas exchange and
regulation of blood pH. Gas exchange is performed by the lungs by eliminating carbon
dioxide, a waste product given off by cellular respiration. As carbon dioxide exits the body,
oxygen needed for cellular respiration enters the body through the lungs. ATP, produced by
cellular respiration, provides the energy for the body to perform many functions, including
nerve conduction and muscle contraction. Lack of oxygen affects brain function, sense of
judgment, and a host of other problems.

9.4.1 Gas Exchange

Gas exchange in the lungs and in the alveoli is between the alveolar air and the blood in the
pulmonary capillaries. This exchange is a result of increased concentration of oxygen, and a
decrease of C02. This process of exchange is done through diffusion.

9.4.2 External Respiration

External respiration is the exchange of gas between the air in the alveoli and the blood within
the pulmonary capillaries. A normal rate of respiration is 12-25 breaths per minute. In
external respiration, gases diffuse in either direction across the walls of the alveoli. Oxygen
diffuses from the air into the blood and carbon dioxide diffuses out of the blood into the air.
Most of the carbon dioxide is carried to the lungs in plasma as bicarbonate ions (HCO3-).
When blood enters the pulmonary capillaries, the bicarbonate ions and hydrogen ions are
converted to carbonic acid (H2CO3) and then back into carbon dioxide (CO2) and water.
This chemical reaction also uses up hydrogen ions. The removal of these ions gives the blood
a more neutral pH, allowing hemoglobin to bind up more oxygen. De-oxygenated blood
"blue blood" coming from the pulmonary arteries, generally has an oxygen partial pressure

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(pp) of 40 mmHg and CO2 pp of 45 mmHg. Oxygenated blood leaving the lungs via the
pulmonary veins has a O2 pp of 100 mmHg and CO2 pp of 40 mmHg. It should be noted
that alveolar O2 pp is 105 mmHg, and not 100 mmHg. The reason why pulmonary venous
return blood has a lower than expected O2 pp can be explained by "Ventilation Perfusion
Mismatch".

9.4.3 Internal Respiration

Internal respiration is the exchanging of gases at the cellular level.
The Passage Way From the Trachea to the Bronchioles
There is a point at the inferior portion of the trachea where it branches into two directions
that form the right and left primary bronchus. This point is called the Carina which is
the keel-like cartilage plate at the division point. We are now at the Bronchial Tree. It
is named so because it has a series of respiratory tubes that branch off into smaller and
smaller tubes as they run throughout the lungs.
Right and Left Lungs

Figure 87

Diagram of the lungs

The Right Primary Bronchus is the first portion we come to, it then branches off into the
Lobar (secondary) Bronchi, Segmental (tertiary) Bronchi, then to the Bronchioles

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which have little cartilage and are lined by simple cuboidal epithelium (See fig. 1). The
bronchi are lined by pseudostratified columnar epithelium. Objects will likely lodge here at
the junction of the Carina and the Right Primary Bronchus because of the vertical structure.
Items have a tendency to fall in it, where as the Left Primary Bronchus has more of a curve
to it which would make it hard to have things lodge there.
The Left Primary Bronchus has the same setup as the right with the lobar, segmental
bronchi and the bronchioles.
The lungs are attached to the heart and trachea through structures that are called the roots
of the lungs. The roots of the lungs are the bronchi, pulmonary vessels, bronchial vessels,
lymphatic vessels, and nerves. These structures enter and leave at the hilus of the lung
which is "the depression in the medial surface of a lung that forms the opening through
which the bronchus, blood vessels, and nerves pass" (medlineplus.gov).
There are a number of terminal bronchioles connected to respiratory bronchioles
which then advance into the alveolar ducts that then become alveolar sacs. Each
bronchiole terminates in an elongated space enclosed by many air sacs called alveoli which
are surrounded by blood capillaries. Present there as well, are Alveolar Macrophages,
they ingest any microbes that reach the alveoli. The Pulmonary Alveoli are microscopic,
which means they can only be seen through a microscope, membranous air sacs within the
lungs. They are units of respiration and the site of gas exchange between the respiratory
and circulatory systems.

9.4.4 Cellular Respiration

First the oxygen must diffuse from the alveolus into the capillaries. It is able to do this
because the capillaries are permeable to oxygen. After it is in the capillary, about 5% will be
dissolved in the blood plasma. The other oxygen will bind to red blood cells. The red blood
cells contain hemoglobin that carries oxygen. Blood with hemoglobin is able to transport 26
times more oxygen than plasma without hemoglobin. Our bodies would have to work much
harder pumping more blood to supply our cells with oxygen without the help of hemoglobin.
Once it diffuses by osmosis it combines with the hemoglobin to form oxyhemoglobin.
Now the blood carrying oxygen is pumped through the heart to the rest of the body. Oxygen
will travel in the blood into arteries, arterioles, and eventually capillaries where it will be
very close to body cells. Now with different conditions in temperature and pH (warmer and
more acidic than in the lungs), and with pressure being exerted on the cells, the hemoglobin
will give up the oxygen where it will diffuse to the cells to be used for cellular respiration,
also called aerobic respiration. Cellular respiration is the process of moving energy from
one chemical form (glucose) into another (ATP), since all cells use ATP for all metabolic
reactions.
It is in the mitochondria of the cells where oxygen is actually consumed and carbon dioxide
produced. Oxygen is produced as it combines with hydrogen ions to form water at the
end of the electron transport chain (see chapter on cells). As cells take apart the carbon
molecules from glucose, these get released as carbon dioxide. Each body cell releases carbon
dioxide into nearby capillaries by diffusion, because the level of carbon dioxide is higher in
the body cells than in the blood. In the capillaries, some of the carbon dioxide is dissolved

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in plasma and some is taken by the hemoglobin, but most enters the red blood cells where
it binds with water to form carbonic acid. It travels to the capillaries surrounding the lung
where a water molecule leaves, causing it to turn back into carbon dioxide. It then enters
the lungs where it is exhaled into the atmosphere.

9.5 Lung Capacity

Figure 88
The normal volume moved in or out of the lungs during quiet breathing is called tidal
volume. When we are in a relaxed state, only a small amount of air is brought in and out,
about 500 mL. You can increase both the amount you inhale, and the amount you exhale,
by breathing deeply. Breathing in very deeply is Inspiratory Reserve Volume and can
increase lung volume by 2900 mL, which is quite a bit more than the tidal volume of 500 mL.
We can also increase expiration by contracting our thoracic and abdominal muscles. This
is called expiratory reserve volume and is about 1400 ml of air. Vital capacity is the
total of tidal, inspiratory reserve and expiratory reserve volumes; it is called vital capacity
because it is vital for life, and the more air you can move, the better off you are. There are
a number of illnesses that we will discuss later in the chapter that decrease vital capacity.
Vital Capacity can vary a little depending on how much we can increase inspiration by
expanding our chest and lungs. Some air that we breathe never even reaches the lungs!

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Stimulation of Breathing
Instead it fills our nasal cavities, trachea, bronchi, and bronchioles. These passages aren't
used in gas exchange so they are considered to be dead air space. To make sure that the
inhaled air gets to the lungs, we need to breathe slowly and deeply. Even when we exhale
deeply some air is still in the lungs,(about 1000 ml) and is called residual volume. This air
isn't useful for gas exchange. There are certain types of diseases of the lung where residual
volume builds up because the person cannot fully empty the lungs. This means that the
vital capacity is also reduced because their lungs are filled with useless air.

9.6 Stimulation of Breathing

There are two pathways of motor neuron stimulation of the respiratory muscles. The first
is the control of voluntary breathing by the cerebral cortex. The second is involuntary
breathing controlled by the medulla oblongata.
There are chemoreceptors in the aorta, the carotid body of carotid arteries, and in the
medulla oblongata of the brainstem that are sensitive to pH. As carbon dioxide levels increase
there is a buildup of carbonic acid, which releases hydrogen ions and lowers pH. Thus, the
chemoreceptors do not respond to changes in oxygen levels (which actually change much
more slowly), but to pH, which is dependent upon plasma carbon dioxide levels. In other
words, CO2 is the driving force for breathing. The receptors in the aorta and the
carotid sinus initiate a reflex that immediately stimulates breathing rate and the receptors
in the medulla stimulate a sustained increase in breathing until blood pH returns to normal.
This response can be experienced by running a 100 meter dash. During this exertion (or any
other sustained exercise) your muscle cells must metabolize ATP at a much faster rate than
usual, and thus will produce much higher quantities of CO2. The blood pH drops as CO2
levels increase, and you will involuntarily increase breathing rate very soon after beginning
the sprint. You will continue to breathe heavily after the race, thus expelling more carbon
dioxide, until pH has returned to normal. Metabolic acidosis therefore is acutely corrected
by respiratory compensation (hyperventilation).

9.7 Regulation of Blood pH

Many of us are not aware of the importance of maintaining the acid/base balance of our
blood. It is vital to our survival. Normal blood pH is set at 7.4, which is slightly alkaline or
"basic". If the pH of our blood drops below 7.2 or rises above 7.6 then very soon our brains
would cease functioning normally and we would be in big trouble. Blood pH levels below
6.9 or above 7.9 are usually fatal if they last for more than a short time. Another wonder of
our amazing bodies is the ability to cope with every pH change large or small. There are
three factors in this process: the lungs, the kidneys and buffers.
So what exactly is pH? pH is the concentration of hydrogen ions (H+). Buffers are molecules
which take in or release ions in order to maintain the H+ ion concentration at a certain level.
When blood pH is too low and the blood becomes too acidic (acidosis), the presence of too
many H+ ions is to blame. Buffers help to soak up those extra H+ ions. On the other hand,
the lack of H+ ions causes the blood to be too basic (alkalosis). In this situation, buffers

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release H+ ions. Buffers function to maintain the pH of our blood by either donating or
grabbing H+ ions as necessary to keep the number of H+ ions floating around the blood at
just the right amount.
The most important buffer we have in our bodies is a mixture of carbon dioxide (CO2) and
bicarbonate ion (HCO3). CO2 forms carbonic acid (H2CO3) when it dissolves in water and
acts as an acid giving up hydrogen ions (H+) when needed. HCO3 is a base and soaks up
hydrogen ions (H+) when there are too many of them. In a nutshell, blood pH is determined
by a balance between bicarbonate and carbon dioxide.
Bicarbonate Buffer System. With this important system our bodies maintain homeostasis. (Note that H2CO3 is Carbonic Acid and HCO3 is Bicarbonate)
CO2 + H2O <---> H2CO3 <---> (H+) + HCO3
If pH is too high, carbonic acid will donate hydrogen ions (H+) and pH will drop.
If pH is too low, bicarbonate will bond with hydrogen ions (H+) and pH will rise.
Too much CO2 or too little HCO3 in the blood will cause acidosis. The CO2 level is
increased when hypoventilation or slow breathing occurs, such as if you have emphysema or
pneumonia. Bicarbonate will be lowered by ketoacidosis, a condition caused by excess fat
metabolism (diabetes mellitus).
Too much HCO3 or too little CO2 in the blood will cause alkalosis. This condition is less
common than acidosis. CO2 can be lowered by hyperventilation.
So, in summary, if you are going into respiratory acidosis the above equation will move to
the right. The body's H+ and CO2 levels will rise and the pH will drop. To counteract this
the body will breathe more and release H+. In contrast, if you are going into respiratory
alkalosis the equation will move to the left. The body's H+ and CO2 levels will fall and the
pH will rise. So the body will try to breathe less to release HCO3. You can think of it like a
leak in a pipe: where ever there is a leak, the body will "fill the hole".

9.8 Problems Associated With the Respiratory Tract and

Breathing
The environment of the lung is very moist, which makes it a hospitable environment for
bacteria. Many respiratory illnesses are the result of bacterial or viral infection of the lungs.
Because we are constantly being exposed to harmful bacteria and viruses in our environment,
our respiratory health can be adversely affected. There are a number of illnesses and diseases
that can cause problems with breathing. Some are simple infections, and others are disorders
that can be quite serious.
Carbon Monoxide Poisoning: caused when carbon monoxide binds to hemoglobin in
place of oxygen. Carbon monoxide binds much tighter, without releasing, causing the
hemoglobin to become unavailable to oxygen. The result can be fatal in a very short amount
of time.
Mild Symptoms: flu like symptoms, dizziness, fatigue, headaches, nausea, and irregular
breathing

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Moderate Symptoms: chest pain, rapid heart beat, difficulty thinking, blurred vision,
shortness of breath and unsteadiness
Severe Symptoms: seizures, palpitations, disorientation, irregular heart beat, low blood
pressure, coma and death.
Pulmonary Embolism: blockage of the pulmonary artery (or one of its branches) by a
blood clot, fat, air or clumped tumor cells. By far the most common form of pulmonary
embolism is a thromboembolism, which occurs when a blood clot, generally a venous
thrombus, becomes dislodged from its site of formation and embolizes to the arterial blood
supply of one of the lungs.
Symptoms may include difficulty breathing, pain during breathing, and more rarely circulatory instability and death. Treatment, usually, is with anticoagulant medication.

9.9 Upper Respiratory Tract Infections

The upper respiratory tract consists of our nasal cavities, pharynx, and larynx. Upper
respiratory infections (URI) can spread from our nasal cavities to our sinuses, ears, and larynx.
Sometimes a viral infection can lead to what is called a secondary bacterial infection."Strep
throat" is a primary bacterial infection and can lead to an upper respiratory infection that
can be generalized or even systemic (affects the body as a whole). Antibiotics aren't used to
treat viral infections, but are successful in treating most bacterial infections, including strep
throat. The symptoms of strep throat can be a high fever, severe sore throat, white patches
on a dark red throat, and stomach ache.
Sinusitis
An infection of the cranial sinuses is called sinusitis. Only about 1-3% of URI's are
accompanied by sinusitis. This "sinus infection" develops when nasal congestion blocks off
the tiny openings that lead to the sinuses. Some symptoms include: post nasal discharge,
facial pain that worsens when bending forward, and sometimes even tooth pain can be a
symptom. Successful treatment depends on restoring the proper drainage of the sinuses.
Taking a hot shower or sleeping upright can be very helpful. Otherwise, using a spray
decongestant or sometimes a prescribed antibiotic will be necessary.
Otitis Media
Otitis media in an infection of the middle ear. Even though the middle ear is not part of the
respiratory tract, it is discussed here because it is often a complication seen in children who
has a nasal infection. The infection can be spread by way of the auditory (Eustachian)
tubethat leads form the nasopharynx to the middle ear. The main symptom is
usually pain. Sometimes though, vertigo, hearing loss, and dizziness may be
present. Antibiotics can be prescribed and tubes are placed in the eardrum to
prevent the buildup of pressure in the middle ear and the possibility of hearing
loss.

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Figure 89

Photo of Tonsillitis.

Tonsillitis
Tonsillitis occurs when the tonsils become swollen and inflamed. The tonsils located in
the posterior wall of the nasopharynx are often referred to as adenoids. If you suffer from
tonsillitis frequently and breathing becomes difficult, they can be removed surgically in a
procedure called a tonsillectomy.
Laryngitis
An infection of the larynx is called laryngitis. It is accompanied by hoarseness and being
unable to speak in an audible voice. Usually, laryngitis disappears with treatment of the
URI. Persistent hoarseness without a URI is a warning sign of cancer, and should be
checked into by your physician.

9.10 Lower Respiratory Tract Disorders

Lower respiratory tract disorders include infections, restrictive pulmonary disorders, obstructive pulmonary disorders, and lung cancer.

9.10.1 Lower Respiratory Infections

Acute bronchitis
An infection that is located in the primary and secondary bronchi is called bronchitis.
Most of the time, it is preceded by a viral URI that led to a secondary bacterial infection.

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Usually, a nonproductive cough turns into a deep cough that will expectorate mucus and
sometimes pus.
Pneumonia
A bacterial or viral infection in the lungs where the bronchi and the alveoli fill with a thick
fluid. Usually it is preceded by influenza. Symptoms of pneumonia include high fever &
chills, with headache and chest pain. Pneumonia can be located in several lobules of the
lung and obviously, the more lobules involved, the more serious the infection. It can be
caused by a bacteria that is usually held in check, but due to stress or reduced immunity
has gained the upper hand.

9.10.2 Restrictive Pulmonary Disorders

Pulmonary Fibrosis
Vital capacity is reduced in these types of disorders because the lungs have lost their
elasticity. Inhaling particles such as sand, asbestos, coal dust, or fiberglass can lead to
pulmonary fibrosis, a condition where fibrous tissue builds up in the lungs. This makes
it so our lungs cannot inflate properly and are always tending toward deflation.

Figure 90

Diagram of the lungs during an asthma attack.

Asthma
Asthma is a respiratory disease of the bronchi and bronchioles. The symptoms include
wheezing, shortness of breath, and sometimes a cough that will expel mucus. The airways
are very sensitive to irritants which can include pollen, dust, animal dander, and tobacco.
Even being out in cold air can be an irritant. When exposed to an irritant, the smooth
muscle in the bronchioles undergoes spasms. Most asthma patients have at least some
degree of bronchial inflammation that reduces the diameter of the airways and contributes
to the seriousness of the attack.

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9.11 Respiratory Distress Syndrome

Pathophysiology
At birth the pressure needed to expand the lungs requires high inspiratory pressure. In
the presence of normal surfactant levels the lungs retain as much as 40% of the residual
volume after the first breath and thereafter will only require far lower inspiratory pressures.
In the case of deficiency of surfactant the lungs will collapse between breaths, this makes
the infant work hard and each breath is as hard as the first breath. If this goes on further
the pulmonary capillary membranes become more permeable, letting in fibrin rich fluids
between the alveolar spaces and in turn forms a hyaline membrane. The hyaline membrane
is a barrier to gas exchange, this hyaline membrane then causes hypoxemia and carbon
dioxide retention that in turn will further impair surfactant production.
Etiology
Type two alveolar cells produce surfactant and do not develop until the 25th to the 28th week
of gestation, in this, respiratory distress syndrome is one of the most common respiratory
disease in premature infants. Furthermore, surfactant deficiency and pulmonary immaturity
together leads to alveolar collapse. Predisposing factors that contribute to poorly functioning
type II alveolar cells in a premature baby are if the child is a preterm male, white infants,
infants of mothers with diabetes, precipitous deliveries, cesarean section performed before
the 38th week of gestation. Surfactant synthesis is influenced by hormones, this ranges
form insulin and cortisol. Insulin inhibits surfactant production, explaining why infants of
mothers with diabetes type 1 are at risk of development of respiratory distress syndrome.
Cortisol can speed up maturation of type II cells and therefore production of surfactant.
Finally, in the baby delivered by cesarean section are at greater risk of developing respiratory
distress syndrome because the reduction of cortisol produced because the lack of stress that
happens during vaginal delivery, hence cortisol increases in high stress and helps in the
maturation of type II cells of the alveoli that cause surfactant.
Treatment
Today to prevent respiratory distress syndrome are animal sources and synthetic surfactants,
and administrated through the airways by an endotracheal tube and the surfactant is
suspended in a saline solution. Treatment is initiated post birth and in infants who are at
high risk for respiratory distress syndrome.

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Sleep Apnea

9.12 Sleep Apnea

Figure 91 CPAP is the most common

treatment for obstructive sleep apnea.

Sleep apnea or sleep apnoea is a sleep disorder characterized by pauses in breathing during
sleep. These episodes, called apneas (literally, "without breath"), each last long enough
so one or more breaths are missed, and occur repeatedly throughout sleep. The standard
definition of any apneic event includes a minimum 10 second interval between breaths, with
either a neurological arousal (3-second or greater shift in EEG frequency, measured at C3,
C4, O1, or O2), or a blood oxygen desaturation of 3-4 percent or greater, or both arousal and
desaturation. Sleep apnea is diagnosed with an overnight sleep test called polysomnogram.
One method of treating central sleep apnea is with a special kind of CPAP, APAP, or VPAP
machine with a Spontaneous Time (ST) feature. This machine forces the wearer to breathe
a constant number of breaths per minute.
(CPAP), or continuous positive airway pressure, in which a controlled air compressor
generates an airstream at a constant pressure. This pressure is prescribed by the patient's
physician, based on an overnight test or titration.

9.13 Nutrition for COPD (Chronic Obstructive Pulmonary

Disease) Patients
Nutrition is particularly important for ventilator-dependent patient. When metabolizing
macronutrients carbon dioxide and water are produced. The respiratory quotient (RQ) is a
ratio of produced carbon dioxide to amount consumed. Carbohydrates metabolism produces
the most amount of carbon dioxide so they have the highest (RQ). Fats produce the least
amount of carbon dioxide along with proteins. Protein has a slightly higher RQ ratio. It is
recommended that this kind of patient not exceed a 1.0 respiratory quotient (RQ). Lowering
carbohydrates and supplementing fat or protein in the diet might not result in maintaining
the desired outcome because, excess amounts fat or protein may also result in a respiratory
quotient (RQ) higher than 1.0.

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The Respiritory System

Please reference source and fact accuracy. It seems like by definition, it is impossible to
exceed a respiratory quotient (RQ) of 1.0. *

9.14 Case Study

Cystic Fibrosis
This disease is most common in Caucasians and will happen to 1 in every 2500 people. It is
most known for its effects on the respiratory tract although it does effect other systems as
well. The respiratory passages become clogged with a thick mucus that is difficult to expel
even with vigorous coughing. Breathing becomes difficult and affected individuals run the
risk of choking to death on their own secretions unless strenuous effort is made to clear the
lungs multiple times every day. Victims frequently will die in the 20's of pneumonia. All of
us secrete mucus by certain cells in the epithelium that line the respiratory passage ways. In
normal cases the cells also secrete a watery fluid that will dilute the mucus making it easier
to pass through the airways. In cystic fibrosis that secretion of watery fluid is impaired.
This makes the mucus thicker and difficult to clear from the passageways. A recent discovery
found that in cystic fibrosis is caused by a defect in a type of chloride protein found in
apical membranes of epithelial calls in the respiratory system and elsewhere. This defect
directly impedes the chlorine ions transport, which will then indirectly effect the transport
of potassium ions. This causes the epithelium, to not create its osmotic gradient necessary
for water secretion. It has been known for a long time that cystic fibrosis is caused by a
recessive gene inheritance. This gene codes for a portion of the chloride channel protein,
which can malfunction in a variety of ways, each with specific treatment required.

9.15 Glossary
9.16 References
Mader, Sylvia S. Human Biology. McGraw Hill Publishing, Burr Ridge, IL. 2004.
Van De Graaff, Kent M. Human Anatomy. McGraw Hill Publishing, Burr Ridge, IL.
2002.
Department of Environmental Biology, University of Adelaide, Adelaide, South Australia
Wikipedia:Lung2
Medlineplus.gov. Hilus. http://www2.merriam-webster.com/cgi-bin/mwmednlm?
book=Medical&va=hilum+
http://www.an-attorney-for-you.com/legal/carbon-monoxide.htm?gg&gclid=
CIbc3P_r-YYCFQwpNAodgmLHJA
www.ineedtoknow.com
"The respiratory system"Authors Mary Kitteredge,intro. by C. Everett Koop, M.D.,SC.D.,
foreword by Sandra Thurman

256

http://en.wikipedia.org/wiki/Lung

External Resources

9.17 External Resources

Eastern Kentucky University Gary Ritchison Lecture Notes: Human Respiration (includes
videos)3
pt:Fisiologia/Sistema respiratrio4

3
4

http://people.eku.edu/ritchisong/301notes6.htm
http://pt.wikibooks.org/wiki/Fisiologia%2FSistema%20respirat%F3rio

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10 The Gastrointestinal System

10.1 Introduction
Which organ is the most important organ in the body? Most people would say the heart or
the brain, completely overlooking the gastrointestinal tract (GI tract). Though definitely
not the most attractive organs in the body, they are certainly among the most important.
The 30+ foot long tube that goes from the mouth to the anus is responsible for the many
different body functions which will be reviewed in this chapter. The GI tract is imperative
for our well being and our life-long health. A non-functioning or poorly functioning GI tract
can be the source of many chronic health problems that can interfere with your quality of
life. In many instances the death of a person begins in the intestines.
The old saying "you are what you eat" perhaps would be more accurate if worded "you
are what you absorb and digest". Here we will be looking at the importance of these two
functions of the digestive system: digestion and absorption.
The Gastrointestinal System is responsible for the breakdown and absorption of various
foods and liquids needed to sustain life. Many different organs have essential roles in the
digestion of food, from the mechanical disrupting by the teeth to the creation of bile (an
emulsifier1 ) by the liver. Bile production of the liver plays a important role in digestion: from
being stored and concentrated in the gallbladder during fasting stages to being discharged
to the small intestine.
In order to understand the interactions of the different components we shall follow the food
on its journey through the human body. During digestion, two main processes occur at the
same time;
Mechanical Digestion: larger pieces of food get broken down into smaller pieces while
being prepared for chemical digestion. Mechanical digestion starts in the mouth and
continues into the stomach.
Chemical Digestion: starts in the mouth and continues into the intestines. Several
different enzymes break down macromolecules into smaller molecules that can be absorbed.
The GI tract starts with the mouth and proceeds to the esophagus, stomach, small intestine
(duodenum, jejunum, ileum), and then to the large intestine (colon), rectum, and terminates
at the anus. You could probably say the human body is just like a big donut. The GI tract
is the donut hole. We will also be discussing the pancreas and liver, and accessory organs of
the gastrointestinal system that contribute materials to the small intestine.

http://en.wikipedia.org/wiki/Emulsifier

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The Gastrointestinal System

10.2 Layers of the GI Tract

The GI tract is composed of four layers or also know as Tunics. Each layer has different
tissues and functions. From the inside out they are called: mucosa, submucosa, muscularis,
and serosa.
Mucosa: The mucosa is the absorptive and secretory layer. It is composed of simple
epithelium cells and a thin connective tissue. There are specialized goblet cells that secrete
mucus throughout the GI tract located within the mucosa. On the mucosa layer there are
Villi and Micro Villi.
Submucosa: The submucosa is relatively thick, highly vascular, and serves the mucosa.
The absorbed elements that pass through the mucosa are picked up from the blood vessels
of the submucosa. The submucosa also has glands and nerve plexuses.
Muscularis: The muscularis is responsible for segmental contractions and peristaltic
movement in the GI tract. The muscularis is composed of two layers of muscle: an inner
circular and outer longitudinal layer of smooth muscle. These muscles cause food to move
and churn with digestive enzymes down the GI tract.
Serosa: The last layer is a protective layer. It is composed of avascular connective tissue
and simple squamous epithelium. It secretes lubricating serous fluid. This is the visible
layer on the outside of the organs.

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Accessory Organs

10.3 Accessory Organs

Figure 92

Teeth, Tongue, and Salivary Glands

1.Salivary glands
Parotid gland, submandibular gland, sublingual gland
Exocrine gland that produces saliva which begins the process of digestion with amylase
2. Tongue
Manipulates food for chewing/swallowing
Main taste organ, covered in taste buds
3. Teeth
For chewing food up
4. Liver
Produces and excretes bile required for emulsifying fats. Some of the bile drains directly
into the duodenum and some is stored in the gall bladder.

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The Gastrointestinal System

Helps metabolize proteins, lipids, and carbohydrates.
Urea, chief end product of mammalian metabolism, is formed in liver from amino acids
and compounds of ammonia.
Breaks down insulin and other hormones.
Produces coagulation factors.
5. Gallbladder
Bile storage.
6. Pancreas
Exocrine functions: Digestive enzyme secretion.
Stores zymogens (inactive enzymes) that will be activated by the brush boarder
membrane in the small intestine when a person eats protein (amino acids).
Trypsinogen Trypsin: digests protein.
Chymotypsinogen Chymotrypsin: digests proteins.
Carboxypeptidases: digests proteins.
Lipase-lipid: digests fats.
Amylase: digests carbohydrates.
Endocrine functions: Hormone secretion.
Somatostatin: inhibits the function of insulin. Produced if the body is getting too
much glucose.
Glucagon: stimulates the stored glycogen in the liver to convert to glucose. Produced
if the body does not have enough glucose.
Insulin: made in the beta cells of the Islets of Langerhans of the pancreas. Insulin is a
hormone that regulates blood glucose.
7. Vermiform appendix
There are a few theories on what the appendix does.
Vestigal organ
Immune function
Helps maintain gut flora

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The Digestive System

10.4 The Digestive System

Figure 93

The first step in the digestive system can actually begin before the food is even in your
mouth. When you smell or see something that you just have to eat, you start to salivate in
anticipation of eating, thus beginning the digestive process.
Food is the body's source of fuel. Nutrients in food give the body's cells the energy they
need to operate. Before food can be used it has to be broken down into tiny little pieces so
it can be absorbed and used by the body. In humans, proteins need to be broken down into
amino acids, starches into sugars, and fats into fatty acids and glycerol.

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The Gastrointestinal System

During digestion two main processes occur at the same time:
Mechanical Digestion: larger pieces of food get broken down into smaller pieces while
being prepared for chemical digestion. Mechanical digestion starts in the mouth and
continues in to the stomach.
Chemical Digestion: several different enzymes break down macromolecules into smaller
molecules that can be more efficiently absorbed. Chemical digestion starts with saliva
and continues into the intestines.
The digestive system is made up by the alimentary canal, or the digestive tract, and other
abdominal organs that play a part in digestion such as the liver and the pancreas. The
alimentary canal is the long tube of organs that runs from the mouth (where the food enters)
to the anus (where indigestible waste leaves). The organs in the alimentary canal include
the mouth( for mastication),esophagus, stomach and the intestines. The average adult
digestive tract is about thirty feet (30') long. While in the digestive tract the food is really
passing through the body rather than being in the body. The smooth muscles of the tubular
digestive organs move the food efficiently along as it is broken down into absorb-able atoms
and molecules. During absorption, the nutrients that come from food (such as proteins, fats,
carbohydrates, vitamins, and minerals) pass through the wall of the small intestine and into
the bloodstream and lymph. In this way nutrients can be distributed throughout the rest
of the body. In the large intestine there is re absorption of water and absorption of some
minerals as feces are formed. The parts of the food that the body passes out through the
anus is known as feces.
Mastication
Digestion begins in the mouth. A brain reflex triggers the flow of saliva when we see or even
think about food. Saliva moistens the food while the teeth chew it up and make it easier to
swallow. Amylase, which is the digestive enzyme found in saliva, starts to break down starch
into simpler sugars before the food even leaves the mouth. The nervous pathway involved in
salivary excretion requires stimulation of receptors in the mouth, sensory impulses to the
brain stem, and parasympathetic impulses to salivary glands.
Swallowing your food happens when the muscles in your tongue and mouth move the food
into your pharynx. The pharynx, which is the passageway for food and air, is about five
inches (5") long. A small flap of skin called the epiglottis closes over the pharynx to prevent
food from entering the trachea and thus choking. For swallowing to happen correctly a
combination of 25 muscles must all work together at the same time. Salivary glands also
produce an estimated three liters of saliva per day.
Enzyme
Carbohydrate Digestion:
Salivary amylase
Pancreatic amylase
Maltase
Protein Digestion:
Pepsin
Trypsin
Peptidases
Nucleic Acid Digestion:

264

Produced In

Site of Release

pH Level

Salivary glands
Pancreas
Small intestine

Mouth
Small intestine
Small intestine

Neutral
Basic
Basic

Gastric glands
Pancreas
Small intestine

Stomach
Small intestine
Small intestine

Acidic
Basic
Basic

Esophagus
Enzyme
Nuclease
Nucleosidases
Fat Digestion:
Lipase

Produced In
Pancreas
Pancreas

Site of Release
Small intestine
Small intestine

pH Level
Basic
Basic

Pancreas

Small intestine

Basic

10.5 Esophagus

Figure 94
The esophagus (also spelled oesophagus/esophagus) or gullet is the muscular tube in
vertebrates through which ingested food passes from the throat to the stomach. The
esophagus is continuous with the laryngeal part of the pharynx at the level of the C6
vertebra. It connects the pharynx, which is the body cavity that is common to both
the digestive and respiratory systems behind the mouth, with the stomach, where the
second stage of digestion is initiated (the first stage is in the mouth with teeth and tongue
masticating food and mixing it with saliva).

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The Gastrointestinal System

After passing through the throat, the food moves into the esophagus and is pushed down
into the stomach by the process of peristalsis (involuntary wavelike muscle contractions
along the G.I. tract). At the end of the esophagus there is a sphincter that allows food into
the stomach then closes back up so the food cannot travel back up into the esophagus.
Histology
The esophagus is lined with mucus membranes, and uses peristaltic action to move swallowed
food down to the stomach.
The esophagus is lined by a stratified squamous epithelium, which is rapidly turned over,
and serves a protective effect due to the high volume transit of food, saliva, and mucus into
the stomach. The lamina propria of the esophagus is sparse. The mucus secreting glands
are located in the submucosa, and are connective structures called papillae.
The muscularis propria of the esophagus consists of striated muscle in the upper third
(superior) part of the esophagus. The middle third consists of a combination of smooth
muscle and striated muscle, and the bottom (inferior) third is only smooth muscle. The
distal end of the esophagus is slightly narrowed because of the thickened circular muscles.
This part of the esophagus is called the lower esophageal sphincter. This aids in keeping
food down and not being regurgitated.
The esophagus has a rich lymphatic drainage as well.

10.6 Stomach
The stomach is a thick walled organ that lies between the esophagus and the first part of
the small intestine (the duodenum). It is on the left side of the abdominal cavity, the fundus
of the stomach lying against the diaphragm. Lying beneath the stomach is the pancreas.
The greater omentum hangs from the greater curvature.
A mucous membrane lines the stomach which contains glands (with chief cells) that secrete
gastric juices, up to three quarts of this digestive fluid is produced daily. The gastric glands
begin secreting before food enters the stomach due to the parasympathetic impulses of the
vagus nerve, making the stomach also a storage vat for that acid.
The secretion of gastric juices occurs in three phases: cephalic, gastric, and intestinal. The
cephalic phase is activated by the smell and taste of food and swallowing. The gastric phase
is activated by the chemical effects of food and the distension of the stomach. The intestinal
phase blocks the effect of the cephalic and gastric phases. Gastric juice also contains an
enzyme named pepsin, which digests proteins, hydrochloric acid and mucus. Hydrochloric
acid causes the stomach to maintain a pH of about 2, which helps kill off bacteria that
comes into the digestive system via food.
The gastric juice is highly acidic with a pH of 1-3. It may cause or compound damage to the
stomach wall or its layer of mucus, causing a peptic ulcer. On the inside of the stomach there
are folds of skin call the gastric rugae. Gastric rugae make the stomach very extendable,
especially after a very big meal.

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Stomach

Figure 95

The stomach is divided into four sections, each of which has different cells and functions.
The sections are: 1) Cardiac region, where the contents of the esophagus empty into the
stomach, 2) Fundus, formed by the upper curvature of the organ, 3) Body, the main central
region, and 4) Pylorus or atrium, the lower section of the organ that facilitates emptying the
contents into the small intestine. Two smooth muscle valves, or sphincters, keep the contents
of the stomach contained. They are the: 1) Cardiac or esophageal sphincter, dividing the
tract above, and 2) Pyloric sphincter, dividing the stomach from the small intestine.
After receiving the bolus (chewed food) the process of peristalsis is started; mixed and
churned with gastric juices the bolus is transformed into a semi-liquid substance called
chyme. Stomach muscles mix up the food with enzymes and acids to make smaller digestible
pieces. The pyloric sphincter, a walnut shaped muscular tube at the stomach outlet, keeps
chyme in the stomach until it reaches the right consistency to pass into the small intestine.
The food leaves the stomach in small squirts rather than all at once.
Water, alcohol, salt, and simple sugars can be absorbed directly through the stomach wall.
However, most substances in our food need a little more digestion and must travel into the
intestines before they can be absorbed. When the stomach is empty it is about the size of
one fifth of a cup of fluid. When stretched and expanded, it can hold up to eight cups of
food after a big meal.
Gastric Glands
There are many different gastric glands and they secret many different chemicals. Parietal
cells secrete hydrochloric acid and intrinsic factor; chief cells secrete pepsinogen; goblet cells
secrete mucus; argentaffin cells secrete serotonin and histamine; and G cells secrete the
hormone gastrin.

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The Gastrointestinal System

Vessels and nerves

Figure 96

Nerves in the lower abdomen.

Arteries: The arteries supplying the stomach are the left gastric, the right gastric and
right gastroepiploic branches of the hepatic, and the left gastroepiploic and short gastric
branches of the lineal. They supply the muscular coat, ramify in the submucous coat, and
are finally distributed to the mucous membrane.
Capillaries: The arteries break up at the base of the gastric tubules into a plexus of
fine capillaries, which run upward between the tubules, anatomizing with each other, and
ending in a plexus of larger capillaries, which surround the mouths of the tubes, and also
form hexagonal meshes around the ducts.

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Stomach
Veins: From these the veins arise, and pursue a straight course downward, between the
tubules, to the submucous tissue; they end either in the lineal and superior mesenteric
veins, or directly in the portal vein.
Lymphatics: The lymphatics are numerous: They consist of a superficial and a deep set,
and pass to the lymph glands found along the two curvatures of the organ.
Nerves: The nerves are the terminal branches of the right and left urethra and other
parts, the former being distributed upon the back, and the latter upon the front part of
the organ. A great number of branches from the celiac plexus of the sympathetic are also
distributed to it. Nerve plexuses are found in the submucous coat and between the layers
of the muscular coat as in the intestine. From these plexuses fibrils are distributed to the
muscular tissue and the mucous membrane.
Disorders of the Stomach
Disorders of the stomach are common. There can be a lot of different causes with a variety
of symptoms. The strength of the inner lining of the stomach needs a careful balance of acid
and mucus. If there is not enough mucus in the stomach, ulcers, abdominal pain, indigestion,
heartburn, nausea and vomiting could all be caused by the extra acid.
Erosions, ulcers, and tumors can cause bleeding. When blood is in the stomach it starts the
digestive process and turns black. When this happens, the person can have black stool or
vomit. Some ulcers can bleed very slowly so the person won't recognize the loss of blood.
Over time, the iron in your body will run out, which in turn, will cause anemia.
There isn't a known diet to prevent against getting ulcers. A balanced, healthy diet is always
recommended. Smoking can also be a cause of problems in the stomach. Tobacco increases
acid production and damages the lining of the stomach. It is not a proven fact that stress
alone can cause an ulcer.
Histology of the human stomach
Like the other parts of the gastrointestinal tract, the stomach walls are made of a number
of layers.
From the inside to the outside, the first main layer is the mucosa. This consists of an
epithelium, the lamina propria underneath, and a thin bit of smooth muscle called the
muscularis mucosa.
The submucosa lies under this and consists of fibrous connective tissue, separating the
mucosa from the next layer, the muscularis externa. The muscularis in the stomach differs
from that of other GI organs in that it has three layers of muscle instead of two. Under
these muscle layers is the adventitia, layers of connective tissue continuous with the omenta.
The epithelium of the stomach forms deep pits, called fundic or oxyntic glands. Different
types of cells are at different locations down the pits. The cells at the base of these pits are
chief cells, responsible for production of pepsinogen, an inactive precursor of pepsin, which
degrades proteins. The secretion of pepsinogen prevents self-digestion of the stomach cells.
Further up the pits, parietal cells produce gastric acid and a vital substance, intrinsic factor.
The function of gastric acid is two fold 1) it kills most of the bacteria in food, stimulates
hunger, and activates pepsinogen into pepsin, and 2) denatures the complex protein molecule
as a precursor to protein digestion through enzyme action in the stomach and small intestines.

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The Gastrointestinal System

Near the top of the pits, closest to the contents of the stomach, there are mucous-producing
cells called goblet cells that help protect the stomach from self-digestion.
The muscularis externa is made up of three layers of smooth muscle. The innermost layer
is obliquely-oriented: this is not seen in other parts of the digestive system: this layer
is responsible for creating the motion that churns and physically breaks down the food.
The next layers are the square and then the longitudinal, which are present as in other
parts of the GI tract. The pyloric antrum which has thicker skin cells in its walls and
performs more forceful contractions than the fundus. The pylorus is surrounded by a thick
circular muscular wall which is normally tonically constricted forming a functional (if not
anatomically discrete) pyloric sphincter, which controls the movement of chyme.
Control of secretion and motility
The movement and the flow of chemicals into the stomach are controlled by both the nervous
system and by the various digestive system hormones.
The hormone gastrin causes an increase in the secretion of HCL, pepsinogen and intrinsic
factor from parietal cells in the stomach. It also causes increased motility in the stomach.
Gastrin is released by G-cells into the stomach. It is inhibited by pH normally less than 4
(high acid), as well as the hormone somatostatin.
Cholecystokinin (CCK) has most effect on the gall bladder, but it also decreases gastric
emptying. In a different and rare manner, secretin, produced in the small intestine, has
most effects on the pancreas, but will also diminish acid secretion in the stomach.
Gastric inhibitory peptide (GIP) and enteroglucagon decrease both gastric motility and
secretion of pepsin. Other than gastrin, these hormones act to turn off the stomach action.
This is in response to food products in the liver and gall bladder, which have not yet been
absorbed. The stomach needs only to push food into the small intestine when the intestine
is not busy. While the intestine is full and still digesting food, the stomach acts as a storage
for food.

270

Small Intestine

10.7 Small Intestine

Figure 97

Diagram showing the small intestine

The small intestine is the site where most of the chemical and mechanical digestion is carried
out. Tiny projections called villi line the small intestine which absorbs digested food into
the capillaries. Most of the food absorption takes place in the jejunum and the ileum.
The functions of a small intestine is, the digestion of proteins into peptides and amino acids
principally occurs in the stomach but some also occurs in the small intestine. Peptides
are degraded into amino acids; lipids (fats) are degraded into fatty acids and glycerol; and
carbohydrates are degraded into simple sugars.
The three main sections of the small intestine is The Duodenum, The Jejunum, The Ileum.

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The Gastrointestinal System

The Duodenum
In anatomy of the digestive system, the duodenum is a hollow jointed tube connecting the
stomach to the jejunum. It is the first and shortest part of the small intestine. It begins with
the duodenal bulb and ends at the ligament of Treitz. The duodenum is almost entirely retro
peritoneal. The duodenum is also where the bile and pancreatic juices enter the intestine.
The Jejunum
The Jejunum is a part of the small bowel, located between the distal end of duodenum
and the proximal part of ileum. The jejunum and the ileum are suspended by an extensive
mesentery giving the bowel great mobility within the abdomen. The inner surface of the
jejunum, its mucous membrane, is covered in projections called villi, which increase the
surface area of tissue available to absorb nutrients from the gut contents. It is different from
the ileum due to fewer goblet cells and generally lacks Peyer's patches.
The Ileum
Its function is to absorb vitamin B12 and bile salts. The wall itself is made up of folds, each
of which has many tiny finger-like projections known as villi, on its surface. In turn, the
epithelial cells which line these villi possess even larger numbers of micro villi. The cells
that line the ileum contain the protease and carbohydrate enzymes responsible for the final
stages of protein and carbohydrate digestion. These enzymes are present in the cytoplasm
of the epithelial cells. The villi contain large numbers of capillaries which take the amino
acids and glucose produced by digestion to the hepatic portal vein and the liver.
The terminal ileum continues to absorb bile salts, and is also crucial in the absorption of
fat-soluble vitamins (Vitamin A, D, E and K). For fat-soluble vitamin absorption to occur,
bile acids must be present.

272

Large Intestine

10.8 Large Intestine

Figure 98

Large Intestinal Tract

The large intestine (colon) extends from the end of the ileum to the anus. It is about 5
feet long, being one-fifth of the whole extent of the intestinal canal. It's caliber is largest
at the commencement at the cecum, and gradually diminishes as far as the rectum, where
there is a dilatation of considerable size just above the anal canal. It differs from the small
intestine in by the greater caliber, more fixed position, sacculated form, and in possessing
certain appendages to its external coat, the appendices epiploic. Further, its longitudinal
muscular fibers do not form a continuous layer around the gut, but are arranged in three
longitudinal bands or tni.
The large intestine is divided into the cecum, colon, rectum, and anal canal. In its course,
describes an arch which surrounds the convolutions of the small intestine. It commences
in the right iliac region, in a dilated part, the cecum. It ascends through the right lumbar
and hypochondriac regions to the under surface of the liver; here it takes a bend, the right
colic flexure, to the left and passes transversely across the abdomen on the confines of the
epigastric and umbilical regions, to the left hypochondriac region; it then bends again, the
left colic flexure, and descends through the left lumbar and iliac regions to the pelvis, where
it forms a bend called the sigmoid flexure; from this it is continued along the posterior wall
of the pelvis to the anus.
There are trillions of bacteria, yeasts, and parasites living in our intestines, mostly in the
colon. Over 400 species of organisms live in the colon. Most of these are very helpful to
our health, while the minority are harmful. Helpful organisms synthesize vitamins, like B12,

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The Gastrointestinal System

biotin, and vitamin K. They breakdown toxins and stop proliferation of harmful organisms.
They stimulate the immune system and produce short chain fatty acids (SCFAs) that are
required for the health of colon cells and help prevent colon cancer. There are many beneficial
bacteria but some of the most common and important are Lactobacillus Acidophilus and
various species of Bifidobacterium. These are available as "probiotics" from many sources.

10.9 Pancreas, Liver, and Gallbladder

The pancreas, liver, and gallbladder are essential for digestion. The pancreas produces
enzymes that help digest proteins, fats, and carbohydrates, the liver produces bile that helps
the body absorb fat, and the gallbladder stores the bile until it is needed. The enzymes and
bile travel through special channels called ducts and into the small intestine where they help
break down the food.
Pancreas
The pancreas is located posterior to the stomach and in close association with the duodenum.
In humans, the pancreas is a 6-10 inch elongated organ in the abdomen located retro
peritoneal. It is often described as having three regions: a head, body and tail. The
pancreatic head abuts the second part of the duodenum while the tail extends towards the
spleen. The pancreatic duct runs the length of the pancreas and empties into the second
part of the duodenum at the ampulla of Vater. The common bile duct commonly joins the
pancreatic duct at or near this point.
The pancreas is supplied arterially by the pancreaticoduodenal arteries, themselves branches
of the superior mesenteric artery of the hepatic artery (branch of celiac trunk from the
abdominal aorta). The superior mesenteric artery provides the inferior pancreaticoduodenal
arteries while the gastroduodenal artery (one of the terminal branches of the hepatic artery)
provides the superior pancreaticoduodenal artery. Venous drainage is via the pancreatic
duodenal veins which end up in the portal vein. The splenic vein passed posterior to the
pancreas but is said to not drain the pancreas itself. The portal vein is formed by the union
of the superior mesenteric vein and splenic vein posterior to the body of the pancreas. In
some people (as many as 40%) the inferior mesenteric vein also joins with the splenic vein
behind the pancreas, in others it simply joins with the superior mesenteric vein instead.
The function of the pancreas is to produce enzymes that break down all categories of digestible
foods (exocrine pancreas) and secrete hormones that affect carbohydrates metabolism
(endocrine pancreas).
Exocrine
The pancreas is composed of pancreatic exocrine cells, whose ducts are arranged in clusters
called acini (singular acinus). The cells are filled with secretory granules containing the
precursor digestive enzymes (mainly trypsinogen, chymotrypsinogen, pancreatic lipase, and
amylase) that are secreted into the lumen of the acinus. These granules are termed zymogen
granules (zymogen referring to the inactive precursor enzymes.) It is important to synthesize
inactive enzymes in the pancreas to avoid auto degradation, which can lead to pancreatitis.

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The pancreas is near the liver, and is the main source of enzymes for digesting fats (lipids)
and proteins - the intestinal walls have enzymes that will digest polysaccharides. Pancreatic
secretions from ductal cells contain bicarbonate ions and are alkaline in order to neutralize
the acidic chyme that the stomach churns out. Control of the exocrine function of the
pancreas are via the hormone gastrin, cholecystokinin and secretin, which are hormones
secreted by cells in the stomach and duodenum, in response to distension and/or food and
which causes secretion of pancreatic juices.
The two major proteases which the pancreas are trypsinogen and chymotrypsinogen. These
zymogens are inactivated forms of trypsin and chymotrypsin. Once released in the intestine, the enzyme enterokinase present in the intestinal mucosa activates trypsinogen by
cleaving it to form trypsin. The free trypsin then cleaves the rest of the trypsinogen and
chymotrypsinogen to their active forms.
Pancreatic secretions accumulate in intralobular ducts that drain the main pancreatic duct,
which drains directly into the duodenum.
Due to the importance of its enzyme contents, injuring the pancreas is a very dangerous
situation. A puncture of the pancreas tends to require careful medical intervention.
Endocrine
Scattered among the acini are the endocrine cells of the pancreas, in groups called the islets
of Langerhans. They are:
Insulin-producing beta cells (50-80% of the islet cells) Glucagon-releasing alpha cells (1520%) Somatostatin-producing delta cells (3-10%) Pancreatic polypeptide-containing PP cells
(remaining %)
The islets are a compact collection of endocrine cells arranged in clusters and cords and
are crisscrossed by a dense network of capillaries. The capillaries of the islets are lined by
layers of endocrine cells in direct contact with vessels, and most endocrine cells are in direct
contact with blood vessels, by either cytoplasmic processes or by direct apposition.
Liver
The liver is an organ in vertebrates, including human. It plays a major role in metabolism
and has a number of functions in the body including glycogen storage, plasma protein
synthesis, and drug detoxification. It also produces bile, which is important in digestion.
It performs and regulates a wide variety of high-volume biochemical reaction requiring
specialized tissues.
The liver normally weighs between 1.3 - 3.0 kilograms and is a soft, pinkish-brown "boomerang
shaped" organ. It is the second largest organ (the largest being the skin) and the largest
gland within the human body. its anatomical position in the body is immediately under the
diaphragm on the right side of the upper abdomen, The liver lies on the right side of the
stomach and makes a kind of bed for the gallbladder.
The liver is supplied by two main blood vessels on its right lobe: the hepatic artery and the
portal vein. The hepatic artery normally comes off the celiac trunk. The portal vein brings
venous blood from the spleen, pancreas, and small intestine, so that the liver can process
the nutrients and byproducts of food digestion. The hepatic veins drain directly into the
inferior vena cava.

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The bile produced in the liver is collected in bile canaliculi, which merge from bile ducts.
These eventually drain into the right and left hepatic ducts, which in turn merge to form
the common hepatic duct. The cystic duct (from the gallbladder) joins with the common
hepatic duct to form the common bile duct. Bile can either drain directly into the duodenum
via the common bile duct or be temporarily stored in the gallbladder via the cystic duct.
The common bile duct and the pancreatic duct enter the duodenum together at the ampulla
of Vater. The branching's of the bile ducts resemble those of a tree, and indeed term "biliary
tree" is commonly used in this setting.
The liver is among the few internal human organs capable of natural regeneration of lost
tissue: as little as 25% of remaining liver can regenerate into a whole liver again. This is
predominantly due to hepatocytes acting as unipotential stem cells. There is also some
evidence of bio potential stem cells, called oval cell, which can differentiate into either
hepatocytes or cholangiocytes (cells that line bile ducts).
The various functions of the liver are carried out by the liver cells or hepatocytes.
The liver produces and excretes bile requires for dissolving fats. Some of the bile drains
directly into the duodenum, and some is stored in the gallbladder
The liver performs several roles in carbohydrate metabolism:
gluconeogenesis (the formation of glucose from certain amino acids, lactate or glycerol)
Glycogenolysis (the formation of glucose from glycogen)
Glycogenesis (the formation of glycogen from glucose)
The breakdown of insulin and other hormones
The liver is responsible for the mainstay of protein metabolism.
The liver also performs several roles in lipid metabolism:
cholesterol synthesis
The production of triglycerides (fats)
The liver produces coagulation factors I (fibrinogen), II (prothrombin), V, VII, IX, X
and XI, as well as protein C, Protein S and antithrombin.
The liver breaks down hemoglobin, creating metabolites that are added to bile as pigment
The liver breaks down toxic substances and most medicinal products in a process called
drug metabolism. This sometimes results in toxication, when the metabolite is more
toxic than its precursor.
The liver converts ammonia to urea.
The liver stores a multitude of substances, including glucose in the form of glycogen,
vitamin B12, iron, and copper
In the first trimester fetus, the liver is the main site of red blood cell production. By the
32nd weeks of gestation, the bone marrow has almost completely taken over that task.
The liver is responsible for immunological effects the reticuloendothelial system if the
liver contains many immunologically active cells, acting as a 'sieve' for antigens carried
to it via the portal system.
Gallbladder
The gallbladder is a pear shaped organ that stores about 50 ml of bile (or "gall") until the
body needs it for digestion. The gallbladder is about 7-10cm long in humans and is dark
green in appearance due to its contents (bile), not its tissue. It is connected to the liver and
the duodenum by biliary tract.

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The gallbladder is connected to the main bile duct through the gallbladder duct (cystic
duct). The main biliary tract runs from the liver to the duodenum, and the cystic duct
is effectively a "cul de sac", serving as entrance and exit to the gallbladder. The surface
marking of the gallbladder is the intersection of the midclavicular line (MCL) and the trans
pyloric plane, at the tip of the ninth rib. The blood supply is by the cystic artery and vein,
which runs parallel to the cystic duct. The cystic artery is highly variable, and this is of
clinical relevance since it must be clipped and cut during a cholecystectomy.
The gallbladder has a epithelial lining characterized by recesses called Aschoff's recesses,
which are pouches inside the lining. Under epithelium there is a layer of connective tissue,
followed by a muscular wall that contracts in response to cholecystokinin, a peptide hormone
by the duodenum.
The gallbladder stores bile, which is released when food containing fat enters the digestive
tract, stimulating the secretion of cholecystokinin (CCK). The bile emulsifies fats and
neutralizes acids in partly digested food. After being stored in the gallbladder, the bile
becomes more concentrated than when it left the liver, increasing its potency and intensifying
its effect in fats.

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10.10 Anus

Figure 99

The human anus is situated between the buttocks, posterior to the perineum. It has
two anal sphincters, one internal, the other external. These hold the anus closed until
defecation occurs. One sphincter consists of smooth muscle and its action is involuntary;
the other consists of striated muscle and its action is voluntary. In many animals, the anus
is surrounded by anal sacs. Role of the anus is when the rectum is full, the increase in
intra-rectal pressure forces the walls of the anal canal apart allowing the fecal matter to
enter the canal. The rectum shortens as material is forced into the anal canal and peristaltic

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waves propel the feces out of the rectum. The internal and external sphincters of the anus
allow the feces to be passed by muscles pulling the anus up over the exiting feces.

10.11 Conditions Affecting the Esophagus

There are two different types of conditions that may affect the esophagus. The first type is
called congenital: meaning a person is born with it. The second type is called non-congenital:
meaning the person develops it after birth. Some examples of these are:
Tracheoesophageal fistula and esophageal atresia
Both of these conditions are congenital. In Tracheoesophageal fistula there is a connection
between the esophagus and the wind pipe (trachea) where there shouldn't be one. In
Esophageal atresia the esophagus of a newborn does not connect to the stomach but comes
to a dead end right before the stomach. Both conditions require corrective surgery and are
usually detected right after the baby is born. In some cases, it can be detected before the
baby is born.
Esophagitis
Esophagitis is inflammation of the esophagus and is a non-congenital condition. Esophagitis
can be caused by certain medications or by infections. It can also be caused by gastroesophageal reflux disease (gerd), a condition where the esophageal sphincter allows the acidic
contents of the stomach to move back up into the esophagus. Gastroesophageal reflux disease
can be treated with medications, but it can also be corrected by changing what you eat.

10.12 Conditions Affecting the Stomach and Intestines

Everybody has experienced constipation or diarrhea in their lifetime. With constipation,
the contents of the large intestines don't move along fast enough and waste material stays
in the large intestines so long. All water is extracted out of the waste and it becomes hard.
With diarrhea you get the exact opposite reaction. Waste moves along too fast and the
large intestines can't absorb the water before the waste is pushed through. Common flora
bacteria assists in the prevention of many serious problems. Here are some more examples
of common stomach and intestinal disorders:

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Figure 100 Acute Appendicitis: An exemplary case of acute appendicitis in a

10-year-old boy. The organ is enlarged and sausage-like (botuliform). This longitudinal
section shows the angry red inflamed mucosa with its irregular luminal surface. Diagnosed
and removed early in the course of the disease, this appendix does not show late
complications, like transmural necrosis, perforation, and abscess formation.
Appendicitis
Appendicitis is the inflammation of the appendix, the finger-like pouch that extends from
the cecum. The most common symptoms are abdominal pain, loss of appetite, fever, and
vomiting. Kids and teenagers are the most common victims of appendicitis and must be
corrected by surgery. While mild cases may resolve without treatment, most require removal
of the inflamed appendix, either by laparotomy or laparoscopy. Untreated, mortality is high,
mainly due to peritonitis and shock.
Celiac Disease
Celiac disease is a disorder in which a person's digestive system is damaged by the response
of the immune system to a protein called gluten, which is found in rye, wheat, and barley,
and also in foods like breakfast cereal and pizza crust. People that have celiac disease
experience abdominal pain, diarrhea, bloating, exhaustion, and depression when they eat
foods with gluten in them. They also have difficulty digesting their food. Celiac disease
runs in families and becomes active after some sort of stress, like viral infections or surgery.
The symptoms can be managed by following a gluten free diet. Doctors can diagnose this
condition by taking a full medical history or with a blood test.
Diverticulitis

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Conditions Affecting the Stomach and Intestines

Figure 101

Benign gastric ulcer

Diverticulitis is a common disease of the bowel, in particular the large intestine. Diverticulitis
develops from diverticulosis, which involves the formation of pouches (diverticula) on the
outside of the colon. Diverticulitis results if one of these diverticula becomes inflamed. In
complicated diverticulitis, bacteria may subsequently infect the outside of the colon if an
inflamed diverticula bursts open. If the infection spreads to the lining of the abdominal
cavity (peritoneum), this can cause a potentially fatal peritonitis. Sometimes inflamed
diverticula can cause narrowing of the bowel, leading to an obstruction. Also, the affected
part of the colon could adhere to the bladder or other organ in the pelvic cavity, causing a
fistula, or abnormal communication between the colon and an adjacent organ.
Gastritis and Peptic ulcers

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Usually the stomach and the duodenum are resistant to irritation because of the strong acids
produced by the stomach. But sometimes a bacteria called Helicobacter pylori or the chronic
use of drugs or certain medications, weakens the mucous layer that coats the stomach and
the duodenum, allowing acid to get through the sensitive lining beneath. This can cause
irritation and inflammation of the lining of the stomach, which is called gastritis, or cause
peptic ulcers, which are holes or sores that form in the lining of the stomach and duodenum
and cause pain and bleeding. Medications are the best way to treat this condition.
Gastrointestinal Infections
Gastrointestinal infections can be caused by bacteria such as Campylobacter, Salmonella, E.
coli, or Shigella. They can also be caused by viruses or by intestinal parasites like amebiasis
and Giardiasis. The most common symptoms of gastrointestinal infections Abdominal pain
and cramps, Diarrhea, and vomiting. These conditions usually go away on there own and
don't need medical attention.
Inflammatory Bowel Disease
Inflammatory bowel disease is the chronic inflammation of the intestines, which usually
affect older kids, teens and adults. There are two major types, ulcerative colitis and Crohn's
disease and indeterminate colitis, which occurs in 10-15% of patients. Ulcerative colitis
usually affects just the rectum and large intestine, while Crohn's disease can affect the whole
gastrointestinal tract from mouth to anus along with some other parts of the body. Patients
with these diseases also suffer from extraintestinal symptoms including joint pain and red
eye, which can signal a flare of the disease. These diseases are treated with medications and
if necessary, Intravenous or IV feeding, or in the more serious cases, surgery to remove the
damaged areas of the intestines.
Polyp
A polyp is an abnormal growth of tissue (tumor) projecting from a mucous membrane. If it
is attached to the surface by a narrow elongated stalk it is said to be pedunculated. If no
stalk is present it is said to be sessile. Polyps are commonly found in the colon, stomach,
nose, urinary bladder and uterus. They may also occur elsewhere in the body where mucous
membranes exist like the cervix and small intestine.

10.13 Disorders of the Pancreas, Liver, and Gallbladder

Disorders of the pancreas, liver, and gallbladder affect the ability to produce enzymes and
acids that aid in digestion. examples of these disorders are.
Cystic Fibrosis
Cystic fibrosis is a chronic, inherited illness where the production of abnormally thick mucous
blocks the duct or passageways in the pancreas and prevents the digestive fluids from entering
the intestines, making it difficult for the person with the disorder to digest protein and fats,
which cause important nutrients to pass through without being digested. People with this
disorder take supplements and digestive enzymes to help manage their digestive problems.
Hepatitis

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Hepatitis is a viral condition that inflames a person's liver which can cause it to lose its
ability to function. Viral hepatitis, like hepatitis A, B, and C, is extremely contagious.
Hepatitis A, which is a mild form of hepatitis, can be treated at home, but more serious
cases that involve liver damage, might require hospitalization.
Cholecystitis
Acute or chronic inflammation if the gallbladder causes abdominal pain. 90% of cases of
acute cholecystitis are caused by the presence of gallstones. The actual inflammation is
due to secondary infection with bacteria of an obstructed gallbladder, with the obstruction
caused by the gallstones. Gallbladder conditions are very rare in kids and teenagers but
can occur when the kid or teenager has sickle cell anemia or in kids being treated with long
term medications.
Cholestasis
Cholestasis is the blockage in the supply of bile into the digestive tract. It can be "intrahepatic"
(the obstruction is in the liver) or "extrahepatic" (outside the liver). It can lead to jaundice,
and is identified by the presence of elevated bilirubin level that is mainly conjugated.
Biliary colic
This is when a gallstone blocks either the common bile duct or the duct leading into it
from the gallbladder. This condition causes severe pain in the right upper abdomen and
sometimes through to the upper back. It is described by many doctors as the most severe
pain in existence, between childbirth and a heart attack. Other symptoms are nausea and
vomiting and diarrhea, bleeding caused by continual vomiting, and dehydration caused by
the nausea and diarrhea. Another more serious complication is total blockage of the bile
duct which leads to jaundice, which if it is not corrected naturally or by surgical procedure
can be fatal as it causes liver damage. The only long term solution is the removal of the
gallbladder.

10.14 Gastrointestinal Dysfunctions

As we age, the amount of digestive enzymes produced by the body drops way down. This leads
to decreased and slower digestion, slower absorption of nutrients and increased accumulation
of fecal mater in the intestinal tract. Undigested food material and metabolic waste can
also build up due to slow elimination, starting of a series of health problems.
When digestion slows, it turns the intestines into a toxic environment. Helpful organisms
cannot live in toxic environments. When the beneficial organisms die they are replaced by
harmful organisms, such as yeasts and parasites, the most common being Candida albicans.
This leads to changes in the intestinal wall which produces leaky gut syndrome which allows
many toxic chemicals to be introduced into the blood stream. As a result the entire toxic
load of the body is increased, which causes a bigger burden on the liver, kidneys and other
body organs. When this happens the organs that are normally used for eliminating waste
and supplying nutrients the GI tract becomes into a large dump for waste. This problem is
made worse by the use of junk food, prescriptions, over the counter medications, antibiotics
and a diet that is too low in fiber.

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Most people never even think about their GI tract. We are all concerned about what the
outside of our body look like, but we completely ignore the inside. Because our bodies a
very resilient. deterioration of the digestive system can go on for years with no symptoms
or side-effect. When symptoms finally do appear they are usually very non-specific, they
include: decreased energy, headaches, diarrhea, constipation, heartburn, and acid reflux.
Over the years these symptoms become more serious, they include: asthma, food allergies,
arthritis, and cancer.
Poor digestion, poor absorption, and bacterial imbalance can be traced to a lot of chronic
conditions. Every organ in the body receives nutrients for the GI tract. I if the GI tract is
malfunctioning then the whole body suffers.
It is possible to return good health to your GI tract by improving digestion, consuming the
right amount of fiber, cutting out junk food and refined sugars.
You can improve the function of the intestines by taking fiber supplements and vitamins
(especially B12 and vitamin K). Some doctors suggest herbal or vitamin enema's to cleanse
and relieve constipation and to help stimulate peristaltic movement which will help to move
the bowels.
Irritable Bowel Syndrome
Irritable Bowel Syndrome (IBS) is a disorder with symptoms that are most commonly
bloating, abdominal pain, cramping, constipation, and diarrhea. IBS causes a lot of pain
and discomfort. It does not cause permanent damage to the intestines and does not lead
to serious diseases such as cancer. Most of the people affected with IBS can control their
symptoms with stress management, diet, and prescription medication. For others IBS can
be debilitating, they may be unable to go to work, travel, attend social events or leave home
for even short periods of time.
About 20 percent of the adult population has some symptoms of IBS, making it one of the
most common intestinal disorders diagnosed by physicians. It is more common in men than
women and in about 50 percent of people affected it starts at about age 35.
Researchers have not found out what exactly causes IBS. One idea is that people with IBS
have a large intestine (colon) that is sensitive to certain foods and stress. The immune
system may also be involved. It has also been reported that serotonin is linked with normal
GI functioning. 95 percent of the body's serotonin is located in the GI tract (the other 5
percent is in the brain). People with IBS have diminished receptor activity, causing abnormal
levels of serotonin in the GI tract. Because of this IBS patients experience problems with
bowel movement, mobility, and sensation having more sensitive pain receptors in their GI
tract. Many IBS patients suffer from depression and anxiety which can make symptoms
worse.
There is no cure for IBS, but medications are an important part of relieving symptoms. Fiber
supplements or laxatives are helpful for constipation. Anti diarrhoeals such as Imodium
can help with diarrhea. An antispasmodic is commonly prescribed for colon muscle spasms.
Antidepressants and pain medication are also commonly prescribed. [12]
Gastrointestinal Stromal Tumor

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Gastrointestinal Dysfunctions
Gastrointestinal Stromal Tumors or GIST is an uncommon type of cancer in the GI tract
(esophagus, stomach, small intestine, and colon). These types of cancers begin in the
connective tissue like fat, muscles, nerves , cartilage, etc.
GIST originates in the stroma cells. Stroma cells are strung along the GI tract and are part
of the system that helps the body to know when to move food through the digestive system.
Over half of Gist's occur in the stomach. Most cases occur in people between the ages of
forty and eighty, but can also show up in a person of any age.
All GIST's of any size or location have the ability to spread. Even if a GIST is removed, it
can reappear in the same area, or may even spread outside of the GI tract.
In the early stages, GIST is hard to diagnose because in the early stages symptoms cannot be
recognized. In the later stages a person can have vague abdominal pain, vomiting, abdominal
bleeding that shows up in stool or vomit, low blood counts causing anemia, and having an
early feeling of being full causing a decrease in appetite.
GIST is now recognized as an aggressive cancer that is able to spread to other parts of the
body. People who have been diagnosed with GIST should get treatment as soon as possible.
Food Allergies
Food allergies occur when the immune system thinks that a certain protein in any kind of
food is a foreign object and will try to fight against it.
Only about eight percent of children and two percent of adults actually have a food allergy.
A person can be allergic to any kind of food, but the most common food allergies are from
nuts, cow's milk, eggs, soy, fish, and shellfish. Most people who have a food allergy are
allergic to less than four different foods.
The most common signs of food allergies are hives, swelling, itchy skin, itchiness, tingling or
swelling in the mouth, coughing, trouble breathing, diarrhea, and vomiting. The two most
common chronic illness that are associated with food allergies are eczema and asthma.
Food allergies can be fatal if it causes the reaction called anaphylaxis. This reaction makes
it hard for the person to breathe. This can be treated by an epinephrine injection.
GERD, Heartburn, Acid Reflux
GERD, or Gastroesophageal Reflux Disease occurs when the lower esophageal sphincter is
not able to close properly. When this happens, contents from the stomach called reflux leak
back into the esophagus and the stomach.
When the stomach refluxes, stomach acid touches the lining of the esophagus and causes it
to have a burning feeling in the throat or the chest. This is what heartburn is. When you
taste the fluid in the back of your throat, it is called acid indigestion. It is common for a
person to get occasional heartburn, but when it occurs more than twice a week it can be
considered as GERD. GERD can occur in people of all ages including infants.
Some symptoms of GERD include having a pain in your chest, hoarseness, having trouble
swallowing, or having the feeling of food being stuck in your throat. The main symptoms
are having persistent heartburn and acid regurgitation. GERD can also cause bad breath
and a dry cough.

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No one knows why people get GERD. Some things that could contribute to GERD are
alcohol use, pregnancy, being overweight and smoking. Certain foods might also contribute
like citrus fruits, caffeine, spicy, fatty, and dried foods, and also mint flavorings.
Over-the-counter antacids or medications that help stop acid production and help the
muscles empty the stomach are commonly used to treat GERD.
Constipation
Not everyone is on the same schedule for having a bowel movement. Depending on the
person, a "normal" schedule can range anywhere from three times a day to three times a
week. If you start having bowel movements less than your own personal schedule, then you
might be getting the signs of constipation.
Constipation is when you have trouble having bowel movements. The stool is very hard
making it hard to pass and causing a person to strain. You may even feel like you have to
have a bowel movement even after you have already had one.
When you digest food, the waste products go through your intestines by the muscles
contracting. When in the large intestine, most of the water and salt from the waste products
are reabsorbed because they are needed by the body for our everyday functions. You can
become constipated if too much water is absorbed, or if waste products move too slowly.
Not getting enough fluids, a low fiber diet, age, not being physically active, depression, stress
and pregnancy can all be causes of constipation. Medications and narcotics can also cause a
person to get constipated. Chronic constipation may be a symptom of a liver problem such
as a urea cycle disorder.
The best way for a person to treat constipation is to make sure that you are getting enough
fluids as well as fiber in your diet. By doing this, the bulk of your stool is increased and also
makes the stool softer so that it can move through your intestines more easily. Being more
active and increasing your daily exercise also helps keep you regulated.
Hemorrhoids
Hemorrhoids (also known as haemorrhoids, emerods, or piles) are varicosities or swelling
and inflammation of veins in the rectum and anus.
Two of the most common types of hemorrhoids are external and internal hemorrhoids.
External hemorrhoids are those that occur outside of the anal verge (the distal end
of the anal canal). They are sometimes painful, and can be accompanied by swelling and
irritation. Itching, although often thought to be a symptom from external hemorrhoids,
is more commonly due to skin irritation.
If the vein ruptures and a blood clot develops, the hemorrhoid becomes a thrombosed
hemorrhoid.
Internal hemorrhoids are those that occur inside the rectum. As this area lacks pain
sensory receptor|receptors, internal hemorrhoids are usually not painful and most people
are not aware that they have them. Internal hemorrhoids, however, may bleed when
irritated.
Untreated internal hemorrhoids can lead to two severe forms of hemorrhoids: prolapsed
and strangulated hemorrhoids.

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Prolapsed hemorrhoids are internal hemorrhoids that are so distended that they
are pushed outside of the anus.
If the anal sphincter muscle goes into spasm and traps a prolapsed hemorrhoid outside
of the anal opening, the supply of blood is cut off, and the hemorrhoid becomes a
strangulated hemorrhoid.

10.15 Bleeding in the Gastrointestinal tract

Bleeding in the gastrointestinal tract doesn't always mean you have a disease, it's usually a
symptom of a digestive problem. The cause of the bleeding may not be that serious, it could
be something that can be cured or controlled such as hemorrhoids. However, locating the
source of the bleeding is very important. The gastrointestinal tract contains many important
organs like the esophagus, stomach, small intestine, large intestine or colon, rectum, and
anus. Bleeding can come from one or more of these area from a small ulcer in the stomach,
or a large surface like the inflammation of the colon. Sometimes a person doesn't even know
they are bleeding. When this happens, it is called hidden, or occult bleeding. Simple tests
can detect hidden blood in the stool.
What Causes Bleeding in the Digestive Tract
Esophageal bleeding may be caused by Mallory-Weiss syndrome which is a tear in the
esophagus. Mallory-Weiss syndrome is usually caused by excessive vomiting or may be
caused by childbirth, a hiatal hernia, or increased pressure in the abdomen caused by
coughing. Various medications can cause stomach ulcers or inflammations. Medications
containing aspirin or alcohol, and various other medications(mainly those used for arthritis)
are some examples of these.
Benign tumors or cancer of the stomach may also cause bleeding. These disorders don't
usually produce massive bleeding. The most common source of bleeding usually occurs
from ulcers in the duodenum. Researchers believe that these ulcers are caused by excessive
stomach acid and a bacteria called Helicobacter Pylori.
In the lower digestive tract, the most common source of bleeding is in the large intestine,
and the rectum. Hemorrhoids are the most common cause of bleeding in the digestive tract.
Hemorrhoids are enlarged veins in the anal area which produces bright red blood that you
see in the toilet or on the toilet paper.
How do you Recognize Bleeding in the Digestive Tract
The signs of bleeding in the digestive tract vary depending on the site and severity of the
bleeding. If the blood is coming from the rectum, it would be bright red blood. If it was
coming from higher up in the colon or from the small intestine, the blood would be darker.
When the blood is coming from the stomach, esophagus, or the duodenum, the stool would
be black and tarry.
If the bleeding is hidden, or occult, a person may not notice changes in the stool color.
If extensive bleeding occurs, a person may feel dizzy, faint, weak, short of breath, have
diarrhea or cramp abdominal pain. Shock can also occur along with rapid pulse, drop in
blood pressure, and difficulty urinating. Fatigue, lethargy, and pallor from anemia will settle

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in if the bleeding is slow. Anemia is when the bloods iron-rich substance, hemoglobin, is
diminished.
Common Causes of Bleeding in the Digestive Tract

Hemorrhoids
Gastritis (inflammation)
Inflammation (ulceratice colitis)
Colo rectal Polyps
Colo rectal Cancer
Duodenal Ulcer
Enlarged Veins
Esophagitis (inflammation of the esophagus)
Mallory-Weiss Syndrome
Ulcers

Iron and beets can also turn the blood red or black giving a false indication of blood in the
stool.
How Bleeding in the Digestive Tract is Diagnosed
To diagnose bleeding in the digestive tract the bleeding must be located and a complete
history and physical are very important. Here are some of the procedures that diagnose the
cause of bleeding.
Endoscopy
An endoscopy is a common diagnostic technique that allows direct viewing of the bleeding
site. Since the endoscope can detect lesions and confirm the absence or presence of bleeding,
doctors often use this method to diagnose acute bleeding, the endoscope can also be used to
treat the cause of bleeding as well.
The endoscope is a flexible instrument that can be inserted through the mouth or rectum. The instrument allows the doctors to see inside the esophagus, stomach, duodenum(esophagoduodenoscopy), sigmoid colon(sigmoidoscopy), and rectum(rectoscopy, to
collect small samples of tissues, take pictures, and stop the bleeding. There is a new procedure out using a long endoscope that can be inserted during surgery to locate a source of
bleeding in the small intestine.
Capsule Endoscopy
Capsule endoscopy helps doctors to see and examine the lining of the middle part of the
gastrointestinal tract, which includes the three parts of the small intestine (duodenum,
jejunum, ileum). The capsule is a small pill sized video camera called an endoscope. It
has its own lens and light that transfers the images to a monitor so the doctor can view
them outside of the body. This process is also referred to as small bowel endoscopy, capsule
endoscopy, or wireless endoscopy.
The most common reason for doing a capsule endoscopy is to look for the causes of bleeding
that is coming from the small intestine. It is also able to help detect ulcers, tumors, and
Crohn's disease.
Angiography

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Colonoscopy
Angiography is a technique that uses dye to highlight blood vessels. This procedure is used
when the patient is bleeding badly enough that it allows the dye to leak out of the blood
vessels and identifies the bleeding site. In some situations, Angiography allows the patient
to have medication injections that may stop the bleeding.
Radionuclide Scanning
Radionuclide scanning is a non-invasive screening technique used for locating sites of acute
bleeding, especially in the lower GI tract. This procedure injects small amounts of radioactive
material that either attach to the persons red blood cells or are suspended in the blood.
Special pictures are taken that allows doctors to see the blood escaping. Barium x-rays,
angiography, and radionuclide scans can be used to locate sites of chronic occult bleeding.
How to Recognize Blood in the Stool and Vomit

Bright red blood coating the stool

Dark blood mixed with the stool
Black or tarry stool
Bright red blood in the vomit
Grainy appearance in vomit

Symptoms of Acute Bleeding

Weakness
Shortness of breath
Dizziness
Cramp abdominal pain
Feeling light headed
Diarrhea

Symptoms of Chronic Bleeding

Fatigue
Shortness of breath
Lethargy
Pallor

10.16 Colonoscopy
A colonoscopy is a test to look at the inside of your colon. Everyone should have a colonoscopy
by the time they are 50 to check for diseases of the colon. Colonoscopy is best known for
its use in early detection of colorectal cancer, the second leading cause of cancer deaths in
the United States. Colon cancer develops from growths like polyps within the intestinal
wall. These growths often take 5-10 years to develop usually without symptoms. You are
at a higher risk to have this disease if you have a close relative who has had it. If you are
going to develop a polyp, you will probably do so after age 50. So the American College
of Gastroenterology (the digestive specialists) recommends screening examinations every 5
years for early detection and removal of these cancer-causing growths after that age. Don't
make excuses! It's not so bad and it may save your life!

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The Gastrointestinal System

10.17 Case Study

Bob had a history of chronic pain in his intestinal area. He wasn't so sure what it was. The
doctor suspected what it was and gave Bob antibiotics. It helped. It so happened that
whenever Bob ate popcorn or nuts he would get this pain. Sometimes it would just go away...
other times he had to go on antibiotics. The doctor ordered some tests. Bob would have
to stay away from nuts, popcorn, tomatoes, strawberries, and anything else with seeds or
hard parts. Seems something in his bowels couldn't tolerate those foods. Bob ate a pretty
healthy diet so he couldn't understand what was happening. A few years later, Bob had
another series of painful episodes. The pain was so great Bob could hardly stand let alone
go to work. This time the doctor did more tests and found out that his lower intestine was
almost blocked. Surgery was ordered. What did Bob have?

10.18 Glossary
Amebiasis
An inflammation if the intestines caused by infestation with Entameba histolytica (a type
of ameba) and characterized by frequent loose stools flecked with blood and mucus
Amylase
An enzyme produces in the pancreas and salivary glands that help in the digestions of
starches.
Bile
A bitter, alkaline, brownish-yellow or greenish-yellow fluid that is secreted by the liver,
stored in the gallbladder, and discharged into the duodenum and aids in the emulsification,
digestion, and absorption of fats. Also called gall.
Biotin
Biotin is used in cell growth, the production of fatty acids, metabolism of fats, and amino
acids. It plays a role in the Krebs Cycle. Biotin is also helpful in maintaining a steady
blood sugar level. It is often recommended for strengthening hair and nails.
B12
A vitamin important for the normal formation of red blood cells and the health of the
nerve tissues. Undetected and untreated B12 deficiency can lead to anemia and permanent
nerve and brain damage
Candida Albicans
Found in animals and in man. Has been isolated from the skin and mucosa of man, but
has also been recovered from leaves, flowers, water, and soil. Reported to be allergenic. A
common cause of superficial infection, oral and vaginal infection, sepsis, and disseminated
disease. Cells from the organism are usually not airborne and are considered to be normal
component of the flora of the mouth and other mucous membranes on the body.
Chemical digestion

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Glossary
Is a chemical breakdown of food when being in the mouth (oral cavity). Is the digestive
secretions of saliva that moistens food and introduces gastric juices and enzymes that are
produced in the stimulation to certain macronutrients, such as, carbohydrates. In this, the
mouth saliva carries an enzyme called amylase for breaking down carbohydrates.
Cholecystokinin (CCK)
Cholecystokinin (also called pancreozymin), this is a hormone in the small intestinal cells
(intestinal mucosa) that is produced in response to food. This hormone regulates the release
of secretions of many organs that aid digestion, such as, bicarbonate from the pancreas to
reduce the acidity of digestive juices like the chyme that enters the small intestine form the
stomach that contains hydrochloric acid (HCL).
Chylomicrons
The lipoproteins first formed after absorption of lipids form food.
Chyme
The thick semi fluid mass of partly digested food that is passed from the stomach to the
duodenum.
Crohn's Disease
Described as skip lessions in the large and small bowel it is a malabsorption disorder that
can affect the gastrointestinal tract for the mouth to the anus.
Deamination
When an amino acid group breaks off an amino acid that makes a molecule of ammonia
and keto acid.
Emulsifier
A mixture of two immiscible (unblendable) substances.
Gastrin
The stomach mucosa secretes a hormone gastrin that increases the release of gastric juices.
GI tract
Gastrointestinal Tract, The tube that extends from the mouth to the anus in which the
movement of muscles and release of hormones and enzymes digest food.
Hydrochloric
The chemical substance hydrochloric acid is the water-based solution of hydrogen chloride
(HCI) gas. It is a strong acid, the major component of stomach acid and of wide industrial
use.
Lactobacillus Acidophilus
Important resident inhabitant of the human small and large intestines, mouth, and vagina.
Secretes natural antibiotic substances which strengthen the body against various diseasecausing microbes
Leaky gut syndrome

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The Gastrointestinal System

Abnormal level of intestinal permeability
Lingual lipase
An enzyme produced only in infancy to aid digestion of long-chain fatty acids.
Lipase
An enzyme produced by microorganisms that split the fat molecules into fatty acids which
create flavor
Mechanical digestion
The crushing of the teeth and rhythms made by the movement of the tongue, the teeth
aid in tearing and pulverizing food, while the tongue helps with peristalsis (movement), of
food down the esophagus.
Micelles
A product of lipids and bile assist in lipid absorption.
Microvilli
On the villi in the small intestine is mivrovilli, these projections called brush border microvilli
secrete specific enzymes for disaccharide hydrolysis, these further aid the absorption of the
carbohydrate by yielding a monosaccharide that then can go through portal circulation to
liver circulation to be further processed into immediate use for energy or glycogen storage.
Peristalsis
The wavelike muscular contractions of the intestine or other tubular structure that propel
the contents onward by alternate contraction and relaxation.
Pharynx
Proliferation
The process of reproduction or division of cells
Proteases
Protein enzyme
Rennin
Only produced during infancy and is a gastric protease and functions with calcium to clot
with milk proteins casein, to slow the movement of milk so that digestion is prolonged.
Serotonin
chemical messenger in the brain that affects emotions, behavior, and thought
Synthesize
To create something, such as chemicals in the body, from simpler, raw materials
Ulcerative Colitis
Villi

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External links
A minute projection arising from a mucous membrane, especially one of the vascular
projections of the small intestine.
Vitamin K
A substance that promotes the clotting of blood
Case Study Answer Bob has diverticulitis. The doctor was afraid that if he had another
bad infection that scar tissue would eventually block his colon completely and burst, which
would necessitate a colostomy. Bob ended up having to have surgery to remove the damaged
part of his colon. The doctor removed almost 18 inches of Bob's large intestine. Bob is doing
fine now and most importantly, he can now eat his favorite food - nuts! Note: Sometimes a
diet rich in fiber can help you avoid this dreaded problem. Sometimes, like in Bob's case,
the predisposition to have this problem runs in the family. All of his siblings and his father
suffered from this same ailment. Stress is another factor that can exacerbate this disease.
So.. don't worry, be happy and eat fiber!

10.19 External links

Appendicitis Update Review2 , An updated Issue on Appendicitis

10.20 References
1: Chen Ts, Chen PS. Intestinal autointoxication: A gastrointestinal leitmotive: Journal
Clinical Gastroenterology
2: Ernst E. Colonic irrigation and the theory of autointoxication: A triumph of ignorance
over science. Journal of Gastroenterology
3: Alvarez WC. Origin of the so-called auto-intoxication symptoms.
4: Donaldson AN. Relation of constipation to intestinal intoxication.
5: Kenney JJ. Fit for Life: Some notes on the book and its roots. Nutrition Forum
6: Use of enemas is limited. FDA consumer
7: Amebiasis associated with colonic irrigation - Colorado. Morbidity and Mortality Weekly
Report
8: Istre GR and others. An outbreak of amebiasis spread by colonic irrigation at a chiropractic
clinic
9: Benjamin R and others. The case against colonic irrigation
10: Eisele JW, Reay DT. Deaths related to coffee enemas
11: Jarvis WT. Colonic Irrigation. National Council Against Health Fraud.
12: National Digestive Disease Information Clearinghouse (NDDIC)
2

http://www.appendicitisreview.com/

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11 Nutrition
11.1 The Community and Nutrition Programs

../images/102.png

Figure 102

Harvard's Food Pyramid

Connections between nutrition and health have probably been understood, at least to some
degree, among all people of all places and times. For example, around 400 BC Hippocrates

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Nutrition
said, "Let food be your medicine and medicine be your food." Understanding the physiological
needs of our cells helps us understand why food has such an impact on overall health. In
this chapter we introduce nutrition by examining how cells use different nutrients and then
discuss disease conditions that are tied to nutritional problems.

11.2 Nutrition and Health in the Community

The nutritional status of people in our communities is a concern not only for quality of life, but
also for economics (treating illness costs far more than preventing it). Various public health
agencies are striving to prevent nutritional deficiencies and improve overall health. In the
U.S., the government supplies a variety of resources such as state assistance, WIC (Women
Infant and Child), and so forth. In addition, there have been many government agencies and
voluntary health and scientific associations, such as the American Heart Association, that
focus on life style and dietary factors that prevent chronic and life-threatening diseases. The
U.S. Department of Agriculture (USDA) and the U.S. Department of Health and Human
Services (USDHHS) developed dietary guidelines in 1977 that were compiled and displayed
as the food guide pyramid. The food guide pyramid was revised as "My Pyramid," but
this new chart is confusing to most people. Harvard School of Public Health developed an
alternative healthy eating pyramid (shown at left) based on long-term nutritional studies.
This pyramid differs from the old USDA pyramid in several key aspects: for example, exercise
is at the bottom to remind us of its important role in our health. Also, not all carbohydrates
are at the bottom (white bread, white rice, and potatoes are now at the top with sugars),
and not all oils are at the top (plant oils are at the bottom). Other resource, such as the
Recommended Daily Allowance (RDA) have helped people become more aware of nutritional
needs, yet obesity and chronic health problems continue to rise.

11.3 Nutritional Requirements

Our bodies have both caloric and nutritional needs. Living tissue is kept alive by the
expenditure of energy in ATP molecules, which energy came from the break down of food
molecules. Caloric need refers to the energy needed each day to carry out the varied chemical
reactions in each cell. When looking at a nutritional label, we can easily see how many
Calories are in a serving. These Calories (big "C") are actually kilocalories (1000 calories).
Technically, a calorie (little "c") is the amount of energy needed to raise the temperature of
1 mL of water by 1 C. How many Calories a person needs daily varies greatly by age, sex,
height, and physical activity levels. If the amount of energy taken in exceeds the amount of
energy used, then the excess energy is stored as adipose tissue (fat), regardless of the source
of the energy.
In addition to daily energy needs, there are nutritional needs to prevent the body from
losing its own fats, carbohydrates, and proteins. Such molecules are continuously broken
down, and must be replaced regularly. Essential amino acids and essential fatty acids are
particularly important building blocks in replacing these molecules. Vitamins and minerals
are not used as energy, but are essential in tissue and enzyme structure or reactions.

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11.4 Carbohydrates
Macronutrient
An energy-yielding nutrient. Macronutrients are those nutrients that together provide the
vast majority of metabolic energy to an organism. The three main macronutrients are
carbohydrates, proteins, and fat.
Micronutrients
Microminerals or trace elements, are dietary minerals needed by the human body in very
small quantities (generally less than 100mg/day) as opposed to macrominerals which are
required in larger quantities.
Functions
Glucose it is the most easily used by the body. It is a simple carbohydrate that circulates
in the blood and is the main source of energy for the muscles, central nervous system, and
brain (the brain can also use ketone bodies).
Carbohydrates are made of organic compounds carbon, hydrogen, and oxygen.
There are three sizes of carbohydrate and they are distinguished by a classification of two
that is, simple carbohydrates (mono saccharides and disaccharides) and complex carbohydrates
(polysaccharides). Polysaccharides are the most abundant carbohydrate in the body along
with glycogen.
The break down of polysaccharides goes as follows: Polysaccharides are digested into
monosaccchorides including glucose which goes into the intestinal epithelium and into the
bloodstream. The molecules of glucose are taken by glucose transporters and delivered into
the cells of the body. While glucose is in the cells it can be oxidized for energy or provide
substrates to other metabolic reactions or of course into glycogen for storage.
A. Monosaccharides = Single carbohydrate unit such as, Glucose, Fructose, and Galactose.
B. Disaccharides = Two single carbohydrates bound together such as, Sucrose, Maltose,
and Lactose.
C. Polysaccharides = Have many units of monosaccharides joined together such as, Starch
and Fiber.
Fiber
Fiber is carbohydrates that cannot be digested. It is in all eatable plants such as fruits
vegetables, grains and Legumes. There are many ways of categorizing fiber types. First,
from the foods they come from such as grains, which is called cereal fiber. Second, if they
are soluble fiber or insoluble fiber. Soluble fiber partially dissolves in water and insoluble
fiber does not.
Adults need about 21-38 grams of fiber a day. Children ages 1 and up need 19 grams a day.
On average Americans eat only 15 grams a day.
Fiber helps reduce the chances of having the following conditions: colon cancer, heart disease,
type 2 diabetes, diverticular disease, and constipation.

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Nutrition
Glycemic Index
Glycemic Index is a new way of classifying carbohydrates. It measures how fast and how far
blood sugar will rise after consuming carbohydrates. Foods that are considered to have a
high glycemic index are converted almost immediately to blood sugar which causes it to rise
rapidly. Foods that are considered to have a low glycemic index are digested slower causing
a slower rise in blood sugar. Examples of high glycemic index foods are potatoes, white rice,
white flour, anything refined, anything with a lot of sugar which includes high fructose corn
syrup. Examples of low glycemic index foods are whole grains (brown rice, 100% whole
wheat bread, whole grain pasta, high fiber cereals), high fiber fruits and vegetables, and
many legumes. According to the Harvard School of Public Health, "The most comprehensive
list of the glycemic index of foods was published in the July, 2002, issue of the American
Journal of Clinical Nutrition. A searchable database maintained by the University of Sydney
is available online."

11.5 Proteins
Functions
Protein forms hormones, enzymes, and antibodies. It is part of fluid and electrolyte
regulation, the buffering effect for pH, and transporter of nutrients. A good example of a
protein is the oxygen carrying hemoglobin found in red blood cells.
Proteins are made of carbon, hydrogen, oxygen, and nitrogen, an inorganic molecule, the
thing that clearly distinguishes them from the other macronutrients.
A. Amino acids are the building blocks of proteins.
B. Polypeptide are a group of amino acids bonded together 10-100 or more.
The body requires amino acids to produce new body protein (protein retention) and to
replace damaged proteins (maintenance) that are lost in the urine.
Proteins are relatively large molecules made of amino acids joined together in chains by
peptide bonds. Amino acids are the basic structural building units of proteins. They form
short polymer chains called peptides or longer poly-peptides which in turn form structures
called proteins. The process of protein synthesis is controlled by an mRNA template. In
this process tRNA transfers amino acids to the mRNA to form protein chains.
There are twenty standard amino acids used by cells in making proteins. Vertebrates,
including humans, are able to synthesize 11 of these amino acids from other molecules. The
remaining nine amino acids cannot be synthesized by our cells, and are termed "'essential
amino acids'". These essential amino acids must be obtained from foods.
The 9 Essential Amino Acids have the following names: Histidine, Isoleucine, Leucine,
Lysine, Methionine, Phenylalanine, Threonine, Tryptophan, Valine
You can remember these with this saying Hey It's Like Lovely Material; Please Touch The
Velvet.
The 11 Non-essential Amino Acids are as follows:

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Proteins
Alanine, Arginine, Aspartic acid, Cysteine, Cystine, Glutamic acid, Glutamine, Glycine,
Proline, Serine, Tyrosine
How about this memory device, "Almost Always Aunt Cindy Can Get Great Gum Popping
Sounds Together" (This section needs to be corrected. Cystine is not one of the 20 common
amino acids. It should be replaced by asparagine which is missing from the list. Also
histidine is not essential for adults while cysteine, tyrosine, histidine, and arginine are
required for infants and growing children. Some amino acids are also essential for specific
subpopulations, e.g., tyrosine for individuals with PKU.)

11.5.1 The 20 Amino Acids and What They Do!

Amino Acid
Alanine

Abbrev.
A
Ala

Cysteine

Cys

Aspartic acid

Asp

Glutamate

Glu

Remarks
Very abundant, very versatile. More stiff than
glycine, but small enough to pose only small
steric limits for the protein conformation. It
behaves fairly neutrally, can be located in both
hydrophilic regions on the protein outside and
the hydrophobic areas inside.
The sulfur atom binds readily to heavy metal
ions. Under oxidizing conditions, two cysteines
can join together in a disulfide bond to form
the amino acid cystine. When cystines are part
of a protein, insulin for example, this stabilizes
tertiary structure and makes the protein more
resistant to denaturation; disulphide bridges are
therefore common in proteins that have to function in harsh environments including digestive
enzymes (e.g., pepsin and chymotrypsin) and
structural proteins (e.g., keratin). Disulphides
are also found in peptides too small to hold a
stable shape on their own (e.g., insulin).
Behaves similarly to glutamic acid. Carries a
hydrophilic acidic group with strong negative
charge. Usually is located on the outer surface
of the protein, making it water-soluble. Binds
to positively-charged molecules and ions, often
used in enzymes to fix the metal ion. When
located inside of the protein, aspartate and
glutamate are usually paired with arginine and
lysine.
Behaves similar to aspartic acid. Has longer,
slightly more flexible side chain. Also serves as
an excitatory neurotransmitter in the CNS.

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Nutrition

Phenylalanine

300

Phe

Glycine

Gly

Histidine

His

Isoleucine

Ile

Lysine

Lys

Essential for humans. Phenylalanine, tyrosine,

and tryptophan contain large rigid aromatic
group on the side chain. These are the biggest
amino acids. Like isoleucine, leucine and valine, these are hydrophobic and tend to orient towards the interior of the folded protein
molecule.
Because of the two hydrogen atoms at the
carbon, glycine is not optically active. It is
the smallest amino acid, rotates easily, adds
flexibility to the protein chain. It is able to fit
into the tightest spaces, e.g., the triple helix
of collagen. As too much flexibility is usually
not desired, as a structural component it is less
common than alanine.
In even slightly acidic conditions protonation
of the nitrogen occurs, changing the properties
of histidine and the polypeptide as a whole. It
is used by many proteins as a regulatory mechanism, changing the conformation and behavior
of the polypeptide in acidic regions such as the
late endosome or lysosome, enforcing conformation change in enzymes. However only a few
histidines are needed for this, so it is comparatively scarce.
Essential for humans. Isoleucine, leucine and
valine have large aliphatic hydrophobic side
chains. Their molecules are rigid, and their
mutual hydrophobic interactions are important for the correct folding of proteins, as these
chains tend to be located inside of the protein
molecule.
Essential for humans. Behaves similarly to
arginine. Contains a long flexible side-chain
with a positively-charged end. The flexibility
of the chain makes lysine and arginine suitable
for binding to molecules with many negative
charges on their surfaces. E.g., DNA-binding
proteins have their active regions rich with arginine and lysine. The strong charge makes these
two amino acids prone to be located on the
outer hydrophilic surfaces of the proteins; when
they are found inside, they are usually paired
with a corresponding negatively-charged amino
acid, e.g., aspartate or glutamate.

Proteins

Leucine

Leu

Methionine

Met

Asparagine

Asn

Proline

Pro

Glutamine

Gln

Arginine
Serine

R
S

Arg
Ser

Threonine

Thr

Valine

Val

Tryptophan

Trp

Tyrosine

Tyr

Essential for humans. Behaves similar to

isoleucine and valine. See isoleucine.
Essential for humans. Always the first amino
acid to be incorporated into a protein; sometimes removed after translation. Like cysteine,
contains sulfur, but with a methyl group instead of hydrogen. This methyl group can be
activated, and is used in many reactions where
a new carbon atom is being added to another
molecule.
Similar to aspartic acid. Asn contains an
amide group where Asp has a carboxyl.
Contains an unusual ring to the N-end amine
group, which forces the CO-NH amide sequence
into a fixed conformation. Can disrupt protein
folding structures like helix or sheet, forcing
the desired kink in the protein chain. Common
in collagen, where it often undergoes a posttranslational modification to hydroxyproline.
Uncommon elsewhere.
Similar to glutamic acid. Gln contains an
amide group where Glu has a carboxyl. Used in
proteins and as a storage for ammonia.
Functionally similar to lysine.
Serine and threonine have a short group ended
with a hydroxyl group. Its hydrogen is easy to
remove, so serine and threonine often act as
hydrogen donors in enzymes. Both are very hydrophilic, therefore the outer regions of soluble
proteins tend to be rich with them.
Essential for humans. Behaves similarly to
serine.
Essential for humans. Behaves similarly to
isoleucine and leucine. See isoleucine.
Essential for humans. Behaves similarly to
phenylalanine and tyrosine (see phenylalanine).
Precursor of serotonin.
Behaves similarly to phenylalanine and tryptophan (see phenylalanine). Precursor of melanin,
epinephrine, and thyroid hormones.

Dietary proteins fall into two categories: complete proteins and incomplete proteins. Complete proteins include ample amounts of all essential amino acids. Examples of foods that
will include these great complete proteins are meat, fish, poultry, cheese, eggs, and milk.
Incomplete proteins contain some but not all of the essential amino acids required by the
human body. Examples of incomplete proteins include legumes, rice, and leafy green veg-

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Nutrition
etables. Someone who chooses a vegan lifestyle must be careful to combine various plant
proteins to obtain all the essential amino acids on a daily basis, but it can be accomplished.
Ingested proteins are broken down into amino acids during digestion. They are then absorbed
by the villi of the small intestine and enter the blood stream. Our cells use these amino
acids to assemble new proteins that are used as enzymes, cell receptors, hormones, and
structural features. Each protein has its own unique amino acid sequence that is specified by
the nucleotide sequence of the gene encoding that protein (see Genetics and Inheritance1 ).
If we are deficient in even a single amino acid, then our cells cannot make the proteins they
require.

11.6 Lipids
Macronutrient
Provide 9 Kcalories per gram; it is an energy-yielding nutrient
Functions are stored energy (adipose tissue), organ protection, temperature regulator,
insulation such as myelin that covers nerve cells, lipid membrane around cells, and emulsifiers
to keep fats dispersed in body fluids.
Lipids are made of organic molecules carbon, hydrogen, and oxygen. Fats consist of glycerol
fatty acids joind by an ester bond.
A. Triglycerides - composed of three fatty acids and one glycerol molecule.
B. Saturated fatty acid - fatty acid with carbon chains fully saturated with hydrogen.
C. Monounsaturated fatty acid - fatty acid that has a carbon chain with one unsaturated
double bond.
D. Polyunsaturated fatty acid - fatty acid that has two or more double bonds on the
carbon chain.
Essential fatty acids part of the polyunsaturated fatty acids
E. Linoleic acid an essential polyunsaturated fatty acid, its first double bond is at the
6th carbon and this is why it can be called Omega 6.
F. Linolenic acid an essential polyunsaturated fatty acid, its first double bond is at the
3rd carbon and this is why it can be called Omega 3, and is the main member of the
omega-3 family.
G. Eicosapentaenoic acid (EPA) , may be derived inefficiently from linolenic acid and is
the main fatty acid found in fish, also called omega 3.
H.Docosahexaenoic acid (DHE), is an omega 3 fatty acid, is synthesized in body from
alph-linolenic acid, and is present in fish. DHA is present in retina and brain.
Nonessential
I.Sterols serve a vital function in the body, are produced by the body, and are not
essential nutrients. This structure of a lipid is cholesterol which is a waxy substance that
doesn't look like a triglyceride. It doesn't have a glycerol backbone or fatty acids, but
because it is impermeable in water, it is a lipid.
1

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Chapter 16 on page 453

Lipids
J.CIS- Trans Fatty acids hydrogenation makes monounsaturated and polyunsaturated
fatty acids go from a state of their original form that is cis to a trans form. Addition
of hydrogen ions will cause vegetable oil to harden. Additionally, they may stimulate
cholesterol synthesis, and are potentially carcinogenic.
Absorption process of triglycerides. This is the fat that your body deals with most of
the time. They are absorbed with the transport of chylomicrons into the lymphatic system
which in turn will pour into the blood stream at the thoracic duct. Once it enters the blood
stream the chylomicrons take the triglycerides into the cells. The triglycerides that are on
the outer part of the chylomicrons are broken down by lipoprotein lipase. Lipoprotein lipase
can be found on the walls of capillaries. It is this enzyme that will break it into fatty acids
and monoglycerides. The fatty acids are taken by the body's cells while the monoglycerides
are taken to the liver to be processed.
More Info on Lipids:
1. Lipids are structural components found in every cell of the human body. That is, they
form the lipid bilayer found in individual cells. They also serve as the myelin sheath
found in neurons.
2. Lipids provide us with energy. Most of that energy is in the form of triacylglycerols.
3. Both lipids and lipid derivatives serve as vitamins and hormones.
4. Lipophilic bile acids aid in lipid solubility.
Recommendations for Fat Intake: Although there are different types of fat the effect
on health and disease, the basic message is simple: leave out the bad fats and replace them
with good fats. Try to limit saturated fats in your diet, and try to eliminate trans fats
from partially hydrogenated oils.Replace saturated and trans fats with polyunsaturated
and monounsaturated fats. As of January 1, 2006, trans fat must be listed on food labels.
More and more "trans-fat" free products are becoming available. Keep in mind, though, that
according to the FDA, a product claiming to have zero trans fat can actually contain up
to a half gram. You may still want to scan the ingredient list for "partially hydrogenated
vegetable oil" and "vegetable shortening," and look for an alternative product without those
words.

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11.7 Vitamins and Minerals

Figure 103
vitamins.

Fruits and vegetables are often a good source of

We all need micronutrients in small quantities to sustain health. Micronutrients include

dietary minerals and vitamins. While all minerals and vitamins can be obtained through
food, many people do not consume enough to meet their micronutrient needs and instead
may take a supplement.
Microminerals or trace elements include at least iron, cobalt, chromium, copper, iodine,
manganese, selenium, zinc, and molybdenum. They are dietary minerals needed by the human
body in very small quantities (generally less than 100mg/day) as opposed to macrominerals
which are required in larger quantities. (Note that the use of the term "mineral" here is
distinct from the usage in the geological sciences.)

11.7.1 Vitamins
Vitamins are organic compounds that are essential for our body to function properly. Most
vitamins are obtained from what you consume, because the body is unable to manufacture
most of the essential vitamins that you need to survive. Here are types of vitamins and their
roles:
Vitamin

304

Food
Sources

Functions

Problems
When Deficient

Problems
With Taking
Too Much

Vitamins and Minerals

Vitamin

Food
Sources

A (retinol)

Ingested
in a precursor form.
Found in animal sources
such as milk
and eggs.
Also found
in carrots
and spinach
(contain pro
vitamin A
carotenoids).

Functions

Vitamin A is
a fat-soluble
vitamin. It
helps cells
differentiate,
also lowering
your risk of
getting cancer. Vitamin
A helps to
keep vision
healthy. It is
required during pregnancy.
Vitamin A
also influences
the function
and development of
sperm, ovaries
and placenta
and is a vital
component of
the reproductive process.

Problems
When Deficient
Night blindness, impaired
growth of
bones and
teeth

Problems
With Taking
Too Much
Headache,
dizziness, nausea, hair loss,
abnormal development of
fetus

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Nutrition
Vitamin

306

Food
Sources

B1 (thiamine)

Found in
wheat germ,
whole wheat,
peas, beans,
enriched flour,
fish, peanuts
and meats.

B2 (riboflavin)

Found in
milk cheese,
leafy green
vegetables,
liver, soybeans yeast
and almonds.
Exposure to
light destroys
riboflavin.

Functions

Problems
When Deficient
Beriberi,
muscular
weakness, enlarged heart

Vitamin B1
is a watersoluble vitamin that the
body requires
to break down
carbohydrates,
fat and protein. The
body needs
vitamin b
in order to
make adenine
triphosphate
(ATP). Vitamin B1 is also
essential for
the proper
functioning of
nerve cells.
Vitamin B2
Dermatitis,
is a waterblurred vision,
soluble vigrowth failure
tamin that
helps the
body process
amino acids
and fats. Activated vitamin
B6 and folic
acid helps
convert carbohydrates
to adenosine
triphosphate
(ATP). Sometimes vitamin
B2 can act
as an antioxidant.

Problems
With Taking
Too Much
Can interfere
with the absorption of
other vitamins

Unknown

Vitamins and Minerals

Vitamin

Food
Sources

B3 (niacin)

Found
in beets,
brewer's yeast,
beef liver,
beef kidney,
pork, turkey,
chicken, veal,
fish, salmon,
swordfish,
tuna, sunflower seeds,
and peanuts.

Functions

Vitamin B3
is required
for cell respiration and
helps release
the energy in
carbohydrates,
fats, and proteins. It helps
with proper
circulation
and healthy
skin, functioning of the nervous system,
and normal
secretion of
bile and stomach fluids. It
is used in the
synthesis of
sex hormones,
treating
schizophrenia and other
mental illnesses, and
as a memoryenhancer.

Problems
When Deficient
Pellagra, diarrhea, mental disorders

Problems
With Taking
Too Much
High blood
sugar and uric
acid, vasodilation

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Nutrition
Vitamin

C (ascorbic
acid)

308

Food
Sources
Found in citrus fruits such
as oranges,
grapefruit and
lemon.

Functions

Vitamin C is
an essential
water-soluble
vitamin. It
is needed to
make collagen. Vitamin
C also aids in
the formation
of liver bile
which helps to
detoxify alcohol and other
substances.
Evidence indicates that
vitamin C
levels in the
eye decrease
with age and
this may be
a cause of
cataracts. Vitamin C has
been reported
to reduce activity of the
enzyme, aldose reductase, which
helps protect
people with
diabetes. It
may also protect the body
against accumulation
or retention
of the toxic
mineral, lead.

Problems
When Deficient
Scurvy, delayed wound
healing, infections

Problems
With Taking
Too Much
Gout, kidney stones,
diarrhea, decreased copper

Vitamins and Minerals

Vitamin

Food
Sources

Functions

Problems
When Deficient
Produced by
Vitamin D is
Lack of Vitathe human
a fat-soluble
min D results
body during
vitamin that
in rickets for
exposure to
helps mainchildren and
the ultraviolet tain blood lev- osteomalacia
rays of the
els of calcium. for adults.
sun.
Vitamin D is
necessary for
healthy bones
and teeth. Vitamin D plays
a role in immunity and
blood cell formation and
also helps
cells differentiate this
lowers your
chance of getting cancer.
Found in veg- Vitamin E
Unknown
etable oils,
is an antioxnuts, and
idant that
green leafy
protects cell
vegetables.
membranes
Fortified ceand other fatreals are also
soluble parts
an important
of the body,
source of vita- such as LDL
min E in the
cholesterol
United States. (the bad
cholesterol),
from damage.

Problems
With Taking
Too Much
Calcification
of soft tissue,
diarrhea, possible renal
damage

Diarrhea,
nausea,
headaches, fatigue, muscle
weakness

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Nutrition
Vitamin

Food
Sources

Found in
kale, collard greens,
spinach, mustard greens,
turnip greens
and Brussels
sprouts. Also
found vegetable oils
such as soybean, canola,
cottonseed,
and olive. Additionally, the
normal flora
of the large
intestine produce vitamin
K, which our
body is able
to absorb and
use
Found in
many vegetables including, broccoli,
peas, asparagus, spinach,
green leafy
types. Also
found in fresh
fruit, liver
and yeast.
Found in
meat, fish,
eggs and milk
but not in
vegetables.

Folic acid

B12

310

Functions

Problems
When Deficient
Easy bruising
and bleeding

Problems
With Taking
Too Much
Can interfere
with anticoagulant medication

Coenzyme
needed for
production of
hemoglobin
and formation
of DNA.

Megaloblastic
anemia, spina
bifida

May mask
B12 deficiency

Vitamin B12
is needed to
make red
blood cells.
Supplements
can help some
types of anemia.

Pernicious
anemia

Unknown

Vitamin K
by helping
transport Ca,
vitamin K
is necessary
for proper
bone growth
and blood
coagulation.

Vitamins and Minerals

Vitamin

B6 (pyridoxine)

Food
Sources
Found in cereals, yeast,
liver, and fish.

Functions

Vitamin B6
is a coenzyme
in amino acid
synthesis.

Problems
When Deficient
Rare to be
deficient, convulsions, vomiting, seborrhea, muscular weakness

Problems
With Taking
Too Much
Insomnia, neuropathy

Folic acid and cancer prevention

Women of childbearing age are often encouraged to take a folic acid supplement to help
reduce the risk of certain birth defects. Research cited by the Harvard School of Public
Health shows that folic acid may have even more benefits, and not just for the developing
fetus. Their study shows that people who get more than the recommended amount of folic
acid due to diet or supplements can actually lower the risk of developing colon or breast
cancer. Since alcohol blocks the absorption of folic acid and inactivates circulating folate,
this can be especially important to those who drink alcohol frequently (more than one drink
per day). The current recommended intake for folic acid is 400 micrograms per day. There
are many excellent sources of folic acid, including prepared breakfast cereals, beans, and
fortified grains. So if you would like to reduce your risk of colon or breast cancer, be sure to
get more than 400 micrograms per day!
Fat soluble vitamins A, D, E, K
With fat soluble vitamins you need the presence of fat in your diet to absorb them, this is
because the bile will not be secreted to help with emulsification and therefore the fat vitamins
will not be broken down for absorption. Fat soluble vitamins are stored in organs such as
the liver, spleen, and other fatty tissues in the body. Because of this, excessive amounts of
fat-soluble vitamins can accumulate in the body resulting in toxicity, but this rarely comes
from excessive dietary intake but rather from improper use of vitamin supplements. The
other, water-soluble vitamins, do not build up to toxic levels because they are regularly
excreted in the urine.

11.7.2 Minerals
Minerals are atoms of certain chemical elements that are essential for body processes.
Minerals are inorganic, meaning that they do not contain the element carbon. They are
either produced by our body, or we obtain them by eating certain foods that contain them.
They are ions found in blood plasma and cell cytoplasm, such as sodium, potassium, and
chloride. In addition, minerals represent much of the chemical composition of bones (calcium,
phosphorus, oxygen). They also contribute to nerve and muscle activity (sodium, potassium,
calcium). Minerals serve several many other functions as well. There are 21 minerals
considered essential for our bodies. Nine of the essential minerals in the body account for
less than .01% of your body weight. Because of the small amount of these minerals that
our body needs, we call them trace minerals. The 12 most important minerals and their
functions are listed below:

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Nutrition
Mineral
Calcium (Ca)

Source
Calcium can be found in
dairy products, dark green
vegetables and legumes.

Chloride (Cl)

Chloride is mainly found in

table salt.

Copper (Cu)

Copper can be found in

seafood, nuts, and legumes.
Flourine is evident in flouridated water, tea, and seafood.

Flourine (F)

Iodine (I)

Iodine is a component in
iodized salt, marine fish and
shellfish.

Iron (Fe)

Iron can be found in green

leafy vegetables, whole grains
foods, legumes, meats, and
eggs.
Magnesium is found in whole
grains foods, and in green
leafy vegetables.
Phosphorus can be found
in meat, poultry, and whole
grain foods.
Potassium is widespread in
the diet, especially in meats
and grains.

Magnesium (Mg)

Phosphorus (P)

Potassium (K)

Sodium (Na)

Sulfur (S)
Zinc (Zn)

312

Sodium is found in table salt,

is a major component of water
and also widespread in the
diet.
Sulfur is found in meat and
diary products.
Zinc is found in whole grain
foods, meats, and seafood.

Use in the body

It contributes to bone and
teeth formation. In addition,
calcium also contributes to
nerve and muscle action, and
blood clotting.
It plays a role in the acidbase balance, stomach acid
formation, and body water
balance.
It participates in the synthesis
of hemoglobin and melanin.
It accounts for the maintenance of teeth, and perhaps
the maintenance of bone as
well.
Although a very small amount
is needed for our body, according to some, iodine still
plays a role in our body's function. It can also be found in
seaweed. It is needed for the
thyroid hormone.
It is needed for composition of
hemoglobin, myoglobin, and
certain enzymes.
It is the coenzyme found in
several enzymes.
It serves as components of
bones, teeth, phospholipids,
ATP, and nucleic acids.
It deals with muscle and nerve
function, and also is a major
component of intracellular
fluid.
It participates in the functioning of muscles and nerves.

It is a component of many
proteins.
It is a component of many
enzymes.

Nutritional Disorders

11.8 Nutritional Disorders

Body Mass Index became popular during the early 1980s as obesity started to become a
discernible issue in prosperous Western society. BMI provided a simple numeric measure
of a person's "fatness" or "thinness", allowing health professionals to discuss the problems
of over- and under-weight more objectively with their patients. However, BMI has become
controversial because many people, including physicians, have come to rely on its apparent
numerical "authority" for medical diagnosis but that has never been the BMI's purpose.
It is meant to be used as a simple means of classifying sedentary (physically inactive)
individuals with an average body composition.[1] For these individuals, the current value
settings are as follows: a BMI of 18.5 to 25 may indicate optimal weight; a BMI lower than
18.5 suggests the person is underweight while a number above 25 may indicate the person
is overweight; a BMI below 15 may indicate the person has an eating disorder; a number
above 30 suggests the person is obese (over 40, morbidly obese).
In physiology the term weight is used interchangeably with mass. For a given body
shape and given density, the BMI will be proportional to weight e.g. if all body weight
increase by 50%, the BMI increases by 50%.
BMI is defined as the individual's body weight divided by the square of their height. The
formulas universally used in medicine produce a unit of measure that is not dimensionless;
it has units of kg/m2. Body mass index may be accurately calculated using any of the
formulas below.
SI units
weight (kg)
BMI = height
2
(m2 )

BMI
Below 18.5
18.5 - 24.9
25.0 - 29.9
30.0 and Above

US units
weight
BMI = 703 height
2

(lb)
(in2 )

UK mixed units
(stone)
BMI = 6.35 weight
height 2 (m2 )

Weight Status
Underweight
Normal
Overweight
Obese

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Nutrition

Figure 104

Either way can be a disorder.

The U.S. National Health and Nutrition Examination Survey of 1994 indicates that 59% of
American men and 49% of women have BMIs over 25. Extreme obesity a BMI of 40 or
more was found in 2% of the men and 4% of the women. There are differing opinions on
the threshold for being underweight in females, doctors quote anything from 18.5 to 20 as
being the lowest weight, the most frequently stated being 19. A BMI nearing 15 is usually
used as an indicator for starvation and the health risks involved, with a BMI <17.5 being
one of the criteria for the diagnosis of anorexia nervosa.
Anorexia nervosa: is a psychiatric diagnosis that describes an eating disorder characterized
by low body weight and body image distortion with an obsessive fear of gaining weight.
Individuals with anorexia often control body weight by voluntary starvation, purging,
vomiting, excessive exercise, or other weight control measures, such as diet pills or diuretic
drugs. It primarily affects young adolescent girls in the Western world and has one of the
highest mortality rates of any psychiatric condition, with approximately 10% of people
diagnosed with the condition eventually dying due to related factors.[1] Anorexia nervosa is a
complex condition, involving psychological, neurobiological, and sociological components.[2]
Bulimia nervosa: commonly known as bulimia, is generally considered a psychological
condition in which the subject engages in recurrent binge eating followed by an intentional
purging. This purging is done in order to compensate for the excessive intake of the food

314

Metabolism
and to prevent weight gain. Purging typically takes the form of vomiting; inappropriate use
of laxatives, enemas, diuretics or other medication, and excessive physical exercise.

11.9 Metabolism
Absorptive and post absorptive stage of metabolism
The body has two phases to its metabolic cycle. The first is known as the absorptive stage.
This stage happens 3-4 hours after a typical meal. During this phase nutrients are absorbed
by the body. In other words this is the stage where energy is stored into macromolecules.
During the post-absorptive stage the nutrients are not being absorbed instead this is the
stage where it is being mobilized.
Insulin
The changes in the body that occur between the absorptive and post-absorptive stages
are triggered by the changes in the plasma concentration of insulin. Insulin encourages
the synthesis of energy storage molecules. When plasma glucose levels in the bloodstream
increase during the absorptive stage, insulin is secreted from the pancreas. When the plasma
glucose levels decrease, the post-absorptive phase begins. Insulin acts on several different
tissues in the body and influences almost every major aspect of energy metabolism. Insulin
supports and promotes all aspects of the absorptive phase by helping store energy in all
tissues. It also inhibits the reactions of the post-absorptive phase. Insulin also affects the
transport of nutrients across the membrane of ALL body cells except for those located in the
liver and CNS. Insulin also has a part in growth where it needs to be present in the blood
stream in order for the hormones to effect normally. Epinephrine and sympathetic
nervous activity on metabolism
The sympathetic system and epinephrine suppress insulin and stimulate glycogen secretion.
This effects the post absorptive phase by making metabolic adjustments. During the post
absorptive phase, plasma glucose levels decrease and cause an increase of glycogen secretion.
It also acts directly on glucose receptors in the CNS. This causes a rise in epinephrine
secretion by the adrenal medulla. The rise in epinephrine creates a cascade event where
the body sends signals to all the tissues (except skeletal muscles) to switch to the post
absorptive phase.

11.10 Diabetes
Diabetes Mellitus
Diabetes is essentially any condition which is characterized by an increase in urine production and secretion. The Random House Webster's Unabridged Dictionary defines it as
the following..."A disorder of carbohydrate metabolism, usually occurring in genetically
predisposed individuals, characterized by inadequate production or utilization of insulin and
resulting in excessive amounts of glucose in the blood and urine, excessive thirst, weight loss,
and in some cases progressive destruction of small blood vessels leading to such complications
as infections and gangrene of the limbs or blindness." In other words, when food is put into

315

Nutrition
the body you get high levels of glucose in your blood stream thus resulting in the release of
Insulin to take up and metabolize this glucose. It also stimulates the liver to store the glucose
as glycogen, thus resulting in the storage of nutrients and the lowering of glucose levels in
the blood. On the flip side you have Glucagon which helps in the breakdown of the stored
nutrients when you need them, thus having the opposite effect of Insulin. People who are
unable to produce insulin on their own, or are lacking/have damaged their insulin receptors
develop what is known as "Diabetes Mellitus." There are two types of Diabetes Mellitus,
Type I, aka, Insulin Dependent Diabetes Mellitus(IDDM), and Type II, aka, Non-Insulin
Dibetes Mellitus(NIDDM).
Type I diabetes is believed to be an autoimmune disease which has been present since
birth or has been brought on by exposure to a virus which causes insulin production by
the pancreas to be impaired. This usually results in a person having to receive insulin
from an external source. Without this external administration, the body would turn to the
metabolism of fat, which leads to the build up of Ketones in the blood, which leads to blood
acidosis and could result in a coma or possible death. The onset of Type I diabetes is most
commonly seen under the age of 25.
Although Type II Diabetes is like Type I in many ways, it's onset is usually the result of
poor lifestyle choices, particularly eating a diet high in sugars and fats while getting little or
no physical exercise. Following this routine will quickly lead to damaging or the shutting
down of your insulin receptors completely, thus resulting in the lack of glucose storage and
the expulsion of essential nutrients from the body via urination. Just like with Type I
Diabetes, Type II can have detrimental effects on the body including blindness, kidney
disease, atherosclerosis, and again, even lead to the loss of extremities due to gangrene.
Doctors have projected that upwards of seven million Americans may have diabetes, yet
many may not know it. If you or someone you know has been suffering from such things
as: frequent urination, especially at night; unusual hunger and/or thirst; unexplained
weight gain or loss; blurred vision; sores that don't heal; or excessive fatigue then it is
highly recommended that you have your fasting blood glucose level checked by a physician.
Maintaining an active lifestyle and making sound nutritional choices may greatly extend
your life by protecting you from the ills of diabetes.

11.11 Calories, Exercise, and Weight

Energy Balance and Body Weight
Energy is measured in units called calories. A calorie is the amount of energy that is needed
to raise the temperature of 1 gram of water by one degree Celsius. Because a calorie is
such a small amount, scientists use a larger unit to measure intake, called a kilocalorie. A
kilocalorie is also referred to often as a capital "C" Calorie, and is equal to 1000 calories.
When we "count" calories, we are actually counting the big Calories.
The old saying, "you are what you eat" is very much true. According to scientists, the
average adult consumes 900,000 calories per year. Most people tend to take in more calories
than their body needs. An intake of 120 extra calories a day, or around 5% excess in calories,
yields an annual increase of 12 extra pounds of body weight. The more developed countries
tend to consume more calories than others because of the increasing availability and dieting

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Calories, Exercise, and Weight

habits of eating refined foods with little nutrition in them and lots of saturated fat. In our
society, there is a huge emphasis put on a person's image and how thin they are, and less
emphasis put on what's most important--the nutrition our body receives. While our body
do need calories every day to keep us going, we need to watch the amount of calories we
consume in order to maintain good health and proper body weight.
Our Caloric intake is linked directly to our health status. Being overweight is generally
defined as being 15-20% above ideal body weight, while obesity is defined as being more than
20% above it. People who weigh 10% less than ideal are considered underweight. This is less
common in the more developed countries. In less developed countries such as South Africa,
being underweight is quite common because they lack the nutrition to maintain good health.
How do we gain weight? When we consume more calories than our body can burn in a
day, the excess energy is stored in specialized cells as fat. It is also important to know that
the three classes of nutrients have different Caloric contents. Carbohydrates and proteins
contain only four Calories per gram, while fat contains about nine. Because of this, it is
essential that we watch our amount of fat intake. If we continuously feed our body more
calories than is needed, our body will produce more fat cells, to store the excess energy.
This contributes to gaining weight.
It is more difficult for chronically overweight persons to lose weight than normal-weight
persons. This is because they are constantly fighting the body's own weight-control system,
which responds as if the excess weight were normal. Our body is capable of measuring how
much we intake, and maintaining our weight. When an overweight person goes on a diet,
and consumes less calories, their body will respond as if they are starving, and try to save
energy where it can to make up for the decrease in received calories.

Figure 105
weight.

Exercise is a great way to maintain healthy body

Maintaining a healthy body weight

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Nutrition
To maintain a stable body weight, our consumption of calories needs to be equal to the
amount of calories we use in a day. You can determine your daily energy needs by determining
your basal metabolic rate (BMR). Your BMR is the energy your body needs to perform
essential activities. Some examples of essential activities are breathing, and maintaining
organ function. Your metabolic rate can be influenced by your age, gender, muscular activity,
body surface area and environmental temperature.
Physical Activity: An efficient way to use calories
Although the BMR stays about the same, we can dramatically change the amount of calories
we burn in a day by participating in physical activity. It is important to note that heavier
people do more work per hour than normal-weight people, for the same level of activity. We
must spend about 3,500 Calories to lose one pound of fat. The best approach to weight loss,
recommended by nutritionists, is to reduce the Caloric intake by a small amount each day
while gradually increasing your amount of physical activity.
BMR: Determining how many calories we need
There are several factors that influence the BMR. Each person's body has different needs.
BMR needs vary with gender and body composition. Muscle tissue consumes more energy
than fat tissue. Typically, males need more calories than females, because they generally
have more muscle tissue. Males use up calories faster than women. BMR also varies with
your age as well. As we age, our body needs less and less calories. In addition, some health
conditions can contribute to our needed calories. Health conditions such as fever, infections,
and hyperthyroidism are examples of health conditions that lower your BMR. Our stress level
effects our needed calorie intake as well. So does our increase or decrease in consumption,
and our rate of metabolism, which varies with individual genetics.
Calculating Your BMR
Here are the steps to determining your BMR, or, the amount of energy your body needs to
perform essential activities:
1. First calculate your weight into kilograms. This is obtained by dividing the number of
pounds by 2.2.
2. For Males: multiply your weight in kilograms by 1.0. For Females: multiply your weight
in kilograms by 0.9.
3. This number approximates the number of Calories you consumer per hour. Now multiply
this number by 24 to estimate how many Calories you need per day to support basic
metabolic functions.
4. The end result is your personal basal metabolic rate!
Exercise
Living a healthy, well-balanced life involves good nutrition and adequate exercise. They
work hand in hand.
There are many benefits to exercising.
Your chances of living longer increases.
You decrease your chances of getting diseases such as:
Heart disease or problems with circulation

318

Glossary

Many types of cancer

Type 2 diabetes
Arthritis
Osteoporosis
Depression
Anxiety
Controls weight
The costs of being physically active far outweigh the medical costs for those who are not
physically active.
Cardiovascular Exercise
Thirty minutes a day of moderate intensity exercise or physical activity has been
shown to make noticeable increases in breathing and heart rate.
METs (metabolic equivalents) are the amount of energy it takes while at rest (1 calorie
per every 2.2 pounds of body weight per hour). Moderate intensity activities can get
you to burn energy 3-6 times more depending upon the activity.
Walking is ideal for everyone.
The MET scale chart on the Harvard School of Public Health web site is interesting.
Feeling whats right
A study suggests that those with disabilities, who are older, or who are out of shape
get the same benefit from 30 minutes of lower intensity exercise as those who are
younger and more fit do from more intense activity.
Beyond the heart
There are other areas that benefit from different types of exercise such as strength
training. These types of exercises help balance, muscle strength, and overall function.
Resistance or strength training can possibly decrease the loss of lean muscle tissue
and even replace some already lost.
It can also decrease fat mass and increase resting metabolic rate.
It is effective in fighting osteoporosis.
It also helps maintain functional tasks in older populations.
Flexibility training or stretching exercises increases range of motion, decrease
soreness, and injury.

11.12 Glossary
Amino acids
The building blocks of protein in the body. There are nine essential amino acids that are
not manufactured by the body and must come from the diet.
Anabolism
Refers the cumulative metabolic intracellular, molecular processes by which every cell
repairs itself and grows.(synthesizing).
Anorexia
A common eating disorder characterized by an abnormal loss of the appetite for food
antioxidants

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Nutrition
Compounds that protect against cell damage inflicted by molecules called oxygen-free
radicals, which are a major cause of disease and aging.
Bulimia Nervosa
Eating disorder characterized by binge eating followed by an intentional purging.
Catabolism
The opposite of Anabolism. The metabolic process that breaks down molecules into smaller
units. It is made up of degradative chemical reactions in the living cell.
Cirrhosis of the liver
An irreversible advanced scarring of the liver as a result of chronic inflammation of the
liver. Can be caused by alcoholism or obesity.
Complete Proteins
Proteins that contain ample amounts of all of the essential amino acids
Deamination
When an amino acid group breaks off an amino acid that makes a molecule of ammonia
and keto acid.
Diverticulosis
A diet low in dietary fiber increases the risk, this is the pouches called diverticula formation
on the outer portion of the large intestine.
Gastric Bypass Surgery
An operation where a small gastric pouch is created and the remainder of the stomach
bypassed
Incomplete Proteins
Proteins that contain some but not all of all of the essential amino acids required by the
body
Ipecac
A drug used to induce vomiting
Kwashiorkor
A childhood form of malnutrition caused by general lack of protein or deficiency in one or
more amino acids. Appearance of a person with this is a swollen belly due to inadequate
production of albumin, which causes the blood to have a lower osmotic pressure, resulting
in more fluids escaping from the plasma.
Marasmus
malnutrition cause by a lack of kcalorie intake. Appearance of a person with this is a
skeletal one.
Malnutrition
An imbalanced nutrient and or energy intake.

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Health Information Online

Obesity
A condition in which the natural energy reserve in fatty tissue increased to a point where
it is thought to be a risk factor for certain health conditions or increased mortality
Peptide
Two or more amino acids linked together by a bond called a peptide bond.
Polypeptide
A string of amino acids linked together by peptide bonds. A protein is an example of a
polypeptide.
Starvation
A severe reduction in vitamin, nutrient, and energy intake, and is the most extreme form
of malnutrition

11.13 Health Information Online

11.14 Review Questions
Answers for these questions can be found here2
1. Nonessential amino acids
A) are stored in the body
B) are only needed occasionally
C) can be produced in the body
D) can be taken in supplements
2. Micronutrients include
A) minerals and vitamins
B) lipids and fatty acids
C) amino acids and proteins
D) vitamins and minerals
3. The body requires amino acids to
A) produce new red blood cells
B) produce new protein
C) replace damaged red blood cells
D) replace damaged protein

http://en.wikibooks.org/wiki/Human_Physiology/Appendix_1:_answers_to_review_
questions#Nutrition

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Nutrition
E) A and C
F) B and D
4. The function of lipids
A) store energy
B) organ protection
C) temperature regulator
D) emulsifiers
E) all of the above
5. This vitamin is a vital component of the reproductive process and lowers the risk of
getting cancer
A) B12
B) Folic Acid
C) Niacin
D) Thiamine
E) Retinol
6. This vitamin is needed to make red blood cells
A) B1
B) B2
C) B6
D) B12
7. This participates in the synthesis of hemoglobin and melanin
A) Copper
B) Chloride
C) Calcium
D) Iron
E) Iodine
8. I go to visit my grandmother and see that she has multiple bruises- from this I may
assume that
A) she has a vitamin A deficiency
B) she is old and just clumsy
C) she has a vitamin K deficiency
D) she has scurvy
E) she has rickets

322

References
9. As a pirate I may get scurvy because
A) I am not getting enough vegetables on the ship
B) I am not getting enough fruit on the ship
C) I am eating too much fish on the ship
D) I am getting too much sun on the ship
E) I am drinking too much rum on the ship
10. I am taking anticoagulant medication and it doesnt seem to be working, this could be
because
A) I have too much vitamin A
B) I have too much B12
C) I have too much sodium
D) I have too much vitamin E
E) I have too much vitamin K
11. Which of these are fat soluble?
A) Vitamin K
B) Vitamin E
C) Vitamin D
D) Vitamin A
E) All of the above

11.15 References
Van De Graaff (2002) Human Anatomy 6th ed. McGraw-Hill Higher Education
Windmaier, P.W. Raff, H. Strang, T.S. (2004) Vander, Sherman, & Luciano's Human
Physiology, the Mechanisms of Body Function 9th ed. Mcgraw-Hill
Starr & McMillan (2001) Human Biology 6th ed. Thomson-Brooks/cole.
Spurlock, Morgan (2004) Super Size Me Hart Sharp Video
Sylvia S. Mader (2006) Human Biology 9th ed. McGraw-Hill Higher Education
Anatomy & Physiology Revealed (2007) McGraw-Hill Higher Education
Random House Webster's Unabridged Dictionary 2nd ed. (2001) Random House

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12 The Endocrine System

12.1 Introduction To The Endocrine System
The endocrine system is a control system of ductless glands that secrete hormones within
specific organs. Hormones act as "messengers," and are carried by the bloodstream to
different cells in the body, which interpret these messages and act on them.
It seems like a far fetched idea that a small chemical can enter the bloodstream and cause
an action at a distant location in the body. Yet this occurs in our bodies everyday of our
lives. The ability to maintain homeostasis and respond to stimuli is largely due to hormones
secreted within the body. Without hormones, you could not grow, maintain a constant
temperature, produce offspring, or perform the basic actions and functions that are essential
for life.
The endocrine system provides an electrochemical connection from the hypothalamus of the
brain to all the organs that control the body metabolism, growth and development, and
reproduction.
There are two types of hormones secreted in the endocrine system: Steroidal (or lipid based)
and non-steroidal, (or protein based) hormones.
The endocrine system regulates its hormones through negative feedback, except in very
specific cases like childbirth. Increases in hormone activity decrease the production of that
hormone. The immune system and other factors contribute as control factors also, altogether
maintaining constant levels of hormones.

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The Endocrine System

12.2 Types of Glands

Figure 106 Major endocrine glands. (Male left,

female on the right.) 1. Pineal gland 2. Pituitary
gland 3. Thyroid gland 4. Thymus 5. Adrenal
gland 6. Pancreas 7. Ovary 8. Testis
Exocrine Glands are those which release their cellular secretions through a duct which
empties to the outside or into the lumen (empty internal space) of an organ. These include
certain sweat glands, salivary and pancreatic glands, and mammary glands. They are not
considered a part of the endocrine system.
Endocrine Glands are those glands which have no duct and release their secretions directly
into the intercellular fluid or into the blood. The collection of endocrine glands makes up
the endocrine system.
The main endocrine glands are the pituitary (anterior and posterior lobes), thyroid,
parathyroid, adrenal (cortex and medulla), pancreas and gonads.

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Hormones and Types

The pituitary gland is attached to the hypothalamus of the lower forebrain.
The thyroid gland consists of two lateral masses, connected by a cross bridge, that are
attached to the trachea. They are slightly inferior to the larynx.
The parathyroid glands are four masses of tissue, two embedded posterior in each lateral
mass of the thyroid gland.
One adrenal gland is located on top of each kidney. The cortex is the outer layer of the
adrenal gland. The medulla is the inner core.
The pancreas is along the lower curvature of the stomach, close to where it meets the first
region of the small intestine, the duodenum.
The gonads (ovaries and testes) are found in the pelvic cavity.

12.3 Hormones and Types

A hormone is a type of chemical signal. They are a means of communication between cells.
The endocrine system produces hormones that are instrumental in maintaining homeostasis
and regulating reproduction and development. A hormone is a chemical messenger produced
by a cell that effects specific change in the cellular activity of other cells (target cells).
Unlike exocrine glands (which produce substances such as saliva, milk, stomach acid and
digestive enzymes), endocrine glands do not secrete substances into ducts (tubes). Instead,
endocrine glands secrete their hormones directly into the surrounding extra cellular space.
The hormones then diffuse into nearby capillaries and are transported throughout the body
in the blood.
The endocrine and nervous systems often work toward the same goal. Both influence other
cells with chemicals (hormones and neurotransmitters). However, they attain their goals
differently. Neurotransmitters act immediately (within milliseconds) on adjacent muscle,
gland, or other nervous cells, and their effect is short-lived. In contrast, hormones take
longer to produce their intended effect (seconds to days), may affect any cell, nearby or
distant, and produce effects that last as long as they remain in the blood, which could be
up to several hours.
In the following table there are the major hormones, their target and their function once in
the target cell.
Endocrine
Gland

Hormone
Released

Chemical
Class

Target Tissue/Organ

Hypothalamus

Hypothalamic releasing
and inhibiting
hormones

Peptide

Anterior pituitary

Major Function of Hormone

Regulate anterior pituitary
hormone

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The Endocrine System

Endocrine
Gland

Hormone
Released

Chemical
Class

Target Tissue/Organ

Posterior
Pituitary

Antidiuretic
(ADH)

Peptide

Kidneys

Oxytocin

Peptide

Uterus, mammary glands

Thyroid stimulating (TSH)

Adrenocorticotropic
(ACTH)
Gonadotropic
(FSH, LH)

Glycoprotein

Thyroid

Peptide

Adrenal cortex

Glycoprotein

Gonads

Prolactin
(PRL)
Growth (GH)

Protein

Mammary
glands
Soft tissue,
bones

Thyroxine
(T4) and Triiodothyronie
(T3)

Iodinated
amino acid

All tissue

Calcitonin

Peptide

Parathyroids

Parathyroid
(PTH)

Peptide

Adrenal
Cortex

Glucocorticoids (cortisol)

Steroid

Bones, kidneys and intestine

Bones, kidneys and intestine
All tissue

Anterior Pituitary

Thyroid

328

Protein

Major Function of Hormone

Stimulates
water reabsorption by
kidneys
Stimulates
uterine muscle
contractions
and release
of milk by
mammary
glands
Stimulates
thyroid
Stimulates
adrenal cortex
Egg and
sperm production, sex
hormone production
Milk production
Cell division,
protein synthesis and
bone growth
Increase
metabolic
rate, regulates
growth and
development
Lowers blood
calcium level
Raises blood
calcium level
Raise blood
gluclose level,
stimulates
breakdown of
protein

Hormones and Types

Endocrine
Gland

Hormone
Released

Chemical
Class

Mineralocorticoids (aldosterone)

Steroid

Sex Hormones

Steroid

Adrenal
Medulla

Epinephrine
and norepinephrine

Modified
amino acid

Pancreas

Insulin

Protein

Glucagon

Protein

Testes

Androgens
(testosterone)

Steroid

Ovaries

Estrogen and
progesterone

Steroid

Thymus

Thymosins

Peptide

Pineal
Gland

Melatonin

Modified
amino acid

Target Tissue/Organ

Major Function of Hormone

Kidneys
Reabsorb
sodium and
excrete potassium
Gonads, skin, Stimulates
muscles and
reproductive
bones
organs and
brings on sex
characteristics
Cardiac and
Released in
other muscles
emergency situations, raises
blood glucose
level, fight
or flight response
Liver, muscles, Lowers blood
adipose tissue glucose levels, promotes
formation of
glycogen
Liver, muscles, Raises blood
adipose tissue glucose levels
Gonads, skin, Stimulates
muscles and
male sex charbone
acteristics
Gonads, skin, Stimulates
muscles and
female sex
bones
characteristics
T lymphoStimulates
cytes
production
and maturation of T
lymphocytes
Brain
Controls circadian and
circannual
rhythms, possibly involved
in maturation
of sexual organs

Hormones can be chemically classified into four groups:

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The Endocrine System

1. Amino acid-derived: Hormones that are modified amino acids.
2. Polypeptide and proteins: Hormones that are chains of amino acids of less than or
more than about 100 amino acids, respectively. Some protein hormones are actually
glycoproteins, containing glucose or other carbohydrate groups.
3. Steroids: Hormones that are lipids synthesized from cholesterol. Steroids are characterized by four interlocking carbohydrate rings.
4. Eicosanoids: Are lipids synthesized from the fatty acid chains of phospholipids found
in plasma membrane.
Hormones circulating in the blood diffuse into the interstitial fluids surrounding the cell.
Cells with specific receptors for a hormone respond with an action that is appropriate for
the cell. Because of the specificity of hormone and target cell, the effects produced by a
single hormone may vary among different kinds of target cells.
Hormones activate target cells by one of two methods, depending upon the chemical nature
of the hormone.
Lipid-soluble hormones (steroid hormones and hormones of the thyroid gland) diffuse
through the cell membranes of target cells. The lipid-soluble hormone then binds to a
receptor protein that, in turn, activates a DNA segment that turns on specific genes. The
proteins produced as result of the transcription of the genes and subsequent translation
of mRNA act as enzymes that regulate specific physiological cell activity.
Water-soluble hormones (polypeptide, protein, and most amino acid hormones) bind
to a receptor protein on the plasma membrane of the cell. The receptor protein, in turn,
stimulates the production of one of the following second messengers:
Cyclic AMP (cAMP) is produced when the receptor protein activates another membranebound protein called a G protein. The G protein activates adenylate cyclase, the enzyme
that catalyzes the production of cAMP from ATP. Cyclic AMP then triggers an enzyme
that generates specific cellular changes.
Inositol triphosphate (IP3) is produced from membrane phospholipids. IP3, in turn, triggers
the release of CA2+ from the endoplasmic reticulum, which then activates enzymes that
generate cellular changes.
Endocrine glands release hormones in response to one or more of the following stimuli:
1. Hormones from other endocrine glands.
2. Chemical characteristics of the blood (other than hormones).
3. Neural stimulation.
Most hormone production is managed by a negative feedback system. The nervous system
and certain endocrine tissues monitor various internal conditions of the body. If action is
required to maintain homeostasis, hormones are released, either directly by an endocrine
gland or indirectly through the action of the hypothalamus of the brain, which stimulates
other endocrine glands to release hormones. The hormones activate target cells, which
initiate physiological changes that adjust the body conditions. When normal conditions
have been recovered, the corrective action - the production of hormones - is discontinued.
Thus, in negative feedback, when the original (abnormal) condition has been repaired, or
negated, corrective actions decrease or discontinue. For example, the amount of glucose in
the blood controls the secretion of insulin and glucagons via negative feedback.

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Endocrine Glands
The production of some hormones is controlled by positive feedback. In such a system,
hormones cause a condition to intensify, rather than decrease. As the condition intensifies,
hormone production increases. Such positive feedback is uncommon, but does occur during
childbirth, where hormone levels build with increasingly intense labor contractions. Also in
lactation, hormone levels increase in response to nursing, which causes an increase in milk
production. The hormone produced by the hypothalamus causing the milk let down and
uterine contraction is oxytocin.

12.4 Endocrine Glands

12.4.1 Pituitary gland
The hypothalamus makes up the lower region of the diencephalons and lies just above the
brain stem. The pituitary gland (hypophysis) is attached to the bottom of the hypothalamus
by a slender stalk called the infundibulum. The pituitary gland consists of two major regions,
the anterior pituitary gland (anterior lobe or adenohypophysis) and the posterior pituitary
gland (posterior lobe or neurohypophysis). The hypothalamus also controls the glandular
secretion of the pituitary gland.
The hypothalamus oversees many internal body conditions. It receives nervous stimuli from
receptors throughout the body and monitors chemical and physical characteristics of the
blood, including temperature, blood pressure, and nutrient, hormone, and water content.
When deviations from homeostasis occur or when certain developmental changes are required,
the hypothalamus stimulates cellular activity in various parts of the body by directing the
release of hormones from the anterior and posterior pituitary glands. The hypothalamus
communicates directives to these glands by one of the following two pathways: The Pituitary
gland is found in the inferior part of the brain and is connected by the Pituitary Stalk.
It can be referred to as the master gland because it is the main place for everything that
happens within the endocrine system. It is divided into two sections: the anterior lobe
(adenohypophysis) and the posterior lobe (neurohypophysis). The Anterior pituitary is
involved in sending hormones that control all other hormones of the body.
Posterior pituitary
Communication between the hypothalamus and the posterior pituitary occurs through
neurosecretory cells that span the short distance between the hypothalamus and the posterior
pituitary. Hormones produced by the cell bodies of the neurosecretory cells are packaged
in vesicles and transported through the axon and stored in the axon terminals that lie in
the posterior pituitary. When the neurosecretory cells are stimulated, the action potential
generated triggers the release of the stored hormones from the axon terminals to a capillary
network within the posterior pituitary. Two hormones, oxytocin and antidiuretic hormone
(ADH), are produced and released this way. Decreased ADH release or decreased renal
sensitivity to ADH produces a condition known as diabetes insipidus. Diabetes insipidus is
characterised by polyuria (excess urine production), hypernatremia (increased blood sodium
content) and polydipsia (thirst).0xytosin is secreated by paraventricular nucleus and a small
quantitis secreted by supraoptic nucleus in hypothalamus.oxytocin is secreted in both males

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The Endocrine System

and females.in female acts on mammaryglands and uterus.in males facilitates release of
sperm in to urethra by causing contraction of vasdeferens.
The posterior lobe is composed of neural tissue [neural ectoderm] and is derived from
hypothalamus. Its function is to store oxytocin and antidiuretic hormone. When the
hypothalamic neurons fire these hormones are release into the capillaries of the posterior
lobe.
The posterior pituitary is, in effect, a projection of the hypothalamus. It does not produce
its own hormones, but only stores and releases the hormones oxytocin and antidiuretic
hormone. ADH is also known as arginine vasopressin (AVP) or simply vasopressin.
Anterior pituitary
The anterior lobe is derived from oral ectoderm and is composed of glandular epithelium.
Communication between the hypothalamus and the anterior pituitary (adenohypophysis)
occurs through hormones (releasing hormones and inhibiting hormones) produced by the
hypothalamus and delivered to the anterior pituitary via a portal network of capillaries.it
consists of three divisions 1.pars distalis,2.pars tuberalis,3.pars intermedia. The releasing
and inhibiting hormones are produced by specialized neurons of the hypothalamus called
neurosecretory cells. The hormones are released into a capillary network or primary plexus,
and transported through veins or hypophyseal portal veins, to a second capillary network or
secondary plexus that supplies the anterior pituitary. The hormones then diffuse from the
secondary plexus aunshine into the anterior pituitary, where they initiate the production of
specific hormones by the anterior pituitary. Many of the hormones produced by the anterior
pituitary are tropic hormones or tropins, which are hormones that stimulate other endocrine
glands to secrete their hormones.
The anterior pituitary lobe receives releasing hormones from the hypothalamus via a portal
vein system known as the hypothalamic-hypophyseal portal system.
The anterior pituitary secretes:

thyroid-stimulating hormone (TSH)

adrenocorticotropic hormone (ACH)
prolactin
follicle-stimulating hormone (FSH)
luteinizing hormone (LH)
growth hormone (GH)
endorphins
and other hormones

It does this in response to a variety of chemical signals from the hypothalamus, which travels
to the anterior lobe by way of a special capillary system from the hypothalamus, down the
median eminence, to the anterior lobe. These include:

thyrotropin-releasing hormone (TRH)

corticotropin-releasing hormone (CRH)
dopamine (DA), also called 'prolactin inhibiting factor' (PIF)
gonadotropin-releasing hormone (GnRH)

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Antagonistic Hormones
growth hormone releasing hormone (GHRH)
These hormones from the hypothalamus cause release of the respective hormone from the
pituitary. The control of release of hormones from the pituitary is via negative feedback
from the target gland. For example homeostasis of thyroid hormones is achieved by the
following mechanism; TRH from the hypothalamus stimulates the release of TSH from the
anterior pituitary. The TSH, in turn, stimulates the release of thyroid hormones form the
thyroid gland. The thyroid hormones then cause negative feedback, suppressing the release
of TRH and TSH.
The heart, gastrointestinal tract, the placenta, the kidneys and the skin, whose major
function is not the secretion of hormones, also contain some specialized cells that produce
hormones.
In addition, all cells, except red blood cells secrete a class of hormones called eicosanoids.
These hormones are paracrines, or local hormones, that primarily affect neighboring cells.
Two groups of eicosanoids, the prostaglandins (PGs) and the leukotrienes (LTs), have a
wide range of varying effects that depend upon the nature of the target cell. Eicosanoid
activity, for example, may impact blood pressure, blood clotting, immune and inflammatory
responses, reproductive processes, and the contraction of smooth muscles.

12.5 Antagonistic Hormones

Maintaining homeostasis often requires conditions to be limited to a narrow range. When
conditions exceed the upper limit of homeostasis, specific action, usually the production of a
hormone is triggered. When conditions return to normal, hormone production is discontinued.
If conditions exceed the lower limits of homeostasis, a different action, usually the production
of a second hormone is triggered. Hormones that act to return body conditions to within
acceptable limits from opposite extremes are called antagonistic hormones. The two
glands that are the most responsible for homeostasis is the thyroid and the parathyroid.
The regulation of blood glucose concentration (through negative feedback) illustrates how
the endocrine system maintains homeostasis by the action of antagonistic hormones. Bundles
of cells in the pancreas called the islets of Langerhans contain two kinds of cells, alpha
cells and beta cells. These cells control blood glucose concentration by producing the
antagonistic hormones insulin and glucagon.
Beta cells secrete insulin. When the concentration of blood glucose raises such in after
eating, beta cells secret insulin into the blood. Insulin stimulates the liver and most other
body cells to absorb glucose. Liver and muscle cells convert glucose to glycogen, for short
term storage, and adipose cells convert glucose to fat. In response, glucose concentration
decreases in the blood, and insulin secretion discontinues through negative feedback from
declining levels of glucose.
Alpha cells secrete glucagon. When the concentration of blood glucose drops such as during
exercise, alpha cells secrete glucagon into the blood. Glucagon stimulates the liver to release
glucose. The glucose in the liver originates from the breakdown of glycogen. Glucagon also
stimulates the production of ketone bodies from amino acids and fatty acids. Ketone bodies

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The Endocrine System

are an alternative energy source to glucose for some tissues. When blood glucose levels
return to normal, glucagon secretion discontinues through negative feedback.
Another example of antagonistic hormones occurs in the maintenance of Ca2+ ion concentration in the blood. Parathyroid hormone (PTH) from the parathyroid glands increases Ca2+
in the blood by increasing Ca2+ absorption in the intestines and reabsorption in the kidneys
and stimulating Ca2+ release from bones. Calcitonin (CT) produces the opposite effect by
inhibiting the breakdown of bone matrix and decreasing the release of calcium in the blood.

12.5.1 Thyroid gland

The Thyroid gland is one of the largest endocrine glands in the body. It is positioned on
the neck just below the Larynx and has two lobes with one on either side of the trachea. It is
involved in the production of the hormones T3 (triiodothyronine) and T4 (thyroxine). These
hormones increase the metabolic activity of the bodys cells. The thyroid also produces
and releases the hormone calcitonin (thyrocalcitonin) which contributes to the regulation of
blood calcium levels. Thyrocalcitonin or calcitonin decreases the concentration of calcium in
the blood. Most of the calcium removed from the blood is stored in the bones.
The thyroid hormone consists of two components, thyroxine and iodine. This hormone
increases the metabolism of most body cells. A deficiency of iodine in the diet leads to
the enlargement of the thyroid gland, known as a simple goiter. Hypothyroidism during
early development leads to cretinism. In adults, it produces myxedema, characterized by
obesity and lethargy. Hyperthyroidism leads to a condition known as exophthalmic goiter,
characterized by weight loss as well as hyperactive and irritable behavior.
The thyroid gland is a two-lobed gland that manifests a remarkably powerful active transport
mechanism for up-taking iodide ions from the blood. As blood flows through the gland, iodide
is converted to an active form of iodine. This iodine combines with an amino acid called
tyrosine. Two molecules of iodinated tyrosine then combine to form thryroxine. Following
its formation, the thyroxine becomes bound to a polysaccharide-protein material called
thyroglobulin. The normal thyroid gland may store several weeks supply of thyroxine in this
bound form. An enzymatic splitting of the thyroxine from the thyroglobulin occurs when a
specific hormone is released into the blood. This hormone, produced by the pituitary gland,
is known as thyroid-stimulating hormone (TSH). TSH stimulates certain major rate-limiting
steps in thyroxine secretion, and thereby alters its rate of release. A variety of bodily defects,
either dietary, hereditary, or disease induced, may decrease the amount of thyroxine released
into the blood. The most popular of these defects is one that results from dietary iodine
deficiency. The thyroid gland enlarges, in the continued presence of TSH from the pituitary,
to form a goiter. This is a futile attempt to synthesize thyroid hormones, for iodine levels
that are too low. Normally, thyroid hormones act via a negative feedback loop on the
pituitary to decrease stimulation of the thyroid. In goiter, the feedback loop cannot be in
operation - hence continual stimulation of the thyroid and the inevitable protuberance on
the neck. Formerly, the principal source of iodine came from seafood. As a result, goiter
was prevalent amongst inland areas far removed from the sea. Today, the incidence of goiter
has been drastically reduced by adding iodine to table salt.
Thyroxine serves to stimulate oxidative metabolism in cells; it increases the oxygen consumption and heat production of most body tissues, a notable exception being the brain.

334

Antagonistic Hormones
Thyroxine is also necessary for normal growth. The most likely explanation being that
thyroxine promotes the effects of growth hormone on protein synthesis. The absence of
thyroxine significantly reduces the ability of growth hormone to stimulate amino acid uptake
and RNA synthesis. Thyroxine also plays a crucial role in the closely related area of organ
development, particularly that of the central nervous system.
If there is an insufficient amount of thyroxine, a condition referred to as hypothyroidism
results. Symptoms of hypothyroidism stem from the fact that there is a reduction in the
rate of oxidative energy-releasing reactions within the body cells. Usually the patient
shows puffy skin, sluggishness, and lowered vitality. Other symptoms of hypothyroidism
include weight gain, decreased libido, inability to tolerate cold, muscle pain and spasm, and
brittle nails. Hypothyroidism in children, a condition known as cretinism, can result in
mental retardation, dwarfism, and permanent sexual immaturity. Sometimes the thyroid
gland produces too much thyroxine, a condition known as hyperthyroidism. This condition
produces symptoms such as an abnormally high body temperature, profuse sweating, high
blood pressure, loss of weight, irritability, insomnia and muscular pain and weakness. It
also causes the characteristic symptom of the eyeballs protruding from the skull called
exopthalmia. This is surprising because it is not a symptom usually related to a fast
metabolism. Hyperthyroidism has been treated by partial removal or by partial radiation
destruction of the gland. More recently, several drugs that inhibit thyroid activity have been
discovered, and their use is replacing the former surgical procedures. Unfortunately thyroid
conditions require lifetime treatment and because of the body's need for a sensitive balance
of thyroid hormone both supplementing and suppressing thyroid function can take months
or even years to regulate.
T3 and T4 Function within the body
The Production of T3 and T4 are regulated by thyroid stimulating hormone (TSH), released
by the pituitary gland. TSH Production is increased when T3 and T4 levels are too low.
The thyroid hormones are released throughout the body to direct the body's metabolism.
They stimulate all cells within the body to work at a better metabolic rate. Without
these hormones the body's cells would not be able to regulate the speed at which they
performed chemical actions. Their release will be increased under certain situations such as
cold temperatures when a higher metabolism is needed to generate heat. When children
are born with thyroid hormone deficiency they have problems with physical growth and
developmental problems. Brain development can also be severely impaired
The significance of iodine
Thyroid hormone cannot be produced without an abundant source of iodine. The iodine
concentration within the body, although significant, can be as little as 1/25th the concentration within the thyroid itself. When the thyroid is low on iodine the body will try harder to
produce T3 and T4 which will often result in a swelling of the thyroid gland, resulting in a
goiter.

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The Endocrine System

12.6 Extrathyroidal iodine

Iodine accounts for 65% of the molecular weight of T4 and 59% of the T3. 1520 mg of
iodine is concentrated in thyroid tissue and hormones, but 70% of the body's iodine is
distributed in other tissues, including mammary glands, eyes, gastric mucosa, the cervix,
and salivary glands. In the cells of these tissues iodide enters directly by sodium-iodide
symporter1 (NIS). Its role in mammary tissue is related to fetal and neonatal development,
but its role in the other tissues is unknown. It has been shown to act as an antioxidant in
these tissues.
The US Food and Nutrition Board and Institute of Medicine recommended daily allowance
of iodine ranges from 150 micrograms /day for adult humans to 290 micrograms /day for
lactating mothers. However, the thyroid gland needs no more than 70 micrograms /day
to synthesize the requisite daily amounts of T4 and T3. These higher recommended daily
allowance levels of iodine seem necessary for optimal function of a number of body systems,
including lactating breast, gastric mucosa, salivary glands, oral mucosa, thymus, epidermis,
choroid plexus, etc.234 Moreover, iodine can add to double bonds of docosahexaenoic
acid and arachidonic acid of cellular membranes, making them less reactive to free oxygen
radicals.5
Calcitonin
Calcitonin is a 32 amino acid polypeptide hormone. It is an additional hormone produced by
the thyroid, and contributes to the regulation of blood calcium levels. Thyroid cells produce
calcitonin in response to high calcium levels in the blood. This hormone will stimulate
movement of calcium into the bone structure. It can also be used therapeutically for the
treatment of hypercalcemia or osteoporosis. Without this hormone calcium will stay within
the blood instead of moving into bones to keep them strong and growing. Its importance in
humans has not been as well established as its importance in other animals.

12.6.1 Parathyroid gland

There are four parathyroid glands. They are small, light-colored lumps that stick out from
the surface of the thyroid gland. All four glands are located on the thyroid gland. They are
butterfly-shaped and located inside the neck, more specifically on both sides of the windpipe.
1
2
3

336

http://en.wikibooks.org/wiki/sodium-iodide%20symporter
Brown-Grant, K.. Extrathyroidal iodide concentrating mechanismsExtrathyroidal iodide concentrating
mechanisms {physrev.physiology.org/cgi/reprint/41/1/189.pdf} . Physiol Rev., 411961
Spitzweg, C., Joba, W., Eisenmenger, W. and Heufelder, A.E. . Analysis of human sodium iodide
symporter gene expression in extrathyroidal tissues and cloning of its complementary deoxyribonucleic
acid from salivary gland, mammary gland, and gastric mucosaAnalysis of human sodium iodide symporter
gene expression in extrathyroidal tissues and cloning of its complementary deoxyribonucleic acid from
salivary gland, mammary gland, and gastric mucosa. J Clin Endocrinol Metab., 831998
Banerjee, R.K., Bose, A.K., Chakraborty, t.K., de, S.K. and datta, A.G. . Peroxidase catalysed
iodotyrosine formation in dispersed cells of mouse extrathyroidal tissues Peroxidase catalysed iodotyrosine
formation in dispersed cells of mouse extrathyroidal tissues. J Endocrinol., 21985
Cocchi, M. and Venturi, S. Iodide, antioxidant function and Omega-6 and Omega-3 fatty acids: a new
hypothesis of a biochemical cooperation? Progress in Nutrition, 2000, 2, 15-19

Extrathyroidal iodine
One of the parathyroid glands most important functions is to regulate the body's calcium
and phosphorus levels. Another function of the parathyroid glands is to secrete parathyroid
hormone, which causes the release of the calcium present in bone to extracellular fluid. PTH
does this by depressing the production of osteoblasts, special cells of the body involved in
the production of bone and activating osteoclasts, other specialized cells involved in the
removal of bone.
There are two major types of cells that make up parathyroid tissue:
One of the major cells is called oxyphil cells. Their function is basically unknown.
The second type are called chief cells. Chief cells produce parathyroid hormone.
The structure of a parathyroid gland is very different from that of a thyroid gland. The
chief cells that produce parathyroid hormone are arranged in tightly-packed nests around
small blood vessels, quite unlike the thyroid cells that produce thyroid hormones, which are
arranged in spheres called the thyroid follicles.
PTH or Parathyroid Hormone is secreted from these four glands. It is released directly
into the bloodstream and travels to its target cells which are often quite far away. It then
binds to a structure called a receptor, that is found either inside or on the surface of the
target cells.
Receptors bind a specific hormone and the result is a specific physiologic response, meaning
a normal response of the body.
PTH finds its major target cells in bone, kidneys, and the gastrointestinal system.
Calcitonin, a hormone produced by the thyroid gland that also regulates ECF calcium levels
and serves to counteract the calcium-producing effects of PTH.
The adult body contains as much as 1 kg of calcium. Most of this calcium is found in bone
and teeth.
The four parathyroid glands secrete the parathyroid hormone (PTH). It opposes the effect
of thyrocalcitonin. It does this by removing calcium from its storage sites in bones, releasing
it into the bloodstream. It also signals the kidneys to reabsorb more of this mineral,
transporting it into the blood. It also signals the small intestine to absorb more of this
mineral, transporting it from the diet into the blood.
Calcium is important for steps of body metabolism. Blood cannot clot without sufficient
calcium. Skeletal muscles require this mineral in order to contract. A deficiency of PTH can
lead to tetany, muscle weakness due to lack of available calcium in the blood.
The parathyroid glands were long thought to be part of the thyroid or to be functionally
associated with it. We now know that their close proximity to the thyroid is misleading:
both developmentally and functionally, they are totally distinct from the thyroid.
The parathyroid hormone, called parathormone, regulates the calcium-phosphate balance
between the blood and other tissues. Production of this hormone is directly controlled by the
calcium concentration of the extracellular fluid bathing the cells of these glands. Parathormne
exerts at least the following five effects: (1) it increases gastrointestinal absorption of calcium
by stimulating the active transport system and moves calcium from the gut lumen into the
blood; (2) it increases the movement of calcium and phosphate from bone into extracellular
fluid. This is accomplished by stimulating osteoclasts to break down bone structure, thus

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liberating calcium phosphate into the blood. In this way, the store of calcium contained
in bone is tapped; (3) it increases re-absorption of calcium by the renal tubules, thereby
decreasing urinary calcium excretion; (4) it reduces the re-absorption of phosphate by the
renal tubules (5)it stimulates the synthesisof 1,25-dihydrixycholecalciferol by the kidney.
The first three effects result in a higher extracellular calcium concentration. The adaptive
value of the fourth is to prevent the formation of kidney stones.
If parathyroid glands are removed accidentally during surgery on the thyroid, there would
be a rise in the phosphate concentration in the blood. There would also be a drop in the
calcium concentration as more calcium is excreted by the kidneys and intestines, and more
incorporated into the bone. This can produce serious disturbances, particularly in the
muscles and nerves, which use calcium ions for normal functioning. Over activity of the
parathyroid glands, which can result from a tumor on the glands, produces a weakening of
the bones. This is a condition that makes them much more vulnerable to fracturing because
of excessive withdrawal of calcium from the bones.

12.6.2 Adrenal glands

Adrenal glands are a pair of ductless glands located above the kidneys. Through hormonal
secretions, the adrenal glands regulate many essential functions in the body, including
biochemical balances that influence athletic training and general stress response. The
glucocorticoids include corticosterone, cortisone, and hydrocortisone or cortisol. These
hormones serve to stimulate the conversion of amino acids into carbohydrates which is a
process known as gluconeogenesis, and the formation of glycogen by the liver. They also
stimulate the formation of reserve glycogen in the tissues, such as in the muscles. The
glucocorticoids also participate in lipid and protein metabolism. The cortex of the adrenal
gland is known to produce over 20 hormones, but their study can be simplified by classifying
them into three categories: glucocorticoids, mineralcorticoids, and sex hormones.
They are triangular-shaped glands located on top of the kidneys. They produce hormones
such as estrogen, progesterone, steroids, cortisol, and cortisone, and chemicals such as
adrenalin (epinephrine), norepinephrine, and dopamine. When the glands produce more or
less hormones than required by the body, disease conditions may occur.
The adrenal cortex secretes at least two families of hormones, the glucocorticoids and mineral corticoids. The adrenal medulla secretes the hormones epinephrine (adrenalin)
and norepinephrine (noradrenalin).
Adrenal Cortex: The hormones made by the Adrenal Cortex supply long-term responses
to stress. The two major hormones produced are theMineral Corticoids and the Glucocorticoids. The Mineral Corticoids regulate the salt and water balance, leading to the
increase of blood volume and blood pressure. The Glucocorticoids are monitoring the
ACTH, in turn regulating carbohydrates, proteins, and fat metabolism. This causes an
increase in blood glucose. Glucocorticoids also reduce the body's inflammatory response.
Cortisol is one of the most active glucocorticoids. It usually reduces the effects of inflammation or swelling throughout the body. It also stimulates the production of glucose from
fats and proteins, which is a process referred to as gluconeogenesis.

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Extrathyroidal iodine
Aldosterone is one example of a mineralcorticoid. It signals the tubules in the kidney
nephrons to reabsorb sodium while secreting or eliminating potassium. If sodium levels are
low in the blood, the kidney secretes more renin, which is an enzyme that stimulates the
formation of angiotensin from a molecule made from the liver. Angiotensin stimulates
aldosterone secretion. As a result, more sodium is reabsorbed as it enters the blood.
Aldosterone, the major mineralcorticoid, stimulates the cells of the distal convoluted tubules
of the kidneys to decrease re-absorption of potassium and increase re-absorption of sodium.
This in turn leads to an increased re-absorption of chloride and water. These hormones,
together with such hormones as insulin and glucagon, are important regulators of the ionic
environment of the internal fluid.
The renin-angiotensin-aldosterone mechanism can raise blood pressure if it tends to drop. It
does this in two ways. Angiotensin is a vasoconstrictor, decreasing the diameter of blood
vessels. As vessels constrict, blood pressure increases. In addition, as sodium is reabsorbed,
the blood passing through the kidney becomes more hypertonic. Water follows the sodium
into the hypertonic blood by osmosis. This increases the amount of volume in the blood
and also increases the blood pressure.
Adrenal Medulla The hypothalamus starts nerve impulses that travel the path from the
bloodstream, spinal cord, and sympathetic nerve fibers to the Adrenal Medulla, which then
releases hormones. The effects of these hormones provide a short-term response to stress
Excessive secretion of the glucocorticoids causes Cushing's syndrome, characterized by
muscle atrophy or degeneration and hypertension or high blood pressure. Under secretion
of these substances produces Addison's disease, characterized by low blood pressure and
stress.
Epinephrine and norepinephrine produce the "fight or flight" response, similar to the effect
from the sympathetic nervous system. Therefore, they increase heart rate, breathing rate,
blood flow to most skeletal muscles, and the concentration of glucose in the blood. They
decrease blood flow to the digestive organs and diminish most digestive processes.

Figure 107

Suprarenal glands viewed from the front.

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The Endocrine System

Figure 108

Suprarenal glands viewed from behind.

The adrenal sex hormones consist mainly of male sex hormones (androgens) and lesser
amounts of female sex hormones (estrogens and progesterone). Normally, the sex hormones
released from the adrenal cortex are insignificant due to the low concentration of secretion.
However, in cases of excess secretion, masculine or feminine effects appear. The most
common syndrome of this sort is "virilism" of the female.
Should there be an insufficient supply of cortical hormones, a condition known as Addison's
disease would result. This disease is characterized by an excessive excretion of sodium ions,
and hence water, due to lack of mineralcorticoids. Accompanying this is a decreased blood
glucose level due to a deficient supply of glucocorticoids. The effect of a decreased androgen
supply cannot be observed immediately. Injections of adrenal cortical hormones promptly
relieve these symptoms.
Hormonal production in the adrenal cortex is directly controlled by the anterior pituitary
hormone called adrenocorticotropic hormone (ACTH).
The two adrenal glands lie very close to the kidneys. Each adrenal gland is actually a
double gland, composed of an inner core like medulla and an outer cortex. Each of these is
functionally unrelated.
The adrenal medulla secretes two hormone, adrenalin or epinephrine and noradrenalin or
norepinephrine, whose functions are very similar but not identical. The adrenal medulla is
derived embriogically from neural tissue. It has been likened to an overgrown sympathetic
ganglion whose cell bodies do not send out nerve fibers, but release their active substances
directly into the blood, thereby fulfilling the criteria for an endocrine gland. In controlling
epinephrine secretion, the adrenal medulla behaves just like any sympathetic ganglion, and
is dependent upon stimulation by sympathetic preganglionic fibers.
Epinephrine promotes several responses, all of which are helpful in coping with emergencies:
the blood pressure rises, the heart rate increases, the glucose content of the blood rises
because of glycogen breakdown, the spleen contracts and squeezes out a reserve supply
of blood, the clotting time decreases, the pupils dilate, the blood flow to skeletal muscles
increase, the blood supply to intestinal smooth muscle decreases and hairs become erect.
These adrenal functions, which mobilize the resources of the body in emergencies, have
been called the fight-or-flight response. Norepinephrine stimulates reactions similar to those
produced by epinephrine, but is less effective in conversion of glycogen to glucose.

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The significance of the adrenal medulla may seem questionable since the complete removal of
the gland causes few noticeable changes; humans can still exhibit the flight-or-fight response.
This occurs because the sympathetic nervous system complements the adrenal medulla in
stimulating the fight-or-flight response, and the absence of the hormonal control will be
compensated for by the nervous system.

12.6.3 Pancreas
The pancreas is very important organ in the digestion system and the circulatory system
because it helps to maintain our blood sugar levels. The pancreas is considered to be part
of the gastrointestinal system. It produces digestive enzymes to be released into the small
intestine to aid in reducing food particles to basic elements that can be absorbed by the
intestine and used by the body. It has another very different function in that it forms insulin,
glucagon and other hormones to be sent into the bloodstream to regulate blood sugar levels
and other activities throughout the body.
It has a pear-shape to it and is approximately 6 inches long. It is located in the middle
and back portion of the abdomen. The pancreas is connected to the first part of the small
intestine, the duodenum, and lies behind the stomach. The pancreas is made up of glandular
tissue: any substance secreted by the cells of the pancreas will be secreted outside of the
organ.
The digestive juices produced by the pancreas are secreted into the duodenum via a Y-shaped
duct, at the point where the common bile duct from the liver and the pancreatic duct join
just before entering the duodenum. The digestive enzymes carried into the duodenum are
representative of the exocrine function of the pancreas, in which specific substances are
made to be passed directly into another organ.
Note:
The pancreas is both an exocrine and an endocrine organ.
The pancreas is unusual among the body's glands in that it also has a very important
endocrine function. Small groups of special cells called islet cells throughout the organ
make the hormones of insulin and glucagon. These, of course, are hormones that are critical
in regulating blood sugar levels. These hormones are secreted directly into the bloodstream
to affect organs all over the body.
No organ except the pancreas makes significant amounts of insulin or glucagon.
Insulin acts to lower blood sugar levels by allowing the sugar to flow into cells. Glucagon
acts to raise blood sugar levels by causing glucose to be released into the circulation from
its storage sites. Insulin and glucagon act in an opposite but balanced fashion to keep blood
sugar levels stable.
A healthy working pancreas in the human body is important for maintaining good health by
preventing malnutrition, and maintaining normal levels of blood sugar. The digestive tract
needs the help of the enzymes produced by the pancreas to reduce food particles to their
simplest elements, or the nutrients cannot be absorbed. Carbohydrates must be broken

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down into individual sugar molecules. Proteins must be reduced to simple amino acids. Fats
must be broken down into fatty acids. The pancreatic enzymes are important in all these
transformations. The basic particles can then easily be transported into the cells that line
the intestine, and from there they can be further altered and transported to different tissues
in the body as fuel sources and construction materials. Similarly, the body cannot maintain
normal blood sugar levels without the balanced action of insulin and glucagon.
The pancreas contains exocrine and endocrine cells. Groups of endocrine cells, the islets of
Langerhans, secrete two hormones. The beta cells secrete insulin; the alpha cells secrete
glucagon. The level of sugar in the blood depends on the opposing action of these two
hormones.
Insulin decreases the concentration of glucose in the blood. Most of the glucose enters the
cells of the liver and skeletal muscles. In these cells, this monosaccharide is converted
to the polysaccharide glycogen. Therefore, insulin promotes glycogenesis or glycogen
synthesis, in which glucose molecules are added to chains of glycogen. Excess glucose is also
stored as fat in adipose tissue cells in response to insulin.
Insulin deficiency leads to the development of diabetes mellitus, specifically type I,
juvenile diabetes. As the pancreas does not produce sufficient insulin, it is treated by insulin
injections. In type II or maturity onset diabetes, the pancreas does produce enough insulin,
but the target cells do not respond to it.
As already stated, the pancreas is a mixed gland having both endocrine and exocrine
functions. The exocrine portion secretes digestive enzymes into the duodenum via the
pancreatic duct. The endocrine portion secretes two hormones, insulin and glucagon, into
the blood.
Insulin is a hormone that acts directly or indirectly on most tissues of the body, with the
exception of the brain. The most important action of insulin is the stimulation of the uptake
of glucose by many tissues, particularly the liver, muscle and fat. The uptake of glucose
by the cells decreases blood glucose and increases the availability of glucose for the cellular
reactions in which glucose participates. Thus, glucose oxidation, fat synthesis, and glycogen
synthesis are all accentuated by an uptake of glucose. It is important to note that insulin
does not alter glucose uptake by the brain, nor does it influence the active transport of
glucose across the renal tubules and gastrointestinal epithelium.
As stated, insulin stimulates glycogen synthesis. In addition, it also increases the activity of
the enzyme that catalyzes the rate-limiting step in glycogen synthesis. Insulin also increases
triglyceride levels by inhibiting triglyceride breakdown, and by stimulating production of
triglyceride through fatty acid and glycerophosphate synthesis. The net protein synthesis is
also increased by insulin, which stimulates the active membrane transport of amino acids,
particularly into muscle cells. Insulin also has effects on other liver enzymes, but the precise
mechanisms by which insulin induces these changes are not well understood.
Insulin is secreted by beta cells, which are located in the part of the pancreas known as
the islets of Langerhans. These groups of cells, which are located randomly throughout the
pancreas, also consist of other secretory cells called alpha cells. It is these alpha cells that
secrete glucagon. Glucagon is a hormone that has the following major effects: it increases
hepatic synthesis of glucose from pyruvate, lactate, glycerol, and amino acids (a process
called gluconeogenesis, which also raises the plasma glucose level); and it increases the

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Extrathyroidal iodine
breakdown of adipose tissue triglyceride, thereby raising the plasma levels of fatty acids and
glycerol. The glucagon secreting alpha cells in the pancreas, like the beta cells, respond to
changes in the concentration of glucose in the blood flowing through the pancreas; no other
nerves or hormones are involved.
It should be noted that glucagon has the opposite effects of insulin. Glucagon elevates the
plasma glucose, whereas insulin stimulates its uptake and thereby reduces plasma glucose
levels; glucagon elevates fatty acid concentrations, whereas insulin converts fatty acids and
glycerol into triglycerides, thereby inhibiting triglyceride breakdown.
The alpha and beta cells of the pancreas make up a push-pull system for regulating the
plasma glucose level.

12.6.4 Sex organs

The Sex organs (Gonads) are the testes in the male, and the ovaries in the female. Both
of these organs produce and secrete hormones that are balanced by the hypothalamus and
pituitary glands.
The main hormones from the reproductive organs are:
Testosterone is more prominent in males. It belongs to the family of androgens, which are
steroid hormones producing masculine effects. Testosterone stimulates the development and
functioning of the primary sex organs. It also stimulates the development and maintenance
of secondary male characteristics, such as hair growth on the face and the deep pitch of the
voice.
Estrogen In females, this hormone stimulates the development of the uterus and vagina. It
is also responsible for the development and maintenance of secondary female characteristics,
such as fat distribution throughout the body and the width of the pelvis.

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Male

Figure 109

framed

The testes produce androgens (i.e., "testosterone"). Testosterone is classified as a steroid

and is responsible for many of the physical characteristics in males like.
Broad shoulders
Muscular body
Hair
Testosterone increases protein production. Hormones that build up protein are called
anabolic steroids. Anabolic steroids are available commercially and are being used by

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athletes because they help improve their physical ability, however, they do have major side
effects such as:

Liver and kidney disorders

Hypertension (high blood pressure)
Decreased sperm count and impotency
Aggressive behavior ("roid mania)
Balding
Acne

Female

Figure 110
anatomy.

Schematic frontal view of female

The ovaries produce estrogen and progesterone. Estrogen increases at the time of
puberty and causes the growth of the uterus and vagina. Without estrogen egg maturation
would not occur. Estrogen is also responsible for secondary sex characteristics such as
female body hair and fat distribution. Estrogen and Progesterone are responsible for the
development of the breast and for the uterine cycle. Progesterone is a female hormone
secreted by the corpus luteum after ovulation during the second half of the menstrual cycle.
It prepares the lining of the uterus for implantation of a fertilized egg and allows for complete
shedding of the endometrium at the time of menstruation. In the event of pregnancy, the
progesterone level remains stable beginning a week or so after conception.

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12.6.5 Pineal gland

The pineal gland (also called the pineal body or epiphysis) is a small endocrine gland in
the brain. It is located near the center of the brain, between the two hemispheres, tucked
in a groove where the two rounded thalamic bodies join.it consists of two types of cells
1.parenchymal cells 2.neuroglial cells.
The pineal gland is a reddish-gray body about the size of a pea (8 mm in humans) located
just rostro-dorsal to the superior colliculus and behind and beneath the stria medullaris,
between the laterally positioned thalamic bodies. It is part of the epithalamus.
The pineal gland is a midline structure, and is often seen in plain skull X-rays, as it is
often calcified. The main hormone produced and secreted by the pineal gland is melatonin.
Secretion is highest at night and between the ages of 0-5.melatonin acts mainly on gonads.

12.7 Glossary
Adrenal Gland: endocrine gland that is located on top of each kidney
Amino Acid-derived: hormones that are modified amino acids
Antagonistic Hormones: hormones that act to return body conditions to within acceptable limits from opposite extremes
Calcitonin: hormone produced by the thyroid; contributes to the regulation of blood
calcium levels
Eicosanoids: lipids that are synthesized from the fatty acid chains of phospholipids found
in plasma membrane
Endocrine Glands: glands that have no duct and release their secretions directly into the
intercellular fluid or into the blood
Endocrine System: a control system of ductless glands that secrete chemical messengers
called hormones
Estrogen: hormone in females; stimulates the development of the uterus and vagina
Exocrine Glands: glands that release their cellular secretions through a duct which
empties to the outside or into the lumen (empty internal space) of an organ
Hormone: a specific chemical substance produced by certain cells that control, or help to
control, cellular processes elsewhere in an organism
Insulin: hormone that acts to lower blood sugar levels by allowing the sugar to flow into
cells
Iodine: chemical in the body; Thyroid hormone can not be produced with out it
Lipid-soluble Hormones: diffuse through the cell membranes of target cells
Parathyroid: four masses of tissue, two embedded posterior in each lateral mass of the
thyroid gland

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Chapter Review Questions

Pancreas: organ involved with the digestion system and the circulatory system; helps to
maintain blood sugar levels
Pineal Gland: small endocrine gland in the brain located near the center of the brain,
between the two hemispheres, tucked in a groove where the two rounded thalamic bodies
join
Pituitary Gland: endocrine gland that is attached to the hypothalamus of the lower
forebrain
Polypeptide and Proteins: hormones that are chains of amino acids of less than or more
than about 100 amino acids
Steroids: hormones that are lipids that are synthesized from cholesterol; characterized by
four interlocking carbohydrate rings
Testosterone: hormone more prominent in males; belongs to the family of androgens,
which are steroid hormones producing masculinizing effects
Thyroid Gland: endocrine gland that consists of two lateral masses that are attached to
the trachea
Thyroxine: serves to stimulate oxidative metabolism in cells; increases the oxygen consumption and heat production of most body tissues
Water-soluble Hormones: bind to a receptor protein on the plasma membrane of the cell

12.8 Chapter Review Questions

Answers for these questions can be found here6
1. My child just fell and was hurt, the anxious feeling that I feel is caused by:
A) glucagon
B) insulin
C) epinephrine
D) adrenocorticotropic
E) None of these
2. All of Bobs life he has had to take insulin shots, this is caused because
A) his beta cells dont function correctly
B) his alpha cells dont function correctly
C) his DA hormone isnt functioning correctly
D) his GHRH hormone isnt functioning correctly

http://en.wikibooks.org/wiki/Human_Physiology/Appendix_1:_answers_to_review_
questions#The_Endocrine_System

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3. The reason iodine is in salt is
A) to prevent diabetes
B) to prevent simple goiters
C) to prevent Addisons disease
D) to prevent Cushing's syndrome
4. All hormones react to a negative feedback except
A) progesterone
B) estrogen
C) prolactin
D) oxytocin
E) none of these
5. If I have a high blood calcium level it may be due to
A) calcitonin
B) parathyroid
C) glucocorticoids
D) glucagon
6. Hormones that are lipids that are synthesized from cholesterol
A) protein
B) amino acid-derived
C) polypeptide
D) steroids
E) eicosanoids
7. This type of hormone must bind to a receptor protein on the plasma membrane of the cell
A) water soluble
B) lipid soluble
C) steroid
D) polypeptide
E) a and d
F) b and c
8. Endocrine glands release hormones in response to
A) Hormones from other endocrine glands
B) Chemical characteristics of the blood

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References
C) Neural stimulation
D) All of the above
9. The anterior pituitary secretes
A) oxytocin
B) endorphins
C) ADH
D) TRH
10. Chief cells produce
A) epinephrine
B) glucagon
C) insulin
D) mineralocorticoids
E) parathyroid hormone
11. Name the eight major endocrine glands.
12. Name the four major groups hormones can be chemically classified into.

12.9 References

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13 The Male Reproductive System

13.1 Introduction
In simple terms, reproduction is the process by which organisms create descendants. This
miracle is a characteristic that all living things have in common and sets them apart from
nonliving things. But even though the reproductive system is essential to keeping a species
alive, it is not essential to keeping an individual alive.
In human reproduction, two kinds of sex cells or gametes are involved. Sperm, the male
gamete, and a secondary oocyte (along with first polar body and corona radiata), the
female gamete must meet in the female reproductive system to create a new individual.
For reproduction to occur, both the female and male reproductive systems are essential. It
is a common misnomer to refer to a woman's gametic cell as an egg or ovum, but this is
impossible. A secondary oocyte must be fertilized by the male gamete before it becomes an
"ovum" or "egg".
While both the female and male reproductive systems are involved with producing, nourishing
and transporting either the oocyte or sperm, they are different in shape and structure. The
male has reproductive organs, or genitals, that are both inside and outside the pelvis, while
the female has reproductive organs entirely within the pelvis.
The male reproductive system consists of the testes and a series of ducts and glands. Sperm
are produced in the testes and are transported through the reproductive ducts. These ducts
include the epididymis, ductus deferens, ejaculatory duct and urethra. The reproductive
glands produce secretions that become part of semen, the fluid that is ejaculated from the
urethra. These glands include the seminal vesicles, prostate gland, and bulbourethral glands.

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The Male Reproductive System

13.2 Structure

Figure 111

The human male reproductive system

13.2.1 Testes
The testes (singular, testis) are located in the scrotum (a sac of skin between the upper
thighs). In the male fetus, the testes develop near the kidneys, then descend into the scrotum
just before birth. Each testis is about 1 1/2 inches long by 1 inch wide. Testosterone is
produced in the testes which stimulates the production of sperm as well as give secondary
sex characteristics beginning at puberty.
Scrotum
The two testicles are each held in a fleshy sac called the scrotum. The major function of
the scrotal sac is to keep the testes cooler than thirty-seven degrees Celsius (ninety-eight
point six degrees Fahrenheit). The external appearance of the scrotum varies at different
times in the same individual depending upon temperature and the subsequent contraction
or relaxation of two muscles. These two muscles contract involuntarily when it is cold to
move the testes closer to the heat of the body in the pelvic region. This causes the scrotum
to appear tightly wrinkled. On the contrary, they relax in warm temperatures causing
the testes to lower and the scrotum to become flaccid. The temperature of the testes is
maintained at about thirty-five degrees Celsius (ninety-five degrees Fahrenheit), which is
below normal body temperature. Temperature has to be lower than normal in order for
spermatogenis (sperm production) to take place.

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Structure

Figure 112 The

human testicle
.
The two muscles that regulate the temperature of the testes are the dartos and cremaster
muscles:
Dartos Muscle
The dartos muscle is a layer of smooth muscle fibers in the subcutaneous tissue of the scrotum
(surrounding the scrotum). This muscle is responsible for wrinkling up the scrotum, in
conditions of cold weather, in order to maintain the correct temperature for spermatogenisis.
Cremaster Muscle
The cremaster muscle is a thin strand of skeletal muscle associated with the testes and
spermatic cord. This muscle is a continuation of the internal oblique muscle of the abdominal
wall, from which it is derived. Seminiferous Tubules
Each testis contains over 100 yards of tightly packed seminiferous tubules. Around 90%
of the weight of each testes consists of seminiferous tubules. The seminiferous tubules
are the functional units of the testis, where spermatogenisis takes place. Once the sperm
are produced, they moved from the seminiferous tubules into the rete testis for further
maturation.
Interstitial Cells (Cells of Leydig)
In between the seminiferous tubules within the testes, are instititial cells, or, Cells of Leydig.
They are responsible for secreting the male sex hormones (i.e., testosterone).
Sertoli Cells
A Sertoli cell (a kind of sustentacular cell) is a 'nurse' cell of the testes which is part of a
seminiferous tubule.
It is activated by follicle-stimulating hormone, and has FSH-receptor on its membranes.
Its main function is to nurture the developing sperm cells through the stages of spermatogenesis. Because of this, it has also been called the "mother cell." It provides both secretory
and structural support.
Other functions During the Maturation phase of spermiogenesis, the Sertoli cells consume
the unneeded portions of the spermatazoa.
Efferent ductules

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The Male Reproductive System

The sperm are transported out of the testis and into the epididymis through a series of
efferent ductules.
Blood Supply
The testes receive blood through the testicular arteries (gonadal artery). Venous blood is
drained by the testicular veins. The right testicular vein drains directly into the inferior
vena cava. The left testicular vein drains into the left renal vein.

13.2.2 Epididymis
The seminiferous tubules join together to become the epididymis. The epididymis is a tube
that is about 2 inches that is coiled on the posterior surface of each testis. Within the
epididymis the sperm complete their maturation and their flagella become functional. This
is also a site to store sperm, nourishing them until the next ejaculation. Smooth muscle in
the wall of the epididymis propels the sperm into the ductus deferens. Vasa efferentia from
the rete testis open into the epididymis which is a highly coiled tubule. The epididymis
has three parts- 1)head or caput epididymis- it is the proximal part of the epididymis. It
caries the sperms from the testis. 2)body or corpus epididymis- it the highly convoluted
middle part of the epididymis 3)tail or cauda epididymis- it is the last part that takes part
in carrying the sperms to the vas deferens. The cauda epididymis continues to form less
convoluted vas deferens.

13.2.3 Ductus Deferens

The ductus (vas) deferens, also called sperm duct, or, spermatic deferens, extends from the
epididymis in the scrotum on its own side into the abdominal cavity through the inguinal
canal. The inguinal canal is an opening in the abdominal wall for the spermatic cord (a
connective tissue sheath that contains the ductus deferens, testicular blood vessels, and
nerves. The smooth muscle layer of the ductus deferens contracts in waves of peristalsis
during ejaculation.

13.2.4 Seminal Vesicles

The pair of seminal vesicles are posterior to the urinary bladder. They secrete fructose to
provide an energy source for sperm and alkalinity to enhance sperm mobility. The duct of
each seminal vesicle joins the ductus deferens on that side to form the ejaculatory duct.

13.2.5 Ejaculatory Ducts

There are two ejaculatory ducts. Each receives sperm from the ductus deferens and the
secretions of the seminal vesicle on its own side. Both ejaculatory ducts empty into the
single urethra.

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Structure

13.2.6 Prostate Gland

The prostate gland is a muscular gland that surrounds the first inch of the urethra as
it emerges from the bladder. The smooth muscle of the prostate gland contracts during
ejaculation to contribute to the expulsion of semen from the urethra.

13.2.7 Bulbourethral Glands

The bulbourethral glands also called Cowper's glands are located below the prostate gland
and empty into the urethra. The alkalinity of seminal fluid helps neutralize the acidic vaginal
pH and permits sperm mobility in what might otherwise be an unfavorable environment.

13.2.8 Penis
The penis is an external genital organ. The distal end of the penis is called the glans penis
and is covered with a fold of skin called the prepuce or foreskin. Within the penis are masses
of erectile tissue. Each consists of a framework of smooth muscle and connective tissue that
contains blood sinuses, which are large, irregular vascular channels.

13.2.9 Urethra
The urethra, which is the last part of the urinary tract, traverses the corpus spongiosum
and its opening, known as the meatus, lies on the tip of the glans penis. It is both a passage
for urine and for the ejaculation of semen.

13.2.10 Overview of Male Reproductive System Structure and Function

STRUCTURE
Bulbourethral glands (2)

Cells of Leydig (Interstitial cells of Leydig)

LOCATION & DESCRIPTION

Pea sized organs posterior to the prostate on
either side of the urethra.

FUNCTION

Secretion of gelatinous
seminal fluid called preejaculate. This fluid helps
to lubricate the urethra
for spermatozoa to pass
through, and to help flush
out any residual urine or
foreign matter. (< 1% of
semen)
Adjacent to the seminifer- Responsible for proous tubules in the testicle. duction of testosterone.
Closely related to nerves.

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The Male Reproductive System

STRUCTURE
Cremaster muscle

LOCATION & DESCRIPTION

Covers the testes.

Dartos muscle

Layer of smooth muscular fiber outside the

external spermatic fascia
but below the skin

Efferent ductules

Part of the testes and

connect the rete testis
with the epididymis
Begins at the vas deferens, passes through the
prostate, and empties into
the urethra at the Colliculus seminalis.
Tightly coiled duct lying
just outside each testis
connecting efferent ducts
to vas deferens.
Three columns of erectile tissue: two corpora
cavernosa and one corpus spongiosum. Urethra
passes through penis.
Surrounds the urethra
just below the urinary
bladder and can be felt
during a rectal exam.

Ejaculatory ducts (2)

Epididymis

Penis

Prostate gland

Scrotum

356

Pouch of skin and muscle

that holds testicles.

FUNCTION
Raises and lowers scrotum to help regulate temperature and promote
spermatogenesis. Voluntary and involuntary
contraction.
Contraction by wrinkling
to decrease surface area
available for heat loss to
testicles, or expansion
to increase surface area
available to promote heat
loss; also helps raise and
lower scrotum to help
regulate temperature
Ducts for sperm to get to
epididymis
Causes reflex for ejaculation. During ejaculation,
semen passes through the
ducts and exits the body
via the penis.
Storage and maturation
of sperm.

Male reproductive organ

and also male organ of
urination.

Stores and secretes a

clear, slightly alkaline
fluid constituting up to
one-third of the volume
of semen. Raise vaginal
pH.(25-30% of semen)
Regulates temperature
at slightly below body
temperature.

Structure
STRUCTURE
Semen

Seminal vesicles (2)

Seminiferous tubules (2)

Sertoli cells

Testes

Testicular arteries (Gonadal arteries)

LOCATION & DESCRIPTION

Usually white but can
be yellow, gray or pink
(blood stained). After
ejaculation, semen first
goes through a clotting
process and then becomes
more liquid.
Convoluted structure
attached to vas deferens
near the base of the urinary bladder.

FUNCTION

Components are sperm,

and "seminal plasma".
Seminal plasma is produced by contributions
from the seminal vesicle, prostate, and bulbourethral glands.
About 65-75% of the
seminal fluid in humans
originates from the seminal vesicles. Contain proteins, enzymes, fructose,
mucus, vitamin C, flavins,
phosphorylcholine and
prostaglandins. High fructose concentrations provide nutrient energy for
the spermatozoa as they
travel through the female
reproductive system.
Long coiled structure con- Meiosis takes place here,
tained in the chambers of creation of gametes
the testis; joins with vas
(sperm).
deferens.
Junctions of the Sertoli
Cells responsible for
cells form the blood-testis nurturing and developbarrier, a structure that
ment of sperm cells , propartitions the interstitial
vides both secretory and
blood compartment of the structural support; actitestis from the adlumivated by FSH. Also called
nal compartment of the
"mother cells" or "nurse
seminiferous tubules.
cells".
Inside scrotum, outside
Gonads that produce
of body.
sperm and male sex hormones.Production of
testosterone by cells of
Leydig in the testicles.
Branch of the abdomiSupplies blood to the
nal aorta. It is a paired
testes.
artery. Each passes
obliquely downward and
laterally behind the peritoneum.

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The Male Reproductive System

STRUCTURE
Urethra

Vas deferens

LOCATION & DESCRIPTION

Connects bladder to outside body, about 8 inches
long.

FUNCTION

Tubular structure that receives urine from bladder

and carries it to outside
of the body. Also passage
for sperm.
Muscular tubes connectDuring ejaculation the
ing the left and right epi- smooth muscle in the vas
didymis to the ejaculadeferens wall contracts,
tory ducts to move sperm. propelling sperm forward.
Each tube is about 30 cm Sperm are transferred
long.
from the vas deferens into
the urethra, collecting
fluids from accessory sex
glands en route

13.2.11 Composition of human semen

The components of semen come from two sources: sperm, and "seminal plasma". Seminal
plasma, in turn, is produced by contributions from the seminal vesicle, prostate, and
bulbourethral glands.
Seminal plasma of humans contains a complex range of organic and inorganic constituents.
The seminal plasma provides a nutritive and protective medium for the spermatozoa during
their journey through the female reproductive tract. The normal environment of the vagina
is a hostile one for sperm cells, as it is very acidic (from the native microflora producing
lactic acid), viscous, and patrolled by immune cells. The components in the seminal plasma
attempt to compensate for this hostile environment. Basic amines such as putrescine,
spermine, spermidine and cadaverine are responsible for the smell and flavor of semen. These
alkaline bases counteract the acidic environment of the vaginal canal, and protect DNA
inside the sperm from acidic denaturation.
The components and contributions of semen are as follows:
GLAND
testes

358

APPROXIMATE
%
2-5%

DESCRIPTION
Approximately 200- to 500-million
spermatozoa (also called sperm or
spermatozoans), produced in the
testes, are released per ejaculation

Structure
GLAND
seminal vesicle

prostate

bulbourethral
glands

APPROXIMATE
%
65-75%

25-30%

< 1%

DESCRIPTION
amino acids, citrate, enzymes,
flavins, fructose (the main energy
source of sperm cells, which rely entirely on sugars from the seminal
plasma for energy), phosphorylcholine, prostaglandins (involved
in suppressing an immune response
by the female against the foreign
semen), proteins, vitamin C
acid phosphatase, citric acid, fibrinolysin, prostate specific antigen,
proteolytic enzymes, zinc (serves to
help to stabilize the DNA-containing
chromatin in the sperm cells. A zinc
deficiency may result in lowered fertility because of increased sperm
fragility. Zinc deficiency can also
adversely affect spermatogenesis.)
galactose, mucus (serve to increase
the mobility of sperm cells in the
vagina and cervix by creating a less
viscous channel for the sperm cells
to swim through, and preventing
their diffusion out of the semen.
Contributes to the cohesive jellylike texture of semen.), pre-ejaculate,
sialic acid

A 1992 World Health Organization report described normal human semen as having a
volume of 2 ml or greater, pH of 7.2 to 8.0, sperm concentration of 20x106 spermatozoa/ml
or more, sperm count of 40x106 spermatozoa per ejaculate or more and motility of 50% or
more with forward progression (categories a and b) of 25% or more with rapid progression
(category a) within 60 minutes of ejaculation.[2]

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The Male Reproductive System

13.3 Functions

Figure 113

13.3.1 Hormone Regulation

Hormones which control reproduction in males are:
Gonadotropin-Releasing Hormone (GnRH):
The hypothalamus secretes this hormone into the pituitary gland in the brain.
There are two gonadotropic hormones, FSH and LH.
Luteinizing Hormone (LH):
The pituitary gland secretes this hormone after receiving a GnRH signal from the
hypothalamus.
LH stimulates Leydig cells, in the testes, telling them to produce testosterone.
Follicle-Stimulating Hormone (FSH):
The pituitary gland also secretes this hormone.
Testosterone helps FSH run through the bloodstream to make Sertoli cells, located in the
seminiferous tubules of the testes, to make immature sperm to mature sperm.

360

Functions
Testosterone:
Also know as "the male hormone" and "androgen".
Testosterone is vital for the production of sperm.

Figure 114 The constituent

cavernous cylinders of the penis.

13.3.2 Erection

Figure 115

Transverse section of the penis.

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The Male Reproductive System

The erection of the penis is its enlarged and firm state. It depends on a complex interaction
of psychological, neural, vascular and endocrine factors. The term is also applied to the
process that leads to this state.
A penile erection occurs when two tubular structures that run the length of the penis, the
corpora cavernosa, become engorged with venous blood. This is a result of parasympathetic
nerve induced vasodilation. This may result from any of various physiological stimuli. The
corpus spongiosum is a single tubular structure located just below the corpora cavernosa,
which contains the urethra, through which urine and semen pass during urination and
ejaculation, respectively. This may also become slightly engorged with blood, but less so
than the corpora cavernosa.
Penile erection usually results from sexual stimulation and/or arousal, but can also occur
by such causes as a full urinary bladder or spontaneously during the course of a day or at
night, often during erotic or wet dreams. An erection results in swelling and enlargement of
the penis. Erection enables sexual intercourse and other sexual activities (sexual functions),
though it is not essential for all sexual activities.

13.3.3 Ejaculation
Emission is the term used when sperm moves into the urethra. Ejaculation is the term
used when sperm is forced out of the urethra and the penis. These are both stimulated by
sympathetic nerves.

13.3.4 Sperm Production

A spermatozoon or spermatozoan (pl. spermatozoa), from the ancient Greek (seed)
and (living being) and more commonly known as a sperm cell, is the haploid cell that
is the male gamete.

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Functions

Figure 116
a

A mature human Spermatozoona

http://en.wikibooks.org/wiki/Spermatozoon

Spermatagonia divides several times during the process of sperm development. The entire
process of sperm formation and maturation takes about 9-10 weeks. The separate divisions
that take place and what happens in each are as follows:
First division: The first division is done by mitosis, and ensures a constant supply of
spermatocytes, each with the diploid number of chromosomes.
Second division: Spermatocytes then undergo a series of two cell divisions during
meiosis to become secondary spermatocytes.
Third division: Secondary Spermatocytes finally become spermatids. Spermatids, which
are haploid cells, mature slowly to become the male gametes, or sperm.

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The Male Reproductive System

The sperm is the main reproductive cell in males. The sperms differ in that each carry a
set of chromosomes dividing each into either a male, or female sperm. The females differ
in that they carry a X gene, while the male sperm carry a Y gene. The female sperm also
differ phenotypically in that they have a larger head in comparison to the male sperms. This
contributes to the male sperm being lighter, and therefore faster and stronger swimmers
than their female counterparts (although statistically there is still a 50% chance of an either
XY or XX embryo forming.
Spermatozoan stream lines are straight and parallel. The tail flagellates, which we now know
propels the sperm cell (at about 1-3 mm/minute in humans) by rotating like a propeller, in
a circular motion, not side to side like a whip. The cell is characterized by a minimum of
cytoplasm. During fertilization, the sperm's mitochondria gets destroyed by the egg cell, and
this means only the mother is able to provide the baby's mitochondria and mitochondrial
DNA, which has an important application in tracing maternal ancestry. However it has
been recently discovered that mitochondrial DNA can be recombinant.
Spermatozoa are produced in the seminiferous tubules of the testes in a process called
spermatogenesis. Round cells called spermatogonia divide and differentiate eventually to
become spermatozoa. During copulation the vagina is inseminated, the spermatozoa move
through chemotaxis (see glossary) to the ovum inside a Fallopian tube or the uterus.

13.3.5 Sperm Pathway

Spermatogenesis takes place inside a males testes, specifically in the walls of the seminiferous
tubules. The epididymis is a tortuously coiled structure topping the testis, it receives
immature sperm from the testis and stores it for several days. When ejaculation occurs,
sperm is forcefully expelled from the tail of the epididymis into the ductus deferens. Sperm
travels through the ductus deferens and up the spermatic cord into the pelvic cavity, over
the ureter to the prostate behind the bladder. Here, the vas deferens joins with the seminal
vesicle to form the ejaculatory duct, which passes through the prostate and empties into the
urethra. Upon the sperm's exit from the testes, into the vas deferens, muscular movements
take over. When ejaculation occurs, rhythmic muscle movements of peristalsis propel the
sperm forward. This continues throughout the remainder of the sperm's journey through
the male reproductive system.
Sperm cells become even more active when they begin to interact with the fertilizing layer
of an egg cell. They swim faster and their tail movements become more forceful and erratic.
This behavior is called "hyper activation."
A recent discovery links hyper activation to a sudden influx of calcium ions into the tails.
The whip-like tail (flagellum) of the sperm is studded with ion channels formed by proteins
called CatSper. These channels are selective, allowing only calcium ion to pass. The opening
of CatSper channels is responsible for the influx of calcium. The sudden rise in calcium levels
causes the flagellum to form deeper bends, propelling the sperm more forcefully through the
viscous environment.

364

Functions

Figure 117

Acrosome reaction on a Sea Urchin cell

The sperm use their tails to push themselves into the epididymis, where they complete their
development. It takes sperm about 4 to 6 weeks to travel through the epididymis. The
sperm then move to the vas deferens, or sperm duct. The seminal vesicles and prostate
gland produce a whitish fluid called seminal fluid, which mixes with sperm to form semen
when a male is sexually stimulated.
The penis, which usually hangs limp, becomes hard when a male is sexually excited. Tissues
in the penis fill with blood and it becomes stiff and erect (an erection). The rigidity of the
erect penis makes it easier to insert into the female's vagina during sexual intercourse, and
the extended length allows it to reach deeper into the female's oviduct, the passage from the
ovaries to the outside of the body (allowing a shorter travel distance for the spermatozoa).
When the erect penis is stimulated to orgasm, muscles around the reproductive organs
contract and force the semen through the duct system and urethra. Semen is pushed out of
the male's body through his urethra - ejaculation. The speed of the semen is about 70 mph
when ejaculation comes and it can contain 100 to 600 million sperm cells. When the male
ejaculates during intercourse, semen is deposited into the fornix at the base of the female's
vagina, near the cervix. From the fornix, the sperm make their way up through the cervix
and move through the uterus with help from uterine contractions.
Sperm hyperactivity is necessary for breaking through two physical barriers that protect
the egg from fertilization. The first barrier to sperm is made up of so-called cumulus cells

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The Male Reproductive System

embedded in a gel-like substance made primarily of hyaluronic acid. The cumulus cells
develop in the ovary with the egg and support it as it grows.
The second barrier coating the oocyte is a thick shell formed by glycoproteins called the
zona pellucida. One of the proteins that make up the zona pellucida binds to a partner
molecule on the sperm. This lock-and-key type mechanism is species-specific and prevents
the sperm and egg of different species from fusing. There is some evidence that this binding
is what triggers the acrosome to release the enzymes that allow the sperm to fuse with the
egg.
When a sperm cell reaches the egg the acrosome releases its enzymes. These enzymes weaken
the shell, allowing the sperm cell to penetrate it and reach the plasma membrane of the egg.
Part of the sperm's cell membrane then fuses with the egg cell's membrane, and the sperm
cell sinks into the egg (at which point the sperm tail falls off).
Upon penetration, the egg cell membrane undergoes a change and becomes impenetrable,
preventing further fertilization.
The binding of the sperm to an ovum is called a zygote. A zygote is a single cell, with a
complete set of chromosomes, that normally develops into an embryo.

13.4 Puberty
In addition to producing sperm, the male reproductive system also produces sex hormones,
which help a boy develop into a sexually mature man during puberty. When a baby boy is
born, he has all the parts of his reproductive system in place, but it isn't until puberty that
his reproductive organs mature and become fully functional. As an newborn FSH and LH
levels are high and after a few weeks levels drop to extremely low. When puberty begins,
usually between the ages of 10 and 14, the pituitary gland - which is located in the brain secretes hormones that stimulate the testicles to produce testosterone. The production of
testosterone brings about many physical changes. Although the timing of these changes is
different for each individual male, the stages of puberty generally follow a set sequence.
First stage: the scrotum and testes grow larger, the apocrine glands develop (see explanation of apocrine glands in glossary).
Second stage: the penis becomes longer, and the seminal vesicles and prostate gland grow.
Hair begins to grow in the pubic region. Reproductive capacity has usually developed by
this stage.
Third stage: hair begins to appear on the face and underarms. During this time, a male's
voice also deepens. Fertility continues to increase.

13.4.1 Testicular size, function, and fertility

In boys, testicular enlargement is the first physical manifestation of puberty (and is termed
gonadarche). Testes in prepubertal boys change little in size from about 1 year of age to the
onset of puberty, averaging about 23 cc in volume and about 1.5-2 cm in length. Testicular
size continues to increase throughout puberty, reaching maximal adult size about 6 years

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Puberty
later. While 18-20 cc is reportedly an average adult size, there is wide variation in the
normal population.
The testes have two primary functions: to produce hormones and to produce sperm. The
Leydig cells produce testosterone (as described below), which in turn produces most of
the changes of male puberty. However, most of the increasing bulk of testicular tissue is
spermatogenic tissue (primarily Sertoli and interstitial cells). The development of sperm
production and fertility in males is not as well researched. Sperm can be detected in the
morning urine of most boys after the first year of pubertal changes (and occasionally earlier).

13.4.2 Genitalia
A boy's penis grows little from the fourth year of life until puberty. Average prepubertal
penile length is 4 cm. The prepubertal genitalia are described as stage 1. Within months
after growth of the testes begins, rising levels of testosterone promote growth of the penis and
scrotum. This earliest discernible beginning of pubertal growth of the genitalia is referred
to as stage 2. The penis continues to grow until about 18 years of age, reaching an average
adult size of about 10-16 cm.
Although erections and orgasm can occur in prepubertal boys, they become much more
common during puberty, accompanied by development of libido (sexual desire). Ejaculation
becomes possible early in puberty; prior to this boys may experience dry orgasms. Emission
of seminal fluid may occur due to masturbation or spontaneously during sleep (commonly
termed a wet dream, and more clinically called a nocturnal emission). The ability to ejaculate
is a fairly early event in puberty compared to the other characteristics, and can occur even
before reproductive capacity itself. In parallel to the irregularity of the first few periods
of a girl, for the first one or two years after a boy's first ejaculation, his seminal fluid may
contain few active sperm.
If the foreskin of a boy does not become retractable during childhood, it normally begins to
retract during puberty. This occurs as a result of the increased production of testosterone
and other hormones in the body.

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The Male Reproductive System

Figure 118 Distribution of

androgenic hair on female and
male body

13.4.3 Genital Erection

The penis contains two chambers called the corpora cavernosa, which run the length of the
organ. A spongy tissue, full of muscle, veins, arteries, etc. fills these chambers. The corpora
cavernosa are surrounded by a membrane, called the tunica albuginea.
Erection begins with sensory or mental stimulation, or both. Impulses from the brain and
local nerves cause the muscles of the corpora cavernosa to relax, allowing blood to flow
in and fill the spaces. The blood creates pressure in the corpora cavernosa, making the
penis expand. The tunica albuginea helps trap the blood in the corpora cavernosa, thereby
sustaining erection. When muscles in the penis contract to stop the inflow of blood and
open outflow channels, erection is reversed.

13.4.4 Pubic hair in boys

Pubic hair often appears on a boy shortly after the genitalia begin to grow. As in girls,
the first appearance of pubic hair is termed pubarche and the pubic hairs are usually first
visible at the dorsal (abdominal) base of the penis. The first few hairs are described as
stage 2. Stage 3 is usually reached within another 6 to 12 months, when the hairs are too
numerous to count. By stage 4, the pubic hairs densely fill the "pubic triangle." Stage 5
refers to spread of pubic hair to the inner thighs and upward towards the umbilicus as part
of the developing abdominal hair.

368

Sexual Homology

13.5 Sexual Homology

Figure 119

The human male reproductive system

369

The Male Reproductive System

../images/120.png

Figure 120

Cross-sectional diagram of the female reproductive organs.

In short, this is a known list of sex organs that evolve from the same tissue in a human life.
Indifferent
Gonad
Mullerian duct
Mullerian duct
Wolffian duct
Mesonephric tubules
Wolffian duct
Wolffian duct
Wolffian duct
Wolffian duct
Urogenital sinus

370

Male
Testis
Appendix testis
Prostatic utricle
Rete testis
Efferent ducts
Epididymis
Vas deferens
Seminal vesicle
Prostate
Bladder, urethra

Female
Ovary
Fallopian tubes
Uterus, proximal vagina
Rete ovarii
Epoophoron
Gartner's duct

Skene's glands
Bladder, urethra, distal vagina

Aging
Indifferent
Urogenital sinus
Genital swelling
Urogenital folds
Genital tubercle
Prepuce

Male
Bulbourethral gland
Scrotum
Distal urethra
Penis
Foreskin
Bulb of penis
Glans penis
Crus of penis

Female
Bartholin's gland
Labia majora
Labia minora
Clitoris
Clitoral hood
Vestibular bulbs
Clitoral glans
Clitoral crura

13.6 Aging
For most men, testosterone secretion continues throughout life, as does sperm production,
though both diminish with advancing age. Probably the most common reproductive problem
for older men is prostatic hypertrophy, enlargement of the prostate gland. This causes the
urethra to compress and urination becomes difficult. Residual urine in the bladder increases
the chance of urinary tract infections. Prostate hypertrophy is usually benign, but cancer of
the prostate is one of the more common cancers in elderly men. A TURP is commonly used
to correct this problem if the symptoms do not improve in response to home treatment and
medication.
Erectile dysfunction (ED) is another common problem seen in aging males. In older men,
ED usually has a physical cause, such as disease, injury, or side effects of drugs. Any disorder
that impairs blood flow in the penis or causes injury to the nerves has the potential to cause
ED. Although it is not an inevitable part of aging, incidences increases with age: About 5
percent of 40-year-old men and between 15 and 25 percent of 65-year-old men experience ED.
As discouraging as Erectile dysfunction may be, it is treatable at any age, and awareness
of this fact has been growing. More men have been seeking help and returning to normal
sexual activity because of improved, successful treatments for ED.

13.7 Things that can go wrong with the male reproductive

system
Boys may sometimes experience reproductive system problems. Below are some examples of
disorders that affect the male reproductive system (Disorders of the Scrotum, Testicles, or
Epididymis). Conditions affecting the scrotal contents may involve the testicles, epididymis,
or the scrotum itself.
Testicular trauma. Even a mild injury to the testicles can cause severe pain, bruising,
or swelling. Most testicular injuries occur when the testicles are struck, hit, kicked, or
crushed, usually during sports or due to other trauma. Testicular torsion, when 1 of the
testicles twists around, cutting off the blood supply, is also a problem that some teen
males experience - although it's not common. Surgery is needed to untwist the cord and
save the testicle.

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The Male Reproductive System

Varicocele1 . This is a varicose vein (an abnormally swollen vein) in the network of veins
that run from the testicles. Varicoceles commonly develop while a boy is going through
puberty. A varicocele is usually not harmful, although in some people it may damage the
testicle or decrease sperm production, so it helps for you to take your child to see his
doctor if he is concerned about changes in his testicles.
Testicular cancer2 . This is one of the most common cancers in men younger than 40.
It occurs when cells in the testicle divide abnormally and form a tumor. Testicular cancer
can spread to other parts of the body, but if it's detected early, the cure rate is excellent.
Teen boys should be encouraged to learn to perform testicular self-examinations.
Epididymitis3 is inflammation of the epididymis, the coiled tubes that connect the
testes with the vas deferens. It is usually caused by an infection, such as the sexually
transmitted disease chlamydia, and results in pain and swelling next to 1 of the testicles.
Hydrocele4 . A hydrocele occurs when fluid collects in the membranes surrounding the
testes. Hydroceles may cause swelling of the testicle but are generally painless. In some
cases, surgery may be needed to correct the condition.
Inguinal hernia5 . When a portion of the intestines pushes through an abnormal opening
or weakening of the abdominal wall and into the groin or scrotum, it is known as an
inguinal hernia. The hernia may look like a bulge or swelling in the groin area. It can be
corrected with surgery.

13.7.1 Disorders of Penis

Disorders of the Penis Disorders affecting the penis include the following:
Inflammation of the penis. Symptoms of penile inflammation include redness, itching,
swelling, and pain. Balanitis occurs when the glans (the head of the penis) becomes
inflamed. Posthitis is foreskin inflammation, which is usually due to a yeast or bacterial
infection.
Hypospadias. This is a disorder in which the urethra opens on the underside of the
penis, not at the tip.
Phimosis. This is a tightness of the foreskin of the penis and is common in newborns
and young children. It usually resolves itself without treatment. If it interferes with
urination, circumcision (removal of the foreskin) may be recommended.
Paraphimosis. This may develop when a boy's uncircumcised penis is retracted but
doesn't return to the unretracted position. As a result, blood flow to the penis may be
impaired, and your child may experience pain and swelling. A doctor may try to use
lubricant to make a small incision so the foreskin can be pulled forward. If that doesn't
work, circumcision may be recommended.

1
2
3
4
5

372

http://en.wikipedia.org/wiki/Varicocele
http://en.wikipedia.org/wiki/Testicular%20cancer
http://en.wikipedia.org/wiki/Epididymitis
http://en.wikipedia.org/wiki/Hydrocele
http://en.wikipedia.org/wiki/Inguinal%20hernia

Review Questions
Ambiguous genitalia. This occurs when a child is born with genitals that aren't clearly
male or female. In most boys born with this disorder, the penis may be very small or
nonexistent, but testicular tissue is present. In a small number of cases, the child may
have both testicular and ovarian tissue.
Micro penis. This is a disorder in which the penis, although normally formed, is well
below the average size, as determined by standard measurements.
Sexually transmitted diseases. Sexually transmitted diseases (STDs) that can affect boys include human immunodeficiency virus/acquired immunodeficiency syndrome
(HIV/AIDS), human papillomavirus (HPV, or genital warts), syphilis, chlamydia, gonorrhea, genital herpes, and hepatitis B. They are spread from one person to another mainly
through sexual intercourse.
Erectile dysfunction. E.D. is the inability to get or keep an erection firm enough
for sexual intercourse. This can also called impotence. The word "impotence" may
also be used to describe other problems that can interfere with sexual intercourse and
reproduction, such as problems with ejaculation or orgasm and lack of sexual desire.
Using the term erectile dysfunction clarifies that those other problems are not involved.

13.7.2 Contraceptive for Men

Vasectomy: In the procedure the vas deferens of each testes is cut and tied off to prevent the
passage of sperm. Sperm is still produced and stored in crypt sites causing inflammation.
Because of this inflammatory response the immune system acts on them destroying them
and then having antisperm antibodies. This causes a lower possibility if the vasectomy is
reversed to becoming fertile again.
Condoms: A device, usually made of latex, or more recently polyurethane, that is used
during sexual intercourse. It is put on a man's penis and physically blocks ejaculated
semen from entering the body of a sexual partner. Condoms are used to prevent pregnancy,
transmission of sexually transmitted diseases (STDs - such as gonorrhea, syphilis, and HIV),
or both.

13.8 Review Questions

Answers for these questions can be found here6
1. This is needed to make immature sperm mature
A) FHS
B) LH
C) FSH
D) HL

http://en.wikibooks.org/wiki/Human_Physiology/Appendix_1:_answers_to_review_
questions#The_male_reproductive_system

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The Male Reproductive System

2. These become engorged with blood in an erection
A) corpora cavernosa
B) fiberous envelope
C) septum pectiniforme
D) integument
E) dorsal veins
3. The difference between male and female sperm
A) female sperm have a larger head
B) male sperm are lighter
C) female sperm are faster
D) male sperm are weaker
E) A and B
F) C and D
4. The entire process of sperm formation takes about
A) 5-6 weeks
B) 7-8 weeks
C) 3-4 weeks
D) 9-10 weeks
5. Hyper Activation occurs when
A) the sperm are introduced into the urethra
B) the sperm are ejaculated into the vaginal canal
C) the sperm begin to interact with the fertilizing layer of an egg cell
D) the sperm reach the cervix
6. It takes sperm ___________weeks to travel through the epididymis
A) 6-8
B) 1-3
C) 2-4
D) 4-6
7. While singing in the choir, Ben suddenly notices his voice is constantly cracking. This is
caused by
A) androgens
B) LH

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Glossary
C) FSH
D) Bens inability to sing
8. In sexual homology, the glans penis in the male is equal to _____________in the
female
A) clitoral hood
B) clitoris
C) clitoral glans
D) clitoral crura
9. In sexual homology, the ___________in the male is equal to the fallopian tubes in
the female
A) testis
B) appendix testis
C) vas deferens
D) seminal vesicle
E) efferent ducts
10. Joe has a bulge in the groin area that seems to get worse when he lifts things. This
most likely is
A) epididymitis
B) testicular cancer
C) varicocele
D) hydrocele
E) inguinal hernia

13.9 Glossary
Androgen: The generic term for any natural or synthetic compound, usually a steroid
hormone, that stimulates or controls the development and maintenance of masculine characteristics in vertebrates by binding to androgen receptors. This includes the activity of
the accessory male sex organs and development of male secondary sex characteristics. They
are also the precursor of all estrogens, the female sex hormones. The primary and most
well-known androgen is testosterone.
Apocrine Glands: Apocrine sweat glands develop during the early to mid puberty ages
approximately around the age of 15 and release more than normal amounts of sweat for
approximately a month and subsequently regulate and release normal amounts of sweat
after a certain period of time. They are located wherever there is body hair. These glands
produce sweat that contains fatty materials. Mainly present in the armpits and around the

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genital area, their activity is the main cause of sweat odor, due to the bacteria that break
down the organic compounds in the sweat.
Bulbourethral Glands: male accessory sex glands that secrete mucus for lubrication
Chemotaxis: Chemotaxis is a kind of taxis, in which bodily cells, bacteria, and other
single-cell or multicellular organisms direct their movements according to certain chemicals
in their environment. This is important for bacteria to find food (for example, glucose)
by swimming towards the highest concentration of food molecules, or to flee from poisons
(for example, phenol). In multicellular organisms, chemotaxis is critical to development as
well as normal function. In addition, it has been recognized that mechanisms that allow
chemotaxis in animals can be subverted during cancer metastasis.
Corpora Cavernosa: one of a pair of a sponge-like regions of erectile tissue which contain
most of the blood in the male penis during erection
Ductus Deferens: epididymal ducts from each testis converge to form a large, thick walled,
muscular duct
Ejaculatory Ducts: two ducts, receive sperm from the ductus deferens and secretions
from the seminal vesicle; the ducts then empty into the urethra
Epididymis: comma shaped and loosely attached to the rear surface of each testis
Erectile Tissue: smooth muscle and connective tissue inside the penis that contain blood
sinuses; large, irregular vascular channels
Erection: the penis at its enlarged and firm state; occurs when the corpora cavernosa
become engorged with venous blood
Flagellum: the whip-like tail of a sperm, propels the sperm towards the egg in hopes of
achieving fertilization
Follicle-Stimulating Hormone (FSH): hormone that stimulates production of sertoli
cells, to make immature sperm to mature sperm
Glans Penis: distal end of the penis, covered with the foreskin
Gonadotropin-Releasing Hormone (GnRH): hormone secreted by the hypothalamus
into the pituitary gland; two types, FSH and LH
Libido: In its common usage, it means sexual desire; however, more technical definitions,
such as those found in the work of Carl Jung, are more general, referring to libido as the
free creativeor psychicenergy an individual has to put toward personal development, or
individuation.
Luteinizing Hormone (LH): hormone that stimulates Leydig cells in the testes to produce
testosterone
Oviduct: the passage in females from the ovaries to the outside of the body.
Penis: external genital organ of the male
Prostate Gland: male accessory sex gland that secretes an alkaline fluid, which neutralizes
acidic vaginal secretions

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Summary
Puberty: the period of maturation and arousal of the dormant and nonfunctional reproductive system; usually occurs in males between the ages of 10 and 15
Scrotum: skin covered sac that houses the male testicles; keeps the testicles away form the
body so that they can stay a few degrees cooler than the body, for better sperm production
Seminal Vesicle: male accessory sex glands that supply fructose to ejaculated sperm and
secrete prostaglandins
Seminiferous Tubules: highly coiled tubules within the testes that produce spermatozoa
Sertoli Cell: A Sertoli cell (a kind of sustentacular cell) is a 'nurse' cell of the testes which
is part of a seminiferous tubule.
It is activated by follicle-stimulating hormone, and has FSH-receptor on its membranes.
Its main function is to nurture the developing sperm cells through the stages of spermatogenesis. Because of this, it has also been called the "mother cell." It provides both secretory
and structural support.
Sexual Homology: sex organs that evolve from the same tissues in both male and females
Sperm: main reproductive cell in males
Spermatogenesis: sperm production
Testes: located in the scrotum, produces testosterone which stimulates production of sperm
Testosterone: male sex hormone secreted by the leydig cells of the testes, vital for the
production of sperm
TURP: transurethral resection of the prostate. During TURP, an instrument is inserted
up the urethra to remove the section of the prostate that is blocking urine flow. This is
most commonly caused by benign prostatic hyperplasia (BPH). A TURP usually requires
hospitalization and is done using a general or spinal anesthetic. It is now the most common
surgery used to remove part of an enlarged prostate.
Urethra: the last part of the urinary tract; in males, it is the passage for both urine and
sperm
Varicocele: varicose vein of the testicles, sometimes a cause of male infertility
Vasectomy: most common sterilization procedure in males; small segment of each ductus
deferens is surgically removed after it passes from the testis

13.10 Summary
Both male and female reproductive systems may seem somewhat isolated from other body
systems in that their purpose is to create new life and not just to maintain existing life.
There are however significant relationships between the reproductive system and other body
systems. All systems relate in one way or another to help our bodies maintain homeostasis.

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13.11 References
"Essentials of Anatomy and Physiology" by Valerie C. Scanlon and Tina Sanders
"Web MD": http://www.webmd.com
Wikibook: Sexual Health7

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14 The Female Reproductive System

14.1 Introduction
All living things reproduce. This is something that sets the living apart from non-living.
Even though the reproductive system is essential to keeping a species alive, it is not essential
to keeping an individual alive. This chapter describes the different parts of the female
reproductive system: the organs involved in the process of reproduction, hormones that
regulate a woman's body, the menstrual cycle, ovulation and pregnancy, the female's role in
genetic division, birth control, sexually transmitted diseases and other diseases and disorders.

14.1.1 Reproduction
Reproduction can be defined as the process by which an organism continues its species. In
the human reproductive process, two kinds of sex cells ( gametes), are involved: the male
gamete (sperm), and the female gamete (egg or ovum). These two gametes meet within
the female's uterine tubes located one on each side of the upper pelvic cavity, and begin
to create a new individual. The female needs a male to fertilize her egg; she then carries
offspring through pregnancy and childbirth.
Similarities between male and female reproductive systems
The reproductive systems of the male and female have some basic similarities and some
specialized differences. They are the same in that most of the reproductive organs of both
sexes develop from similar embryonic tissue, meaning they are homologous. Both systems
have gonads that produce (sperm and egg or ovum) and sex organs. And both systems
experience maturation of their reproductive organs, which become functional during puberty
as a result of the gonads secreting sex hormones.

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The Female Reproductive System

Figure 121

380

The human male reproductive system

Introduction

../images/122.png

Figure 122

Cross-sectional diagram of the female reproductive organs.

In short, this is a known list of sex organs that evolve from the same tissues in a human life.
Undifferentiated
Gonad
Mullerian duct
Mullerian duct
Wolffian duct
Mesonephric tubules
Wolffian duct
Wolffian duct
Wolffian duct
Wolffian duct
Urogenital sinus

Male
Testis
Appendix testis
Prostatic utricle
Rete testis
Efferent ducts
Epididymis
Vas deferens
Seminal vesicle
Prostate
Bladder, urethra

Female
Ovary
Fallopian tubes
Uterus, proximal
Rete ovarii
Epoophoron
Gartner's duct

Skene's glands
Bladder, urethra, distal

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The Female Reproductive System

Undifferentiated
Urogenital sinus
Genital swelling
Urogenital folds
Genital tubercle
Prepuce

Male
Bulbourethral gland
Scrotum
Distal urethra
Penis
Bulb of penis
Glans penis
Crus of penis

Female
Bartholin's gland
Labia majora
Labia minora
Clitoris
Clitoral hood
Vestibular bulbs
Clitoral glans
Clitoral crura

Differences between male and female reproductive systems

The differences between the female and male reproductive systems are based on the functions
of each individual's role in the reproduction cycle. A male who is healthy, and sexually
mature, continuously produces sperm. The development of women's "eggs" are arrested
during fetal development. This means she is born with a predetermined number of oocytes
and cannot produce new ones.
At about 5 months gestation, the ovaries contain approximately six to seven million oogonia,
which initiate meiosis. The oogonia produce primary oocytes that are arrested in prophase
I of meiosis from the time of birth until puberty. After puberty, during each menstrual
cycle, one or several oocytes resume meiosis and undergo their first meiotic division during
ovulation. This results in the production of a secondary oocyte and one polar body. The
meiotic division is arrested in metaphase II. Fertilization triggers completion of the second
meiotic division and the result is one ovum and an additional polar body.
The ovaries of a newborn baby girl contain about one million oocytes. This number declines
to 400,000 to 500,000 by the time puberty is reached. On average, 500-1000 oocytes are
ovulated during a woman's reproductive lifetime.
When a young woman reaches puberty around age 10 to 13, a promary oocyte is discharged
from one of the ovaries every 28 days. This continues until the woman reaches menopause,
usually around the age of 50 years. Occytes are present at birth, and age as a woman ages.
Female Reproductive System

Produces eggs (ova)

Secretes sex hormones
Receives the male spermatazoa during
Protects and nourishes the fertilized egg until it is fully developed
Delivers fetus through birth canal
Provides nourishment to the baby through milk secreted by mammary glands in the
breast

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External Genitals

14.2 External Genitals

Figure 123
Vulva
The external female genitalia is referred to as vulva. It consists of the labia majora and
labia minora (while these names translate as "large" and "small" lips, often the "minora"
can protrude outside the "majora"), mons pubis, clitoris, opening of the urethra (meatus),
vaginal vestibule, vestibular bulbs, vestibular glands.
The term "vagina" is often improperly used as a generic term to refer to the vulva or female
genitals, even though - strictly speaking - the vagina is a specific internal structure and the
vulva is the exterior genitalia only. Calling the vulva the vagina is akin to calling the mouth
the throat.
Mons Veneris
The mons veneris, Latin for "mound of Venus" (Roman Goddess of love) is the soft mound
at the front of the vulva (fatty tissue covering the pubic bone). It is also referred to as
the mons pubis. The mons veneris protects the pubic bone and vulva from the impact of
sexual intercourse. After puberty, it is covered with pubic hair, usually in a triangular shape.
Heredity can play a role in the amount of pubic hair an individual grows.
Labia Majora

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The Female Reproductive System

The labia majora are the outer "lips" of the vulva. They are pads of loose connective and
adipose tissue, as well as some smooth muscle. The labia majora wrap around the vulva
from the mons pubis to the perineum. The labia majora generally hides, partially or entirely,
the other parts of the vulva. There is also a longitudinal separation called the pudendal cleft.
These labia are usually covered with pubic hair. The color of the outside skin of the labia
majora is usually close to the overall color of the individual, although there may be some
variation. The inside skin is usually pink to light brown. They contain numerous sweat and
oil glands. It has been suggested that the scent from these oils are sexually arousing.
Labia Minora
Medial to the labia majora are the labia minora. The labia minora are the inner lips of
the vulva. They are thin stretches of tissue within the labia majora that fold and protect
the vagina, urethra, and clitoris. The appearance of labia minora can vary widely, from
tiny lips that hide between the labia majora to large lips that protrude. There is no pubic
hair on the labia minora, but there are sebaceous glands. The two smaller lips of the labia
minora come together longitudinally to form the prepuce, a fold that covers part of the
clitoris. The labia minora protect the vaginal and urethral openings. Both the inner and
outer labia are quite sensitive to touch and pressure.
Clitoris

Figure 124
The clitoris, visible as the small white oval between the top of the labia minora and the
clitoral hood, is a small body of spongy tissue that functions solely for sexual pleasure.
Only the tip or glans of the clitoris shows externally, but the organ itself is elongated and
branched into two forks, the crura, which extend downward along the rim of the vaginal
opening toward the perineum. Thus the clitoris is much larger than most people think it is,
about 4" long on average.
The clitoral glans or external tip of the clitoris is protected by the prepuce, or clitoral hood,
a covering of tissue similar to the foreskin of the male penis. However, unlike the penis, the
clitoris does not contain any part of the urethra.
During sexual excitement, the clitoris erects and extends, the hood retracts, making the
clitoral glans more accessible. The size of the clitoris is variable between women. On some,
the clitoral glans is very small; on others, it is large and the hood does not completely cover
it.

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Internal Genitals
Urethra
The opening to the urethra is just below the clitoris. Although it is not related to sex or
reproduction, it is included in the vulva. The urethra is actually used for the passage of
urine. The urethra is connected to the bladder. In females the urethra is 1.5 inches long,
compared to males whose urethra is 8 inches long. Because the urethra is so close to the
anus, women should always wipe themselves from front to back to avoid infecting the vagina
and urethra with bacteria. This location issue is the reason for bladder infections being
more common among females.
Hymen
The hymen is a thin fold of mucous membrane that separates the lumen of the vagina from
the urethral sinus. Sometimes it may partially cover the vaginal orifice. The hymen is
usually perforated during later fetal development.
Because of the belief that first vaginal penetration would usually tear this membrane and
cause bleeding, its "intactness" has been considered a guarantor of virginity. However, the
hymen is a poor indicator of whether a woman has actually engaged in sexual intercourse
because a normal hymen does not completely block the vaginal opening. The normal hymen
is never actually "intact" since there is always an opening in it. Furthermore, there is not
always bleeding at first vaginal penetration. The blood that is sometimes, but not always,
observed after first penetration can be due to tearing of the hymen, but it can also be from
injury to nearby tissues.
A tear to the hymen, medically referred to as a "transection," can be seen in a small
percentage of women or girls after first penetration. A transection is caused by penetrating
trauma. Masturbation and tampon insertion can, but generally are not forceful enough to
cause penetrating trauma to the hymen. Therefore, the appearance of the hymen is not a
reliable indicator of virginity or chastity.
Perineum
The perineum is the short stretch of skin starting at the bottom of the vulva and extending
to the anus. It is a diamond shaped area between the symphysis pubis and the coccyx. This
area forms the floor of the pelvis and contains the external sex organs and the anal opening.
It can be further divided into the urogenital triangle in front and the anal triangle in back.
The perineum in some women may tear during the birth of an infant and this is apparently
natural. Some physicians however, may cut the perineum preemptively on the grounds that
the "tearing" may be more harmful than a precise cut by a scalpel. If a physician decides
the cut is necessary, they will perform it. The cut is called an episiotomy.

14.3 Internal Genitals

14.3.1 Vagina
The vagina is a muscular, hollow tube that extends from the vaginal opening to the cervix
of the uterus. It is situated between the urinary bladder and the rectum. It is about three
to five inches long in a grown woman. The muscular wall allows the vagina to expand and

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The Female Reproductive System

contract. The muscular walls are lined with mucous membranes, which keep it protected
and moist. A thin sheet of tissue with one or more holes in it, called the hymen, partially
covers the opening of the vagina. The vagina receives sperm during sexual intercourse from
the penis. The sperm that survive the acidic condition of the vagina continue on through to
the fallopian tubes where fertilization may occur.
The vagina is made up of three layers, an inner mucosal layer, a middle muscularis layer,
and an outer fibrous layer. The inner layer is made of vaginal rugae that stretch and allow
penetration to occur. These also help with stimulation of the penis. microscopically the
vaginal rugae has glands that secrete an acidic mucus (pH of around 4.0.) that keeps
bacterial growth down. The outer muscular layer is especially important with delivery of a
fetus and placenta.
Purposes of the Vagina

Receives a male's erect penis and semen during sexual intercourse.

Pathway through a woman's body for the baby to take during childbirth.
Provides the route for the menstrual blood (menses) from the uterus, to leave the body.
May hold forms of birth control, such as a diaphragm, FemCap, Nuva Ring, or female
condom.

Clinical Application:
Pelvic inflammatory disease (PID) is a widespread infection that originates in the vagina
and uterus and spreads to the uterine tubes, ovaries, and ultimately the pelvic peritoneum.
This condition, which occurs in about 10% of women is usually caused by chlamydial or
gonorrheal infection, other bacteria infecting the vagina may be involved as well. Signs
and symptoms include tenderness of the lower abdomen, fever, and a vaginal discharge.
Even a single episode of PID can cause infertility, due to scarring that blocks the uterine
tubes. Therefore, patients are immediately given broad-spectrum antibiotics whenever
PID is suspected.

14.3.2 Cervix
The cervix (from Latin "neck") is the lower, narrow portion of the uterus where it joins
with the top end of the vagina. Where they join together forms an almost 90 degree curve.
It is cylindrical or conical in shape and protrudes through the upper anterior vaginal wall.
Approximately half its length is visible with appropriate medical equipment; the remainder
lies above the vagina beyond view. It is occasionally called "cervix uteri", or "neck of the
uterus".
During menstruation, the cervix stretches open slightly to allow the endometrium to be shed.
This stretching is believed to be part of the cramping pain that many women experience.
Evidence for this is given by the fact that some women's cramps subside or disappear after
their first vaginal birth because the cervical opening has widened.
The portion projecting into the vagina is referred to as the portio vaginalis or ectocervix.
On average, the ectocervix is three cm long and two and a half cm wide. It has a convex,
elliptical surface and is divided into anterior and posterior lips. The ectocervix's opening is
called the external os. The size and shape of the external os and the ectocervix varies widely

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Internal Genitals
with age, hormonal state, and whether the woman has had a vaginal birth. In women who
have not had a vaginal birth the external os appears as a small, circular opening. In women
who have had a vaginal birth, the ectocervix appears bulkier and the external os appears
wider, more slit-like and gaping.
The passageway between the external os and the uterine cavity is referred to as the endocervical canal. It varies widely in length and width, along with the cervix overall. Flattened
anterior to posterior, the endocervical canal measures seven to eight mm at its widest in
reproductive-aged women. The endocervical canal terminates at the internal os which is the
opening of the cervix inside the uterine cavity.
During childbirth, contractions of the uterus will dilate the cervix up to 10 cm in diameter
to allow the child to pass through. During orgasm, the cervix convulses and the external os
dilates.

14.3.3 Uterus
The uterus is shaped like an upside-down pear, with a thick lining and muscular walls.
Located near the floor of the pelvic cavity, it is hollow to allow a blastocyte, or fertilized
egg, to implant and grow. It also allows for the inner lining of the uterus to build up until a
fertilized egg is implanted, or it is sloughed off during menses.
The uterus contains some of the strongest muscles in the female body. These muscles are
able to expand and contract to accommodate a growing fetus and then help push the baby
out during labor. These muscles also contract rhythmically during an orgasm in a wave
like action. It is thought that this is to help push or guide the sperm up the uterus to the
fallopian tubes where fertilization may be possible.
The uterus is only about three inches long and two inches wide, but during pregnancy it
changes rapidly and dramatically. The top rim of the uterus is called the fundus and is a
landmark for many doctors to track the progress of a pregnancy. The uterine cavity refers
to the fundus of the uterus and the body of the uterus.
Helping support the uterus are ligaments that attach from the body of the uterus to the
pelvic wall and abdominal wall. During pregnancy the ligaments prolapse due to the growing
uterus, but retract after childbirth. In some cases after menopause, they may lose elasticity
and uterine prolapse may occur. This can be fixed with surgery.
Some problems of the uterus include uterine fibroids, pelvic pain (including endometriosis,
adenomyosis), pelvic relaxation (or prolapse), heavy or abnormal menstrual bleeding, and
cancer. It is only after all alternative options have been considered that surgery is recommended in these cases. This surgery is called hysterectomy. Hysterectomy is the removal of
the uterus, and may include the removal of one or both of the ovaries. Once performed it is
irreversible. After a hysterectomy, many women begin a form of alternate hormone therapy
due to the lack of ovaries and hormone production.

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The Female Reproductive System

Figure 125

14.3.4 Fallopian Tubes

At the upper corners of the uterus are the fallopian tubes. There are two fallopian tubes,
also called the uterine tubes or the oviducts. Each fallopian tube attaches to a side of the
uterus and connects to an ovary. They are positioned between the ligaments that support
the uterus. The fallopian tubes are about four inches long and about as wide as a piece of
spaghetti. Within each tube is a tiny passageway no wider than a sewing needle. At the
other end of each fallopian tube is a fringed area that looks like a funnel. This fringed area,
called the infundibulum, lies close to the ovary, but is not attached. The ovaries alternately
release an egg. When an ovary does ovulate, or release an egg, it is swept into the lumen of
the fallopian tube by the fimbriae.
Once the egg is in the fallopian tube, tiny hairs in the tube's lining help push it down the
narrow passageway toward the uterus. The oocyte, or developing egg cell, takes four to
five days to travel down the length of the fallopian tube. If enough sperm are ejaculated
during sexual intercourse and there is an oocyte in the fallopian tube, fertilization will occur.
After fertilization occurs, the zygote, or fertilized egg, will continue down to the uterus and
implant itself in the uterine wall where it will grow and develop.
If a zygote doesn't move down to the uterus and implants itself in the fallopian tube, it is
called a ectopic or tubal pregnancy. If this occurs, the pregnancy will need to be terminated
to prevent permanent damage to the fallopian tube, possible hemorrhage and possible death
of the mother.

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Internal Genitals

14.3.5 Mammary glands

Figure 126 Cross section of the breast of a

human female.
Mammary glands are the organs that produce milk for the sustenance of a baby. These
exocrine glands are enlarged and modified sweat glands.
Structure
The basic components of the mammary gland are the alveoli (hollow cavities, a few
millimetres large) lined with milk-secreting epithelial cells and surrounded by myoepithelial
cells. These alveoli join up to form groups known as lobules, and each lobule has a
lactiferous duct that drains into openings in the nipple. The myoepithelial cells can
contract, similar to muscle cells, and thereby push the milk from the alveoli through the
lactiferous ducts towards the nipple, where it collects in widenings (sinuses) of the ducts. A
suckling baby essentially squeezes the milk out of these sinuses.
The development of mammary glands is controlled by hormones. The mammary glands exist
in both sexes, but they are rudimentary until puberty when - in response to ovarian hormones
- they begin to develop in the female. Estrogen promotes formation, while testosterone
inhibits it.
At the time of birth, the baby has lactiferous ducts but no alveoli. Little branching occurs
before puberty when ovarian estrogens stimulate branching differentiation of the ducts into
spherical masses of cells that will become alveoli. True secretory alveoli only develop in
pregnancy, where rising levels of estrogen and progesterone cause further branching and

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The Female Reproductive System

differentiation of the duct cells, together with an increase in adipose tissue and a richer
blood flow.
Colostrum is secreted in late pregnancy and for the first few days after giving birth. True milk
secretion (lactation) begins a few days later due to a reduction in circulating progesterone
and the presence of the hormone prolactin. The suckling of the baby causes the release of
the hormone oxytocin which stimulates contraction of the myoepithelial cells.
The cells of mammary glands can easily be induced to grow and multiply by hormones.
If this growth runs out of control, cancer results. Almost all instances of breast cancer
originate in the lobules or ducts of the mammary glands.
STRUCTURE
Breasts

Cervix

Clitoris

Fallopian tubes

Hymen

Labia majora

Labia minora

Mons

390

LOCATION & DEFUNCTION

SCRIPTION
Upper chest one on each
Lactation milk/nutrition
side containing alveolar
for newborn.
cells (milk production), myoepithelial cells (contract
to expel milk), and duct
walls (help with extraction
of milk).
The lower narrower porDuring childbirth, contion of the uterus.
tractions of the uterus will
dilate the cervix up to 10
cm in diameter to allow
the child to pass through.
During orgasm, the cervix
convulses and the external
os dilates
Small erectile organ diSexual excitation, enrectly in front of the
gorged with blood.
vestibule.
Extending upper part of
Egg transportation from
the uterus on either side.
ovary to uterus (fertilization usually takes place
here).
Thin membrane that partially covers the vagina in
young females.
Outer skin folds that surLubrication during matround the entrance to the
ing.
vagina.
Inner skin folds that surLubrication during matround the entrance to the
ing.
vagina.
Mound of skin and underlying fatty tissue, central
in lower pelvic region

The Female Reproductive Cycle

STRUCTURE
Ovaries (female gonads)

Perineum

Urethra
Uterus

LOCATION & DESCRIPTION

Pelvic region on either
side of the uterus.

Short stretch of skin starting at the bottom of the

vulva and extending to the
anus.
Pelvic cavity above bladder, tilted.
Center of pelvic cavity.

Vagina

Canal about 10-8 cm long

going from the cervix to
the outside of the body.

Vulva

Surround entrance
to the reproductive
tract.(encompasses all external genitalia)
The innermost layer of
uterine wall.

Endometrium

Myometrium

Smooth muscle in uterine

wall.

FUNCTION
Provides an environment
for maturation of oocyte.
Synthesizes and secretes
sex hormones (estrogen
and progesterone).

Passage of urine.
To house and nourish developing human.
Receives penis during mating. Pathway through a
womans body for the baby
to take during childbirth.
Provides the route for the
menstrual blood (menses)
from the uterus, to leave
the body. May hold forms
of birth control, such as an
IUD, diaphragm, neva ring,
or female condom

Contains glands that secrete fluids that bathe the

utrine lining.
Contracts to help expel the
baby.

14.4 The Female Reproductive Cycle

Towards the end of puberty, girls begin to release eggs as part of a monthly period called
the female reproductive cycle, or menstrual cycle (menstrual referring to "monthly").
Approximately every 28 days, during ovulation, an ovary sends a tiny egg into one of the
fallopian tubes. Unless the egg is fertilized by a sperm while in the fallopian in the two to
three days following ovulation, the egg dries up and leaves the body about two weeks later
through the vagina. This process is called menstruation. Blood and tissues from the inner
lining of the uterus (the endometrium) combine to form the menstrual flow, which generally
lasts from four to seven days. The first period is called menarche. During menstruation

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The Female Reproductive System

arteries that supply the lining of the uterus constrict and capillaries weaken. Blood spilling
from the damaged vessels detaches layers of the lining, not all at once but in random patches.
Endometrium mucus and blood descending from the uterus, through the liquid creates the
menstruation flow.

Figure 127

Menstrual cycle

The reproductive cycle can be divided into an ovarian cycle and a uterine cycle (compare
ovarian histology and uterine histology in the diagram on the right). During the uterine
cycle, the endometrial lining of the uterus builds up under the influence of increasing
levels of estrogen (labeled as estradiol in the image). Follicles develop, and within a few
days one matures into an ovum, or egg. The ovary then releases this egg, at the time
of ovulation. After ovulation the uterine lining enters a secretory phase, or the ovarian
cycle, in preparation for implantation, under the influence of progesterone. Progesterone is
produced by the corpus luteum (the follicle after ovulation) and enriches the uterus with
a thick lining of blood vessels and capillaries so that it can sustain the growing fetus. If
fertilization and implantation occur, the embryo produces Human Chorionic Gonadotropin

392

The Female Reproductive Cycle

(HCG), which maintains the corpus luteum and causes it to continue producing progesterone
until the placenta can take over production of progesterone. Hence, progesterone is "pro
gestational" and maintains the uterine lining during all of pregnancy. If fertilization and
implantation do not occur the corpus luteum degenerates into a corpus albicans, and
progesterone levels fall. This fall in progesterone levels cause the endometrium lining to
break down and sluff off through the vagina. This is called menstruation, which marks the
low point for estrogen activity and is the starting point of a new cycle.
Common usage refers to menstruation and menses as a period. This bleeding serves as a
sign that a woman has not become pregnant. However, this cannot be taken as certainty,
as sometimes there is some bleeding in early pregnancy. During the reproductive years,
failure to menstruate may provide the first indication to a woman that she may have become
pregnant.
Menstruation forms a normal part of a natural cyclic process occurring in healthy women
between puberty and the end of the reproductive years. The onset of menstruation, known
as menarche, occurs at an average age of 12, but is normal anywhere between 8 and
16. Factors such as heredity, diet, and overall health can accelerate or delay the onset of
menarche.
Signs of ovulation
The female body produces outward signs that can be easily recognized at the time of
ovulation. The two main signs are thinning of the cervical mucus and a slight change in
body temperature.
Thinning of the Cervical Mucus
After menstruation and right before ovulation, a woman will experience an increase of
cervical mucus. At first, it will be thick and yellowish in color and will not be very plentiful.
Leading up to ovulation, it will become thinner and clearer. On or around the day of
ovulation, the cervical mucus will be very thin, clear and stretchy. It can be compared to
the consistency of egg whites. This appearance is known as 'spinnbarkeit'.
Temperature Change
A woman can also tell the time of ovulation by taking her basal body temperature daily.
This is a temperature taken with a very sensitive thermometer first thing in the morning
before the woman gets out of bed. The temperature is then tracked to show changes. In the
uterine cycle, a normal temperature will be around 97.0 98.0. The day of ovulation the
temperature spikes down, usually into the 96.0 97.0 range and then the next morning it
will spike up to normal of around 98.6 and stay in that range until menstruation begins.
Both of these methods are used for conception and contraception. They are more efficient in
conception due to the fact that sperm can live for two to three days inside of the fallopian
tubes. A woman could be off by a couple of days in her calculations and still become
pregnant.
Menopause is the physiological cessation of menstrual cycles associated with advancing age.
Menopause is sometimes referred to as "the change of life" or climacteric. Menopause occurs
as the ovaries stop producing estrogen, causing the reproductive system to gradually shut
down. As the body adapts to the changing levels of natural hormones, vasomotor symptoms
such as hot flashes and palpitations, psychological symptoms such as increased depression,

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The Female Reproductive System

anxiety, irritability, mood swings and lack of concentration, and atrophic symptoms such
as vaginal dryness and urgency of urination appear. Together with these symptoms, the
woman may also have increasingly scanty and erratic menstrual periods.
Technically, menopause refers to the cessation of menses; the gradual process through which
this occurs, which typically takes a year but may last as little as six months or more than
five years, is known as climacteric. A natural or physiological menopause is that which
occurs as a part of a woman's normal aging process. However, menopause can be surgically
induced by such procedures as hysterectomy.
The average onset of menopause is 50.5 years, but some women enter menopause at a younger
age, especially if they have suffered from cancer or another serious illness and undergone
chemotherapy. Premature menopause is defined as menopause occurring before the age of
40, and occurs in 1% of women. Other causes of premature menopause include autoimmune
disorders, thyroid disease, and diabetes mellitus.
Premature menopause is diagnosed by measuring the levels of follicle stimulating hormone
(FSH) and luteinizing hormone (LH). The levels of these hormones will be higher if menopause
has occurred. Rates of premature menopause have been found to be significantly higher in
both fraternal and identical twins; approximately 5% of twins reach menopause before the
age of 40. The reasons for this are not completely understood. Post-menopausal women are
at increased risk of osteoporosis.
Perimenopause refers to the time preceding menopause, during which the production of
hormones such as estrogen and progesterone diminish and become more irregular. During
this period fertility diminishes. Menopause is arbitrarily defined as a minimum of twelve
months without menstruation. Perimenopause can begin as early as age 35, although it
usually begins much later. It can last for a few months or for several years. The duration of
perimenopause cannot be predicted in advance.
Premenstrual Syndrome (PMS) It is common for women to experience some discomfort
in the days leading up to their periods. PMS usually is at its worst the seven days before a
period starts and can continue through the end of the period. PMS includes both physical
and emotional symptoms: acne, bloating, fatigue, backaches, sore breasts, headaches,
constipation, diarrhea, food cravings, depression, irritability, difficulty concentrating or
handling stress.

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Ovarian and Uterine Cycles in the Nonpregnant Woman

14.5 Ovarian and Uterine Cycles in the Nonpregnant

Woman

Figure 128

An ovary about to release an egg.

Ovarian Cycle
Follicular phase Days 1-13

Events
FSH secretion
begins.
Follicle maturation occurs.

Uterine Cycle
Menstruation Days 2-5
Proliferative
phase - Days 6-13

Events
Endometrium
breaks down.
Endometrium
rebuilds.

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The Female Reproductive System

Ovarian Cycle

Ovulation - Day
14*
Luteal phase Days 15-28

Events
Estrogen secretion is prominent.
LH spike occurs.

Uterine Cycle

LH secretion continues.

Secretory phase Days 15-28

Events

Endometrial
thickens, and
glands are secretory.

Corpus luteum
forms.
Progesterone secretion is prominent.
(*)Assuming a 28 day cycle.
There are two phases of the ovarian cycle the follicular phase and the luteal phase. In the
follicular phase about 10-25 follicles are taken from preantral or early antrial follicles to
develop further. Seven days later the dominant follicle is selected to develop to full maturity.
This is the pre-cursor for ovulation. Follicles themselves secrete FSH and estrogen, and these
two hormones stimulate follicular growth and development. Ovulation marks the beginning
of the luteal phase. This is started by the wall of the Graffian follicle to rupture and cause a
flow of antral fluid that will carry the oocyte to the ovary's surface. The ruptured follicle
is then turned into a gland (corpus luteum). Which secretes estrogens and progesterone.
This is all triggered by and abrupt change in plasma LH levels. After ovulation the released
oocyte enters the uterine tube, where it will be either fertilized or discarded.
The uterine cycle operates in sync with the ovarian cycle and is divided into three phases. The
first phase in the menstrual phase. It is named the menstrual phase because in corresponds
with the shedding the the uterine lining or more commonly called menstruation. The corpus
luteum degenerates causing plasma estrogen and progesterone levels to decrease and in turn
causes menstruation. Blood vessels in the outer most layer of the endometrium constrict
and decrease blood flow to the tissues killing these tissues. After the tissues die they start
to separate from the underlying endometrail tissues. Eventually the dead tissue is shed.
This shedding of the tissues ruptures blood vessels and causes bleeding. Now we have the
proliferative phase. During this phase the uterus renews itself and prepares for pregnancy.
The endomitrial tissue that is left after menstruation begins to grow. The endometrial glands
grow and enlarge causing more blood vessels. The cervical canal has glands that secrete a
thin mucous that helps deposited sperm. Estrogen promotes uterine changes in this phase.
The last phase is the secretory phase. This is where the endometrium is transformed to
make it the best environment for implantation and subsequent housing and nourishment of
the developing embryo. By doing this the endometrium will do things like have an enriched
blood supply, begin to secrete fluids rich in glycogen, and even form a plug at the end of the
cervical canal so that microorganisms can not enter. These changes in the uterus are caused
by progesterone, due to the corpus luteum. At the end of the secretory phase the corpus
luteum degenerates, and progesterone levels fall. This will trigger menstruation.

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Sexual Reproduction

14.6 Sexual Reproduction

Sexual reproduction is a type of reproduction that results in increasing genetic diversity
of the offspring. In sexual reproduction, genes from two individuals are combined in random
ways with each new generation. Sex hormones released into the body by the endocrine
system signal the body when it is time to start puberty. The female and male reproductive
systems are the only systems so vastly different that each sex has their own different organs.
All other systems have "unisex" organs.
Reproduction is characterized by two processes. The first, meiosis, involves the halving of
the 46 of chromosomes. The second process, fertilization, leads the fusion of two gametes and
the restoration of the original number of chromosomes: 23 chromosomes from the paternal
side and 23 from the maternal side. During meiosis, the chromosomes of each pair usually
cross over to achieve genetic recombination.
Sexual reproduction cannot happen without the sexual organs called gonads. Both sexes
have gonads: in females, the gonads are the ovaries. The female gonads produce female
gametes (eggs); the male gonads produce male gametes (sperm). After an egg is fertilized
by the sperm, the fertilized egg is called the zygote.
The fertilization usually occurs in the oviducts, but can happen in the uterus itself. The zygote
then implants itself in the wall of the uterus, where it begins the processes of embryogenesis
and morphogenesis. The womens body carries out this process of reproduction for 40 weeks,
until delivery of the fetus from the uterus through the vagina (birth canal). Even after birth,
the female continues with the reproduction process by supplying the milk to nourish the
infant.

14.7 Infertility
Infertility is the inability to naturally conceive a child or the inability to carry a pregnancy
to term. There are many reasons why a couple may not be able to conceive without medical
assistance. Infertility affects approximately 15% of couples. Roughly 40% of cases involve a
male contribution or factor, 40% involve a female factor, and the remaining 20% involve
both sexes. Healthy couples in their mid-20s having regular sex have a one-in-four chance of
getting pregnant in any given month. This is called "Fecundity".

14.7.1 Primary vs. secondary

According to the American Society for Reproductive Medicine, infertility affects about 6.1
million people in the United States, equivalent to 10% of the reproductive age population.
Female infertility accounts for one third of infertility cases, male infertility for another
third, combined male and female infertility for another 15%, and the remainder of cases are
"unexplained.
"Secondary infertility" is difficulty conceiving after already having conceived and carried a
normal pregnancy. Apart from various medical conditions (e.g. hormonal), this may come as

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The Female Reproductive System

a result of age and stress felt to provide a sibling for their first child. Technically, secondary
infertility is not present if there has been a change of partners.

14.7.2 Factors of Infertility

Factors relating to female infertility are:
General factors
Diabetes mellitus,thyroid disorders,adrenal disease
Significant liver,kidney disease
Psychological factors
Hypothalamic-pituitary factors:
Kallmann syndrome
Hypothalamic dysfunction
Hyperprolactinemia
Hypopituitarism
Ovarian factors
Polycystic ovary syndrome
Anovulation
Diminished ovarian reserve
Luteal dysfunction
Premature menopause
Gonadal dysgenesis (Turner syndrome)
Ovarian neoplasm
Tubal/peritoneal factors
Endometriosis
Pelvic adhesions
Pelvic inflammatory disease(PID, usually due to chlamydia)
Tubal occlusion
Uterine factors
Uterine malformations
Uterine fibroids (leiomyoma)
Asherman's Syndrome
Cervical factors
Cervical stenosis
Antisperm antibodies
Insufficient cervical mucus (for the travel and survival of sperm)
Vaginal factors
Vaginismus
Vaginal obstruction
Genetic factors
Various intersexuality|intersexed conditions, such as androgen insensitivity syndrome

14.7.3 Combined Infertility

In some cases, both the man and woman may be infertile or sub-fertile, and the couple's
infertility arises from the combination of these factors. In other cases, the cause is suspected

398

Infertility
to be immunological or genetic; it may be that each partner is independently fertile but the
couple cannot conceive together without assistance.

14.7.4 Unexplained Infertility

In about 15% of cases of infertility, investigation will show no abnormalities. In these
cases abnormalities are likely to be present but not detected by current methods. Possible
problems could be that the egg is not released at the optimum time for fertilization, that
it may not enter the fallopian tube, sperm may not be able to reach the egg, fertilization
may fail to occur, transport of the zygote may be disturbed, or implantation fails. It is
increasingly recognized that egg quality is of critical importance.

14.7.5 Diagnosis of Infertility

Diagnosis of infertility begins with a medical history and physical exam. The healthcare
provider may order tests, including the following:

an endometrial biopsy, which tests the lining of the uterus

hormone testing, to measure levels of female hormones
laparoscopy, which allows the provider to see the pelvic organs
ovulation testing, which detects the release of an egg from the ovary
Pap smear, to check for signs of infection
pelvic exam, to look for abnormalities or infection
a postcoital test, which is done after sex to check for problems with secretions
special X-ray tests

14.7.6 Treatment
Fertility medication which stimulates the ovaries to "ripen" and release eggs (e.g.
Clomifene|clomifene citrate, which stimulates ovulation)
Surgery to restore potency of obstructed fallopian tubes (tuboplasty)
Donor insemination which involves the woman being artificially inseminated or artificially
inseminated with donor sperm.
In vitro fertilization (IVF) in which eggs are removed from the woman, fertilized and
then placed in the woman's uterus, bypassing the fallopian tubes. Variations on IVF
include:
Use of donor eggs and/or sperm in IVF. This happens when a couple's eggs and/or
sperm are unusable, or to avoid passing on a genetic disease.
Intracytoplasmic sperm injection (ICSI) in which a single sperm is injected directly
into an egg; the fertilized egg is then placed in the woman's uterus as in IVF.
Zygote intrafallopian transfer(ZIFT) in which eggs are removed from the woman,
fertilized and then placed in the woman's fallopian tubes rather than the uterus.
Gamete intrafallopian transfer(GIFT) in which eggs are removed from the woman,
and placed in one of the fallopian tubes, along with the man's sperm. This allows
fertilization to take place inside the woman's body.
Other assisted reproductive technology (ART):

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The Female Reproductive System

Assisted hatching
Fertility preservation
Freezing (cryopreservation) of sperm, eggs, & reproductive tissue
Frozen embryo transfer (FET)
Alternative and complimentary treatments
Acupuncture Recent controlled trials published in Fertility and Sterility have shown
acupuncture to increase the success rate of IVF by as much as 60%. Acupuncture
was also reported to be effective in the treatment of female anovular infertility, World
Health Organization, Acupuncture: Review and Analysis of Reports on Controlled
Trials (2002).
Diet and supplements
Healthy lifestyle

14.8 Types of Birth Control

Birth control is a regimen of one or more actions, devices, or medications followed in order
to deliberately prevent or reduce the likelihood of a woman becoming pregnant. Methods
and intentions typically termed birth control may be considered a pivotal ingredient to
family planning. Mechanisms which are intended to reduce the likelihood of the fertilization
of an ovum by a sperm may more specifically be referred to as contraception. Contraception
differs from abortion in that the former prevents fertilization, while the latter terminates
an already established pregnancy. Methods of birth control (e.g. the pill, IUDs, implants,
patches, injections, vaginal ring and some others) which may prevent the implantation of an
embryo if fertilization occurs are medically considered to be contraception. It is advised to
talk with a doctor before choosing a contraceptive. If you have genetics problems or blood
conditions, such as factor V leiden, certain contraceptives can be deadly.
Type

Procedure

Method

Abstinence

Refrain from
sexual intercourse
Intercourse
is avoided
for about an
8-day span every month in
middle of her
cycle, from
about five
days before
ovulation to
three days after ovulation.

No sperm in
vagina

Rhythm
Method

400

fertilization
is only possible during
8-day span
in middle of
menstrual cycle

Effectiveness
100%

Risks

70-80%

None

None

Types of Birth Control

Type

Procedure

Method

Withdrawal

The man
withdraws
his penis from
the vagina
at just the
right moment
before ejaculation.
Oviducts are
cut and tied

sperm are unable to enter

vagina if male
penis is removed at the
right time

Tubal Ligation (Vasectomy)

Hormonal
IUD (intrauterine
device)

Oral Contraceptive

Contraceptive
Implants

Flexible, plastic coil inserted by

physician

No eggs in
oviduct

Releases small
amounts of
estrogen. In
most cases,
stops egg
from developing and
being released,
but can also
operate by
killing a fertilized egg by
preventing its
implantation
Hormone med- Stops release
ication taken
of FSH and
daily
LH, but can
also operate
by killing a
fertilized egg
by preventing
its implantation
Tubes of pro- Stops release
gesterone imof FSH and
planted under LH, but can
the skin
also operate
by killing a
fertilized egg
by preventing
its implantation

Effectiveness
70-80%

Risks

Almost 99%

About 75%
Irreversible

About 99%

May cause
infections,
uterine perforation

More than
90%

Blood clots,
especially in
smokers

More than
90%

None known

None

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The Female Reproductive System

Type

Procedure

Method

Effectiveness
About 99%

Risks

Contraceptive
Injections

Injections of
hormones

Diaphragm

Latex cup inserted into

vagina to
cover cervix
before intercourse
Latex cup
held by suction over
cervix
Polyurethane
liner fitted
inside vagina

Stops release
of FSH and
LH, but can
also operate
by killing a
fertilized egg
by preventing
its implantation
Blocks entrance of
sperm into
uterus

With spermicide, about

90%

Latex or spermicide allergy

Delivers spermicide near

cervix

Almost 85%

UTI, latex or
spermicide
allergy

Blocks entrance of
sperm into
uterus and
prevents
STDs
Male Condom soft sheath,
Blocks enmade of latrance of
tex or animal sperm into
membrane, en- vagina and
closes penis,
prevents
trapping ejac- STD's
ulated sperm
Jellies, Cream, Spermicidal
Kills large
Foams
products innumber of
serted before
sperm
intercourse
Natural Fam- Keep record
Avoid sexual
ily Planning
of ovulation
intercourse
using various
near ovulation
methods
Douche
Vagina
Washes out
cleansed afsperm
ter intercourse

Almost 85%

None

90%

None

About 75%

UTI, allergy
to spermicides

About 70%

None known

Less than
70%

None known

Cervical Cap

Female Condom

402

Possible osteoporosis

Sexually Transmitted Diseases

Type

Procedure

Method

Plan B Pill

Pill taken after intercourse

Prevents release of egg,

fertilization of
egg, but can
also operate
by killing a
fertilized egg
by preventing
its implantation

Effectiveness
About 89%

Risks
Same as oral
contraceptive

14.9 Sexually Transmitted Diseases

Sexually transmitted diseases (STDs) are diseases or infections that have a significant
probability of transmission between humans by means of sexual contact: vaginal intercourse,
oral sex, and/or anal sex. Many STDs are (more easily) transmitted through the mucous
membranes of the penis, vulva, and (less often) the mouth. The visible membrane covering
the head of the penis is a mucous membrane, though, for those who are circumcised it is
usually dry and produces no mucus (similar to the lips of the mouth). Mucous membranes
differ from skin in that they allow certain pathogens (viruses or bacteria) into the body
(more easily).
The probability of transmitting infections through sex is far greater than by more casual
means of transmission, such as non-sexual contacttouching, sharing cutlery, and shaking
hands. Although mucous membranes exist in the mouth as well as in the genitals, many
STDs are more likely to be transmitted through oral sex than through deep kissing. Many
infections that are easily transmitted from the mouth to the genitals or from the genitals to
the mouth, are much harder to transmit from one mouth to another. With HIV, genital
fluids happen to contain a great deal more of the pathogen than saliva. Some infections
labeled as STDs can be transmitted by direct skin contact. Herpes simplex and HPV are
both examples. Depending on the STD, a person who has has the disease but has no
symptoms may or may not be able to spread the infection. For example, a person is much
more likely to spread herpes infection when blisters are present than when they are absent.
However, a person can spread HIV infection at any time, even if he/she has not developed
symptoms of AIDS.
All sexual behaviors that involve contact with the bodily fluids of another person should
be considered to hold some risk of transmission of sexually transmitted diseases. Most
attention has focused on controlling HIV, which causes AIDS, but each STD presents a
different situation.
As may be noted from the name, sexually transmitted diseases are transmitted from one
person to another by certain sexual activities rather than being actually caused by those
sexual activities. Bacteria, fungi, protozoa or viruses are still the causative agents. It is
not possible to catch any sexually transmitted disease from a sexual activity with a person

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The Female Reproductive System

who is not carrying a disease; conversely, a person who has an STD received it from contact
(sexual or otherwise) with someone who is infected.
Although the likelihood of transmitting diseases by sexual activities varies a great deal, in
general, all sexual activities between two (or more) people should be considered as being a
two-way route for the transmission of STDs (i.e. "giving" or "receiving" are both risky).

14.9.1 Prevention of Sexually Transmitted Diseases

Although healthcare professionals suggest that safer sex, such as the use of condoms, as
the most reliable way of decreasing the risk of contracting sexually transmitted diseases
during sexual activity, safer sex should by no means be considered an absolute safeguard.
The transfer of and exposure to bodily fluids, such as blood transfusions and other blood
products, sharing injection needles, needle-stick injuries (when medical staff are inadvertently
jabbed or pricked with needles during medical procedures), sharing tattoo needles, and
childbirth are all avenues of transmission. These means put certain groups, such as doctors,
haemophiliacs and drug users, particularly at risk.

14.9.2 Human Papillomavirus (HPV)

There are over 100 types of this virus which is often asymptomatic. Nearly 3 out of 4
Americans between ages 15 and 49 have been infected. It can be contracted through one
partner and remain dormant allowing it to be transmitted to another. Some types can cause
cervical cancer.
Genital HPV infection is a sexually transmitted disease that is caused by human papillomavirus. Human papillomavirus is the name of a group of viruses that includes more than
100 different strains. More than 30 of these are sexually transmitted and they can infect
the genital area of men and women. Approximately 20 million people are currently infected
with HPV and at least 50% of sexually active men and women will acquire HPV at some
point in their lives. By age 50 at least 80% of women will have acquired HPV and about 6.2
million Americans get a new HPV infection each year. Most people who have HPV don't
know that they are infected. The virus lives in the skin or mucous membranes and usually
causes no symptoms. Commonly some people get visible genital warts or have pre-cancerous
changes in the cervix, vulva, anus, or penis. Very rarely, HPV results in anal or genital
cancers. Genital warts usually appear soft, moist, pink, or flesh colored swellings. They can
be raised, flat, single, or multiple, small or large and sometimes cauliflower shaped. Warts
may not appear for weeks or months or not at all and the only way to diagnose them is
by visible inspection. Most women are diagnosed with HPV on the basis of abnormal pap
tests and there are no tests available for men. There is no cure for HPV. The surest way
to eliminate risk for HPV is to refrain from any genital contact with another individual.
For those who choose to be sexually active, a long term monogamous relationship with an
uninfected partner is the strategy most likely to prevent future HPV infections.The next
best way to help reduce risk is using a condom but the effectiveness is unknown.
What is the connection between HPV and cervical cancer? All types of HPV cause
mild pap test abnormalities which do not have serious consequences. Approximately 10 of
the 30 identified HPV types can lead to development of cervical cancer. Research as shown

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Diseases and Disorders of the Female Reproductive System

that for most women, 90% cervical HPV infection becomes undetectable within two years.
Although only a small proportion of women have persistent infection, persistent infection
with the high risk types of HPV is the main risk factor for cervical cancer.
A pap test can detect pre-cancerous and cancerous cells on the cervix. Regular pap testing
and careful medical follow up, with treatment if necessary, can help ensure that pre-cancerous
changes in the cervix caused by HPV infection do not develop into life threatening cervical
cancer. The pap test used in the U.S. cervical cancer screening programs is responsible for
greatly reducing deaths from cervical cancer.

14.10 Diseases and Disorders of the Female Reproductive

System
Women are commonly dealing with many different diseases and disorders that pertain to
the reproductive system. Here are some of the most common:
1. Vulvovaginitis (pronounced:vul-vo-vah-juh-ni-tus) is an inflammation of the vulva
and vagina. It may be caused by irritating substances such as laundry soap, bubble
baths or poor hygiene such as wiping from back to front. Symptoms include redness
and itching in these areas and sometimes vaginal discharge. It can also be caused by
an overgrowth of candida, a fungus normally present in the vagina.
2. Nonmenstrual vaginal bleeding is most commonly due to the presence of a foreign
body in the vagina. It may also be due to urethral prolapse, a condition in which the
mucous membranes of the urethra protrude into the vagina and forms a tiny, donut
shaped mass of tissue that bleeds easily. It can also be due to a straddle injury or
vaginal trauma from sexual abuse.
3. Ectopic Pregnancy occurs when a fertilized egg or zygote doesn't travel into the
uterus, but instead grows rapidly in the fallopian tube. Women with this condition
can develop severe abdominal pain and should see a doctor because surgery may be
necessary.
4. Ovarian tumors,although rare, can occur. Women with ovarian tumors may have
abdominal pain and masses that can be felt in the abdomen. Surgery may be needed
to remove the tumor.
5. Ovarian cysts are noncancerous sacs filled with fluid or semi-solid material. Although
they are common and generally harmless, they can become a problem if they grow
very large. Large cysts may push on surrounding organs, causing abdominal pain. In
most cases, cysts will pass or disappear on their own and treatment is not necessary.
If the cysts are painful and occur frequently, a doctor may prescribe birth control pills
to alter their growth and occurrences. Surgery is also an option if they need to be
removed.
6. Polycystic ovary syndrome is a hormone disorder in which too many hormones
are produced by the ovaries. This condition causes the ovaries to become enlarged
and develop many fluid filled sacs or cysts. It often first appears during the teen years.
Depending on the type and the severity of the condition, it may be treated with drugs
to regulate hormone balance and menstruation.
7. Trichomonas vaginalis inflammatory condition of the vagina usually a bacterial
infection also called vaginosis.

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The Female Reproductive System

8. Dysmenorrhea is painful periods.
9. Menorrhagia is when a woman has very heavy periods with excess bleeding.
10. Oligomenorrhea is when a woman misses or has infrequent periods, even though she
has been menstruating for a while and is not pregnant.
11. Amenorrhea is when a girl has not started her period by the time she is 16 years
old or 3 years after puberty has started, has not developed signs of puberty by 14, or
has had normal periods but has stopped menstruating for some reasons other than
pregnancy.
12. Toxic shock syndrome is caused by toxins released into the body during a type of
bacterial infection that is more likely to develop if a tampon is left in too long. It can
produce high fever, diarrhea, vomiting, and shock.
13. Candidasis symptoms of yeast infections include itching, burning and discharge.
Yeast organisms are always present in all people, but are usually prevented from
"overgrowth" (uncontrolled multiplication resulting in symptoms) by naturally occurring
microorganisms.
At least three quarters of all women will experience candidiasis at some point in their lives.
The Candida albicans organism is found in the vaginas of almost all women and normally
causes no problems. However, when it gets out of balance with the other "normal flora,"
such as lactobacilli (which can also be harmed by using douches), an overgrowth of yeast
can result in noticeable symptoms. Pregnancy, the use of oral contraceptives, engaging in
vaginal sex after anal sex in an unhygienic manner, and using lubricants containing glycerin
have been found to be causally related to yeast infections. Diabetes mellitus and the use
of antibiotics are also linked to an increased incidence of yeast infections. Candidiasis can
be sexually transmitted between partners. Diet has been found to be the cause in some
animals. Hormone Replacement Therapy and Infertility Treatment may be factors.
There are also cancer's of the female reproductive system, such as:
1.
2.
3.
4.

Cervical cancer
Ovarian cancer
Uterine cancer
Breast cancer

Endometriosis
Endometriosis is the most common gynecological diseases, affecting more than 5.5 million
women in North America alone! The two most common symptoms are pain and infertility.
In this disease a specialized type of tissue that normally lines the inside of the uterus,(the
endometrium) becomes implanted outside the uterus, most commonly on the fallopian tubes,
ovaries, or the tissue lining the pelvis. During the menstrual cycle, hormones signal the
lining of the uterus to thicken to prepare for possible pregnancy. If a pregnancy doesn't
occur, the hormone levels decrease, causing the thickened lining to shed.
When endometrial tissue is located in other parts it continues to act in it's normal way: It
thickens, breaks down and bleeds each month as the hormone levels rise and fall. However,
because there's nowhere for the blood from this mislocated tissue to exit the body, it becomes
trapped and surrounding tissue becomes irritated. Trapped blood may lead to growth of
cysts. Cysts in turn may form scar tissue and adhesions. This causes pain in the area of
the misplaced tissue, usually the pelvis. Endometriosis can cause fertility problems. In fact,
scars and adhesions on the ovaries or fallopian tubes can prevent pregnancy. Endometriosis

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Check Your Understanding

can be mild, moderate or severe and tends to get worse over time without treatment. The
most common symptoms are:
1. Painful periods Pelvic pain and severe cramping, intense back pain and abdominal
pain.
2. Pain at other times Women may experience pelvic pain during ovulation, sharp
deep pain in pelvis during intercourse, or pain during bowel movements or urination.
3. Excessive bleeding Heavy periods or bleeding between periods.
4. Infertility Approximately 30-40% of women
The cause of endometriosis remains mysterious. Scientists are studying the roles that
hormones and the immune system play in this condition. One theory holds that menstrual
blood containing endometrial cells flows back through the fallopian tubes, takes root and
grows. Another hypothesis proposes that the bloodstream carries endometrial cells to other
sites in the body. Still another theory speculates that a predisposition toward endometriosis
may be carried in the genes of certain families.
Other researchers believe that certain cells present within the abdomen in some women
retain their ability to specialize into endometrial cells. These same cells were responsible for
the growth of the woman's reproductive organs when she was an embryo. It is believed that
genetic or environmental influences in later life allow these cells to give rise to endometrial
tissue outside the uterus.
Experts estimate that up to one in ten American women of childbearing age have endometriosis. There is some thinking that previous damage to cells that line the pelvis can lead to
endometriosis. There are several ways to diagnose endometriosis:
1.
2.
3.
4.

Pelvic exam
Ultrasound
Laparoscopy Usually used, most correct diagnosis
Blood test

Endometriosis can be treated with:

1. Pain medication
2. Hormone therapy
a) Oral contraceptives
b) Gonadotropin-releasing hormone(Gn-Rh)agonists and antagonists
c) Danazol(Danocrine)
d) Medroxyprogesterone(Depo-Provera)
3. Conservative surgery which removes endometrial growths.
4. Hysterectomy

14.11 Check Your Understanding

Answers for these questions can be found here1
1. In homology, the ___________in the female is equal to the penis in the male
1

http://en.wikibooks.org/wiki/Human_Physiology/Appendix_1:_answers_to_review_
questions#The_female_reproductive_system

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The Female Reproductive System

A) labia majora
B) clitoral hood
C) clitoris
D) labia minora
E) none of the above
2. This contains some of the strongest muscles in the human body
A) uterus
B) clitoris
C) cervix
D) labia majora
3. This protects the vaginal and urethral openings
A) labia majora
B) labia minora
C) clitoris
D) urethra
4. Sally has noticed that her cervical mucus has changed and now resembles egg whitesfrom this Sally could assume
A) her period will begin soon
B) nothing, this is a normal occurrence
C) she has a yeast infection
D) she is ovulating
5. Debbie recently went to the OBGYN and was diagnosed with PCOD (polycystic ovary
syndrome) because of this she has
A) nothing, its normal in women
B) antisperm antibodies
C) an overproduction of LH
D) leaking of milk from her mammary glands
E) problems becoming pregnant
6. Angie went to the doctor because she has had pain in her leg recently- this could be
caused by
A) ovulation pain
B) her period that will be starting tomorrow
C) premenstrual syndrome

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Check Your Understanding

D) a blood clot resulting from her birth control pill
7. Sue recently started her period and has noticed that they are very heavy and painful,
and that they are inconsistent in their timing. One explanation could be
A) endometriosis
B) ovarian cancer
C) candidasis
D) toxic shock syndrome
E) amenorrhea
8. Mary is getting married and is not ready to become a mother- she chooses this birth
control because of its high effectiveness
A) natural family planning
B) a diaphragm
C) contraceptive injections
D) a spermicide foam
9. The release of LH in woman causes
A) menstration
B) ovulation
C) increase of endometrial lining
D) decrease of endometrial lining
E) nothing LH only does something in the male reproductive system
10. When the ovaries stop producing estrogen, this occurs
A) ovulation
B) implantation
C) premenstrual syndrome
D) menopause
11. Infertility affects what percentage of couples?
A) 5%
B) 10%
C) 15%
D) 20%
12. What is the only 100% effective form of birth control?
A) Tubal ligation
B) IUD

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The Female Reproductive System

C) Natural family planning
D) Abstinence

14.12 Glossary
Adhesions: Abnormal tissue that binds organs together
Alveoli: Basic components of the mammary glands; lined with milk-secreting epithelial
cells
Birth Control: regimen of one or more actions, devices, or medications followed in order
to deliberately prevent or reduce the likelihood of a woman becoming pregnant
Cervical Mucus: Mucus secreted by the cervix, near ovulation it helps to lower the acidity
of the vagina
Cervix: Lower, narrow portion of the uterus where it joins with the top of the vagina
Clitoris: Small body of spongy tissue that functions solely for sexual pleasure
Chromosomes: Structures in the nucleus that contain the genes for genetic expression
Ectocervix: Portion of the cervix projecting into vagina
Endocervical Canal: Passageway between the external os and the uterine cavity
Endometrium: The inner lining of the uterus
Fallopian Tubes: Located at the upper end of the vagina, passage way for the egg from
the ovary
Factor V Leiden: This is the name given to a variant of human factor V that causes
a hypercoagulability disorder. In this disorder the Leiden variant of factor V, cannot
be inactivated by activated protein C. Factor V Leiden is the most common hereditary
hypercoagulability disorder amongst Eurasians. It is named after the city Leiden (The
Netherlands), where it was first identified in 1994 by Prof R. Bertina et al.
Gamete: A haploid sex cell; either an egg cell or a sperm cell
Gene: That portion of the DNA of a chromosome containing the information needed to
synthesize a particular protein molecule
Gonad: A reproductive organ, testis or ovary that produces gametes and sex hormones
Hormone: A chemical substance produced in an endocrine gland and secreted into the
bloodstream that acts on target cells to produce a specific effect
Hymen: Thin fold of mucous membrane that separates the lumen of the vagina from the
urethral sinus
Infertility: Inability to naturally conceive a child or the inability to carry a pregnancy to
term
Labia Majora: Outer "lips" of the vulva, made of loose connective tissue and adipose tissue
with some smooth muscle

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Glossary
Labia Minora: Inner lips of the vulva, folds and protects the vagina, urethra and clitoris
Mammary Glands: Organs that produce milk for the sustenance of a baby
Meiosis: A specialized type of cell division by which gametes, or haploid sex cells, are
formed
Menarche: The first menstrual discharge; occurs normally between the ages of 9 and 17
Menopause: The period marked by the cessation of menstrual periods in the human female
Menstrual Cycle: The rhythmic female reproductive cycle characterized by physical
changes in the uterine lining
Menstruation: The discharge of blood and tissue from the uterus at the end of menstrual
cycle
Mittelschmerz: Pain near the lower abdomen site at the time of ovulation; German for
ovulation pain
Mons Veneris: soft mound at the front of the vulva (fatty tissue covering the pubic bone)
Ovarian Cycle: Last phase of the reproductive cycle; if no implantation occurs, causes the
breakdown of the endometrial lining and causes menstruation
Ovulation: The rupture of an ovarian follicle with the release of an ovum
Perineum: External region between the scrotum and the anus in a male or between the
vulva and anus in a female
Premenstrual Syndrome (PMS): Time leading up to menstruation; includes both
physical and emotional symptoms: acne, bloating, fatigue, backaches, sore breasts, headaches,
constipation, diarrhea, food cravings, depression, irritability, difficulty concentrating or
handling stress
Puberty: The period of development in which the reproductive organs become functional
and the secondary sex characteristics are expressed
Reproduction: Process by which an organism continues its species
Sexually transmitted diseases (STDs): diseases or infections that have a significant
probability of transmission between humans by means of sexual contact
Urethra: Located below the clitoris, used for the passage of urine
Uterine Cycle: First part of the reproductive cycle; the time when the endrometrial lining
builds up and follicles develop
Uterus: Major reproductive organ, receives fertilized eggs which become implanted in the
lining, the lining (endometrium) provides nourishment to developing fetus; contains some of
the strongest muscles in the female body and is able to stretch during fetus development
Vagina: Muscular, hollow tube that extends from the vaginal opening to the cervix
Vulva: External female genitals, includes labia majora, labia minora, mons pubis, clitoris,
meatus, vaginal vestibule, vestibule bulbs and vestibular glands

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The Female Reproductive System

14.13 References
Essentials of Anatomy and Physiology. Fourth Edition. Valerie C. Scanlon and Tina
Sanders.
Human Anatomy. Sixth Edition. Van De Graaff.
Wikibook: Sexual Health2
http://www.fda.gov/cder/drug/infopage/planBQandAhtm
http://www.goplanb.com/Forconsumers
American Social Health Association;ashastd.org
http://www.cdc.gov
http://www.mayoclinic.com

412

http://en.wikibooks.org/wiki/Sexual%20Health

15 Pregnancy and Birth

15.1 Introduction
In this chapter we will discuss the topics covering pregnancy, from conception to birth. The
chapter will cover fertilization, implantation of the zygote, to becoming a fetus, the three
trimesters, and the progressive development of the fetus through the weeks of pregnancy. It
will cover the topic of birth and different birthing methods.

15.2 Fertilization

Figure 129

A sperm fertilizing an ovum

Fertilization is the joining of a sperm and an egg. A sperm is a male gamete that is released
into the vagina of a female during intercourse. In order for fertilization to occur there must

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Pregnancy and Birth

be a mature ovum present. Every month one of the ovaries releases an egg which will meet
one of the A 4 million sperm the male ejaculates into the vagina. The sperm swim through
the cervix and into the uterus which lead to the fallopian tubes. This is where fertilization
is most likely to take place. The high amount of sperm in the ejaculate is needed because
only around 100 survive to enter reach the fertilization site. In order to penetrate the egg
the sperm must first break through 2 barriers surrounding the ovum. The acrosome of
sperm comes in contact with the corona radiata and releases digestive enzymes that break
down a gelatinous layer around the egg called, the zona pellucida. Once a sperm reaches
the plasma membrane of the egg it sets off a reaction that spreads across the membrane
of the egg preventing other sperm from breaking through the egg membrane. Once the
sperm reaches the inside of the egg it sheds its tail and the two nuclei fuse and now the 23
chromosomes from the egg and the 23 chromosomes of the sperm join and they become a
zygote. Chromosomes contain all the information needed to determine the genetic structure
of the new baby. Normally all human beings have two chromosomes that determine sex:
A combination of X and Y makes a male or a combination of X and X makes a female.
All ovum have X sex chromosomes where as sperm have both X or Y sex chromosomes.
Therefore, the male gametes determine the sex of the baby.

Figure 130

An 8-cell embryo in the process of cleavage.

15.3 Pre-embryonic Period

After fertilization, the zygote begins a process of dividing by mitosis in a process called
cleavage. It divides until it reaches 16 cells. It is now referred to as a morula. As the morula
floats freely within the uterus, it starts to bring nutrients into the cells. The morula fills
with fluid and the cells inside start to form two separate groups. At this stage it is now
a blastocyst. The inner layer of cells is called the embryoblast, and will become the fetus.

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Pre-embryonic Period
The outer layer is called a trophoblast which will develop into part of the placenta. At this
point the zona pellucida is disintegrating. The trophoblast contains specialized cells that
become extensions, like fingers, that grow into the endometrium once in contact with the
well thickened endometrium.

15.3.1 Implantation
The blastocyst preserves itself by secreting a hormone that indirectly stops menstruation.
The trophoblast cells secrete hCG hormones that help maintain the corpus luteum that
would normally regress. In turn, the corpus luteum continues to secrete progesterone, which
maintains the endometrium of the uterus in the secretory phase. This helps the blastocyst
to continue to grow and stay embedded within the endometrium. The fetal life support
system and the placenta begin to form, and eventually the placenta will take over the job of
producing progesterone.
Gastrulation and Formation
The embryoblast within the blastocyst forms 3 primary germs layers: ectoderm, mesoderm,
and endoderm.
Ectoderm
This forms the nervous tissue and the epithelium covering the outer body surface. Epidermis
of skin, including hair and nails, glands of skin, linings of oral cavity, nasal cavity, anal
canal, vagina, brain, spinal cord, sensory organs, lens of eye and epithelium of conjunctiva (a
membrane that covers the sclera and lines the inside of the eyelids), pituitary gland, adrenal
medulla, and enamel of teeth.
Mesoderm
This forms all of the muscle tissue and the connective tissue of the body, as well as the
kidneys and the epithelium of the serous membranes and blood vessels. All muscle tissue
(skeletal, smooth, cardiac), all connective tissue (fibrous connective tissue, bone, blood,
cartilage), dentin of teeth, adrenal cortex, kidneys and ureters, internal reproductive viscera,
epithelium lining vessels, joint cavities, and the serous body cavities.
Endoderm
Forms the lining epithelium and glands of the visceral body systems. Lining epithelium and
glands of digestive, respiratory, and parts of urogenital systems, thyroid and parathyroid
glands, and thymus.

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15.4 Formation of Placenta

As changes to the endometrium occur, cellular growth and the accumulation of glycogen
cause fetal and maternal tissue to come together. This formation makes the functional
unit called the placenta. The placenta does not mix blood between mother and fetus, but
allows nutrients and waste products to diffuse between the two blood systems. The placenta
provides protection by filtering out many harmful substances that the mother comes in
contact with. Unfortunately the placenta cannot protect against some teratogens including
but not limited to:

Thalidomide
Heroin
Cocaine
Aspirin
Alcohol
Chemicals in cigarette smoke
Propecia, also known as Finasteride, which can cause birth defects simply by a woman
handeling a broken pill during pregnancy.

15.5 Amniotic Fluid

Attached to placenta is the membranous sac which surrounds and protects the embryo. This
sac is called the amnion. It grows and begins to fill, mainly with water, around two weeks
after fertilization. This liquid is called Amniotic fluid, it allows the fetus to move freely,
without the walls of the uterus being too tight against its body. Buoyancy is also provided
here for comfort. After a further 10 weeks the liquid contains proteins, carbohydrates, lipids
and phospholipids, urea and electrolytes, all which aid in the growth of the fetus. In the
late stages of gestation much of the amniotic fluid consists of fetal urine. The fetus swallows
the fluid and then voids it to prepare its digestive organs for use after birth. The fetus also
"breathes" the fluid to aid in lung growth and development.

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Amniotic Fluid

Figure 131 A small part of the placenta is shown at the bottom, while the fluid-filled
amnion surrounds it
Not enough amniontic fluid, or oligohydramnios, can be a concern during pregnancy. Oligohydramnios can be caused by infection, kidney dysfunction or malformation (since much
of the late amniotic fluid volume is urine), procedures such as chorionic villus sampling
(CVS), and preterm, premature rupture of membranes (PPROM). One possible outcome
of oligohydramnios can cause is underdeveloped, or hypoplastic, lungs. This condition is
potentially fatal and the baby can die shortly after birth. Babies with too little amniotic
fluid can also develop contractures of the limbs, including clubbing of the feet and hands.
As with too little fluid, too much fluid or polyhydramnios, can be a cause or an indicator of
problems for the mother and baby. Polyhydramnios is a predisposing risk factor for cord

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Pregnancy and Birth

prolapse and is sometimes a side effect of a macrosomic pregnancy. In both cases, however,
the majority of pregnancies proceed normally and the baby is born healthy.
Preterm, premature rupture of membranes (PPROM) is a condition where the amniotic sac
leaks fluid before 38 weeks of gestation. This can be caused by a bacterial infection or by a
defect in the structure of the amniotic sac, uterus, or cervix. In some cases the leak can
spontaneously heal, but in most cases of PPROM, labor begins within 48 hours of membrane
rupture. When this occurs, it is necessary that the mother receive treatment immediately to
postpone labor if the fetus is not viable, for as long as is safe, and for antibiotic treatments
to avoid possible infection in the mother and baby. If rupture occures too early in pregnancy
little can be done to save the fetus.
A very rare and most often fatal obstetric complication is an amniotic fluid embolism, or
leakage of amniotic fluid into the mothers vascular systems causing an allergic reation. This
allergic reaction results in cardiorespiratory (heart and lung) collapse, developing into a
condition known as disseminated intravascular coagulation in which the mothers blood looses
it's ability to clot.
Amniotic band syndrome, or ABS, occurs when the inner fetal membrane (amnion) ruptures
without injury to the outer membrane (chorion). Fibrous bands from the ruptured amnion
float in the amniotic fluid and can entangle the fetus, reducing blood supply and causing
congenital limb abnormalities dysmelia. In some cases a complete "natural" amputation of
a digit(s) or limb may occur before birth or the digit(s) or limbs may be necrotic (dead)
requiring surgical removal.

15.6 Endocrine Function of the Placenta

There are pituitary like hormones and steroid hormones secreted from the placenta. The
pituitary like hormones are hCG and hCS. HCG is similar to LH and helps maintain the
mothers corpus luteum. HCS is like prolactin and growth hormone and help aid in increasing
fat breakdown that spares the use of glucose from the mothers tissues. This effect leaves
more glucose available to the placenta and the fetus for necessary growth. The steroid
hormones are progesterone and estrogen. Progesterone helps maintain the endrometrium and
supports the growth of mammary glands. Estrogen also helps maintain the endrometrium
and growth of mammary glands as well as inhibits prolactin secretion.

15.7 Developing Baby

The womb is expanding, the baby is growing and taking all the nourishment from the mother.
What once started as a microscopic two-celled egg, will be formed into a baby in just 12
weeks. The baby develops from conception to term, in a month-to-month progress.

15.7.1 Overview of Developmental Milestones

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Developing Baby
WEEK

CHANGES IN MOTHER

1 week

Ovulation Occurs

2 weeks

Symptoms of early pregnancy

(nausea, breast swelling and tenderness, fatigue); blood pregnancy tests may show positive
First period missed; urine pregnancy test may show positive;
early pregnancy symptoms continue

3 weeks

4 weeks

5 weeks

Uterus is the size of a hen's egg;

mother may need to urinate
frequently

6 weeks

Uterus is the size of an orange

8 weeks

Uterus can be felt above the

pubic bone

12 weeks

Uterus is the size of a grapefruit

16 weeks

Fetal movement can be felt

20-22 weeks

Uterus reaches up to the level

of umbilicus and pregnancy is
obvious

DEVELOPMENT OF
BABY
Pre-embryonic Development
Fertilization occurs, cell division
begins and continues, chorion
appears
Embryonic Development
Implantation occurs; amnion
and yolk sac appear; embryo has
tissue; placenta begins to form
Nervous system begins to develop; allantois and blood vessels
are present and placenta is well
formed
Limb buds form; heart is beating; nervous system further develops; embryo has tail; other
systems are forming
Embryo is curved, head is large,
limb buds are showing division,
nose, ears and eyes are noticeable
Fingers and toes are present and
skeleton is cartilaginous
Fetus begins to look human;
limbs are developing and major
organs forming; facial features
are becoming refined
Fetal Development
Head grows faster than the
rest of the body; facial features
are apparent, but there is no
layer of fat yet and the skin is
translucent; gender can be distinguished via ultrasound; fingernails appear
Fine hair (lanugo) grows over
the body; fetus resembles a tiny
human being; skeleton is visible
Vernix caseosa, the protective
fatty coating, begins to be deposited; heartbeat can be heard

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Pregnancy and Birth

WEEK

CHANGES IN MOTHER

24 weeks

Doctor can tell where baby's

head, back and limbs are;
breasts have enlarged and
nipples and areola are darker,
colostrum is produced

32 weeks

Uterus reaches halfway between

umbilicus and rib cage

36 weeks

Weight gain is averaging about

a pound a week; standing and
walking are becoming very difficult because the center of gravity is thrown forward
Uterus is up to the rib cage,
causing shortness of breath and
heartburn; sleeping is very difficult

40 weeks

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DEVELOPMENT OF
BABY
Fully formed but still thin; much
larger and very active, all major
organs are working, the lungs
and digestive system need more
time to develop; body is covered
in fine hair called lanugo
Most babies are in a head down
position in the womb; head is
more in proportion to the body;
eyes are open; babies born at
this stage have a good chance of
living
Body hair begins to disappear,
fat is being deposited

Not much room to move in the

womb; fully mature, baby moves
less, and the surrounding fluid
reduces and the womb expands
its limits

Embryonic Development at Specific Stages

15.8 Embryonic Development at Specific Stages

15.8.1 First trimester

Figure 132 An embryo this tiny shows very distinct anatomic

features, including tail, limb buds, heart (which actually protrudes
from the chest), eye cups, cornea/lens, brain, and prominent
segmentation into somites. The gestational sac is surrounded by a
myriad of chorionic villi resembling elongate party balloons. This
embryo is about five weeks old (or seven weeks in the biologically
misleading but eminently practical dating system used in obstetrics).
4 Weeks
There are only the beginnings of facial features. All the major organs are starting to
form. Gill-like folds that develop into facial features, beginnings of the spinal cord, skin
is translucent, and rudimentary (basic; minimal) heart develops.
6 Weeks
The length from crown to rump is about the size of a finger tip,
all the major organs will have formed.

3
4

". The beginnings of

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Pregnancy and Birth

The embryo floats in a fluid filled bubble that will develop into the amniotic sac. The sac
is covered by a protective layer of cells, called chorion. The yolk sac supplies the embryo
with all its nutrients until the placenta is fully developed and takes over at around the
twelfth week. During the first 12 weeks, the embryo will develop features and major
organs of a human being. The embryo is susceptible to harmful environmental influences.
This is a vital time for the embryo to develop healthily; taking supplements of folic acid,
avoiding certain foods, and eliminating alcohol, cigarettes, and any unnecessary drugs or
medicines.
9 Weeks
The length from crown to rump approximately 1 1/4". The facial features are becoming
more distinct, and the tail has disappeared. The muscles are also developing. Eyes
are formed but eyelids are still closed over them. Arms now bend at the elbow and
rudimentary hands and fingers develop. Knees will have formed and developing feet with
distinct toes.
Heart- is now a four-chambered and fully formed organ; it beats about 180 times per
minute.
Brain and nervous system- is four times the size it was at 6 weeks. Special glial cells are
being formed within the neural tube; they allow nerve cells to be joined so that messages
can be transmitted from the brain to the body.
Digestive system- the mouth, intestine, and stomach are developing very rapidly, but do
not function yet.
The fetal life-support system- the placental tissue that initially surrounds the fetus and
the amniotic sac is becoming concentrated in one circular area on the womb wall to form
the placenta.

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Embryonic Development at Specific Stages

Figure 133

Sonogram of a fetus at 14 weeks (Profile)

12 Weeks
At twelve weeks the fetus looks like a tiny human. It is about 2 1/2" long and weighs 1/2
oz. Arms and legs are now beginning to move. Skin is red and translucent. Fingers and
toes are more defined, and nails are starting to grow.
Heart is complete and working, pumping blood to all parts of the body. Digestive system
has formed and is linked to the mouth and intestines. Sexual organs have formed inside
the body, but cannot yet establish the sex of the baby.

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Pregnancy and Birth

15.8.2 Second Trimester

20 Weeks
By 20 weeks the fetus will be about 6 1/3" long and weighs 12 oz. Movements are for
more coordinated. The sexual organs are well developed and are usually visible on ultra
sound.
The fetus is growing very quickly. At this stage, the mother should feel the movements
of the fetus. Movements are more noticeable as the fetus's leg bones achieve their final
relative proportions in a process called quickening. Quickening is the process of muscles
contracting that cause movement at the fetus's synovial joints. The joint movement
enhances the nutrition of the articular cartilage and prevents the fusion of connective
tissues within the joint. It also promotes bone hardening.
From now on, the fully developed placenta will provide all the fetus' needs until birth;
oxygen, nutrients and protective antibodies.

Figure 134

424

Fetus at 29 weeks gestation in 3D

Embryonic Development at Specific Stages

15.8.3 Third Trimester

29 Weeks
By 29 weeks the baby is about 10" long and weighs about 2 lbs. 7 oz.
The brain grows much larger, and fatty protective sheath covers the nerve fibers; this
important development allows brain impulses to travel faster, enhancing the ability to
learn. The lungs have developed most of their airways and air sacs. The placenta is quite
selective in what it allows to pass from the mother to the baby's blood, stopping some
harmful substances, such as certain drugs, from crossing over.
40 Weeks
The baby is now ready to be born. When the head of the baby moves down from high in
the mother's abdomen and settles deeper into her pelvis in preparation for birth, it is
called engagement. This can happen any time between 36 weeks and labor.
In the last four weeks of pregnancy the baby puts on a lot of weight and develops a thick
layer of fat. All organs are completely formed and functioning.

15.8.4 Umbilical Cord

This is the life support for a growing embryo. The umbilical cord stretches between the
placenta and the fetus. This cord contains the umbilical arteries and vein. The umbilical
cord forms by week 5 of conception. The average cord is close to 22 inches long and may
have the appearance of a coil. The umbilical cord is very rich in stem cells and is often used
for parents who choose to store their stem cells in a blood bank or donate it to a blood bank.
These stem cells can be used to treat over 45 disorders and is an alternative from extracting
the stem cells from a donor.

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Pregnancy and Birth

Figure 135 Human placenta shown a few minutes after birth. The side shown
faces the baby with the umbilical cord top right. The unseen side connects to
the uterine wall. The white fringe surrounding the bottom is the remnants of
the amniotic sac. You can see the differences in the umbilical vein and arteries.
Umbilical Arteries
The exchange of gases, nutrients and oxygen takes place between the maternal blood and
fetal blood. There are 2 main arteries.
Umbilical Vein
Vein that carries nutrients and oxygen away from the placenta to the growing fetus. It also
carries oxygen and nutrient rich blood. There is only 1 main vein.
Fetus doesn't use its lungs for gas exchange, only a small amount of blood is pumped to
fetal lungs in order to support their development.
Umbilical Abnormalities
Single Umbilical Artery
One artery instead of two will result in chromosomal abnormalities. Some of these defects
include poor fetal growth, preterm delivery, and still births. This can be detected by a
routine ultrasound. If an ultrasound is done and no other complications or abnormalities
are detected, the baby will usually be born healthy.
Umbilical Prolapse

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This condition usually happens when a cord is too long. The baby may be born prematurely
or will be breech.
Umbilical Nuchal Loops
This condition happens when the umbilical cord is wrapped around the baby's head at least
one or more times. This can be detected when a baby is in stress or by a simple ultrasound.
In most cases the mother will have a cesarean delivery. In other cases the cord may be
wrapped around the hands or feet.
Vasa Previa
This occurs in one in every 3,000 births, which can become life threatening for the unborn
baby. This complication happens when the umbilical cord inserts abnormally in the fetal
membranes of the placenta, which appears abnormally shaped or positioned. Major risks
include unprotected fetal blood vessels cross the cervix, oftentimes rupturing the membranes.
Also, lack of blood pressure due from pressure, causes the loss of oxygen to the baby. Women
who will be at risk for this would be those who already have experienced placenta previa or
have used in vitro fertilization.
Umbilical Cord Knots
About 1% of babies are born with one or more knots in their umbilical cord. Some knots
happen during labor; others happen from moving around in the womb. Most knots occur
when the umbilical cord is too long. In some cases the knots can become tight, cutting off
the oxygen supply to the baby. Cord knots result in miscarriages and stillbirth in 5% and
10% of most cases. Most will require a cesarean delivery.
Umbilical Clotting
This is more common with genetic defects, such as Factor V Leiden. This complication will
prevent blood flow to and from the baby and many times will cause the placenta to also clot
and die. If this is not caught early enough, the baby will die of starvation in the womb. A
simple ultrasound can determine if there are problems with the blood flow.

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15.9 Pregnancy from the mother's perspective

Figure 136

Growth of the uterus in a pregnant female.

An initial sign of pregnancy is amenorreah, or the absence of menstruation. Menses cease

because the blastocyte begins the release of hCG or human chorionic gonadotropin. Most
pregnancy tests are specifically designed to recognize the presence of hCG, and hCG levels
can be tested through the mothers blood to learn whether or not a pregnancy is progressing
normally.
Human pregnancy lasts approximately 40 weeks from the time of the last menstrual cycle
to childbirth (38 weeks from fertilization). The medical term for a pregnant woman is

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genetalian, just as the medical term for the potential baby is embryo (early weeks) and then
fetus (until birth). A woman who is pregnant for the first time is known as a primigravida
or gravida 1: a woman who has never been pregnant is known as a gravida 0; similarly, the
terms para 0, para 1 and so on are used for the number of times a woman has given birth.
In many societies' medical and legal definitions, human pregnancy is somewhat arbitrarily
divided into three trimester periods, as a means to simplify reference to the different stages
of fetal development. The first trimester period carries the highest risk of miscarriage
(spontaneous death of embryo or fetus). During the second trimester the development of the
fetus can start to be monitored and diagnosed. The third trimester marks the beginning of
viability, which means the fetus might survive if an early birth occurs.

15.9.1 Changing Body

Figure 137

As soon as a woman becomes pregnant, her body begins to change so that it can support
both herself and the unborn baby. All of the body functions start to work much harder.
The heart has to pump more blood around the body, in particular to the womb, placenta,
and the fetus. As well as physical demands, pregnancy also causes a range of emotional
reactions.
The first trimester, the first twelve weeks, little is visible.
The second trimester, 13-27 Weeks, the waistline is rapidly growing, the abdomen becomes
noticeably pregnant.

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The third trimester, 28-40 weeks, the body expands rapidly and the womb enlarges and
presses against the diaphragm.
First Trimester
In the early weeks the mother is likely to be more tired. As the uterus begins to grow, the
"bump" becomes noticeable. This is a good time to start looking into options on birthing
and doctors.
Physical feelings: tiredness, nausea, constipation, frequent urination, food cravings,
change in size of breasts, fainting or dizziness, bloated stomach, and high emotions.
Second Trimester
The mother will probably be feeling full of energy and excitement.
Physical feelings: More energy, constipation, heartburn, and indigestion. The breasts
continue to grow, as does an increase in appetite. There is mild swelling in the feet,
ankles, hands, and face. There is also more baby movement. There may be emotional
ups and downs in the feeling of pregnancy, and short-term memory may be poor.
The hormones estrogen, progesterone, human placental lactogen, oxytocin, and prolactin
prepare the body for feeding the baby, and cause the breasts to enlarge, becoming
painful and tender.
The fetus, placenta, and amniotic fluid account for just over a third of the weight gain
during pregnancy. The remaining weight comes from increased blood volume, fluid
retention, and extra body fat. The suggested weight gain in most pregnancies is between
25-40 lbs.
Third Trimester
Physical feelings
Shortness of breath, tiredness, difficulty in moving and sleeping, and frequent urination.
The emotional mood swings ease off, but the mother begins to feel less enthusiastic about
being pregnant. She may become impatient and restless and just wants for the birth to be
over.
The body is changing to cope with the ever increasing size of the womb. The baby
grows and pushes out the lower back of the mother. The breathing rate of the baby is
growing very quickly. At this stage, the mother should feel the movements of the fetus.
Other signs may be the nipples secreting colostrum, Braxton-Hicks' contractions may
begin, and blood flow to the womb has increased tenfold since conception.

15.9.2 Prenatal Care

Once the female confirms her pregnancy, she will need to find out her physical condition
and what to expect in the coming months. Women typically begin pre-natal care at

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approximately 8-10 weeks gestation, and pregnancy care should continue until approximately
6 weeks postpartum. The main purpose of the prenatal visits is to perform preventative
medicine. Most complications in pregnancy are best treated if they are caught early on. A
series of tests will be performed throughout the pregnancy to judge the mother and fetus'
well-being including:

Mother's history
Urine tests for glucose, protein, and infection
The mother's weight
Blood tests such as a complete blood count, HIV test, or the triple screen which is test
used most commonly to look for neural tube defects and Downs Syndrome.
Physical examination
Blood pressure
Fetal heart monitoring
Ultrasound scans
Non-stress tests

Continuous care is the best way to ensure a healthy mother and baby.

15.10 Labor and Birth

Labor is defined as contractions and cervical change, contractions alone are not labor.
Pre-Labor Signs: as your body is preparing for labor, there are a few things that should
be expected to happen within four to six weeks of labor.
1.
2.
3.
4.
5.
6.

Pressure on the pelvic area

Occasional brownish discharge
Energy level is noticeably increasing or decreasing
Loss of the mucus plug (does not always exist)/increasing discharge
Braxton Hicks contractions (painless contraction of the uterus)
Movement of the baby into the pelvis

False Labor Signs: there are a few signs that indicate false labor.
1. Timing of the contractions are irregular and do not become more frequent or more
intense
2. Contractions stop during rest, stopping what the mother is doing, walking, or changing
position
3. Inconsistent in strength (strong one minute then weak the next)
4. Location of pain is in the front only
True Labor
1. Pain in the lower back, radiating towards the front abdomen, possibly also the legs
2. Contractions increase in strength and are closer together; coming now on a regular
basis, 30 to 70 seconds apart
3. The mucous plug is detached, showing bloody discharge
4. The water breaks (usually this does not break until the doctor does it), when this
happens, contractions become much stronger

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5. Some women have the sudden need to go to the bathroom, diarrhea is common
6. Contractions continue despite movement
7. The cervix is thinning and dilating
When the contractions of labor begin, the walls of the uterus start to contract. They are
stimulated by the release of the pituitary hormone oxytocin. The contractions cause the
cervix to widen and begin to open. As labor progresses the amniotic sac can rupture causing
a slow or a fast gush of fluids. Labor usually begins within a 24 hour period after the
amniotic sac has ruptured. As contractions become closer and stronger the cervix will
gradually start to dilate. The first stage of labor is broken into three parts:
Early Phase First is the early phase of labor, when the cervix dilates from 1-4 centimeters,
this can be the longest and most exhausting part for the mother.
Active Phase The cervix dilates on average 1 cm per hour in the active phase of labor
dilating from 4-7 centimeters. If an epidural is requested it is usually given in this phase.
Transition This is often considered the most intense part of labor with contractions
lasting longer and having shorter rest periods in between them. Dilation from 8-10
centimeters occurs during transition. Some women experience nausea and vomiting
during this phase as well as rectal pressure and an urge to push.
At this point the labor enters the second stage, or the birth of the baby. The mother begins
pushing to aid in the birth of the baby, this part of labor can last minutes, or even hours. A
fetus usually delivered head first. 'Crowning' is the term used when the fetus' head can be
seen between the mothers labia as it emerges. At this point if necessary the birth attendant
may perform an episiotomy, which is a small surgical incision in the peritoneum. This
procedure is usually done to deliver the baby more quickly in response to fetal distress.

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Figure 138

Diagram showing an episiotomie

The third stage of labor is the delivery of the afterbirth (placenta).

Oxytocin continues to be released to shrink the size of the uterus and aid in the limiting of
blood loss from the site of the placenta. As the uterus shrinks the attachment site blood
vessels, some of which can be as large as an adult finger, shrink also. The average blood loss
in a routine vaginal delivery is 400-500 cc.
There are times when a mother may need outside aid in the delivery of the baby, some of
these methods include:
Forceps, an instrument used to cradle the fetus' head and manipulate the head under the
pubic bone to more easily pass through the birth canal.
Vacuum Extraction, a suction cup is applied to the baby's head, and a plunger is used
to suck any air from between the suction cup and the head to create a good seal. The
babies head is then manipulated through the birth canal. This usually leaves a baby's
head bruised, but the mark fades within weeks after birth.

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Figure 139

C-section Birth

Cesarean section, or C-section, is the delivery of a baby through a surgical abdominal

incision (Abdominal delivery - Abdominal birth - Cesarean section). A C-section delivery
is performed when a vaginal birth is not possible or is not safe for the mother or child.
Surgery is usually done while the woman is awake but anesthetized from the chest to
the legs by epidural or spinal anesthesia. An incision is made across the abdomen just
above the pubic area. The uterus is opened, and often brought through the incision after
delivery for better visualization. The amniotic fluid is drained, and the baby is delivered.
The baby's mouth and nose are cleared of fluids, and the umbilical cord is clamped and
cut. After delivery a nursery nurse or pediatrician check the make sure that the baby is
breathing and responding. Due to a variety of medical and social factors, C-sections have
become fairly common; around 25% of births are performed by C-section. C-sections
carry some risks to mother and baby. Compared to a vaginal birth, the risks to mother
include increased risk of death, surgical injury, infection, postpartum depression, and
hemorrhage, although these are rare. Babies born by c-section are more likely to be
admitted to the ICU for breathing problems. Mothers are advised to carefully weigh the
risks of C-section versus vaginal birth.

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Figure 140

Newborn baby

15.10.1 Delivery Options

Hospital Births
The chances of having natural, uncomplicated birth are optimized by carefully selecting
your obstetrician and hospital. Doctors who work with midwives have lower cesarean
section rates because midwives handle less complicated pregnancies. Delivering babies by
abdominal surgery has been steadily rising in America over the past two decades, so that
now 22-30% of births in American hospitals are cesarean section. The U.S., despite having

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the most advanced technology and highly trained medical personnel, ranks 23rd in infant
mortality and 18th in perinatal mortality.
Medical interventions such as epidural anesthesia, pitocin augmentation of labor, vacuum
extraction of fetus, episiotomy and separation of newborn and mother are common in
American hospitals. There are circumstances where medical procedures such as these
are necessary, but many parents and professionals now question the routine use of such
interventions. In some cases, the routine use of these procedures have lead to further
complications. For example, the epidural anesthetic, while providing pain relief, has shown
to increase the operative vaginal delivery rate (i.e. forceps and vacuum extraction rates
slightly) especially in first time mothers. Epidurals have not been shown to increase the
cesarean section rate in recent well documented studies.
Freestanding Birth Centers & Water Birth
"Freestanding" Birth Centers are not inside of or affiliated with a hospital. They are run
by collaboration of midwives or physicians. This is an alternative choice for the woman
who does not wish to birth in a hospital environment yet is not comfortable giving birth at
home. Birth centers do not provide any additional measure of safety than most planned
home births with qualified midwives; they may provide the expectant couple with the
physiological comfort necessary to enable the mother to relax.
Out of hospital birth centers are designed for women having low-risk pregnancies who want
drug-free birth with minimal intervention in a home-like environment. Family members
may participate in the birth. C-sections rates are lower than most hospitals because the
pregnancies are low risk. Freestanding Birth Centers are an alternative choice for a woman
who has had a previous cesarean and wishes to maximize her chances of a vaginal delivery.
However, vaginal birth attempts after a prior cesarean section have a 1-2% risk of uterine
rupture. Heath insurance may cover costs. Many birth centers offer birthing tubs where
one can give birth in water.
Homebirth
Birth at home provides parents with intimacy, privacy, comfort and family-centered experience. Childbirth at home may be a safe option for healthy women having normal
pregnancies. It is for those who have a very strong desire for natural childbirth and who
are willing to take high degree of responsibility for their health care and baby's birth. At
home, the parents and midwife are in control of the birthing environment, and strict time
perimeters for length of labor are not imposed, or routine medical interventions such as
IVs done. However, the World Health Organization (WHO) states that "giving birth in a
health facility (not necessarily a hospital) with professional staff is safer by far than doing
so at home." (The World Health Report 2005). Also, the American College of Obstetricians
and Gynecologists (ACOG) opposes out of hospital births. In choosing the comfort of home
parents are also choosing to be further away from lifesaving measures should complications
arise.
Homebirth midwives provide complete prenatal care including monthly visits, laboratory
tests, screening for infections. They provide nutritional counseling and support for psychosocial issues. There is a chance that a rare, but critical emergency might occur during
the birth where hospital services may not be able to be obtained quick enough. Again,
the WHO states that "it is just before, during, and in the very first hours and days after

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birth that life is most at risk," (The World Health Report 2005) and that "many of the
complications that result in maternal deaths and many that contribute to perinatal deaths
are unpredictable, and their onset can be both sudden and severe." (WHO Birth and
Emergency Preparedness in Antenatal Care, 2006) Home birth midwives are trained to
know when an emergency requires medical interface and can provide stabilizing measures
until critical care can be obtained. While homebirth midwives generally have the training,
equipment, and medicine to handle many complications, there is great variation in training
and skill level among midwives. In choosing a homebirth midwife one should careful
examine credentials and training.

Figure 141 A newborn with umbilical

cord still attached (3 minutes.)

15.10.2 Postpartum care

After the baby is born the umbilical cord is clamped and cut and the baby is looked over by
a doctor or nurse. The baby is given an APGAR score at one and five minutes after birth.
This is an analysis of how well the baby is performing its vital functions.
The five criteria of the Apgar score:
Score of 0
Skin color
blue all over
Heart rate
absent

Score of 1
blue at extremities
<100

Score of 2
normal
>100

Acronym
Appearance
Pulse

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Reflex irritability

no response
to stimulation

grimace/feeble cry
when stimulated

Muscle tone
Respiration

none
absent

some flexion
weak or irregular

sneeze/cough/pulls
away
when stimulated
active movement
strong

Grimace

Activity
Respiration

If tearing, or an episiotomy occurs the wound is closed with absorbable suture. The mother is
closely watched for blood loss, infection, or any other possible complications. Breastfeeding
should be initiated as soon as possible after delivery as the stimulation of oxytocin in the
mother aids in hemostasis.

15.11 Risks in Pregnancy

Pregnancies that warrant close attention usually come from an existing medical condition
such as asthma, diabetes, epilepsy, or a condition developed because of pregnancy. Conditions
that arise during pregnancy will require special treatment. The purpose of prenatal care is
to detect these conditions, and to monitor and deal with them before they become serious.
Preeclampsia is the medical term for high blood pressure during pregnancy. It is also
characterized by edema, blurry vision, liver pain, and can progress into Eclampsia in
which the mother can experience seizures, coma or even death.
Gestational Diabetes is diabetes mellitus that develops during pregnancy. All women
should be tested for the condition at about 28 weeks gestation. Gestational and preexisting diabetes can cause large for gestational age babies, a sudden drop in a neonates
blood sugar after birth, and has a high risk for stillbirth
Other serious risks include:
Teratogens (substances that cause birth defects including alcohol and certain prescription
and recreational drugs)
Infection (such as rubella or cytomegalovirus) An infection in the eleventh week is less
likely to damage the heart, but the baby may be born deaf.
Genetics (such as Factor V Leiden) Diabetes, blood conditions, etc.
Radiation (ionizing radiation such as X-rays, radiation therapy, or accidental exposure
to radiation)
Nutritional deficiencies
Fetal Alcohol Syndrome or FAS exposure is the leading known cause of mental
retardation in the Western world. It is a disorder of permanent birth defects that occurs
in the offspring of women who drink alcohol during pregnancy, depending on the amount,
frequency, and timing of alcohol consumption. Alcohol crosses the placental barrier and
can stunt fetal growth or weight, create distinctive facial stigmata, damage neurons and
brain structures, and cause other physical, mental, or behavioral problems. Drinking
during pregnancy should be avoided. Women who drink more than 4 or 5 drinks per day
may cause permanent damage to their fetus, including, behavioral problems, sight and
hearing loss, deformed organs and central nervous system dysfunction.

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Risks in Pregnancy
Smoking can cause low birth weight, still birth, birth defects, preterm births and
immature lung development. It can also contribute to addiction in the child's later teen
years.
Illegal Drugs can be the most devastating. Risks include SIDS (Sudden Infants Death
Syndrome), learning disorders, birth defects, uncontrollable trembling, hyperactive, and
drug dependency. Most drugs can be tested by a simple urine or blood test.
Medications. All medication use should be discussed with your doctor. Many over the
counter and prescription drugs have warning labels. Follow these precautions to help
avoid birth defects or other related problems.

15.11.1 Miscarriage
Miscarriage or spontaneous abortion is the natural or spontaneous end of a pregnancy at a
stage where the embryo or the fetus is incapable of surviving, generally defined in humans
at a gestation of prior to 20 weeks. Miscarriages are the most common complication of
pregnancy. Basic Facts: 15-20% of pregnancies end in miscarriage, 70% of the time there is
a chromosomal abnormality with the fetus, and one miscarriage does not increase your risk
in the next pregnancy. Miscarriage is almost never the mother's fault.
If the products of conception are not completely expelled after fetal death this is known
as a missed abortion and is usually treated surgically by a procedure known as a D&C or
dilation and curettage.

15.11.2 Bleeding During Pregnancy

Vaginal bleeding at any stage should be taken seriously. Severe bleeding in the early weeks
may be a sign of miscarriage. However, 25% of pregnant patient bleed in the first trimester.
After 24 weeks the mother should seek medical advice immediately. Third trimester bleeding
in pregnancy is often one of the first signs of placenta previa; placenta is across the opening
of the cervix. An ultrasound should be performed to establish the location. Other causes of
late term bleeding include:
Preterm Labor or labor that occurs before 38 weeks gestation that can have multiple
causes
Placental Abruption is a condition in which the placenta is torn away from the uterine
wall causing loss of oxygen and nutrients to the baby, and hemorrhage of mother and
baby from the large blood vessels in the placenta. Most women, but not all experience
heavy bleeding and abdominal pain. This is a life threatening emergency as a fetus can
only survive as long as 50% of the placenta is still attached.

15.11.3 Blood Conditions

Individuals either have, or do not have, the Rhesus factor (or Rh D antigen) on the surface
of their red blood cells. This is usually indicated by 'RhD positive' (does have the RhD
antigen) or 'RhD negative' (does not have the antigen) suffix to the ABO blood type i.e.

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A+ B- blood typing. This is a problem only when an Rh-negative woman has a partner
who is Rh-positive resulting in an Rh-positive baby. If the mother's and the baby's blood
come into contact during the birth, her body produces antibodies against the baby's blood.
This problem usually does not affect the current pregnancy but can be dangerous for future
pregnancies as the antibodies stay in the blood causing an immune response against future
Rh+ fetus. In essence the mother's body "rejects" the fetus as it would a foreign body. A
drug called Rhogam is now given by injection given at 28-30 weeks gestation and given again
if there is confirmation that the baby is Rh positive within 24 hours after birth to protect
the future pregnancies. Rh isoimmunization is rare in our day. Rh- mothers should also be
given the injection after miscarriage or abortion.
If a mother is untreated they are at risk to subsequently deliver babies who suffer from
hemolytic disease of the newborn. Hemolytic disease of the newborn, also known as HDN, is
an alloimmune condition that develops in a fetus, when the IgG antibodies that have been
produced by the mother and have passed through the placenta include ones which attack
the red blood cells in the fetal circulation. The red cells are broken down and the fetus can
develop reticulocytosis and anemia. This fetal disease ranges from mild to very severe, and
fetal death from heart failure (hydrops fetalis) can occur. When the disease is moderate or
severe, many erythroblasts are present in the fetal blood and so these forms of the disease can
be called erythroblastosis fetalis (or erythroblastosis foetalis). Hemolysis leads to elevated
bilirubin levels. After delivery bilirubin is no longer cleared (via the placenta) from the
neonate's blood and the symptoms of jaundice (yellowish skin and yellow discoloration of
the whites of the eyes) increase within 24 hours after birth. Like any other severe neonatal
jaundice, there is the possibility of acute or chronic kernicterus. Profound anemia can cause
high-output heart failure, with pallor, enlarged liver and/or spleen, generalized swelling, and
respiratory distress. The prenatal manifestations are known as hydrops fetalis; in severe
forms this can include petechiae and purpura. The infant may be stillborn or die shortly
after birth.

15.11.4 Other Abnormalities

Physical and Genetic Defects: Physical anomalies are present at birth. Examples are; cardiac,
facial (such as cleft palate), club foot, etc. These do not always endanger the baby's life.
1-2% of babies are born with a significant congenital abnormality. 4-6% with something
relatively minor.
Chromosomal Abnormalities: Occur when there is a problem in the baby's genetic makeup;
these include conditions such as Down syndrome. Other genetic defects, such as cystic
fibrosis, can be inherited from the parents.

15.12 Staying Healthy

Pregnancy and childbirth place great demands, it is important to keep healthy. The more
healthy and relaxed the mother is, the better it will be to cope with the demands of pregnancy.
A healthy lifestyle combines many factors:
Balanced Diet

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A poor diet can cause a low birth weight. Excessive weight gain during pregnancy can cause
back problems, varicose veins, or indicate preclampsia. Advice on diet often includes to eat
foods that are high in nutritional content. Sufficient protein, vitamins, carbohydrates, fats,
and minerals, as well as fiber. Limit intake of saturated fats and sugar, and salt. Drink
plenty of fluids.
Regular Exercise
Mild exercise, such as walking or swimming, is beneficial and will help cope with the
workload of pregnancy and the demands of labor. Mother's should listen to her body and
stop exercising when it tells her to. Exercise should never be painful.
Baby's Health
Smoking reduces the oxygen and nutrients passing via the placenta to the baby. Avoid
alcohol to avoid serious birth defects.

15.13 In vitro Fertilization and Artificial Implantation

Figure 142

Oocyte is injected with sperm outside of the womb.

An alternative when other methods of achieving contraception have failed.

In vitro fertilization (IVF) is a technique in which egg cells are fertilized by sperm outside
the woman's womb. IVF is a major treatment in infertility when other methods of achieving
conception have failed. The process involves hormonally controlling the ovulatory process,
removing ova (eggs) from the woman's ovaries and letting sperm fertilize them in a fluid
medium. The fertilized egg (zygote) is then transferred to the patient's uterus with the
intent to establish a successful pregnancy.

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The term in vitro, from the Latin root, is used, because early biological experiments involving
cultivation of tissues outside the living organism from which they came, were carried out in
glass containers such as beakers, test tubes, or petri dishes.
While the overall live birth rate via IVF in the U.S. is about 27% per cycle (33% pregnancy
rate), the chances of a successful pregnancy via IVF vary widely based on the age of the
woman (or, more precisely, on the age of the eggs involved). Where the woman's own
eggs are used as opposed to those of a donor, for women under 35, the pregnancy rate is
commonly approximately 43% per cycle (37% live birth), while for women over 40, the rate
falls drastically - to only 4% for women over 42. Other factors that determine success rates
include the quality of the eggs and sperm, the duration of the infertility, the health of the
uterus, and the medical expertise. It is a common practice for IVF programmes to boost
the pregnancy rate by placing multiple embryos during embryo transfer. A flip side of this
practice is a higher risk of multiple pregnancy, itself associated with obstetric complications.
Embryo cryopreservation If multiple embryos are generated, patients may choose to
freeze embryos that are not transferred. Those embryos are placed in liquid nitrogen and
can be preserved for a long time. There are currently 500,000 frozen embryos in the United
States. The advantage is that patients who fail to conceive may become pregnant using such
embryos without having to go through a full IVF cycle. Or, if pregnancy occurred, they
could return later for another pregnancy.

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15.14 Embryonic stem cells

Figure 143 Pluripotent, embryonic stem cells originate as inner mass cells with in a
blastocyst. The stem cells can become any tissue in the body, excluding a placenta. Only
the morula's cells are totipotent, able to become all tissues and a placenta.

Embryonic celtic cell lines (ES cell lines) are cultures of cells derived from the epiblast
tissue of the inner cell mass (ICM) of a blastocyst. A blastocyst is an early stage embryo
- approximately 4 to 5 days old in humans and consisting of 50-150 cells. ES cells are
pluripotent, and give rise during development to all derivatives of the three primary germ
layers: ectoderm, endoderm and mesoderm. In other words, they can develop into each of the
more than 200 cell types of the adult body when given sufficient and necessary stimulation
for a specific cell type. They do not contribute to the extra-embryonic membranes or the
placenta. This means they can become any kind of human tissue (ie. heart tissue, nerve
tissue, etc.).

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When given no stimuli for differentiation, ES cells will continue to divide in vitro and each
daughter cell will remain pluripotent. The pluripotency of ES cells has been rigorously
demonstrated in vitro and in vivo, thus they can be indeed classified as stem cells.
Because of their unique combined abilities of unlimited expansion and pluripotency, embryonic stem cells are a potential source for regenerative medicine and tissue replacement
after injury or disease. To date, no approved medical treatments have been derived from
embryonic stem cell research. This is not surprising considering that many nations currently
have moratoria (suspension of practices) on either ES cell research or the production of new
ES cell lines.
There exists a widespread controversy over stem cell research that emanates from the
techniques used in the creation and usage of stem cells. Embryonic stem cell research is
particularly controversial because, with the present state of technology, starting a stem cell
line requires the destruction of a human embryo and/or therapeutic cloning. Opponents of the
research argue that this practice is a slippery slope to reproductive cloning and tantamount
to the instrumentalization of a human being. Contrarily, some medical researchers in the
field argue that it is necessary to pursue embryonic stem cell research because the resultant
technologies are expected to have significant medical potential, and that the embryos used for
research are only those meant for destruction anyway (as a product of in vitro fertilization).
This in turn, conflicts with opponents in the pro-life movement, who argue that an embryo
is a human being and therefore entitled to dignity even if legally slated for destruction. The
ensuing debate has prompted authorities around the world to seek regulatory frameworks
and highlighted the fact that stem cell research represents a social and ethical challenge.
Reproductive Cloning
Reproductive Cloning is a technology used to generate an animal that contains the same
nuclear DNA as another currently or previously existing animal. Scientists transfer the
genetic material from the nucleus of a donor adult cell to an egg whose nucleus, and thus its
genetic material has been removed. The egg containing the DNA, now reconstructed, has to
be treated with chemicals or electric current in order to stimulate cell division. Once the
cloned embryo reaches a suitable stage, it is transferred to the uterus of a female host to
continue development until birth. Currently this is illegal to practice in the United States.
Therapeutic Cloning
Recent research by researchers led by Anthony Atala of Wake Forest University and a team
from Harvard University has found that amniotic fluid, in addition to its main functions
of cushioning a growing fetus and providing buoyancy, is also a plentiful source of nonembryonic stem cells. These cells have demonstrated the ability to differentiate into a
number of different cell-types, including brain, liver and bone.
Therapeutic Cloning refers to a procedure that allows the cloning of specific body parts and
organs to be used for medical purposes. Although this has not been realized, much research
is being done on the subject.

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15.15 Pregnancy and Lactation

A mother's milk is ideal because it meets the baby's specific needs. Lactation is a neuroendocrine response in milk production. Sucking stimulates the sensory nerve endings in the
nipples and sends stimulus to the hypothalamus. The hypothalamus stimulates anterior
pituitary and prolactin is released. In milk let-down the sucking stimulates sensory nerves in
the nipples. This stimulates the hypothalamus which then stimulates the posterior pituitary
and releases oxytocin. Sucking also stimulates contraction of the cells around the alveoli in
the mammary cells. Milk then flows into the milk ducts causing milk let-down.
Breast milk provides all the nutrients required for the first 4-6 months. It contains carbohydrates (such as lactose), fats (such as linoleic acid), and easily digestible proteins (such as
alpha-lactalbumin). Breast milk also contains an adequate supply of vitamins and minerals,
digestive enzymes, hormones and immunological factors.
The first milk produced after birth is called colostrum. This is synthesized during the
end of pregnancy and 3-5 days of postpartum. It is very high in protein and low in fat
and carbohydrates, and contains immunoglobulins. This help the baby have a first bowel
movement and prevent jaundice. The bowel movement that results from the colostrum is a
different color and consistency than future bowel movements once the mother's milk comes
in. In some cultures the colostrum is discarded because of the difference, but what they do
not know is that it is the best thing for the baby.
The composition varies in breast milk during feeding, and over time with development of
the baby. When breastfeeding there are three names for the composition of the milk: the
fore milk, present during the beginning of breastfeeding; mid is the middle of feeding; and
hind which is toward the end of the feeding and contains a composition high in fat.
When breastfeeding the female should consider the types of food that will be consumed.
If the mother is on a low fat diet or if foods like garlic, broccoli, and onions are eaten, it
may affect the baby's preference for breast feeding. Also, the mother should consider not
breastfeeding after the consumption of alcohol, caffeine, smoking, and certain medications.
Barriers of breastfeeding are lack of professional and social support, misinformation, embarrassment, early discharge form the hospital without instruction, and returning to work or
school without adequate lactation rooms and if the mother refuses to tend breastfed infant.
When breastfeeding initiate as soon after delivery as possible, position the baby correctly,
feed on demand from both breasts at each feeding and at least 10 minutes on each breast.
Additionally there should be a good educator in the case the infant is not latching on.
A common problem that may happen when breastfeeding is mastitis, which is an inflammation
of one or both breasts and is usually associated with the infection of a blocked milk duct
during lactation. The symptoms include flu-like symptoms, red streaks on the breast, and
hot skin. Antibiotics may be necessary to clear the infection. Thrush may also happen and
could be passed between mom and baby. A symptom of thrush includes white flecks on
tongue, and the baby and mother should be treated by a doctor.
Breast milk is recommended through the first 12 months. Supplementation of cow's milk is
not recommended due to the high protein that would cause liver damage to the baby.
Why breastfeed?

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Pregnancy and Birth

It is easily digested
Composition changes with infant needs
Changes during a feeding, high in fat at the end of feeding
Antibodies in milk
Breastfeeding moms miss less work because babies are sick less
Fewer allergies
Less spit-up
Less constipation and diarrhea
Better jaw development
Decreased risk of SIDS (Sudden Infant Death Syndrome)
Higher IQ
Decreased risk of diabetes, Crohn's Disease, Celiac Sprue
Bonding
Convenient, always at the correct temperature and ready to go
Less expensive
Helps the uterus return to normal size more quickly
Less incidence of postpartum blues
Lower risk of breast cancer
Lower risk of osteoporosis

15.16 Postpartum Depression

Having a baby is usually one of the happiest times in a woman's life, but for some women, it
can include times of sadness and depression. More women actually suffer from postpartum
depression than we really know. Women usually ignore the emotional and physical signs,
dealing with their feelings on their own.
Postpartum depression affects approximately 10 to 15 percent of new mothers. It often
causes anxiety and obsession about caring for the baby or the cleanliness of the home. It
may cause changes in sleep patterns and affect relationships including the ability to form a
bond with the baby and other family members. Some mothers with postpartum depression
have thoughts of wanting to die or of hurting the baby. If the symptoms are so severe that
they keep the mother from being able to function, medical treatment is necessary.
Baby blues are common due to rapid hormonal changes but resolve after 1-2 weeks. Postpartum depression is characterized by persisting symptoms, and the mother should notify
her provider immediately.

15.17 Testing Your Knowledge

Answers for these questions can be found here1
1. Is at this stage that an egg implants in the uterine lining

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http://en.wikibooks.org/wiki/Human_Physiology/Appendix_1:_answers_to_review_
questions#Pregnancy_and_birth

Testing Your Knowledge

A) morula
B) zygote
C) blastocyst
D) embryoblast
2. Which part of the embryoblast will become the central nervous system in development
A) ectogerm
B) mesoderm
C) endoderm
3. This hormone is only produced in the human body when a woman is pregnant
A) estrogen
B) HCG
C) progesterone
D) FSH
E) LH
4. By this week of pregnancy, the beginnings of all major organs have formed
A) 4
B) 7
C) 5
D) 6
E) 8
5. Stem cells are found in the embryoblast and use of them is very controversial, another
place to find stem cells that are usable to treat leukemia and other disorders is the
A) morula
B) chorion
C) amnion
D) amniotic fluid
E) umbilical cord
6. The cervix dilates on an average of ______per hour in the active phase of labor
A) 2 mm
B) 2 cm
C) 1mm
D) 1 cm

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Pregnancy and Birth

7. The contractions of the uterus are stimulated by the release of
A) oytocin
B) FSH
C) LH
D) prolactin
E) estrogen
8. A sign of pre-labor is
A) irregular contractions
B) pain in the front only
C) loss of the mucas plug
D) contractions stop during rest
9. This is the most common complication of pregnancy
A) preclampcia
B) miscarriage
C) smoking
D) Rh factor
E) teratogens
10. Sue decides to breastfeed because she has been told that colostrum contains
A) high protein
B) low fat
C) immunoglobulins
D) all of the above
E) none of the above
11. What is the first milk after birth called?
A) thrush
B) mastitis
C) colostrum
D) milk let down

15.18 Glossary
Abruption: Premature separation of the placenta from the wall of the womb

448

Glossary
Amnion: An embryonic membrane that encircles a developing fetus and contains amniotic
fluid.
Amniocentesis: A procedure in which a small sample of amniotic fluid is removed from
around the fetus
Amniotic fluid: The fluid surrounding the fetus
Amniotomy: (artificial rupture of membranes, ARM) Breaking the membranes using a
special plastic hook
Anemia: Lack of hemoglobin in red blood cells, due to iron deficiency or disease
Antepartum Hemorrhage: (APH) Vaginal bleeding that happens after 24 weeks of
pregnancy and before delivery
Breech: The baby is lying bottom down in the womb
Celiac sprue: Nutrient absorption impairment which is improved when gluten is removed
form the diet. Characteristic mucosal lesion of the small intestine.
Cephalic: The baby is lying head down in the womb
Chorion: The embryonic membrane that forms the outermost covering around the developing fetus.
Chorion Villus Sampling: (CVS) A method for sampling placental tissue for genetic or
chromosome studies.
Colostrum the fluid that is made late in pregnancy and the first few days postpartum in
the breast that contains immunologic substances and essential nutrients.
Cleavage: The early successive divisions of embryonic cells into smaller and smaller cells.
Cilia: The fine hairs that line the fallopian tubes'
Cordocentesis: The procedure for taking blood from the fetal umbilical cord via a needle
through the mothers abdomen
Copulation: (Coitus, sexual intercourse) is the procreative act of a man's erect penis is
inserted into a woman's vagina. At climax, semen is ejaculated from the penis at the cervix
of the uterus. Sperm then propel themselves into the uterine tubes where fertilization may
occur if an eg
Crohn's disease: Skip lesions in the colon and is a malabsorptive disease.
Cystitis: Infection of the bladder
Dizygous: Not identical (fraternal) twins
Doppler: A form of ultrasound used specially to investigate blood flow in the placenta or
in the fetus
Down Syndrome: (Trisomy 21) A disorder caused by the presence of an extra chromosome
21 in the cells
Ectopic Pregnancy: A pregnancy that develops outside of the womb
Edema: Swelling of the fingers, legs, toes, and face.

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Pregnancy and Birth

Embryo: The medical term for the baby from conception to about six weeks
Engagement: The process in which the head of the baby moves down from high in the
mother's abdomen and settles deeper into her pelvis in preparation for birth. This can
happen any time between 36 weeks and labor.
Epidural Anesthesia: A method of numbing the nerves of the lower spinal cord to ensure
a pain-free labor
Episiotomy: A cut of the perineum and vagina performed to make the delivery easier
External Fetal Monitor: An electronic monitor used to record the fetal heartbeat and
mothers contractions
Fallopian Tubes: (uterine tubes) Two tubular structures (one on each side of the womb)
leading from the ovaries to the uterus
Fertilization: The union of an egg cell and a sperm cell is present wherein 23 chromosomes
from each parent come together to form a zygote. After sperm penetrates, the ovum
undergoes a chemical change to prevent other sperm from entering. Multiple births can
occur from complete division of the conceptus during early cleavage or from fertilization
of multiple ova. Birth control techniques are designed to prevent ovulation or to prevent
fertilization by barriers, that keep sperm and ova separated.
Fetus: Medical term for the baby from six weeks after conception until birth
Forceps: Metal instruments that fit on either side of the baby's head and are used to help
deliver the baby
Fundus: The top of the womb
Germ layer: Layers of cells within an embryo that form the body organd during development.
Glial Cells (neuroglia; glia): Non-neuronal cells that provide support and nutrition,
maintain homeostasis, form myelin, and participate in signal transmission in the nervous
system. In the human brain, glia are estimated to outnumber neurons by about 10 to 1.
Glial cells provide support and protection for neurons, the other main type of cell in the
central nervous system. They are thus known as the "glue" of the nervous system. The
four main functions of glial cells are to surround neurons and hold them in place, to supply
nutrients and oxygen to neurons, to insulate one neuron from another, and to destroy
pathogens and remove dead neurons.
Hemoglobin: (Hb)The oxygen carrying constituent of red blood cells
Induction of labor: (IOL) the procedure for initiating labor artificially
In utero death: (IUD)the death of the unborn fetus after 24 weeks
In vitro fertilization: (IVF) a method of assisted conception in which fertilization occurs
outside the mother's and the embryo is replaced in the womb
Lanugo: fine hair that covers the fetus in the womb
Lochia: blood loss after birth

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Reference
Mastitis inflammation of the breast most frequently in lactation.
Neonatal: baby less than 28 days old
Nuchal scan: special ultrasound scan that gives an estimate of the risk of Down syndrome
Oocyte: one egg that is released from the ovary at each ovulation
Placenta: The structure by which an unborn child is attached to it's mother's uterine wall
and through which it is nourished.
Postnatal: After birth
Prenatal: Before birth
Quickening: The process that occurs between the seventeenth and twentieth weeks of fetal
development, the fetus's leg bones achieve their final relative proportions. In this process
the muscles contract, causing movement at the fetus's sinovial joints. The joint movement
enhances the nutrition of the articular cartilage and prevents the fusion of connective tissues
within the joint. It also promotes bone hardening. It is this stage, where the fetus's bones
become more developed and harder, that the mother begins to notice fetal movement.
Rudimentary: Basic; minimal; with less than, or only the minimum, necessary
Thrush: Creamy white flakes on a red papillae on tongue and tongue may be enlarged.
Umbilical cord: The cord like structures that connects the fetus to the placenta.
Zygote: A cell produced by the fusion of an egg and a sperm; a fertilized egg cell.

15.19 Reference
"as your baby grows From Conception to Birth"published by American Baby
http://www.babybluesconnection.com
"Pregnancy and Birth" authors: Dr. Karina Reynolds, Dr. Christoph Lees, Grainne
McCartan
"Fundamental Concepts of Human Anatomy" authors: M.J. Shively D.V.M., M.S., Ph.D.
and D.P. Homan B.S., M.S.
"Essentials of Anatomy and Physiology" authors:Valerie C. Scanlon and Tina Sanders,
fourth edition
http://www.MERLOT.com Stanford Site
"The New Parent" author DR. Miriam Stoppard
www.marchofdimes.com
http: // health. allrefer. com/ health/ fetal-development-info. html
American Pregnancy Association
Internet groups: International Awareness Network: www.ican-online.org

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16 Genetics and Inheritance

16.1 Introduction
w:Natural Selection1 Genetics is the science of the way traits are passed from parent to
offspring. For all forms of life, continuity of the species depends upon the genetic code being
passed from parent to offspring. Evolution by natural selection is dependent on traits being
heritable. Genetics is very important in human physiology because all attributes of the
human body are affected by a persons genetic code. It can be as simple as eye color, height,
or hair color. Or it can be as complex as how well your liver processes toxins, whether you
will be prone to heart disease or breast cancer, and whether you will be color blind. Defects
in the genetic code can be tragic. For example: Down Syndrome, Turner Syndrome, and
Klinefelter's Syndrome are diseases caused by chromosomal abnormalities. Cystic fibrosis is
caused by a single change in the genetic sequence. Genetic inheritance begins at the time
of conception. You inherited 23 chromosomes from your mother and 23 from your father.
Together they form 22 pairs of autosomal chromosomes and a pair of sex chromosomes (either
XX if you are female, or XY if you are male). Homologous chromosomes have the same
genes in the same positions, but may have different alleles (varieties) of those genes. There
can be many alleles of a gene within a population, but an individual within that population
only has two copies, and can be homozygous (both copies the same) or heterozygous (the
two copies are different) for any given gene.
w:Human Genome Project2 Genetics is important to medicine. As more is understood about
how genetics affects certain defects and diseases, cures and treatments can be more readily
developed for these disorders. The sequence of the human genome (approximately 3 billion
base pairs in a human haploid genome with an estimated 20,000-25,000 protein-coding genes)
was completed in 2003, but we are far from understanding the functions and regulations of
all the genes. In some ways medicine is moving from diagnosis based on symptoms towards
diagnosis based on genetics, and we are moving into what many are calling the age of
personalized medicine.

16.1.1 DNA
Deoxyribonucleic acid (DNA) is the macromolecule that stores the information necessary
to build structual and functional cellular components. It also provides the basis for inheritance
when DNA is passed from parent to offspring. The union of these concepts about DNA
allows us to devise a working definition of a gene. A gene is a segment of DNA that codes
for the synthesis of a protein and acts as a unit of inheritance that can be transmitted from
1
2

http://en.wikipedia.org/wiki/Natural%20Selection
http://en.wikipedia.org/wiki/Human%20Genome%20Project

453

Genetics and Inheritance

generation to generation. The external appearance (phenotype) of an organism is determined
to a large extent by the genes it inherits (genotype). Thus, one can begin to see how variation
at the DNA level can cause variation at the level of the entire organism. These concepts
form the basis of genetics and evolutionary theory.

16.1.2 Gene

Figure 144

rotating animation of a DNA molecule.

A gene is made up of short sections of DNA which are contained on a chromosome within
the nucleus of a cell. Genes control the development and function of all organs and all

454

Introduction
working systems in the body. A gene has a certain influence on how the cell works; the
same gene in many different cells determines a certain physical or biochemical feature of the
whole body (e.g. eye color or reproductive functions). All human cells hold approximately
30,000 different genes. Even though each cell has identical copies of all of the same genes,
different cells express or repress different genes. This is what accounts for the differences
between, let's say, a liver cell and a brain cell . Genotype is the actual pair of genes that a
person has for a trait of interest. For example, a woman could be a carrier for hemophilia
by having one normal copy of the gene for a particular clotting protein and one defective
copy. A Phenotype is the organisms physical appearance as it relates to a certain trait.
In the case of the woman carrier, her phenotype is normal (because the normal copy of
the gene is dominant to the defective copy). The phenotype can be for any measurable
trait, such as eye color, finger length, height, physiological traits like the ability to pump
calcium ions from mucosal cells, behavioral traits like smiles, and biochemical traits like
blood types and cholesterol levels. Genotype cannot always be predicted by phenotype (we
would not know the woman was a carrier of hemophilia just based on her appearance), but
can be determined through pedigree charts or direct genetic testing. Even though genotype
is a strong predictor of phenotype, environmental factors can also play a strong role in
determining phenotype. Identical twins, for example, are genetic clones resulting from the
early splitting of an embryo, but they can be quite different in personality, body mass, and
even fingerprints. hi

16.1.3 Genetics
Genetics (from the Greek genno = give birth) is the science of genes, heredity, and the
variation of organisms. The word "genetics" was first suggested to describe the study of
inheritance and the science of variation by prominent British scientist William Bateson in
a personal letter to Adam Sedgwick, dated April 18, 1905. Bateson first used the term
"genetics" publicly at the Third International Conference on Genetics (London, England) in
1906.
Heredity and variations form the basis of genetics. Humans apply knowledge of genetics in
prehistory with the domestication and breeding of plants and animals. In modern research,
genetics provide important tools for the investigation of the function of a particular gene,
e.g., analysis of genetic interactions. Within organisms, genetic information is generally
carried in chromosomes, where it is represented in the chemical structure of particular DNA
molecules.

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Genetics and Inheritance

Figure 145

diagram showing the seven characters observed by Mendel

Genes encode the information necessary for synthesizing the amino-acid sequences in proteins,
which in turn play a large role in determining the final phenotype, or physical appearance
of the organism. In diploid organisms, a dominant allele on one chromosome will mask
the expression of a recessive allele on the other. While most genes are dominant/recessive,
others may be codominant or show different patterns of expression. The phrase "to code for"
is often used to mean a gene contains the instructions about a particular protein, (as in the
gene codes for the protein). The "one gene, one protein" concept is now known to be the
simplistic. For example, a single gene may produce multiple products, depending on how
its transcription is regulated. Genes code for the nucleotide sequence in mRNA and rRNA,
required for protein synthesis.
Gregor Mendel researched principals of heredity in plants. He soon realized that these
principals also apply to people and animals and are the same for all living animals.
Gregor Mendel experimented with common pea plants. Over generations of the pea plants,
he noticed that certain traits can show up in offspring with out blending any of the parent's
characteristics. This is a very important observation because at this point the theory was
that inherited traits blend from one generation to another.

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Introduction

Figure 146

Mendelian inheritance 1 2 1

Pea plant reproduction is easily manipulated. They have both male and female parts and
can easily be grown in large numbers. For this reason, pea plants can either self-pollinate or
cross-pollinate with other pea plants.
In cross pollinating two true-breeding plants, for example one that came from a long line
of yellow peas and the other that came from a long line of green peas, the first generation
of offspring always came out with all yellow peas. The following generations had a ratio
of 3:1 yellow to green. In this and in all of the other pea plant traits Mendel observed,
one form was dominant over another so it masked the presence of the other allele. Even

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Genetics and Inheritance

if the phenotype (presence) is covered up, the genotype (allele) can be passed on to other
generations.
Time line of notable discoveries
1859 Charles Darwin3 publishes "The Origin of Species"4
1865 Gregor Mendel's5 paper, Experiments on Plant Hybridization6
1903 Chromosomes are discovered to be hereditary units
1906 The term "genetics" is first introduced publicly by the British biologist William Bateson7
at the Third International Conference on Genetics in London, England
1910 Thomas Hunt Morgan8 shows that genes reside on chromosomes, and discovered linked
genes on chromosomes that do NOT follow Mendel's law of independent allele segregation
1913 Alfred Sturtevant9 makes the first genetic map of a chromosome
1913 Gene maps show chromosomes contain linear arranged genes
1918 Ronald Fisher10 publishes On the correlation between relatives on the supposition of
Mendelian inheritance - the modern synthesis starts.
1927 Physical changes in genes are called mutations
1928 Fredrick Griffith discovers a hereditary molecule that is transmissible between bacteria
1931 Crossing over is the cause of recombination
1941 Edward Lawrie Tatum11 and George Wells Beadle12 show that genes code for proteins
1944 Oswald Theodore Avery13 , Colin McLeod14 and Maclyn McCarty15 isolate DNA16 as
the genetic material (at that time called transforming principle)
1950 Erwin Chargaff17 shows that the four nucleotides are not present in nucleic acid in
stable proportions, but that some general rules appear to hold. (e.g., the nucleotide bases
Adenine-Thymine and Cytosine-guanine always remain in equal proportions)
1950 Barbra McClintock discovers transposons in maize

3
4
5
6
7
8
9
10
11
12
13
14
15
16
17

458

http://en.wikipedia.org/wiki/Charles%20Darwin
http://en.wikipedia.org/wiki/The%20Origin%20of%20Species
http://en.wikipedia.org/wiki/Gregor%20Mendel
http://en.wikipedia.org/wiki/Experiments%20on%20Plant%20Hybridization
http://en.wikipedia.org/wiki/William%20Bateson
http://en.wikipedia.org/wiki/Thomas%20Hunt%20Morgan
http://en.wikipedia.org/wiki/Alfred%20Sturtevant
http://en.wikipedia.org/wiki/Ronald%20Fisher
http://en.wikipedia.org/wiki/Edward%20Lawrie%20Tatum
http://en.wikipedia.org/wiki/George%20Wells%20Beadle
http://en.wikipedia.org/wiki/Oswald%20Theodore%20Avery
http://en.wikipedia.org/wiki/Colin%20McLeod
http://en.wikipedia.org/wiki/Maclyn%20McCarty
http://en.wikipedia.org/wiki/DNA
http://en.wikipedia.org/wiki/Erwin%20Chargaff

Introduction
1952 The Hershey-Chase experiment18 proves the genetic information of phages (and all
other organisms) to be DNA
1953 DNA structure is resolved to be a double helix by James D. Watson19 and Francis
Crick20 , with help from Rosalind Franklin21
1956 Jo Hin Tjio and Albert Levan22 established the correct chromosome number in humans
to be 46
1958 The Meselson-Stahl experiment23 demonstrates that DNA is semi-conservatively replicated
1961 The genetic code is arranged in triplets
1964 Howard Temin24 showed using RNA viruses that Watson's central dogma is not always
true
1970 Restriction enzymes were discovered in studies of a bacterium Haemophilus influenzae,
enabling scientists to cut and paste DNA
1977 DNA is sequenced for the first time by Fred Sangr, Walter Gilbert25 , and Allan Maxam
working independently. Sanger's lab complete the entire genome of sequence of Bacteriophage
1983 Kary Banks Mullis26 discovers the polymerase chain reaction (PCR) enabling the easy
amplification of DNA
1985 Alec Jeffreys27 discovers genetic finger printing
1989 The first human gene is sequenced by Francis Collin and Lap-Chee Tsui28 . It encodes
the CFTR protein. Defect in this gene causes Cystic Fibrosis29
1995 The genome of Haemophilus30 influenza is the first genome of a free living organism to
be sequenced.
1996 Saccharomyces31 cerevisiae is the first eukaryote genome sequence to be released.
1998 The first genome sequence for a multicellular eukaryote, C. elegans32 is released.
2001 First draft sequences of the human genome are released simultaneously by the Human
Genome Project33 and Celera Genomic

18
19
20
21
22
23
24
25
26
27
28
29
30
31
32
33

http://en.wikipedia.org/wiki/Hershey-Chase%20experiment
http://en.wikipedia.org/wiki/James%20D.%20Watson
http://en.wikipedia.org/wiki/Francis%20Crick
http://en.wikipedia.org/wiki/Rosalind%20Franklin
http://en.wikipedia.org/wiki/Albert%20Levan
http://en.wikipedia.org/wiki/Meselson-Stahl%20experiment
http://en.wikipedia.org/wiki/Howard%20Temin
http://en.wikipedia.org/wiki/Walter%20Gilbert
http://en.wikipedia.org/wiki/Kary%20Banks%20Mullis
http://en.wikipedia.org/wiki/Alec%20Jeffreys
http://en.wikipedia.org/wiki/Lap-Chee%20Tsui
http://en.wikipedia.org/wiki/Cystic%20Fibrosis
http://en.wikipedia.org/wiki/Haemophilus
http://en.wikipedia.org/wiki/Saccharomyces
http://en.wikipedia.org/wiki/C.%20elegans
http://en.wikipedia.org/wiki/Human%20Genome%20Project

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Genetics and Inheritance

2003 (14 April) Successful completion of Human Genome Project with 99% of the genome
sequenced to a 99.99% accuracy
2006 Marcus Pembrey and Olov Bygren publish Sex-specifics, male line trans-generational
responses in humans, a proof of epigenetics

16.2 Transcription and Translation

Figure 147
Transcription is the process of making RNA. In response to an enzyme RNA polymerase
breaks the hydrogen bonds of the gene. A gene is a segment of DNA which contains the
information for making a protein. As it breaks the hydrogen bonds it begins to move down
the gene. Next the RNA polymerase will line up the nucleotides so they are complementary.
Some types of RNA will leave the nucleus and perform a specific function.
Translation is the synthesis of the protein on the ribosome as the mRNA moves across the
ribosome. There are eleven basic steps to translation.
1. The mRNA base sequence determines the order of assembling of the amino acids to form
specific proteins.

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Inheritance
2. Transcription occurs in the nucleus, and once you have completed transcription the
mRNA will leave the nuecleus, and go into the cytoplasm where the mRNA will bind to a
free floating ribosome, where it will attach to a small ribosomal subunit.
3. Methionine-tRNA binds to the nucleotides AUG. AUG is known as the start codon and
is found at the beginning of each mRNA.
4. The complex then binds to a large ribosomal subunit. Methionine-tRNA is bound to the
P site of the ribosome.
5. Another tRNA containing a second amino acid (lysine) binds to the second amino acid.
Binding to the second condon of mRNA (on the A-site of the ribosome).
6. Peptidyl transferase, forms a peptide3 bond between the two amino acids (methionine
and lysine)
7. The first amino tRNA is released and mRNA is translocated one codon carrying the
second tRNA (still carrying the two amino acids) to the P site.
8. Another tRNA with attached amino acid (glutamine) moves into the A site and binds to
that codon.
9. It will now form a peptide bond with lysine and glutamine
10. Now the tRNA in the P site will be let go, and mRNA is translocated one codon, (the
tRNA with three amino acids) to the P site.
11. This will continue going until it reaches the stop codon (UAG) on the mRNA. Then this
codon will tell it to release the polypeptide chain.
These are some good sites to visit
A http://www.studiodaily.com/main/technique/tprojects/6850.html
B http://multimedia.mcb.harvard.edu/media.html
Select A the video of the Inner Life of a Cell. If you want to hear the descriptions in this
process go to B web site and select the Inner Life: view the animation.

16.3 Inheritance
Children inherit traits, disorders, and characteristics from their parents. Children tend to
resemble their parents especially in physical appearance. However they may also have the
same mannerisms, personality, and a lot of the time the same mental abilities or disabilities.
Many negatives and positives tend to "run in the family". A lot of the time people will use
the excuse "It runs in the family" for things that have alternative reasons, such as a whole
family may be overweight, yes it may "run in the family" but it could also be because of
all the hamburgers and extra mayo that they all eat. Or the fact that after they eat the
hamburgers they all sit on the couch and don't move for the rest of the evening. Children
may have the same habits (good or bad) as their parents, like biting their nails or enjoying
reading books. These things aren't inherited they are happening because children imitate
their parents, they want to be like mom or dad. Good examples are just as important as
good genes.

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Inheritance pattern
Autosomal dominant

Autosomal recessive

462

Description

Examples

Only one mutated copy of

the gene is needed for a person to be affected by an autosomal dominant disorder.
Each affected person usually has one affected parent.
There is a 50% chance that
a child will inherit the mutated gene. Many disease
conditions that are autosomal dominant have low penetrance, which means that
although only one mutated
copy is needed, a relatively
small proportion of those
who inherit that mutation
go on to develop the disease,
often later in life.
Two copies of the gene must
be mutated for a person to
be affected by an autosomal
recessive disorder. An affected person usually has
unaffected parents who
each carry a single copy
of the mutated gene (and
are referred to as carriers).
Two unaffected people who
each carry one copy of the
mutated gene have a 25%
chance with each pregnancy
of having a child affected by
the disorder.

Huntingtons disease, Neurofibromatosis 1, HBOC

syndrome, Hereditary nonpolyposis colorectal cancer

Cystic fibrosis, Sickle cell

anemia, Tay-Sachs disease,
Spinal muscular atrophy,
Muscular dystrophy

Inheritance
Inheritance pattern
X-linked dominant

Description

Examples

X-linked dominant disorders

are caused by mutations in
genes on the X chromosome.
Only a few disorders have
this inheritance pattern. Females are more frequently
affected than males, and
the chance of passing on
an X-linked dominant disorder differs between men
and women. The sons of a
man with an X-linked dominant disorder will not be
affected, and his daughters
will all inherit the condition.
A woman with an X-linked
dominant disorder has a 50%
chance of having an affected
daughter or son with each
pregnancy. Some X-linked
dominant conditions, such as
Aicardi Syndrome, are fatal
to boys, therefore only girls
have them (and boys with
Klinefelter Syndrome).

Hypophosphatemia, Aicardi
Syndrome

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Inheritance pattern
X-linked recessive

Y-linked

Mitochondrial

464

Description

Examples

X-linked recessive disorders are also caused by mutations in genes on the X

chromosome. Males are
more frequently affected
than females, and the chance
of passing on the disorder
differs between men and
women. The sons of a man
with an X-linked recessive
disorder will not be affected,
and his daughters will carry
one copy of the mutated
gene. With each pregnancy,
a woman who carries an Xlinked recessive disorder has
a 50% chance of having sons
who are affected and a 50%
chance of having daughters
who carry one copy of the
mutated gene.
Y-linked disorders are
caused by mutations on the
Y chromosome. Only males
can get them, and all of the
sons of an affected father
are affected. Since the Y
chromosome is very small, Ylinked disorders only cause
infertility, and may be circumvented with the help of
some fertility treatments.
This type of inheritance,
also known as maternal inheritance, applies to genes
in mitochondrial DNA. Because only egg cells contribute mitochondria to the
developing embryo, only
females can pass on mitochondrial conditions to their
children.

Hemophilia A, Duchenne
muscular dystrophy, Color
blindness, Turner Syndrome

Male Infertility

Leber's Hereditary Optic

Neuropathy (LHON)

Inheritance

16.3.1 Mechanisms of inheritance

A person's cells hold the exact genes that originated from the sperm and egg of his parents
at the time of conception. The genes of a cell are formed into long strands of DNA. Most of
the genes that control characteristic are in pairs, one gene from mom and one gene from dad.
Everybody has 22 pairs of chromosomes (autosomes) and two more genes called sex-linked
chromosomes. Females have two X (XX) chromosomes and males have an X and a Y (XY)
chromosome. Inherited traits and disorders can be divided into three categories: unifactorial
inheritance, sex-linked inheritance, and multifactor inheritance.

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16.3.2 Unifactorial Inheritance

Figure 148 Chart showing the possibilities of contracting a recessive defect, from two
carrier parents.

Traits such as blood type, eye color, hair color, and taste are each thought to be controlled
by a single pair of genes. The Austrian monk Gregor Mendel was the first to discover this
phenomenon, and it is now referred to as the laws of Mendelian inheritance. The genes
deciding a single trait may have several forms (alleles). For example, the gene responsible
for hair color has two main alleles: red and brown. The four possibilities are thus
Brown/red, which would result in brown hair, Red/red, resulting in red hair, Brown/brown,
resulting in brown hair, or Red/brown, resulting in red hair.

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Inheritance
The genetic codes for red and brown can be either dominant or recessive. In any case, the
dominant gene overrides the recessive.
When two people create a child, they each supply their own set of genes. In simplistic cases,
such as the red/brown hair, each parent supplies one "code", contributing to the child's hair
color. For example, if dad has brown/red he has a 50% chance of passing brown hair to his
child and a 50% of passing red hair. When combined with a mom who has brown/brown
(who would supply 100% brown), the child has a 75% chance of having brown hair and a
25% chance of having red hair. Similar rules apply to different traits and characteristics,
though they are usually far more complex.

16.3.3 Multifactorial inheritance

Some traits are found to be determined by genes and environmental effects. Height for
example seems to be controlled by multiple genes, some are "tall" genes and some are "short"
genes. A child may inherit all the "tall" genes from both parents and will end up taller than
both parents. Or the child my inherit all the "short" genes and be the shortest in the family.
More often than not the child inherits both "tall" and "short" genes and ends up about
the same height as the rest of the family. Good diet and exercise can help a person with
"short" genes end up attaining an average height. Babies born with drug addiction or alcohol
addiction are a sad example of environmental inheritance. When mom is doing drugs or
drinking, everything that she takes the baby takes. These babies often have developmental
problems and learning disabilities. A baby born with Fetal alcohol syndrome is usually
abnormally short, has small eyes and a small jaw, may have heart defects, a cleft lip and
palate, may suck poorly, sleep poorly, and be irritable. About one fifth of the babies born
with fetal alcohol syndrome die within the first weeks of life, those that live are often mentally
and physically handicapped.

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16.3.4 Sex-linked Inheritance

Figure 149

X-linked recessive inheritance

Sex-linked inheritance is quite obvious, it determines your gender. Male gender is caused
by the Y chromosome which is only found in males and is inherited from their fathers.
The genes on the Y chromosomes direct the development of the male sex organs. The x
chromosome is not as closely related to the female sex because it is contained in both males
and females. Males have a single X and females have double XX. The X chromosome is to
regulate regular development and it seems that the Y is added just for the male genitalia.
When there is a default with the X chromosomes in males it is almost always persistent
because there is not the extra X chromosome that females have to counteract the problem.

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Inheritance
Certain traits like colorblindness and hemophilia are on alleles carried on the X chromosome.
For example if a woman is colorblind all of her sons will be colorblind. Whereas all of her
daughters will be carriers for colorblindness.

16.3.5 Exceptions to simple inheritance

Our knowledge of the mechanisms of genetic inheritance has grown a lot since Mendel's
time. It is now understood, that if you inherit one allele, it can sometimes increase the
chance of inheriting another and can affect when or how a trait is expressed in an individuals
phenotype. There are levels of dominance and recessiveness with some traits. Mendel's
simple rules of inheritance does not always apply in these exceptions.

16.3.6 Polygenic Traits

Polygenic traits are traits determined by the combined effect of more than one pair of
genes. Human stature is an example of this trait. The size of all body parts from head to
foot combined determines height. The size of each individual body part are determined
by numerous genes. Human skin, eyes, and hair are also polygenic genes because they are
determined by more than one allele at a different location.

16.3.7 Intermediate Expressions

When there is incomplete dominance, blending can occur resulting in heterozygous individuals.
An example of intermediate expression is the pitch of a human male voice. Homozygous men
have the lowest and highest voice for this trait (AA and aa). The child killer Tay- Sachs is
also characterized by incomplete dominance.

16.3.8 Co-dominance
For some traits, two alleles can be co-dominant. Were both alleles are expressed in heterozygous individuals. An example of that would be a person with AB blood. These people have
the characteristics of both A and B blood types when tested.

16.3.9 Multiple-Allele Series

There are some traits that are controlled by far more alleles. For example, the human HLA
system, which is responsible for accepting or rejecting foreign tissue in our bodies, can have
as many as 30,000,000 different genotypes! The HLA system is what causes the rejection
of organ transplants. The multiple allele series is very common, as geneticists learn more
about genetics, they realize that it is more common than the simple two allele ones.

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16.3.10 Modifying and Regulator Genes

Modifying and regulator genes are the two classes of genes that may have an effect on how the
other genes function. Modifying Genes alter how other genes are expressed in the phenotype.
For example, a dominant cataracts gene may impair vision at various degrees, depending on
the presence of a specific allele for a companion modifying gene. However, cataracts can also
come from excessive exposure to ultraviolet rays and diabetes. Regulator Genes also known
as homoerotic genes, can either initiate or block the expression of other genes. They also
control a variety of chemicals in plants and animals. For example, Regulator genes control
the time of production of certain proteins that will be new structural parts of our bodies.
Regulator genes also work as a master switch starting the development of our body parts
right after conception and are also responsible for the changes in our bodies as we get older.
They control the aging processes and maturation.

16.3.11 Incomplete penetrates

Some genes are incomplete penetrate. Which means, unless some environmental factors are
present, the effect does not occur. For example, you can inherit the gene for diabetes, but
never get the disease, unless you were greatly stressed, extremely overweight, or didn't get
enough sleep at night.

16.4 Inherited Genetic Disease

Some of the most common inherited diseases are hemochromatosis, cystic fibrosis, sickle cell
anemia and hemophilia. They are all passed along from the parents and even if the parents
don't show signs of the disease they may be carriers which mean that all of the children they
have may be born with the disease. There is genetic testing that may be done prenatally to
determine if the baby is conflicted with one of these diseases.

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Inherited Genetic Disease

16.4.1 Hemochromatosis

Figure 150
a

Haemochromatosis types 1-3 are inherited in an autosomal recessivea fashion.

http://en.wikibooks.org/wiki/Recessive%20gene

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Genetics and Inheritance

Figure 151
a

Haemochromatosis type 4 is inherited in an autosomal dominanta fashion.

http://en.wikibooks.org/wiki/autosomal%20dominant

Even though most people have never heard of hemochromatosis it is the most common
inherited disease. About 1 in 300 are born with hemochromatis and 1 in 9 are carriers. The
main characteristic is the intake of too much iron into the inflicted body. Iron is crucial
to the workings of hemoglobin but too much iron is just as bad as too little iron. With
hemochromatosis deposits of iron form on almost every major organ especially the liver,
heart and pancreas, which causes complete organ failure. Hemochromatosis patients usually
absorb two or three times the iron that is needed for normal people. Hemochromatosis

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Inherited Genetic Disease

was first discovered in 1865 and most patients have Celtic ancestry dating back 60 or 70
generations.
Treatments for hemochromatosis
The most common treatment for hemochromatosis is to induce anemia and maintain it until
the iron storage is reduced. This is done by therapeutic phlebotomy. Phlebotomy is the
removal of a unit of blood (about 500 mls.) This must be done one to two times a week
and can take weeks, months, or years to complete. After this treatment some patients will
never have to do it again and others will have to do it many times over the course of their
life. Patients who undergo their recommended treatments usually go on to live a long and
healthy life. Patients who decide against treatment increase their chances of problems such
as organ failure -- or even death. Along with phlebotomy treatment, patients should stick
to a low iron diet and should not cook with iron cookware.

16.4.2 Cystic Fibrosis (CF)

Cystic fibrosis is a disease that causes thick, sticky mucus to build up in the lungs and
digestive tract. It is the most common lung disease in children and young adults and may
cause early death. The mucus builds up in the breathing passages of the lungs and in the
pancreas. The build up of the mucus results in terrible lung infections and digestion problems.
Cystic fibrosis may also cause problem with the sweat gland and a man's reproductive
system. There are more than 1,000 mutations of the CF gene, symptoms vary from person
to person. The most common symptoms are: No bowel movements for the first 24 to 48
hours of life, stools that are pale or clay colored, foul smelling or that float, infants that have
salty-tasting skin, recurrent respiratory infections like pneumonia, coughing or wheezing,
weight loss or low weight gain in childhood, diarrhea, delayed growth, and excessive fatigue.
Most patients are diagnosed by their first birthday but less severe cases sometimes aren't
caught until after 18 years of age. 40% of patients are over 18 years old and the average life
span of CF patients is about 35 years old, which is a huge increase over the last 30 years.
Patients usually die of lung complications.

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Genetics and Inheritance

Figure 152

CFTR protein - Molecular structure of the CFTR protein

Treatment for cystic fibrosis

In 2005 the U.S food and drug administration approved the first DNA based blood test to help
detect CF. Other tests to help detect CF include: Sweat chloride test, which is the standard
test for CF. High salt levels in the patients sweat is an indication of CF, Fecal fat test,
upper GI and small bowel series, and measurements of pancreatic function. After a diagnosis
has been made there are a number of treatments available, these include: Antibiotics for
respiratory infections, pancreatic enzyme replacement, vitamin supplements (mostly A, D,
E, and K), inhalers to open the airways, enzyme replacement therapy which makes it easier
to cough up the mucus, pain relievers, and in very severe cases, lung transplants.

16.4.3 Sickle cell anemia

Sickle cell anemia is an inherited disease of the red blood cells which causes abnormally
shaped red cells. A typical red blood cell has about 270 million hemoglobin molecules, which
bind with oxygen. In a person with sickle cell disease, one amino acid is changed in the
hemoglobin molecule, and the end result is misshapen red blood cells. In a patient with
sickle cell disease the red blood cells change from the normal round shape to the shape of a
sickle or "C" shaped. The abnormal shape causes the cells to get stuck in some blood vessels
which causes blockage in the vessel. This causes pain and can destroy organs because of the
lack of oxygen. Sickle cells live only 10 to 20 days and a normal cell lives about 120 days.

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Inherited Genetic Disease

Figure 153

Red blood cells with sickle-cell mutations.

This rapid death of blood cells leads to chronic anemia. Complications can include severe
pain, terrible infection, swelling of the feet and hands, stroke, damage to the eyes, and
damaged body organs. These effects can vary from person to person depending on the type
of sickle cell disease they have. Some patients are mostly healthy and others are in the
hospital more than they are out. Thanks to diagnosis and treatment advancements, most
children born with sickle cell grow up to have a normal and relatively healthy life. The
form of sickle cell is determined by which genes they inherit from the parents. When a
child inherits a sickle cell gene (hemoglobin gene) from each parent it is called hemoglobin
SS disease ( which is the formal name for sickle cell). When a child inherits a sickle cell
gene from one parent and a different abnormal gene from the other parent, it is a form

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of disease called hemoglobin SC disease or hemoglobin S-thalassemia. If a child inherits a
normal gene from one parent and a sickle cell gene from the other, the child will not have
sickle cell but will be a carrier and may pass it to their children. Sickle cell affects mostly
African Americans and some Latino Americans. A person who is a carrier (has one copy
of the gene) is resistant to malaria. This heterozygote advantage explains why the gene is
more common in people in equatorial regions, or who are descendants of such people (such
as African Americans).
Treatment for Sickle cell anemia
Sickle cell is diagnosed at birth with a simple blood test. If the first blood test is positive
then a second test is done just for confirmation. Because of the high risk of infections
that occur with sickle cell, early diagnosis is very important. Other than a bone marrow
transplant there is no known cure for sickle cell. Bone marrow transplants have a high risk
of rejection and aren't an available option for every patient. The patient would need a bone
marrow donor match with a low risk of rejection. Even without a cure, with the use of pain
medications and antibiotic treatments, children with sickle cell can live a long and happy
life. Blood transfusions are sometimes used to treat episodes of severe pain. For adults
who have recurrent pain episodes (at least 3 yearly), a cancer drug, hydroxyurea (marketed
as Droxia), has been approved to relieve symptoms. It appears to work by increasing the
flexibility of sickle cells.

16.4.4 Hemophilia
About two thirds of people who have Hemophilia have inherited it. For the other third,
there is no known cause for possessing the disorder. There are two types of hemophilia,
Type A and Type B. Both are caused by a low level or a complete absence of protein in the
blood. Without this protein, blood is not able to clot.
Some of the symptoms of Hemophilia are bleeding in the joints, knees, and ankles. Stiffness
without pain in the joints, stiffness with a lot of warmth,(most ability for movement is lost
due to swelling) blood in the urine or stool, excessive bleeding after surgery or loosing a
tooth, excessive bruising, abnormal menstrual bleeding, and nose bleeds that last for long
periods of time.
Hemophiliacs blood does not coagulate like a normal persons. Coagulation controls bleeding,
it changes blood from a liquid to a solid. Within seconds of a cut or scrape, platelets,
calcium and other tissue factors start working together to form a clot. Over a short time
the clot strengthens and then dissolves as the injury heals. Hemophiliacs are missing the
clotting factor, or it isn't working correctly which causes them to bleed for a longer time.
The most common myth is that a person with a bleeding disorder will bleed to death from a
minor wound or that their blood flows faster than somebody without a bleeding disorder.
Some of the risks hemophilia are: Scarring of the joints or joint disease, vision loss from
bleeding of the eyes, chronic anemia from blood loss, a neurological or psychiatric problem,
death which may occur from large amounts of blood loss or bleeding in the brain or other
vital organs. Most cases of hemophilia are caused from inherited disorders but sometimes
people can get it from vitamin K deficiency, liver disease, or treatments like prolonged use

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Inherited Genetic Disease

of antibiotics or anti coagulation drugs. Hemophilia is the best known bleeding disorder and
it has had the most research done on it, so hemophiliacs have a slight advantage over people
with other bleeding disorders.
Treatment for hemophilia
To treat Hemophilia, a Clotting Factor is needed. It is in the shape of powder kept in a
small, sterile glass bottle. It has to be kept in the fridge. When needed, The Clotting Factor
is mixed with sterile water, then one minute later it can be injected into a vein. It may also
be mixed with a large amount of water and injected through an IV.
There are over 140 centers that specialize in hemophilia. Most of these centers are "Comprehensive Care Facilities". Comprehensive care facilities provide all the services needed
by a hemophiliac and their family. Services provided include: Primary physician, nurse
coordinator, physiotherapist, and dentist. Hemophiliacs require a special dentist because
of the higher risk of bleeding. It is recommended that hemophiliacs go to the treatment
centers twice a year for a complete check-up.
The basic and most common treatment for patients with hemophilia A and B is factor
replacement therapy. Factor replacement therapy is the IV injection of Factor VIII and IX
concentrates which help control bleeding. This concentrate comes from two sources: human
plasma and genetically engineered cells made by DNA technology. This concentrate is what
the hemophiliac is lacking in their own genes. After the injection is given the patients blood
becomes "normal" for a couple of hours which gives time for a clot to from at the site of a
damaged blood vessel. This treatment is not a permanent cure, within about 3 days there is
no trace left in the system. Today's Factor treatments are much more concentrated than
they were in the past so very little is required even if the patient is going in for major surgery
or has a major injury. Treatments are also very convenient, they can be stored at home
in the fridge for up to 6 months. So if the patient is injured they don't need to go to the
hospital they can give themself an injection at home. After the injection it only takes about
15-20 minutes for the clotting process to begin. There is a risk of contracting other disease
such as AIDS from Factor VIII that is made from human plasma, but as technology gets
better the cases of AIDS has dropped. There is no possibility of contracting diseases from
genetic engineering Factor VIII.
Hemophiliacs can live a long life. The most common reason for early death among patients
has been from AIDS related complications.

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Genetics and Inheritance

16.5 Non-heritable Genetic Disorders

Figure 154

Karyotype of 21 trisomy-Down syndrome

Any disorder caused totally or in part by a fault (or faults) of the genetic material passed
from parent to child is considered a genetic disorder. The genes for many of these disorders
are passed from one generation to the next, and children born with a heritable genetic
disorder often have one or more extended family members with the same disorder. There
are also genetic disorders that appear due to spontaneous faults in the genetic material, in
which case a child is born with a disorder with no apparent family history.
Down Syndrome, also known as Trisomy 21, is a chromosome abnormality that effects one
out of every 800-1000 newborn babies. During anaphase II of meiosis the sister chromatids
of chromosome 21 fail to separate, resulting in an egg with an extra chromosome, and a fetus
with three copies (trisomy) of this chromosome. At birth this defect is recognizable because
of the physical features such as almond shaped eyes, a flattened face, and less muscle tone
than a normal newborn baby. During pregnancy, it is possible to detect the Down Syndrome
defect by doing amniocentesis testing. There is a risk to the unborn baby and it is not
recommended unless the pregnant mother is over the age of thirty-five. Other non-lethal
chromosomal abnormalities include additional osex chromosome abnormalities which is when
a baby girl (about 1 in 2,500)is born with one x instead of two (xx) this can cause physical
abnormalities and defective reproduction systems. Boys can also be born with extra X's
(XXY or XXXY) which will cause reproductive problems and sometimes mental retardation.
Chromosomal Abnormalities In most cases with a chromosomal abnormality all the
cells are affected. Defects can have anywhere from little effect to a lethal effect depending
on the type of abnormality. Of the 1 in 200 babies born having some sort of chromosomal
abnormality, about 1/3 of these results in spontaneous abortion. Abnormalities usually
form shortly after fertilization and mom or dad usually has the same abnormality. There is

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Mutant Genes
no cure for these abnormalities. Tests are possible early in pregnancy and if a problem is
detected the parents can choose to abort the fetus.

16.6 Mutant Genes

Mutation is a permanent change in a segment of DNA.
Mutations are changes in the genetic material of the cell. Substances that can cause genetic
mutations are called mutagen agents. Mutagen agents can be anything from radiation
from x-rays, the sun, toxins in the earth, air, and water viruses. Many gene mutations are
completely harmless since they do not change the amino acid sequence of the protein the
gene codes for.
Mutations can be good, bad, or indifferent. They can be good for you because their mutation
can be better and stronger than the original. They can be bad because it might take away
the survival of the organism. However, most of the time, they are indifferent because the
mutation is no different than the original.
The not so harmless ones can lead to cancer, birth defects, and inherited diseases. Mutations
usually happen at the time of cell division. When the cell divides, one cell contracts a defect,
which is then passed down to each cell as they continue to divide.
Teratogens refers to any environmental agent that causes damage during the prenatal period.
Examples of Common Teratogens:

drugs: prescription, non-prescription, and illegal drugs

tobacco, alcohol,
radiation,
environmental pollution,
infectious disease,
STD's,
Aids,
Parasites,

Sensitive period to teratogen exposure, in the embryonic period is most vital. Fetal damage
is minor.

16.7 Genetic Engineering

w:Genetic Engineering34 Genetic Engineering is where the DNA or gene gets changed by a
scientist to make a gene with the characteristics that they want it to have, and to get rid
of the characteristics that they don't want the gene to have. This process can be applied
towards any plant, animal, or person.
The main reason for genetic engineering is to "mass produce" a certain protein. Each cell
is responsible for producing a certain protein and these proteins can be used for medical

34

http://en.wikipedia.org/wiki/Genetic%20Engineering

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Genetics and Inheritance

treatment and diagnosis. The job of each gene is to control the production of a particular
protein in a living cell. If the gene responsible for synthesizing a important or useful protein
can be found, and if that gene can be inserted into another cell that can be made to
reproduce, then a colony of cells containing that gene can be grown and the protein will
be manufactured in large quantities. This process is responsible for insulin and growth
hormones and it is also used in vaccines to help prevent hepatitis and a treatment to help
prevent viral infections. It also helps in genetically engineering Factor VIII which is a
treatment for hemophilia.
The first step is to find the gene in the DNA of a cell that is responsible for the manufacturing
of the desired protein. Then that gene is either extracted or the exact chemical structure is
figures out to be synthesized. The last step is to insert the DNA into the recipient which is
done by using special enzymes to split a molecule of the recipients cell and inserting the
new gene.
There have been many steps taken to bring technology closer to being able to fix genetically
inherited diseases. Hopefully someday there will be a lot less babies born with genetic
diseases and disorders.

16.8 Gene Therapy

Gene therapy is a way to correct the defective genes that are the cause of disease development.
When the genes are altered proteins are not able to function normally and as a result of
this, defects can occur. Current gene therapy is still being experimented with, but in some
cases it is very effective.
Genes are carried on chromosomes and are the basic physical and functional parts of
hereditary. When there is a genetic disorder, gene therapy can help fix the problem either
permanently or at least temporarily. The most common form of gene therapy is to insert
a gene into a nonspecific place to replace a malfunctioning gene. Another method is gene
swapping, where an abnormal gene is replaced by a normal gene. Genes could also be
repaired through "selective reverse mutation" which returns the gene to it's original function.
The degree to which a gene is turned on or off can also be altered.
Gene therapy works on the principle belief that a virus genome can be manipulated to
remove disease causing genes and new therapeutic genes can be inserted in their place. These
new genes are called gene therapy vectors. (The virus container is the vector and the new
gene is the payload.)
[[Image:Gene therapy.jpg|right|thumb|340px|Gene therapy using an Adenovirus35 vector.
A new gene is inserted into an adenovirus vector, which is used to introduce the modified
DNA36 into a human cell. If the treatment is successful, the new gene will make a functional
protein37 .]]
A few of the different viruses used as gene therapy vectors are: Retroviruses - A class of
viruses that can create double-stranded DNA copies of their original RNA genomes. Theses
35
36
37

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http://en.wikibooks.org/wiki/Adenovirus
http://en.wikibooks.org/wiki/DNA
http://en.wikibooks.org/wiki/protein

Genetic Regulation of Development and Homeostasis

copies of its genomes can be mixed into the chromosomes of "host" cells. HIV is a type of
retrovirus. Adenoviruses - A class of viruses with double-stranded DNA genome that cause
respiratory, intestinal, and eye infections in humans. The common cold is an adenovirus.
Adeno-associated viruses - A class of small, single-stranded DNA viruses that can insert their
genetic material at a specific site on chromosome 19. (chromosome 19 represents about 2%
of the human genome and contains about 1,500 genes. Some of the genes included are genes
that code for insulin-dependent diabetes, myotonic dystrophy, migraines, and inherited high
blood cholesterol). A class of double-stranded DNA viruses that infect a particular cell type,
neurons, called Herpes simplex viruses is another common virus used in gene therapy.
It is the virus that causes cold sores.
Major advancements have been made in gene therapy. There are many new discoveries in
helping cure and treat diseases that claim millions of lives. Some of the disease that have
cures or treatments because of gene therapy include: Parkinson's, Huntington's, Cystic
Fibrosis, Some cancers, "Bubble Boy" syndrome and sickle cell. With technology jumping
ahead, maybe someday there will be a cure for every life threatening disease.

16.9 Genetic Regulation of Development and Homeostasis

It is very easy to think of Genetics as why I have blue eyes while both of my parents have
brown eyes. Or how hemophilia is passed down from mother to son, and not mother to
daughter. But Genetics is more in depth than that. At conception you started as a single
cell. That cell started to divide. You didnt increase in mass just in the number of cells.
Once the bundle of cells reached a certain number, things changed. You started gaining mass
by acquiring new resources (from your mother) and increasing in cell number. Your cells
specialized. Some cells became the liver. Others became heart, lungs, brain, and so forth.
Why is this? How did that little bundle of cells "know" when it was time to specialize? It is
because your DNA has regulatory control over your entire system. If it didnt, that bundle of
cells would just keep dividing as undifferentiated cells and never specialize, never gain form
or function. Thanks to the genetic regulatory control over your system, your anatomy forms
correctly with everything in its proper place. Even after fetal development gene regulation
still controls what each cell produces and how it functions. Puberty just doesnt happen
at the age of twelve. Puberty happens because genes in your genetic code are triggered by
your growth and development, causing your endocrine system to start producing the proper
hormones, thus causing you to mature sexually. w:Regulation of gene expression38 Even aging
is genetically controlled. The mechanisms of genetic regulation are not discussed here, but
it is worth noting that any step of gene expression may be modulated, from the DNA-RNA
transcription step to post-translational modification of a protein. Gene regulation gives the
cell control over structure and function, and is the basis for cellular differentiation. A cell
can also respond to changes in its environment by altering gene expression. For example, a
pancreatic cell exposed to high glucose levels releases pre-formed insulin that it was storing.
Yet, if the high levels of glucose continue, the cell will transcribe additional copies of the gene
for making insulin and thus increase insulin production to meet demand. This is homeostasis
in action.

38

http://en.wikipedia.org/wiki/Regulation%20of%20gene%20expression

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16.10 Glossary
Allele: one member of a pair of genes that occupy a specific position on a specific chromosome
Autosome: chromosome that is not a sex chromosome
Chromosome: threadlike strand of DNA and associated proteins in the nucleus of cells
that carries the genes and functions in the transmission of heredity information
Cystic Fibrosis: recessive genetic disorder affecting the mucus lining of the lungs, leading
to breathing problems and other difficulties
Fetal Alcohol Syndrome: combination of birth defects resulting form high (sometimes
low) alcohol consumption by the mother during pregnancy
Gene: is a segment of nucleic acid that contains the information necessary to produce a
functional product, usually a protein.
Genetics: is the science of genes, heredity, and the variation of organisms.
Genome: complete set of genetic information of an organism including DNA and RNA
Genotype: actual set of genes an organism has. It is the blue print of gentic material.
Hemochromatosis: metabolic disorder that causes increased absorption of iron, which is
deposited in the body tissues and organs; the iron accumulates in the body where it may
become toxic and causes damage
Hemoglobin: component of red blood cells that carries oxygen
Hemophilia: group of heredity disorders in which affected individuals fail to make enough
of certain proteins needed to form blood clots
Inheritance: characteristics given to a child by a parent
Modifying Gene: alters how other genes are expressed in the phenotype
Multifactorial Inheritance: trait or disorder determined by multiple genes and/or environmental effects
Phenotype: organisms physical appearance
Polygenic: trait whose expression is influenced by more than one gene
Regulator Genes: initiate or block the expression of other genes.
Sex-linked: pertaining to a trait of a disorder determined by the sex chromosome in a
persons cells or by the genes carried on those chromosomes
Sickle Cell Anemia: recessive disorder in which red blood cells take on an unusual shape,
leading to other problems with the blood
Synthesize: to make using biochemical processes
Unifactorial Inheritance: trait or disorder determined by a single pair of genes
Zygote: cell formed by the union of male and female gametes. A Zygote is a cell that is
the result of fertilization.

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Review questions

16.11 Review questions

Answers for these questions can be found here39
1. DNA is found on
A) endoplasmic reticulum
B) ribosomes
C) chromosomes
D) cytoplasm
2. Even though each cell has identical copies of all of the same genes, different cells
__________or ___________different genes
A) express, repress
B) genotype, phenotype
C) dominant, recessive
3. In diploid organisms, a dominant allele on one chromosome will
A) show the expression of a recessive allele
B) mask the expression of a recessive allele
C) show that there are dominant alleles on both chromosomes
D) none of the above
4. Transcription occurs in the
A) cytoplasm
B) golgi apparatus
C) mitochondria
D) nucleus
5. This is the start codon and is found at the beginning of each mRNA
A) AGU
B) GAU
C) UAG
D) GUA
E) AUG
6. Sara was born with cystic fibrosis, from this we could assume that
A) all of her siblings also have cystic fibrosis

39

http://en.wikibooks.org/wiki/Human_Physiology/Appendix_1:_answers_to_review_
questions#Genetics_and_inheritance

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Genetics and Inheritance

B) only her dad is a carrier
C) only her mom is a carrier
D) both of her parents are carriers
7. Jesse was born with a flattened face, almond eyes and less muscle tone; it could be
assumed that he has
A) a chromosome abnormality on chromosome 21
B) a chromosome abnormality on chromosome 19
C) a chromosome abnormality on chromosome 20
D) a chromosome abnormality on chromosome 22
E) No chromosome abnormality, these are his inherited traits
8. The most common inherited disease is
A) hemochromatosis
B) cystic fibrosis
C) sickle cell anemia
D) hemophilia
E) all of the above
9. Being a carrier of sickle cell anemia means that the person will
A) also be a carrier of hemophilia
B) be resistant to malaria
C) have children that all have sickle cell anemia
D) have children that all have malaria
E) none of the above
10. Hemophilia is
A) a Y linked disease
B) an XY linked disease
C) an X linked disease

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17 Human Development
17.1 Overview
We are born, we grow up, we age, and then we die. Unless disease or trauma occurs, most
humans go through the various stages of life described above. Human Development is the
process of growing to maturity. Traditionally, theories that explain senescence have generally
been divided between the programmed and stochastic theories of aging. Programmed theories
imply that aging is regulated by biological clocks operating throughout the life span. This
regulation would depend on changes in gene expression that affect the systems responsible for
maintenance, repair and defense responses. Stochastic theories blame environmental impacts
on living organisms that induce cumulative damage at various levels as the cause of aging.
Examples of environmental impacts range from damage to deoxyribonucleic acid (DNA),
damage to tissues and cells by oxygen radicals (widely known as free radicals countered by
the even more well known antioxidants), and cross-linking. However, aging is now seen as a
combination of genetic and environmental processes; a progressive failure of homeostatic
mechanisms involving maintenance and repair genes, stochastic events leading to molecular
damage and molecular heterogeneity, and chance events determining the probability of death.
Homeostasis, as we have seen throughout this book, is maintained through complex and
interacting systems, and aging is considered to be a progressive shrinkage of homeostatic
capabilities, mainly due to increased molecular heterogeneity. In this chapter we explore
the physiology of all stages of human development, with a particular emphasis on the aging
process.

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17.2 Apoptosis

Figure 155 A cell undergoing apoptosis.

In just one of many scenarios of apoptosis, the
process is triggered by another neighboring
cell; the dying cell eventually transmits
signals that tell the phagocytes, which are a
part of the immune system, to engulf it.

Apoptosis is the process of regulated cell death and removal. In some cases cell damage
can trigger apoptosis, but it is usually a normal function of the cell. Apoptosis results in
controlled auto digestion of the cells content. The cell membrane stays in place and the
cells contents are not dispersed. When this process is near completion, "eat me" signals,
like phosphatidylserine, appear on the surface of the cell membrane. This in turn attracts
phagocytic scavengers that complete the process of removing the dead cell without eliciting
an inflammatory response. Unlike necrosis, which is a form of cell death that results from
acute cellular injury, apoptosis is carried out in an ordered process that generally confers
advantages during an organism's life cycle.
Apoptosis Rates
The rate at which cells of the body die varies widely between different cell types. Some
cells, such as white blood cells, live for only a matter of hours while other cells can live
throughout the duration of the lifespan of the individual.
Homeostasis
Apoptosis is a regulated function that results in a relatively consistent number of cells in
the body. This balancing act is part of homeostasis (see chapter 1) that is required by

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living organisms. An example of this is that blood cells are constantly being produced
and apoptosis takes place to eliminate a similar number of older cells. Homeostasis was
discovered by Claude Bernard around the year 1851.
Development
Apoptosis also plays a key role in growth and development. An example of how apoptosis enables development is the differentiation of human fingers in a developing embryo.
Apoptosis is the function that enables the embryos fingers to separate.
Disorders
Too much apoptosis causes cell-loss disorders such as osteoporosis, whereas too little
apoptosis results in uncontrolled cell proliferation, namely cancer.

17.3 Growth and development

Growth and development is an ongoing process that begins at conception and continues
through the remainder of our lives. There is a broad spectrum of physical and psychological
changes that are part of the maturation and life of the individual.
Growth is a physical change that can be weighed and measured. Development is psychological
and social changes to the individual such as behaviors and thinking patterns. Growth and
development are two complimentary processes that together make up the individual.
Examples of this difference are all around us. One notable example involves infants. Infants
understand speech much earlier than their bodies have matured enough to physically perform
it. Thus it is evident that their speech patterns develop before the physical growth of their
vocal chords is adequate to facilitate speech.
The rate of development and growth varies dependent on many factors such as age and
genetic disposition. Babies grow at roughly the same pace and benchmarks for their physical
and social development are roughly standard. However, as any parent can tell you, no two
children develop exactly within the same time frame. Thus an appropriate time span should
be used. For example: one brother may gain weight faster than another. Growth spurts can
vary. Some children can speak entire sentences before their first year while others may not
speak at all until two or three. This creates a greater diversity among human beings.
The following chart focuses on reflexes of the developing infant.
Reflex
Eye blink

Stimulation
Bright light
shinning in
eyes or clap
hands by eyes

Response
closes eyelids
quickly

Age of disappearance
Permanent

Function
This reflex
protects the
infant from a
lot of stimulation

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Human Development
Reflex
Withdrawal

Stick sole
of foot with
stimulus like a
pin

Rooting

Touch cheek
near the corner of the
mouth

Sucking

Place fingers
in infant's
mouth

Swimming

Place the
baby in pool
of water face
down

Moro

Hold infant
in a cradling
horizontal
position and
slightly lower
the baby in
a fast motion
toward the
ground while
making a loud
sound supporting the
baby
Place the finger in baby's
palm and
press against
the palm

Palmar grasp

488

Stimulation

Response
This cause
the foot to
withdraw,
this occurs
with the use
of flexing of
the knee to
hip
The infants
head will turn
towards the
site of stimulation

The infant
will suck finger rhythmically
The baby
paddles and
kicks in swimming movements
The baby
will make a
embracing
motion and
arch its back
extending its
legs throwing its arms
outward, and
finally it will
bring arms
in toward its
body
The baby
will immediately grasp
the finger

Age of disappearance
Decreases
after the 10th
day of birth

3 weeks (due
to the voluntary response
that is now
capable for infant to do at
this time)
4 months
(voluntary
sucking will
come about)
4 to 6 month

6 months

3 to 4
months

Function
This is a protection for
the infant in
the instance
of unpleasant
tactile stimulation
This reflex
helps baby to
find the mothers nipple

This helps
with feeding

This helps
baby to
survive if
dropped into
the water
In the evolutionary past
this may have
helped the
baby cling to
the mother

This prepares
infant for
when voluntary grasping
comes about

Neonatal
Reflex

Stimulation

Tonic neck

Turn the
baby's head
to one side
while the
baby is awake

Stepping/marching

When you
hold the baby
under the arm
and permit
the bare feet
of the baby to
touch a flat
surface

Babinski

Touch the
foot in a
stroking manner form the
toe toward
the heel

Response
This will
cause the
baby to extend one arm
in front of its
eye on one
arm to the
side to which
the head has
been turned
The baby
will lift one
foot after the
other in a
stepping fashion

The baby's
toes will fan
out and curl
as the foot
twists in

Age of disappearance
4 months

2 months
(this applies
to a baby who
has gained
weight a baby
who is not
as heavy this
reflex may be
submissive)
8 to 12
months

Function
This may
prepare for
voluntary
reaching

This prepares
the baby for
voluntary
walking

Unknown

17.4 Neonatal
The neonatal period extends from birth to somewhere between 2 weeks and 1 month.
Immediately after the baby is born, uterine contractions force blood, fluid, and the placenta
from the mother's body. The umbilical cordthe baby's lifeline to it's motheris now
severed. Without the placenta to remove waste, carbon dioxide builds up in the baby's
blood. This fact, along with the actions of medical personnel, stimulates the control center
in the brain, which in turn responds by triggering inhalation. Thus the newborn takes its
first breath. As the newborn's lungs begin to function, the bypass vessels of fetal circulation
begin to close. The bypass connecting the atria of the heart, known as the foramen ovale,
normally closes slowly during the first year.
During this period the body goes through drastic physiological changes. The most critical
need is for the body to get enough oxygen as well as an adequate supply of blood. (The
respiratory and heart rate of a newborn is much faster than that of an adult.)

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Figure 156
delivery.

Newborn infant, just seconds after vaginal

17.4.1 The newborn's appearance

A newborn's skin is oftentimes grayish to dusky blue in color. As soon as the newborn
begins to breathe, usually within a minute or two of birth, the skin's color returns to normal
tones. Newborns are wet, covered in streaks of blood, and coated with a white substance
known as vernix caseosa, which is believed to act as an antibacterial barrier. The newborn
may also have Mongolian spots, various other birthmarks, or peeling skin, particularly at
the wrists, hands, ankles, and feet.
A newborn's shoulders and hips are narrow, the abdomen protrudes slightly, and the arms
and legs are relatively short. The average weight of a full-term newborn is approximately 7
1
2 pounds (3.2kg), but can be anywhere from 5.510 pounds (2.74.6kg). The average total
body length is 1420 inches (35.650.8cm), although premature newborns may be much
smaller. The Apgar score is a measure of a newborn's transition from the womb during the
first ten minutes of life.
A newborn's head is very large in proportion to the rest of the body, and the cranium is
enormous relative to his or her face. While the adult human skull is about 1/8 of the total
body length, the newborn's is twice that. At birth, many regions of the newborn's skull have
not yet been converted to bone. These "soft spots" are known as fontanels; the two largest
are the diamond-shaped anterior fontanel, located at the top front portion of the head, and
the smaller triangular-shaped posterior fontanel, which lies at the back of the head.
During labor and birth, the infant's skull changes shape to fit through the birth canal,
sometimes causing the child to be born with a misshapen or elongated head. This will
usually return to normal on its own within a few days or weeks. Special exercises sometimes
advised by physicians may assist the process.
Some newborns have a fine, downy body hair called lanugo. It may be particularly noticeable
on the back, shoulders, forehead, ears and face of premature infants. Lanugo disappears

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Neonatal
within a few weeks. Likewise, not all infants are born with lush heads of hair. Some may be
nearly bald while others may have very fine, almost invisible hair. Some babies are even
born with a full head of hair. Amongst fair-skinned parents, this fine hair may be blond,
even if the parents are not. The scalp may also be temporarily bruised or swollen, especially
in hairless newborns, and the area around the eyes may be puffy.

Figure 157
newborn

Traces of vernix caseosa on a full term

A newborn's genitals are enlarged and reddened, with male infants having an unusually
large scrotum. The breasts may also be enlarged, even in male infants. This is caused
by naturally-occurring maternal hormones and is a temporary condition. Females (and
even males) may actually discharge milk from their nipples, and/or a bloody or milky-like
substance from the vagina. In either case, this is considered normal and will disappear in
time.
The umbilical cord of a newborn is bluish-white in color. After birth, the umbilical cord
is normally cut, leaving a 12 inch stub. The umbilical stub will dry out, shrivel, darken,
and spontaneously fall off within about 3 weeks. Occasionally, hospitals may apply triple
dye to the umbilical stub to prevent infection, which may temporarily color the stub and
surrounding skin purple.
Newborns lose many of the above physical characteristics quickly. Thus prototypical older
babies look very different. While older babies are considered "cute", newborns can be
"unattractive" by the same criteria and first time parents may need to be educated in this
regard.
Neonatal jaundice
Neonatal jaundice is usually harmless: this condition is often seen in infants around the
second day after birth, lasting until day 8 in normal births, or to around day 14 in premature
births. Serum Bilirubin initially increase because a newborn does not need as many red
blood cells as it did as a fetus (since there is a higher concentration of oxygen in the air
than what was available through the umbilical vein). The newborn's liver processes the

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Human Development
breakdown of the extra red blood cells, but some bilirubin does build up in the blood.
Normally bilirubin levels drop to a low level without any intervention required. In babies
where the bilirubin levels are a concern (particularly in pre-term infants), a common
treatment is to use UV lights ("bili lights") on the newborn baby.

17.5 Changes in body Size and Muscle fat makeup

By the end of the first year an infant's height is increased by 50% and by the age of 2 the
baby will have grown 75% greater.
By 5 months a baby will have doubled its weight, and tripled its weight by the first year.
By the age of 2, a baby's weight will have quadrupled.
Infants and toddlers grow in little spurts over the first 21 months of life. A baby can go
through periods of 7 to 63 days with no growth but they can add as much as an inch in
one 24 hour period. During the day before a growth spurt, parents describe their babies as
irritable and very hungry.
The best way to estimate a child's physical maturity is to use skeletal age, a measure of
bone development. This is done by having a x-ray of the long bones of the body to see the
extent to which soft, pliable cartilage has hardened into bone.
Changes in body Proportions
Cephalocaudal trend means that growth occurs from head to tail. The head develops
more rapidly than the lower part of the body. At birth the head takes up to one fourth of
the total body length and legs only one third. The lower body catches up by age 2 and the
head accounts for only one fifth and legs for nearly one half of the body length.
Proximodistal trend means that head growth proceeds literally form near to far or from
center of the body outward.
At birth the brain is nearer its adult shape and size than any other physical structure. The
brain continues to develop at an astounding pace throughout infancy and toddlerhood.
The Brain Development
The neurons of infants and adults differ in 2 significant ways: Growth of neural fibers and
synapses increases connective structures. When synapses are formed, many surrounding
neurons die. This occurs in 20 to 80 percent of the brain region.
Dendrites synapses: Synapses are tiny gaps between neurons where fiber from different
neurons come close together but do not touch. Neurons release chemicals that cross the
synapses sending messages to one another. During the prenatal period the neural tube
produces far more neurons than the brain will ever need. Myelinization: The coating
of neural fibers with a fatty sheath called myelin that improves the efficiency of message
transfer. Multi-layered lipid cholesterol and protein covering produced by neuralgia cause a
rapid gain in overall size of brain due to neural fibers and myelination.
Synaptic pruning: Neurons seldom stimulated soon loose their synapses. Neurons not
needed at the moment return to an uncommitted state so they can support future development. However, if synaptic pruning occurs in old age neurons will lose their synapses.

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Infancy
If neurons are stimulated at a young age, even though neurons were pruned, they will be
stimulated again.
Cerebral Cortex: Surrounding the brain, it is the largest most complex brain structure.
The cortex is divided into four major lobes: occipital lobe, parietal lobe, temporal lobe, and
frontal lobe which is the last to develop.
Brain plasticity: The brain is highly plastic. Many areas are not yet committed to specific
functions. If a part of the brain is damaged, other parts can take over tasks that they would
not normally have handled.
Changing states of Arousal
How children develop more regular sleep patterns around 4 to 6 months of age: Sleep
patterns are more developed as the brain develops. It is not until the first year of life that
the secretion of melatonin, a hormone produced in the brain, affects more drowsiness in the
night than in the day. In addition, REM is decreased.

17.6 Infancy

Figure 158

Infant

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Human Development
Infancy is the period that follows the neonatal period and includes the first two years of life.
During this time tremendous growth, coordination and mental development occur. Most
infants learn to walk, manipulate objects and can form basic words by the end of infancy.
Another characteristic of infancy is the development of deciduous teeth.
Deciduous Teeth
Deciduous teeth, otherwise known as milk teeth, baby teeth, or primary teeth, are the first
set of teeth in the growth development of humans and many other animals. They develop
during the embryonic stage of development and erupt - become visible in the mouth - during
infancy. They are usually lost and replaced by permanent teeth, but in the absence of
permanent replacements, they can remain functional for many years. (Concise)
Deciduous teeth start to form during the embryo phase of pregnancy. The development
of deciduous teeth starts at the sixth week of development as the dental lamina. This
process starts at the midline and then spreads back into the posterior region. By the time
the embryo is eight weeks old, there are ten areas on the upper and lower arches that will
eventually become the deciduous dentition. These teeth will continue to form until they
erupt in the mouth. In the deciduous dentition there are a total of twenty teeth: five per
quadrant and ten per arch. In most babies the eruption of these teeth begins at the age of
six months and continues until twenty-five to thirty-three months of age. The first teeth
seen in the mouth are the mandibular centrals and the last are the maxillary second molars.
However it is not unheard of for a baby to be born with teeth.

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Infancy

Figure 159

Deciduous teeth.

The deciduous dentition is made up of centrals, laterals, canines, first molars, and second
molars; there is one in each quadrant, making a total of four of each tooth. All of these
are replaced with a permanent counterpart except for the first and second molars; they
are replaced by premolars. These teeth will remain until the age of six. At that time, the
permanent teeth start to appear in the mouth resulting in mixed dentition. The erupting
permanent teeth causes root resorption, where the permanent teeth push down on the
roots of the deciduous teeth causing the roots to be dissolved and become absorbed by the
forming permanent teeth. The process of shedding deciduous teeth and the replacement by
permanent teeth is called exfoliation. This will last from age six until age twelve. By age
twelve there are only permanent teeth remaining.
Deciduous teeth are considered essential in the development of the oral cavity by dental
researchers and dentists. The permanent teeth replacements develop from the same tooth
bud as the deciduous teeth; this provides a guide for permanent teeth eruption. Also the
muscles of the jaw and the formation of the jaw bones depend on the primary teeth in order
to maintain the proper space for permanent teeth. The roots of deciduous teeth provide
an opening for the permanent teeth to erupt through. These teeth are also needed in the
development of a childs ability to speak and chew their food correctly.

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17.7 Adolescence

Figure 160

American high school students

Adolescence is the period of psychological and social transition between childhood and
adulthood. Adolescence is the transitional stage of human development in which a juvenile
matures into an adult. This transition involves biological, social, and psychological changes,
though the biological ones are the easiest to measure objectively. The time is identified
with dramatic changes in the body, along with developments in a person's psychology and
academic career. In the onset of adolescence, children usually complete elementary school
and enter secondary education, such as middle school or high school. A person between
early childhood and the teenage years is sometimes referred to as a pre-teen or 'tween.
Physical maturation resulting from puberty leads to an interest in sexual activities, sometimes
leading to teenage pregnancy. Since teens may not be emotionally or mentally mature
enough or financially able to support children, sexual activity among adolescents is considered
problematic.
At this age there is also a greater probability of drug and alcohol use, mental health disorders
such as schizophrenia, eating disorders such as anorexia, and clinical depression. The
unstable emotions or lack of emotional intelligence among some adolescents may also lead
to youth crime.
Searching for a unique identity is one of the problems that adolescents often face. Some,
but not all, teenagers often challenge the authority or the rules as a way to establish their
individuality. They may crave adulthood and be eager to find their place in society. While
adolescents are eager to grow up and be treated like adults, they also idolize athletes, movie
stars and celebrities. They want to be like these role models - whether or not these role
models actually have qualities that should be aspired to.

17.7.1 Female
In females, puberty is caused by alterations in brain functions that result in increased
secretion by the hypothalamus of gonadotropin-releasing hormone (GnRH). Increased levels

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Adolescence
of GnRH stimulate secretion of pituitary gonadatrophins FSH and LH which cause follicle
development and estrogen secretion. Estrogen is responsible for accessory sex organs and
secondary sex characteristics. Menarche, the first menstrual cycle, occurs at about 12.5
years of age as a result of the release of FSH.
Breast development
The first physical sign of puberty in girls is usually a firm, tender lump under the center
of the areola(e) of one or both breasts, occurring on average at about 10.5 years. This is
referred to as thelarche. By the widely used Tanner staging of puberty, this is stage 2 of
breast development (stage 1 is a flat, prepubertal breast). Within 6-12 months, the swelling
has clearly begun in both sides, softened, and can be felt and seen extending beyond the
edges of the areolae. This is stage 3 of breast development. By another 12 months (stage
4), the breasts are approaching mature size and shape, with areolae and papillae forming a
secondary mound. In most young women, this mound disappears into the contour of the
mature breast (stage 5), although there is so much variation in sizes and shapes of adult
breasts that distinguishing advanced stages is of little clinical value.
Pubic hair in girls
Pubic hair is often the second unequivocal change of puberty. It is referred to as pubarche
and the pubic hairs are usually visible first along the labia. The first few hairs are described
as Tanner stage 2. Stage 3 is usually reached within another 612 months, when the hairs
are too numerous to count and appear on the mons as well. By stage 4, the pubic hairs
densely fill the "pubic triangle." Stage 5 refers to spread of pubic hair to the thighs and
sometimes as abdominal hair upward towards the umbilicus. In about 15% of girls, the
earliest pubic hair appears before breast development begins.
Vagina, uterus, ovaries
The mucosal surface of the vagina also changes in response to increasing levels of estrogen,
becoming thicker and a duller pink in color (in contrast to the brighter red of the prepubertal
vaginal mucosa). Whitish secretions (physiologic leukorrhea) are a normal effect of estrogen
as well. In the next 2 years following thelarche, the uterus and ovaries increase in size. The
ovaries usually contain small cysts visible by ultrasound.
Menstruation and fertility
w:Menarche1
The first menstrual bleeding is referred to as menarche. The average age of menarche in
American girls is about 12.7 years, usually about 2 years after thelarche. Menses (menstrual
periods) are not always regular and monthly in the first 2 years after menarche. Ovulation
is necessary for fertility, and may or may not accompany the earliest menses. By 2 years
after menarche, most girls are ovulating at least several times a year. Over 90% of girls
who experience menarche before age 13 years are experiencing very regular, predictable
menses accompanied by ovulation within 2 years, and a higher proportion of those with
later menarche may not establish regular ovulation for 4 years or more. However, initiation
of ovulation after menarche is not inevitable, and a high proportion of girls with continued

http://en.wikipedia.org/wiki/Menarche

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Human Development
irregularity several years from menarche will continue to have prolonged irregularity and
anovulation, and are at higher risk for reduced fertility.
Pelvic shape, fat distribution, and body composition
During this period, also in response to rising levels of estrogen, the lower half of the pelvis
widens. This prepares the body for the time when she will give birth by enlarging the birth
canal. Fat tissue increases to a greater percentage of the body composition than in males,
especially in the typical female distribution of breasts, hips, and thighs. This produces the
typical female body shape. Also, the fat goes to the buttocks of a girl, giving their buttocks
more shape and curve.
Body and facial hair in girls
In the months and years following the appearance of pubic hair, other areas of skin which
respond to androgens develop heavier hair (androgenic hair) in roughly the following sequence:
underarm (axillary) hair, perianal hair, upper lip hair, sideburn (preauricular) hair, and
periareolar hair. Arm and leg hair becomes heavier gradually over a period of 10 years or
more. While the appearance of hair in some of these areas is not always wanted, particularly
in Western culture, it rarely indicates a hormone imbalance unless it occurs elsewhere as
well, such as under the chin and in the midline of the chest.
Height growth in girls
The estrogen-induced pubertal growth spurt in girls begins at the same time the earliest
breast changes begin, or even a few months before, making it one of the earliest manifestations
of puberty in girls. Growth of the legs and feet accelerates first, so that many girls have
longer legs in proportion to their torso in the first year of puberty. The rate of growth tends
to reach a peak velocity (as much as 7.5-10 cm or 3-4 inches per year) midway between
thelarche and menarche and is already declining by the time menarche occurs. In the 2
years following menarche most girls grow about 5 cm (2 inches) before growth ceases at
maximal adult height. This last growth primarily involves the spine rather than the limbs.
Body odor, skin changes, and acne

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Adolescence

Figure 161

Acne on the face and body.

Rising levels of androgens can change the fatty acid composition of perspiration, resulting in
a more "adult" body odor. This often precedes thelarche and pubarche by 1 or more years.
Another androgen effect is increased secretion of oil (sebum) from the skin. This change
increases the susceptibility to acne vulgaris, a characteristic affliction of puberty greatly
variable in its severity.

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17.7.2 Male
The onset of puberty for males is similar to that of females. GnRH secretion from the
hypothalamus results in an increase in pituitary gonadatropins secretion of LH / ICSH
and FSH. The pituitary gonadatropins stimulate the seminiferous tubules and testosterone
secretion. Testosterone causes changes in the accessory reproductive organs, secondary sex
characteristics and male sex drive.
Testicular size, function, and fertility
In boys, testicular enlargement is the first physical manifestation of puberty. It is termed
gonadarche. The testes in prepubertal boys change little in size from about 1 year of age
to the onset of puberty, averaging about 23 cc in volume and about 1.5-2 cm in length.
Testicular size continues to increase throughout puberty, reaching maximal adult size about
6 years later. While 18-20 cc is reportedly an average adult size, there is wide variation in
the normal population.
The testes have two primary functions: to produce hormones and to produce sperm. The
Leydig cells produce testosterone (as described below), which in turn produces most of
the changes of male puberty. However, most of the increasing bulk of testicular tissue is
spermatogenic tissue (primarily Sertoli and interstitial cells). The development of sperm
production and fertility in males is not as well documented. Sperm can be detected in the
morning urine of most boys after the first year of pubertal changes (and occasionally earlier).
Genitalia
A boy's penis grows little from the fourth year of life until puberty. Average prepubertal
penile length is 4 cm. The prepubertal genitalia are described as stage 1. Within months
after growth of the testes begins, rising levels of testosterone promote growth of the penis and
scrotum. This earliest discernible beginning of pubertal growth of the genitalia is referred
to as stage 2. The penis continues to grow until about 21 years of age, reaching an average
adult size of about 7-15.5 cm.
Although erections and orgasms occur in prepubertal boys, they become much more common
during puberty, accompanied by a markedly increased libido. Ejaculation becomes possible
early in puberty; prior to this boys may experience dry orgasms. Emission of seminal fluid
may occur due to masturbation or spontaneously during sleep (commonly termed a wet
dream, and more clinically called a nocturnal emission). The ability to ejaculate is a fairly
early event in puberty compared to the other characteristics. However, in parallel to the
irregularity of the first few periods of a girl, for the first one or two years after a boy's first
ejaculation, his seminal fluid may contain few active sperm.
Pubic hair in boys
Pubic hair often appears on a boy shortly after the genitalia begin to grow. As in girls, the
first appearance of pubic hair is termed pubarche and the pubic hairs are usually first visible
at the dorsal (abdominal) base of the penis. The first few hairs are described as stage 2.
Stage 3 is usually reached within another 612 months, when the hairs are too numerous to
count. By stage 4, the pubic hairs densely fill the "pubic triangle." Stage 5 refers to spread
of pubic hair to the thighs and upward towards the umbilicus as part of the developing
abdominal hair.

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Body and facial hair in boys
In the months and years following the appearance of pubic hair, other areas of skin which
respond to androgens develop heavier hair (androgenic hair) in roughly the following
sequence: underarm (axillary) hair, perianal hair, upper lip hair, sideburn (preauricular)
hair, periareolar hair, and the rest of the beard area. Arm, leg, chest, abdominal, and back
hair become heavier more gradually. There is a large range in amount of body hair among
adult men, and significant differences in timing and quantity of hair growth among different
ethnic groups.
Voice change
Under the influence of androgens, the voice box, or larynx, grows in both genders. This
growth is far more prominent in boys, causing the male voice to drop, rather abruptly, about
one octave, because the larger vocal folds have a lower fundamental frequency. Occasionally,
this is accompanied by cracking and breaking sounds in the early stages. Most of the voice
change happens during stage 4 of male puberty around the time of peak growth. However,
it usually precedes the development of significant facial hair by several months to years.
Height growth in boys
Compared to girls' early growth spurt, growth accelerates more slowly in boys and lasts
longer, resulting in a taller adult stature among males than females (on average about 10 cm
or 4 inches). The difference is attributed to the much greater potency of estradiol compared
to testosterone in promoting bone growth, maturation, and epiphyseal closure. In boys,
growth begins to accelerate about 9 months after the first signs of testicular enlargement and
the peak year of the growth spurt occurs about 2 years after the onset of puberty, reaching
a peak velocity of about 8.512 cm or 3.55 inches per year. The feet and hands experience
their growth spurt first, followed by the limbs, and finally ending in the trunk. Epiphyseal
closure and adult height are reached more slowly, at an average age of about 17.5 years. As
in girls, this last growth primarily involves the spine rather than the limbs.
Male musculature and body shape
By the end of puberty, adult men have heavier bones and nearly twice as much skeletal
muscle. Some of the bone growth (e.g., shoulder width and jaw) is disproportionately greater,
resulting in noticeably different male and female skeletal shapes. The average adult male
has about 150% of the lean body mass of an average female, and about 50% of the body fat.
This muscle develops mainly during the later stages of puberty, and muscle growth can
continue even after a male is biologically adult. The peak of the so-called "strength spurt,"
the rate of muscle growth, is attained about one year after a male experiences his peak
growth rate.
Breast development in boys: pubertal gynecomastia
Estradiol is produced from testosterone in male puberty as well as female, and male breasts
often respond to the rising estradiol levels. This is termed gynecomastia. In most boys, the
breast development is minimal, similar to what would be termed a "breast bud" in a girl,
but in many boys, breast growth is substantial. It usually occurs after puberty is underway,
may increase for a year or two, and usually diminishes by the end of puberty. It is increased
by extra adipose tissue if the boy is overweight.

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Although this is a normal part of male puberty, breast development for some boys is as
unwelcome as upper lip hair in girls. If the boy's distress becomes too substantial during
development, breast tissue can be removed and corrected surgically.

17.8 Adulthood
w:adult2 The term "adult" generally refers to a fully developed person from maturity (the
end of puberty) onward. The age at which a person is physiologically an adult is age 17
for females and age 18 for males. Adulthood can also refer to a person's ability to care for
them self independently, and raise a family of their own; or it can simply mean reaching a
specified age. Graduating high school, residing in one's own residence and attaining financial
independence are all synonymous with adulthood in the United States.

17.8.1 Adult characteristics

There are some qualities that symbolize adultness in most cultures. Not always is there a
concordance between the qualities and the physical age of the person.
The adult character is comprised of:

Self-control - restraint, emotional control.

Stability - stable personality, strength.
Independence - ability to self-regulate.
Seriousness - ability to deal with life in a serious manner.
Responsibility - accountability, commitment and reliability.
Method/Tact - ability to think ahead and plan for the future, patience.
Endurance - ability and willingness to cope with difficulties that present themselves.
Experience - breadth of mind, understanding.
Objectivity - perspective and realism.

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Adulthood

Figure 162 This diagram shows Maslow's hierarchy of needs, represented as a pyramid
with the more primitive needs at the bottom.

Abraham Maslow, a psychologist, developed Maslow's Hierarchy of Needs. It is a chart

outlining basic needs that a person must meet to function and survive in life. It also attempts
to explain what motivates people in life. The needs on the lower level must be met before
moving up the ladder, as the higher needs only come into focus once all the needs that are
lower down in the pyramid are satisfied. People can get stuck on levels and some people
may never reach certain levels because of circumstances in their life. When one stage is
fulfilled you naturally move to the next.
Physical or Physiological: These include shelter, oxygen, food, water, rest and elimination, all of which are vital to a person's life and essential to survival.
Security or Safety: This involves not only actually being secure and safe, but also the
feeling of safety and security. This is something that people typically learn from their
childhood and something that helps lay the groundwork for developing other skills and
moving up to the next step in the ladder.
Social (Love/Belonging): This involves developing friendships and eventually relationships. This involves emotionally-based relationships in general, such as friendship, sexual
intimacy, and having a supportive and communicative family.
Esteem: This is where people learn to develop self-esteem and confidence. According
to Maslow, all humans have a need to be respected, to have self-respect, and to respect
others. People need to engage themselves in order to gain recognition and have an activity
or activities that give the person a sense of contribution, be it in a profession or hobby,

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Self-Actualization: The highest level you can reach according to Maslow. Maslow writes
the following of self-actualizing people:
They embrace the facts and realities of the world (including themselves) rather than
denying or avoiding them.
They are spontaneous in their ideas and actions.
They are creative.
They are interested in solving problems; this often includes the problems of others.
Solving these problems is often a key focus in their lives.
They feel a closeness to other people, and generally appreciate life.
They have a system of morality that is fully internalized and independent of external
authority.
They have discernment and are able to view all things in an objective manner. Prejudices
are absent.
In short, self-actualization is reaching one's fullest potential.
Most people accomplish the two lower levels in their lifetime, but may get stuck on upper
levels. While self-actualization is a useful concept to many, others insist there is no proof
that every individual has this capacity or even the goal to achieve it.

17.9 Menopause
w:Menopause3
Menopause occurs as the ovaries stop producing estrogen, causing the reproductive system
to gradually shut down. As the body adapts to the changing levels of natural hormones,
vasomotor symptoms such as hot flashes and palpitations, psychological symptoms such
as increased depression, anxiety, irritability, mood swings and lack of concentration, and
atrophic symptoms such as vaginal dryness and urgency of urination appear. Together
with these symptoms, the woman may also have increasingly scanty and erratic menstrual
periods.
Technically, menopause refers to the cessation of menses; whereas the gradual process
through which this occurs, which typically takes a year but may last as little as six months
or more than five years, is known as climacteric. Popular use, however, replaces climacteric
with menopause. A natural or physiological menopause is that which occurs as a part of
a woman's normal aging process. However, menopause can be surgically induced by such
procedures as hysterectomy (when this procedure includes oophorectomy, removal of the
ovaries).
The average onset of menopause is 50.5 years, but some women enter menopause at a younger
age, especially if they have suffered from cancer or another serious illness and undergone
chemotherapy. Premature menopause (or premature ovarian failure) is defined as menopause
occurring before the age of 40, and occurs in one percent of women. Other causes of
premature menopause include autoimmune disorders, thyroid disease, and diabetes mellitus.
Premature menopause is diagnosed by measuring the levels of follicle stimulating hormone

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Menopause
(FSH) and luteinizing hormone (LH); the levels of these hormones will be higher if menopause
has occurred. Rates of premature menopause have been found to be significantly higher in
both fraternal and identical twins; approximately five percent of twins reach menopause
before the age of 40. The reasons for this are not completely understood. Transplants of
ovarian tissue between identical twins have been successful in restoring fertility.
Post-menopausal women, especially Caucasian women of European descent, are at increased
risk of osteoporosis.
Animals other than human beings rarely experience menopause, possibly because they simply
do not live long enough to reach it. However, recent studies have shown menopause in
gorillas, with an average age of 44 at onset.
Perimenopause refers to the time preceding menopause, during which the production of
hormones such as estrogen and progesterone diminishes and becomes more irregular. During
this period fertility diminishes. Menopause is arbitrarily defined as a minimum of twelve
months without menstruation. Perimenopause can begin as early as age 35, although it
usually begins much later. It can last for a few months or for several years. The duration of
perimenopause cannot be predicted in advance.

17.9.1 Grandmother Hypothesis

Human females have the unique distinction of being one of the only species to stop reproduction well before the end of their life span. This evolutionary distinction is odd because most
other species continue to reproduce until death, thus maximizing the number of offspring they
produce. The grandmother hypothesis essentially states that the presence of a grandmother
has beneficial effect on the survival of an infant. Humans are one of the slowest developing
species in the animal kingdom, and unlike many species, infants, toddlers and children must
be continuously cared for to ensure their survival. (Compare that to the salmon that swims
up stream, spawns and dies.)

17.9.2 Etiology
The cessation of menses is the result of the eventual atresia (degeneration and reabsorption)
of almost all oocytes in the ovaries. This causes an increase in circulating FSH and LH levels
as there are a decreased number of oocytes responding to these hormones and producing
estrogen. This decrease in the production of estrogen leads to the post-menopausal symptoms
of hot flashes, insomnia, osteoporosis, atherosclerosis, vaginal atrophy and depression.
Cigarette smoking has been found to decrease the age of menopause by as much as one year
however, premature menopause (before the age of 40) is generally idiopathic.

17.9.3 Symptoms
The clinical features of menopause are caused by the estrogen deficiency.
vasomotor instability
hot flashes, hot flushes

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sleep disturbances
Urogenital atrophy
dyspareunia
itching
dryness
bleeding
urinary frequency
urinary urgency
urinary incontinence
skeletal

Breast Atrophy
skin thinning
decreased elasticity
Psychological
Mood Disturbance

irritability
fatigue
decreased libido
memory loss
depression

Treatments: Medical treatments for menopausal symptoms have been developed. Most
notably, Hormone Replacement Therapy (HRT), has been used to reduce the weakening of
bones (known as osteoporosis). However, some women have resisted the implication that
menopause is a disorder, seeing it as a natural stage of life. There has also been scientific
controversy over whether the benefits of HRT outweigh the risks. For many years, women
were advised to take hormone therapy after menopause to reduce their risk of heart disease
and various aspects of aging. However, a large, randomized, controlled trial (the Women's
Health Initiative) found that women undergoing HRT had an increased risk of Alzheimer's
disease, breast cancer, heart disease and stroke.

17.9.4 Osteoporosis
Osteoporosis is a skeletal disease resulting in bone loss and changes in the bone quality that
leads to diminished bone strength and an increased risk to sustain fractures. The main
cause of osteoporosis is a loss estrogen following menopause. Osteoporosis can be prevented
and treated using a number of different drugs and lifestyle modifications including proper
diet, exercise and hormone replacement therapy. The link to Wikipedia Osteoporosis is a
great source of additional information.
Preventing Osteoporosis The old saying that an ounce of prevention is worth a pound
of cure holds true for osteoporosis. In researching osteoporosis I found that while there are
some treatments for osteoporosis, a healthy lifestyle throughout your life is a much more
effective way of combating the effects of this disease. It is generally acknowledged that
a regular weight bearing exercise plan is helpful in maintaining bone mass. Additionally,

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adequate dietary calcium and vitamin D intake throughout ones life are important factors
in building up and maintaining bone mass.
Estrogen and progesterone treatments in postmenopausal women have proven to be effective
in treating bone loss. There are also two groups of drugs that interfere with the re-absorption
of bone by osteoclasts called bisphosphonates and lective estrogen receptor modulators
(SERMS).
An estimated 52 million men and woman will be afflicted with crumbling, weakened bone's
by the year 2010. Osteoporosis is three to four times more common in woman than men.
While some men do get osteoporosis, they are less likely to do so because men have frames
that are 25 percent larger and heavier than women. Women are also more susceptible to
the disease because they are more likely than a man to go on crash diets. This kind of diet
may interfere with the three main factors associated with osteoporosis and having healthy
bones: having enough vitamin D, having enough calcium, and having enough estrogen.
There are approximately 1 million to 1.3 million hip fractures every year that are related to
osteoporosis. Men on steroids, people with arthritis, people undergoing chemotherapy, along
with those suffering from anorexia all have an increased chance of having osteoporosis.
Osteoporosis related links
Wikipedia Osteoporosis Page4 This is a wikipedia link with a complete discussion of osteoporosis.
National Osteoporosis Foundation5 This page links to the National Osteoporosis Foundation

17.10 Old Age

Figure 163

4
5

Hmong women

http://en.wikipedia.org/wiki/Osteoporosis
http://www.nof.org/osteoporosis/

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17.10.1 Why do people age?

Some researchers believe we are programmed by an internal biological clock to age. The
idea is that each type of cell, tissue and organ is like a clock that ticks at its own pace. In
the body our cells divide 80 to 90 times at the most. At the end of each chromosome there
are repeated stretches of DNA called telomeres. A bit of each telomere is lost during every
cell division. When only a nub remains the cells stop dividing and die.
A different hypothesis is that aging is a result of accumulated damage to DNA from
environmental attacks and a decline in DNA's mechanism of self repair. Things such as
free radicals attack DNA and other molecules causing structural changes. These changes in
DNA endanger the synthesis of enzymes and other proteins that are required for life. This
damage interferes with cell division.
Most researchers believe that aging is a combination of an internal clock that ticks out the
life span of cells and the accumulation damage to DNA.

17.11 Old Age Diseases

17.11.1 Diabetes
Diabetes mellitus is a disease characterized by persistent hyperglycemia (high blood sugar
levels), resulting either from inadequate secretion of the hormone insulin, an inadequate
response of target cells to insulin, or a combination of these factors. Diabetes is a metabolic
disease requiring medical diagnosis, treatment and lifestyle changes
Type 1 diabetes mellitus is characterized by loss of the insulin-producing beta cells of the
islets of Langerhans of the pancreas. Sensitivity and responsiveness to insulin are usually
normal, especially in the early stages. This type comprises up to 10% of total cases in North
America and Europe, though this varies by geographical location. This type of diabetes can
affect children or adults, but has traditionally been termed "juvenile diabetes" because it
represents a majority of cases of diabetes affecting children. The most common cause of beta
cell loss leading to type 1 diabetes is autoimmune destruction, accompanied by antibodies
directed against insulin and islet cell proteins. The principal treatment of type 1 diabetes,
even from the earliest stages, is replacement of insulin. Without insulin, ketosis and diabetic
ketoacidosis can develop.
Type 2 diabetes mellitus is due to a combination of defective insulin secretion and defective
responsiveness to insulin (often termed reduced insulin sensitivity). In early stages the
predominant abnormality is reduced insulin sensitivity, characterized by elevated levels of
insulin in the blood. The initial defect of insulin secretion is subtle and initially involves only
the earliest phase of insulin secretion. In the early stages, hyperglycemia can be reversed
by a variety of measures and medications that improve insulin sensitivity or reduce glucose
production by the liver, but as the disease progresses the impairment of insulin secretion
worsens, and therapeutic replacement of insulin often becomes necessary. Type 2 diabetes is
quite common, comprising 90% or more of cases of diabetes in many populations. There is a
strong association with obesity and with aging, although in the last decade it has increasingly

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begun to affect older children and adolescents. In the past, this type of diabetes was often
termed adult-onset diabetes or maturity-onset diabetes.
Gestational diabetes, Type III, also involve a combination of inadequate insulin secretion and
responsiveness, resembling type 2 diabetes in several respects. It develops during pregnancy
and may improve or disappear after delivery. Even though it may be transient, gestational
diabetes may damage the health of the fetus or mother, and about 40% of women with
gestational diabetes develop type 2 diabetes later in life.

17.11.2 Congestive Heart Failure

Congestive heart failure (CHF), also called congestive cardiac failure (CCF) or just heart
failure, is a condition that can result from any structural or functional cardiac disorder that
impairs the ability of the heart to fill with or pump a sufficient amount of blood throughout
the body. It is not to be confused with "cessation of heartbeat", which is known as asystole,
or with cardiac arrest, which is the cessation of normal cardiac function in the face of heart
disease. Because not all patients have volume overload at the time of initial or subsequent
evaluation, the term "heart failure" is preferred over the older term "congestive heart failure".
Congestive heart failure is often undiagnosed due to a lack of a universally agreed definition
and difficulties in diagnosis, particularly when the condition is considered "mild".

17.11.3 Stroke

Figure 164

Stroke

A stroke, also known as cerebrovascular accident (CVA), is an acute neurologic injury

whereby the blood supply to a part of the brain is interrupted. Stroke can also be said to be
a syndrome of sudden loss of neuronal function due to disturbance in cerebral perfusion.
This disturbance in perfusion is commonly on the arterial side of the circulation, but can be
on the venous side.
The part of the brain with disturbed perfusion can no longer receive adequate oxygen carried
by the blood; brain cells are therefore damaged or die, impairing function from that part of
the brain. Stroke is a medical emergency and can cause permanent neurologic damage or
even death if not promptly diagnosed and treated. It is the third leading cause of death and
adult disability in the US and industrialized European nations. On average, a stroke occurs

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every 45 seconds and someone dies every 3 minutes. Of every 5 deaths from stroke, 2 occur
in men and 3 in women.

17.11.4 Progeria
The term Progeria narrowly refers to Hutchinson-Gilford Progeria syndrome, but the term
is also used more generally to describe any of the so-called "accelerated aging diseases". The
word progeria is derived from the Greek for "prematurely old". Because the "accelerated
aging" diseases display different aspects of aging, but never every aspect, they are often
called "segmental progerias" by biogerontologists. Hutchinson-Gilford Progeria syndrome
is an extremely rare genetic condition which causes physical changes that resemble greatly
accelerated aging in sufferers. The disease affects between 1 in 4 million (estimated actual)
and 1 in 8 million (reported) newborns. Currently, there are approximately 40-45 known
cases in the world. There is no known cure. Most people with progeria die around 13 years
of age. Progeria is of interest to scientists because the disease may reveal clues about the
process of aging. Unlike most other "accelerated aging diseases" (such as Werner's syndrome,
Cockayne's syndrome or xeroderma pigmentosum), progeria is not caused by defective DNA
repair. It is caused by mutations in a LMNA (Lamin A protein) gene on chromosome 1.
Nuclear lamina is a protein scaffold around the edge of the nucleus that helps organize
nuclear processes such as RNA and DNA synthesis.

17.12 The effects of Aging on the Body

17.12.1 Cardiovascular System
The heart loses about 1% of its reserve plumbing capacity every year after we turn 30.
Change in blood vessels that serve brain tissue reduce nourishment to the brain, resulting in
the malfunction and death of brain cells. By the time we turn 80, cerebral blood flow is 20%
less, and renal blood flow is 50% less than when we were age 30. As we age our heart goes
through certain structural changes: the walls of the heart thicken and the heart becomes
heavier, heart valves stiffen and are more likely to calcify, and the aorta, the major vessel
carrying blood out of the heart, becomes larger. w:Heart Attack6
Heart Attack / Myocardial infarction
Acute myocardial infarction (AMI or MI), commonly known as a heart attack, is a disease
that occurs when the blood supply to a part of the heart is interrupted, causing death
of heart tissue. It is the leading cause of death for both men and women all over the
world. The term myocardial infarction is derived from myocardium (the heart muscle) and
infarction (tissue death). The phrase "heart attack" sometimes refers to heart problems
other than MI, such as unstable angina pectoris and sudden cardiac death.
Congestive Heart Failure

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In the elderly, ventricular diastolic stiffness can lead to pulmonary circulatory congestion.
Aortic stenosis and aortic insufficiency, elevate left ventricular preload to the point where
the left ventricle becomes stiff and noncompliant, and is common in people 75 years of
age or older. Elevated pressures are transmitted to the pulmonary vasculature and lead to
pulmonary edema.

17.12.2 Musculoskeletal System

Bones
Aging is accompanied by the loss of bone tissue. The haversian systems in compact bone
undergo slow erosion, lacunae are enlarged, canals become widened, and the endosteal
cortex converts to spongy bone. The endosteal surface gradually erodes until the rate
of loss exceeds the rate of deposition. Bone remodeling cycle takes longer to complete
because bone cells slow in the rate of resorption and deposition of bone tissue. The rate
of mineralization also slows down. The number of bone cells also decreases because the
bone marrow becomes fatty and unable to provide an adequate supply of precursor cells.
Because bones become less dense, they become more prone to fractures. Although bone
degeneration is inevitable, it is variable if steps are taken before the mid-twenties -around
this time our bones break down faster than they rebuild. Bone density increases when our
bones are stressed, so physical activity is important. Vitamins and good diet also help
build up bone mass.
Joints
Cartilage becomes more rigid, fragile, and susceptible to fibrillation. Loss of elasticity
and resiliency is attributed to more cross-linking of collagen to elastin, decrease in water
content, and decreasing concentrations of glycosaminoglycans. Joints are also more prone
to fracture due to the loss of bone mass.
Muscles
Decrease in the range of motion of the joint is related to the change of ligaments and
muscles. As the body ages, muscle bulk and strength declines especially after the age of
70. As much as 30% of skeletal muscle are lost by age 80. Muscle fibers, RNA synthesis
and mitochondrial volume loss may all be contributors to muscle decline. Other factors
that could contribute to muscle loss of the aged are: change in activity level, reduced
nerve supply to muscle, cardiovascular disease, and nutritional deficiencies. In women,
menopause will cause muscle mass to decrease significantly, especially in the first three
post-menopausal years.

17.12.3 Nervous System

One of the effects of aging on the nervous system is the loss of neurons. By the age of 30,
the brain begins to lose thousands of neurons each day. The cerebral cortex can lose as
much as 45% of its cells and the brain can weigh 7% less than in the prime of our lives.
Associated with the loss of neurons comes a decreased capacity to send nerve impulses to
and from the brain. Because of this the processing of information slows down. In addition
the voluntary motor movement's slow down, reflex time increases, and conduction velocity

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decreases. Parkinson's disease is the most common movement disorder of the nervous system.
As we age there are some degenerative changes along with some disease's involving the sense
organ's that can alter vision, touch, smell, and taste. Loss of hearing is also associated with
aging. It is usually the result of changes in important structures of the inner ear.
Dementia
Dementia (from Latin de- "apart, away" + mens (genitive mentis) "mind") is the progressive
decline in cognitive function due to damage or disease in the brain beyond what might be
expected from normal aging. Particularly affected areas may be memory, attention, language
and problem solving, although particularly in the later stages of the condition, affected
persons may be disoriented in time (not knowing what day, week, month or year it is),
place (not knowing where they are) and person (not knowing who they are). Symptoms of
dementia can be classified as either reversible or irreversible depending upon the etiology of
the disease. Less than 10% of all dementias are reversible. Dementia is a non-specific term
that encompasses many disease processes, just as fever is attributable to many etiologies.
Alzheimers disease
Alzheimer's disease (AD) is a neurodegenerative disease characterized by progressive cognitive
deterioration together with declining activities of daily living and neuropsychiatric symptoms
or behavioral changes. It is the most common cause of dementia. The most striking early
symptom is short term memory loss (amnesia), which usually manifests as minor forgetfulness
that becomes steadily more pronounced with illness progression, with relative preservation
of older memories. As the disorder progresses, cognitive (intellectual) impairment extends to
the domains of language (aphasia), skilled movements (apraxia), recognition (agnosia), and
those functions (such as decision-making and planning) closely related to the frontal and
temporal lobes of the brain as they become disconnected from the limbic system, reflecting
extension of the underlying pathological process. This consists principally of neuronal loss or
atrophy, together with an inflammatory response to the deposition of amyloid plaques and
neurofibrillary tangles. Genetic factors are known to be important, and autosomal dominant
mutations in three different genes (presenilin 1, presenilin 2, and amyloid precursor protein)
have been identified that account for a small number of cases of familial, early-onset AD. For
late onset AD (LOAD), only one susceptibility gene has so far been identified: the epsilon 4
allele of the apolipoprotein E gene. Age of onset itself has a heritability of around 50%.

17.12.4 Digestive System

The changes associated with aging of the digestive system include loss of strength and tone of
muscular tissue and supporting muscular tissue, decreased secretory mechanisms, decreased
motility of the digestive organs, along with changes in neurosensory feedback regarding
enzyme and hormone release, and diminished response to internal sensations and pain. In
the upper GI tract common changes include periodontal disease, difficulty in swallowing,
reduced sensitivity to mouth irritations and sores, loss of taste, gastritis, and peptic ulcer
disease. Changes that may appear in the small intestine include, appendicitis, duodenal
ulcers, malabsoration, and maldigestion. Other pathologies that increase in occurrence with

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age are acute pancreatitis, jaundice, and gallbladder problems. Large intestinal changes such
as hemorrhoids and constipation may also occur. Cancer of the rectum are quite common.

17.12.5 Urinary System

As we get older kidney function diminishes. By the age of 70, the filtering mechanism is only
about half as effective as it was at age 40. Because water balance is altered and the sensation
of thirst diminishes with age, older people are more susceptible to dehydration. This causes
more urinary tract infections in the elderly. other problems may include nocturia (excessive
urination at night), increased frequency of urination, polyuria (excessive urine production),
dysuria (painful urination), incontinence, and hematuria (blood in the urine). Some kidney
diseases that are common as we age include acute and chronic kidney inflammations and
renal calculi (kidney stones). The prostate gland is often implicated in various disorders of
the urinary tract. Prostate cancer is the most common cancer in elderly males. Because the
prostate gland encircles part of the urethra, an enlarged prostate gland may cause difficulty
in urination

17.12.6 Respiratory Systems

With the advancing of age, the airways and tissue of the respiratory tract become less elastic
and more rigid. The walls of the alveoli break down, so there is less total respiratory surface
available for gas exchange. This decreases the lung capacity by as much as 30% by the age
of 70. Therefore, elderly people are more susceptible to pneumonia, bronchitis, emphysema,
and other pulmonary disorders. For a more complete discussion of the respiratory system
please visit Chapter 12 The Respiratory System.7

http://en.wikibooks.org/wiki/Human_Physiology/The_respiratory_system

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Human Development
Lung cancer

Figure 165

Correlation between lung cancer and smoking tobacco.

Lung cancer is a cancer of the lungs characterized by the presence of malignant tumors.
Most commonly it is bronchogenic carcinoma (about 90%). Lung cancer is one of the most
lethal forms of cancer worldwide, causing up to 3 million deaths annually. Only one in ten
patients diagnosed with this disease will survive the next five years. Although lung cancer
was previously an illness that affected predominately men, lung cancer rate for women has
been increasing in the last few decades. This has been attributed to the rising ratio of
female to male smokers. More women die of lung cancer than any other cancer, including
breast cancer, ovarian cancer and uterine cancers combined. Current research indicates that
the factor with the greatest impact on risk of lung cancer is long-term exposure to inhaled
carcinogens. The most common means of such exposure is tobacco smoke.

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The effects of Aging on the Body

Vision
Changes in vision begin at an early age. The cornea becomes thicker and less curved. The
anterior chamber decreases in size and volume. The lens becomes thicker and more opaque,
and also increases rigidity and loses elasticity. The ciliary muscles atrophy and the pupil
constricts. There is also a reduction of rods and nerve cells of the retina.
Hearing
Approximately one third of people over the age of 65 have hearing loss. The ability to
distinguish between high and low frequency diminishes with age. Loss of hearing for sounds
of high-frequency (presbycusis) is the most common, although the ability to distinguish
sound localization also decreases. It is believed that the hearing loss isn't so much an age
change as it is due to the accumulation of noise damage.
Taste and Smell
Sensitivity to odors and taste decline with age. The sense of smell begins to degenerate with
the loss of olfactory sensory neurons and loss of cells from the olfactory bulb. The decline in
taste sensation is more gradual than that of smell. The elderly have trouble differentiating
between flavors. The number of fungiform papillae of the tongue decline by 50% by the age
of 50. Taste could also be affected by the loss of salivary gland secretions, notably amylase.
This loss of taste and smell can have a significant effect on an elder's health. With the
reduced ability to taste and smell, it is difficult to adjust food intake as they can no longer
rely on their taste receptors to tell them if something is too salty, or too sweet. This can also
cause the problem in that they might not be able to detect if something is spoiled, making
them at a higher risk for food poisoning.

17.12.7 Cellular Aging

As people age, oxygen intake decreases as well as the basal metabolic rate. The decrease in
the metabolic rate, delayed shivering response, sedentary lifestyle, decreased vasoconstrictor
response, diminished sweating, and poor nutrition are reasons why the elderly cannot
maintain body temperature. There is also a decrease in total body water (TBW). In
newborns, TBW is 75% to 80%. TBW continues to decline in childhood to 60% to 65%, to
less than 60% in adults.

17.12.8 Organism Aging

Aging is generally characterized by the declining ability to respond to stress, increasing
homeostatic imbalance and increased risk of disease. Because of this, death is the ultimate
consequence of aging. Differences in maximum life span between species correspond to
different "rates of aging". For example, inherited differences in the rate of aging make
a mouse elderly at 3 years and a human elderly at 90 years. These genetic differences

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Human Development
affect a variety of physiological processes, probably including the efficiency of DNA repair,
antioxidant enzymes, and rates of free radical production.

17.13 Life Expectancy

http://www.senescence.info/definitions.html

17.14 Stages of Grief- Death and Dying

We go through several stages of grief as we near death, receive catastrophic news, or go
through some type of life-altering experience. There are five defined stages according to
Elisabeth Kbler-Ross. She states, however, that these steps don't always come in order,
and are not always experienced all together by everyone. She does claim that a person will
always experience at least two of the stages.
The stages are:
Denial- This isn't happening, there must have been some mistake.
Anger- Why me? It's not fair, how could you do this to me?!? (aimed toward some other
"responsible" party)
Bargaining- Just give me 2 more years...let me live to see________.
Depression- extreme sadness, lack of motivation or desire to fight anymore
Acceptance- I'm ok with this.

17.15 Sidenotes: Aubrey de Grey

Aubrey David Nicholas Jasper de Grey, Ph.D., (born 20 April 1963 in London, England)
is a controversial biomedical gerontologist who lives in the city of Cambridge, UK. He is
working to expedite the development of a cure for human aging, a medical goal he refers to
as engineered negligible senescence. To this end, he has identified what he concludes are
the seven areas of the aging process that need to be addressed medically before this can
be done. He has been interviewed in recent years in many news sources, including CBS 60
Minutes, BBC, the New York Times, Fortune Magazine, and Popular Science. His main
activities at present are as chairman and chief science officer of the Methuselah Foundation
and editor-in-chief of the academic journal Rejuvenation Research. Here are the seven
biological causes of senescence and possible solutions:
1. Cell loss or atrophy. Cell depletion can be partly corrected by therapies involving
exercise and growth factors. But stem cell therapy is almost certainly required for any
more than just partial replacement of lost cells. This research would involve a large
number of details, but is occurring on many fronts.

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Discoveries In Growth And Development

2. Nuclear mutations and epimutations. A mutation in a functional gene of a cell can
cause that cell to malfunction or to produce a malfunctioning product. Because of the
sheer number of cells Dr. de Grey believes that redundancy takes care of this problem,
although cells that have mutated to produce toxic products might have to be disabled.
In Dr. de Grey's opinion, the effect of mutations and epimutations that really matters
is cancer, since if even one cell turns into a cancer cell it might spread and become
deadly. This is to be corrected by whole-body interdiction of lengthening telomeres, or
any other cure for cancer, if any is ever found.
3. Mutant mitochondria. Because of the highly oxidative environment in mitochondria and
their lack of the sophisticated repair systems found in the cell nucleus, mitochondrial
mutations are believed to a be a major cause of progressive cellular degeneration.
This is to be corrected by moving the DNA for mitochondria completely within the
cellular nucleus, where it is better protected. In humans all but 13 proteins are already
protected in this way. It has been experimentally shown the operation is feasible.
4. Cellular senescence. Cellular senescence might be corrected by forcing senescent cells
to destroy themselves, a process called apoptosis. Cell killing with suicide genes or
vaccines was suggested for making the cells do apoptosis. Healthy cells would multiply
to replace them.
5. Extracellular cross-links. These are chemical bonds between structures that are part
of the body, but not within a cell. In senescent people many of these become brittle
and weak. The proposal is to further develop small-molecular drugs and enzymes to
break links caused by sugar-bonding (glycation), and other common forms of chemical
linking.
6. Junk outside cells. Junk outside cells might be removed by enhanced phagocytosis (the
normal process used by the immune system), and small drugs able to break chemical
beta-bonds. The large junk in this class can be removed surgically. Junk here means
useless things accumulated by a body, but which cannot be digested or removed by
its processes, such as the amyloid plaques characteristic of Alzheimer's disease. The
oft-mentioned 'toxins' that people claim cause many diseases would probably also fit
under this class.
7. Junk inside cells. Junk inside cells might be removed by adding new enzymes to the
cell's natural digestion organ, the lysosome. These enzymes would be taken from
bacteria, molds and other organisms that are known to completely digest animal
bodies.
Dr. de Grey's research proposals are highly controversial, with many critics arguing the highly
complicated biomedical phenomena involved contain too many unknowns for intervention to
be considered remotely foreseeable.

17.16 Discoveries In Growth And Development

Medieval times
In this time the thought was once children emerged form infancy, they were regarded as
miniature already formed adults.
Religious influence of parenting 16th Century

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Human Development
Puritan belief harsh restrictive parenting practices were recommended as the most efficient
means of taming the depraved child.
John Locke's 17th Century
Tabula Rosa = Blank slate in this the thought was that children are to begin with nothing at
all and all kinds of experiences can shape their characters. This is seen as a negative vision
of the development of children because children do contribute to his or her own development.
Jean Jacques Rousseau 18th Century
Noble savages = endowed with a sense of right or wrong. Children have built in moral sense
1st concept of stage, 2nd maturation of growth refers to genetically determined naturally
unfolding course. He saw development as a discontinuous stagenise process mapped cut by
nature.
Charles Darwin the forefather of Scientific Child Study 1859-1936, 19th century
The famous theory of evolution, the survival of the fittest, and natural selection.
G. Stanley Hall regarded as the founder of the child study movement 18461924
One of the most influential American psychologists of the early twentieth century. The
Normative Approach = normative period measures of large numbers of individuals and age
related averages are computed to represent typical development.
The mental testing movement early 20th Century
French psychologist Alfred Binet and Colleague Theodore Simon were the first to come up
with a successful intelligence test IQ at Stanford University.
Sigmund Freud 1856-1939
Theory psychosexual theory, ID, Ego, and Superego.
Erik Erikson 1902-1994
Theory psychosocial theory
John Watson 1978-1958
Behaviorism and Social earing Theory
Ivan Pavlov
Classical conditioning
B.F. Skinner
Operant Conditioning
Albert Bandura
Social learning theory
Jean Piaget's
Cognitive-developmental theory

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Review Questions

17.17 Review Questions

Answers for these questions can be found here8
1. Growth is the most rapid in
A) puberty
B) childhood
C) infancy
D) adulthood
E) Growth is always the same
2. This hormone stimulates puberty
A) GnRH
B) LH
C) FSH
D) TSH
3. Compared to girls' early growth spurt, growth __________in boys and __________
A) is quicker, lasts longer
B) accelerates more slowly, lasts longer
C) is slower, shorter
D) None of the above
4. This quality symbolizes adulthood in most cultures
A) stability
B) method/tact
C) endurance
D) objectivity
E) all of the above
5. Susie has a very hard time keeping friends, according to Maslow, this could be because
A) as a child she had a supportive family
B) she likes to help solve the problems of others
C) as a teenager her self-esteem was low
D) as a baby she wasnt breastfed

http://en.wikibooks.org/wiki/Human_Physiology/Appendix_1:_answers_to_review_
questions#Development:_birth_through_death

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Human Development
E) as a child she lived in an environment that never made her feel safe
6. According to Maslow, in order for me to reach my full potential of self-actualization I
must first
A) feel safe
B) gain self-esteem
C) have friendship
D) have food
E) all of the above
7. Humans are one of the _________developing species in the animal kingdom
A) slowest
B) quickest
C) average
D) none of the above
8. Jenny thinks that she might be going through menopause, a symptom of this is
A) bleeding
B) frequent urination
C) itchiness
D) none of the above
E) all of the above
9. It is estimated that 52 million people will be afflicted with this by 2010
A) Progeria
B) osteoporosis
C) Alzheimers
D) dementia
10. This is the leading cause of death for both men and women
A) progeria
B) cancer
C) congestive heart failure
D) osteoporosis
E) heart attack

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Glossary

17.18 Glossary
Alzheimer's disease
The most common form of dementia. It is a progressive condition that destroys brain cells,
resulting in the loss of intellectual abilities
Apoptosis
The process of regulated cell death
Appositional bone growth
The growth in diameter of bones around the diaphysis occurs by deposition of bone beneath
the periosteum.
Bilirubin
A chemical breakdown product of hemoglobin.
canaliculi
small channels or canals in bone.
Deciduous teeth
The first set of teeth in the growth development of humans and many other animals. (milk
teeth, baby teeth, or primary teeth)
Dementia
The progressive decline in cognitive function due to damage or disease in the brain beyond
what might be expected from normal aging.
Epiphyseal Plate
The cartilage in growing long bones that allows lengthwise growth. The plate ossifies at
the end of puberty.
Haversian system
The basic structual unit of compact bone which includes a central canal, lamellae, lacunae,
osteocytes, and canaliculi.
Intramembranous ossification
The type of bone formation responsible for the development of flat bones, especially those
found in the skull. In intramembranous ossification mesenchymal cells develop into bone
without first going through a cartilage stage.
lacunae
spaces between bone lamellae.
lamellae
cocentric layers of bone matrix.
Menopause

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Human Development
The permanent cessation of menstrual cycles.
Menarche
The first menstrual bleeding, usually occurs at about 12.7 years of age.
Mongolian spots
are common among darker-skinned races, such as Asian, East Indian, and African. They are
flat, pigmented lesions with unclear borders and irregular shape. They appear commonly
at the base of the spine, on the buttocks and back. They may also can appear as high
as the shoulders and elsewhere. Mongolian spots are benign skin markings and are not
associated with any conditions or illnesses.
Necrosis
A form of cell death that results from acute cellular injury.
Osteoporosis
A condition that is characterized by a decrease in bone mass and density, causing bones to
become fragile.
Puberty
The process of physical changes by which a child's body becomes an adult body capable of
reproduction
Pyloric Stenosis
Narrowing of the pyloric sphincter that reduces or eliminates the passage of food from the
stomach to the small intestine, often causing projectile vomiting in infants.
Trabeculae
spongy bones that make plates or bars instead of cocentric layers.

17.19 References
Methuselahmouse.org9
Van De Graaff (2002) Human Anatomy 6th ed. McGraw-Hill Higher Education
Windmaier, P.W. Raff, H. Strang, T.S. (2004) Vander, Sherman, & Luciano's Human
Physiology, the Mechanisms of Body Function 9th ed. Mcgraw-Hill
Starr & McMillan (2001) Human Biology 6th ed. Thomson-Brooks/cole.
McCance, Kathryn L., Heuther, Sue E. (1994) Pathophysiology: the biological basis for
diseases in adults and children. Mosby-Year Book, Inc.

522

http://www.methuselahmouse.org

18 Notes and Resources

18.1 Authors
1. Kevin Young1 , U.S. Citizen and resident thereof. I was teaching pre-nursing students
of Provo College2 through distance education technology, while working at the Utah
State University3 Brigham City campus (as of Jan 2011 I teach at Arizona Western
College4 ). This textbook was created as a class project. I created the chapter pages,
but the students are the primary authors (hopefully some of them will list themselves
here). The fall 2006 class created the initial structure and content, while the spring
2007 students went through each chapter making improvements.
2. Nursing student, Provo College Stephanie Greenwood5 18:13, 30 April 2007 (UTC)
3. Nursing Student, Provo College Danette Seyffert 16:07, 1 May 2007 (UTC)
Hopefully this project expands far beyond our classroom. If you wish to be listed specifically
as a contributing author, then please include your name above this paragraph. We
also thank all those who wrote Wikipedia articles that we borrowed from extensively, and
all anonymous contributors.

18.2 Content and Contributions

To the best of our knowlege, this is the world's first and only open content6 human
physiology textbook. Not only will this be the most affordable introductory physiology
textbook available, but we anticipate that it will become the best one available. We will focus
all our efforts for two months on providing valuable content and organizing and explaining
information clearly. We anticipate the book becoming increasingly better as worldwide
awareness and participation spread.
The original text of this work, and the home of the project, can be found at:
Wikibooks: Human Physiology7
http://en.wikibooks.org/wiki/Human_Physiology
Notes on the preferred style and formatting of each page can be at:

1
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7

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http://www.trade-schools.net/provo-college/default.asp
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http://azwestern.edu
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http://en.wikipedia.org/wiki/Open_content
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Wikibooks: Human Physiology/Formatting8
http://en.wikibooks.org/wiki/Human_Physiology/Formatting

18.3 License
All content contained herein is available under the GNU free documentation license9 . You
can copy it, print it, sell it, and create derivative works from it, in accordance with that
license.
This book links to several outside sources, and these links are designed to be illustrative
learning tools. Links to outside content do not represent an endorsement of that content.
Any of the content not found under the Wikimedia site and subsites is not guaranteed to be
under the GDFL10 ; they are most likely not.

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http://en.wikibooks.org/wiki/Human%20Physiology%2FFormatting
http://en.wikibooks.org/wiki/GNU%20Free%20Documentation%20License
http://en.wikibooks.org/wiki/GNU%20Free%20Documentation%20License

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http://en.wikibooks.org/w/index.php?title=User:Galaxy_sm
http://en.wikibooks.org/w/index.php?title=User:Gartoly
http://en.wikibooks.org/w/index.php?title=User:Gayad
http://en.wikibooks.org/w/index.php?title=User:General_Tojo
http://en.wikibooks.org/w/index.php?title=User:Geoffy
http://en.wikibooks.org/w/index.php?title=User:GeorgHH
http://en.wikibooks.org/w/index.php?title=User:Gopherusagassizii
http://en.wikibooks.org/w/index.php?title=User:HMman
http://en.wikibooks.org/w/index.php?title=User:Hagindaz
http://en.wikibooks.org/w/index.php?title=User:Harrissc
http://en.wikibooks.org/w/index.php?title=User:Hasdo456
http://en.wikibooks.org/w/index.php?title=User:Henkeldg
http://en.wikibooks.org/w/index.php?title=User:Herbythyme
http://en.wikibooks.org/w/index.php?title=User:Hethrir
http://en.wikibooks.org/w/index.php?title=User:Hoggle
http://en.wikibooks.org/w/index.php?title=User:Horn_Eaas
http://en.wikibooks.org/w/index.php?title=User:Hubie_224
http://en.wikibooks.org/w/index.php?title=User:Hytham
http://en.wikibooks.org/w/index.php?title=User:Iamunknown
http://en.wikibooks.org/w/index.php?title=User:Islam.badreldin
http://en.wikibooks.org/w/index.php?title=User:JackBot
http://en.wikibooks.org/w/index.php?title=User:Jacquel

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Jami 799
Jandreakeller100
Jaredjohnson101
Jcran69102
Jeeny103
Jen A104
JenVan105
Jennifer72106
Jennifermorley107
Jenny2288108
Jessewin109
Jessewinfield110
Jguk111
Jimmy112
Jokes Free4Me113
Jomegat114
Jtervortn115
Juliedulany116
Jusjih117
Kansing Lansing118
Kayau119
Kaye120
Keith davis121

http://en.wikibooks.org/w/index.php?title=User:JamBam
http://en.wikibooks.org/w/index.php?title=User:JamBam16
http://en.wikibooks.org/w/index.php?title=User:Jami_7
http://en.wikibooks.org/w/index.php?title=User:Jandreakeller
http://en.wikibooks.org/w/index.php?title=User:Jaredjohnson
http://en.wikibooks.org/w/index.php?title=User:Jcran69
http://en.wikibooks.org/w/index.php?title=User:Jeeny
http://en.wikibooks.org/w/index.php?title=User:Jen_A
http://en.wikibooks.org/w/index.php?title=User:JenVan
http://en.wikibooks.org/w/index.php?title=User:Jennifer72
http://en.wikibooks.org/w/index.php?title=User:Jennifermorley
http://en.wikibooks.org/w/index.php?title=User:Jenny2288
http://en.wikibooks.org/w/index.php?title=User:Jessewin
http://en.wikibooks.org/w/index.php?title=User:Jessewinfield
http://en.wikibooks.org/w/index.php?title=User:Jguk
http://en.wikibooks.org/w/index.php?title=User:Jimmy
http://en.wikibooks.org/w/index.php?title=User:Jokes_Free4Me
http://en.wikibooks.org/w/index.php?title=User:Jomegat
http://en.wikibooks.org/w/index.php?title=User:Jtervortn
http://en.wikibooks.org/w/index.php?title=User:Juliedulany
http://en.wikibooks.org/w/index.php?title=User:Jusjih
http://en.wikibooks.org/w/index.php?title=User:Kansing_Lansing
http://en.wikibooks.org/w/index.php?title=User:Kayau
http://en.wikibooks.org/w/index.php?title=User:Kaye
http://en.wikibooks.org/w/index.php?title=User:Keith_davis

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530

Kfarnham7122
Klaitaka123
Kmarv84124
Kpjas125
Krstnplmr126
LAURIELL127
Lafadam128
LathLyd129
Leilijohnson130
Linsey8131
Linsey88132
Lotje133
Macp134
Macsking135
MadeofPlants136
Makecat137
MarksJonson138
Mattb112885139
Melaniep140
Melissasmith141
Meric-lmt142
MichaelJoseph143
Michelleamills144
Mike.lifeguard145
Mike6271146

http://en.wikibooks.org/w/index.php?title=User:Kfarnham7
http://en.wikibooks.org/w/index.php?title=User:Klaitaka
http://en.wikibooks.org/w/index.php?title=User:Kmarv84
http://en.wikibooks.org/w/index.php?title=User:Kpjas
http://en.wikibooks.org/w/index.php?title=User:Krstnplmr
http://en.wikibooks.org/w/index.php?title=User:LAURIELL
http://en.wikibooks.org/w/index.php?title=User:Lafadam
http://en.wikibooks.org/w/index.php?title=User:LathLyd
http://en.wikibooks.org/w/index.php?title=User:Leilijohnson
http://en.wikibooks.org/w/index.php?title=User:Linsey8
http://en.wikibooks.org/w/index.php?title=User:Linsey88
http://en.wikibooks.org/w/index.php?title=User:Lotje
http://en.wikibooks.org/w/index.php?title=User:Macp
http://en.wikibooks.org/w/index.php?title=User:Macsking
http://en.wikibooks.org/w/index.php?title=User:MadeofPlants
http://en.wikibooks.org/w/index.php?title=User:Makecat
http://en.wikibooks.org/w/index.php?title=User:MarksJonson
http://en.wikibooks.org/w/index.php?title=User:Mattb112885
http://en.wikibooks.org/w/index.php?title=User:Melaniep
http://en.wikibooks.org/w/index.php?title=User:Melissasmith
http://en.wikibooks.org/w/index.php?title=User:Meric-lmt
http://en.wikibooks.org/w/index.php?title=User:MichaelJoseph
http://en.wikibooks.org/w/index.php?title=User:Michelleamills
http://en.wikibooks.org/w/index.php?title=User:Mike.lifeguard
http://en.wikibooks.org/w/index.php?title=User:Mike6271

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Mkyashar147
Mohborg148
Mperkins149
Mseliw150
Mshahin151
Msol152
Nataliehaveron153
Neoptolemus154
Never2late155
Nikkjeppson156
NipplesMeCool157
Nprasunpriya158
Osandyoo159
Panic2k4160
Princess8107161
Prispartlow162
Provophys163
Pwoodson164
QUBot165
QuiteUnusual166
Ramac167
Randomraccoon168
Read-write-services169
Recent Runes170
Red4tribe171

http://en.wikibooks.org/w/index.php?title=User:Mkyashar
http://en.wikibooks.org/w/index.php?title=User:Mohborg
http://en.wikibooks.org/w/index.php?title=User:Mperkins
http://en.wikibooks.org/w/index.php?title=User:Mseliw
http://en.wikibooks.org/w/index.php?title=User:Mshahin
http://en.wikibooks.org/w/index.php?title=User:Msol
http://en.wikibooks.org/w/index.php?title=User:Nataliehaveron
http://en.wikibooks.org/w/index.php?title=User:Neoptolemus
http://en.wikibooks.org/w/index.php?title=User:Never2late
http://en.wikibooks.org/w/index.php?title=User:Nikkjeppson
http://en.wikibooks.org/w/index.php?title=User:NipplesMeCool
http://en.wikibooks.org/w/index.php?title=User:Nprasunpriya
http://en.wikibooks.org/w/index.php?title=User:Osandyoo
http://en.wikibooks.org/w/index.php?title=User:Panic2k4
http://en.wikibooks.org/w/index.php?title=User:Princess8107
http://en.wikibooks.org/w/index.php?title=User:Prispartlow
http://en.wikibooks.org/w/index.php?title=User:Provophys
http://en.wikibooks.org/w/index.php?title=User:Pwoodson
http://en.wikibooks.org/w/index.php?title=User:QUBot
http://en.wikibooks.org/w/index.php?title=User:QuiteUnusual
http://en.wikibooks.org/w/index.php?title=User:Ramac
http://en.wikibooks.org/w/index.php?title=User:Randomraccoon
http://en.wikibooks.org/w/index.php?title=User:Read-write-services
http://en.wikibooks.org/w/index.php?title=User:Recent_Runes
http://en.wikibooks.org/w/index.php?title=User:Red4tribe

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Reece172
RiRi82173
Robisabi174
Ruhidoc175
Ruter176
SB Johnny177
SBJohnny178
SKvalen179
SPat180
Savh181
Scottholmes182
Scout21972183
Sethwoodworth184
Shakah185
Shaleneroberts186
Shanannie187
Shanowac188
Shellybird2189
Sigma 7190
Sincade191
Smootswiki192
Soeb193
Spamduck194
Spazzi195
Srayhamlin196

http://en.wikibooks.org/w/index.php?title=User:Reece
http://en.wikibooks.org/w/index.php?title=User:RiRi82
http://en.wikibooks.org/w/index.php?title=User:Robisabi
http://en.wikibooks.org/w/index.php?title=User:Ruhidoc
http://en.wikibooks.org/w/index.php?title=User:Ruter
http://en.wikibooks.org/w/index.php?title=User:SB_Johnny
http://en.wikibooks.org/w/index.php?title=User:SBJohnny
http://en.wikibooks.org/w/index.php?title=User:SKvalen
http://en.wikibooks.org/w/index.php?title=User:SPat
http://en.wikibooks.org/w/index.php?title=User:Savh
http://en.wikibooks.org/w/index.php?title=User:Scottholmes
http://en.wikibooks.org/w/index.php?title=User:Scout21972
http://en.wikibooks.org/w/index.php?title=User:Sethwoodworth
http://en.wikibooks.org/w/index.php?title=User:Shakah
http://en.wikibooks.org/w/index.php?title=User:Shaleneroberts
http://en.wikibooks.org/w/index.php?title=User:Shanannie
http://en.wikibooks.org/w/index.php?title=User:Shanowac
http://en.wikibooks.org/w/index.php?title=User:Shellybird2
http://en.wikibooks.org/w/index.php?title=User:Sigma_7
http://en.wikibooks.org/w/index.php?title=User:Sincade
http://en.wikibooks.org/w/index.php?title=User:Smootswiki
http://en.wikibooks.org/w/index.php?title=User:Soeb
http://en.wikibooks.org/w/index.php?title=User:Spamduck
http://en.wikibooks.org/w/index.php?title=User:Spazzi
http://en.wikibooks.org/w/index.php?title=User:Srayhamlin

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Sterlingsilver199
Steve3562200
Sullyz0r201
Sundance Raphael202
Sunlight2203
TATENSMOM204
Tammishamo205
Tannersf206
Taxman207
Thatgadgetgirl208
Thenub314209
Theornamentalist210
Toriloveless211
Tradimus212
Trevan5213
Trisha83214
Truckies daughter94215
Truthspeaks216
Unknownfigure01217
VSimonian218
VWilkes219
Valerie795220
Van der Hoorn221

http://en.wikibooks.org/w/index.php?title=User:Staticshakedown
http://en.wikibooks.org/w/index.php?title=User:Stephanie_greenwood
http://en.wikibooks.org/w/index.php?title=User:Sterlingsilver
http://en.wikibooks.org/w/index.php?title=User:Steve3562
http://en.wikibooks.org/w/index.php?title=User:Sullyz0r
http://en.wikibooks.org/w/index.php?title=User:Sundance_Raphael
http://en.wikibooks.org/w/index.php?title=User:Sunlight2
http://en.wikibooks.org/w/index.php?title=User:TATENSMOM
http://en.wikibooks.org/w/index.php?title=User:Tammishamo
http://en.wikibooks.org/w/index.php?title=User:Tannersf
http://en.wikibooks.org/w/index.php?title=User:Taxman
http://en.wikibooks.org/w/index.php?title=User:Thatgadgetgirl
http://en.wikibooks.org/w/index.php?title=User:Thenub314
http://en.wikibooks.org/w/index.php?title=User:Theornamentalist
http://en.wikibooks.org/w/index.php?title=User:Toriloveless
http://en.wikibooks.org/w/index.php?title=User:Tradimus
http://en.wikibooks.org/w/index.php?title=User:Trevan5
http://en.wikibooks.org/w/index.php?title=User:Trisha83
http://en.wikibooks.org/w/index.php?title=User:Truckies_daughter94
http://en.wikibooks.org/w/index.php?title=User:Truthspeaks
http://en.wikibooks.org/w/index.php?title=User:Unknownfigure01
http://en.wikibooks.org/w/index.php?title=User:VSimonian
http://en.wikibooks.org/w/index.php?title=User:VWilkes
http://en.wikibooks.org/w/index.php?title=User:Valerie795
http://en.wikibooks.org/w/index.php?title=User:Van_der_Hoorn

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Vkghai223
Voidxor224
Webaware225
Whiteknight226
Whiterose227
Whoop whoop pull up228
Whtndks229
Whym230
WiKiMi3231
Winn232
Wutsje233
Xania234
Xxagile235
YMS236
Zakiyang237

http://en.wikibooks.org/w/index.php?title=User:VernoWhitney
http://en.wikibooks.org/w/index.php?title=User:Vkghai
http://en.wikibooks.org/w/index.php?title=User:Voidxor
http://en.wikibooks.org/w/index.php?title=User:Webaware
http://en.wikibooks.org/w/index.php?title=User:Whiteknight
http://en.wikibooks.org/w/index.php?title=User:Whiterose
http://en.wikibooks.org/w/index.php?title=User:Whoop_whoop_pull_up
http://en.wikibooks.org/w/index.php?title=User:Whtndks
http://en.wikibooks.org/w/index.php?title=User:Whym
http://en.wikibooks.org/w/index.php?title=User:WiKiMi3
http://en.wikibooks.org/w/index.php?title=User:Winn
http://en.wikibooks.org/w/index.php?title=User:Wutsje
http://en.wikibooks.org/w/index.php?title=User:Xania
http://en.wikibooks.org/w/index.php?title=User:Xxagile
http://en.wikibooks.org/w/index.php?title=User:YMS
http://en.wikibooks.org/w/index.php?title=User:Zakiyang

List of Figures
GFDL: Gnu Free Documentation License. http://www.gnu.org/licenses/fdl.html
cc-by-sa-3.0: Creative Commons Attribution ShareAlike 3.0 License.
creativecommons.org/licenses/by-sa/3.0/

http://

cc-by-sa-2.5: Creative Commons Attribution ShareAlike 2.5 License.

creativecommons.org/licenses/by-sa/2.5/

http://

cc-by-sa-2.0: Creative Commons Attribution ShareAlike 2.0 License.

creativecommons.org/licenses/by-sa/2.0/

http://

cc-by-sa-1.0: Creative Commons Attribution ShareAlike 1.0 License.

creativecommons.org/licenses/by-sa/1.0/

http://

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org/licenses/by/2.0/
cc-by-2.0: Creative Commons Attribution 2.0 License. http://creativecommons.
org/licenses/by/2.0/deed.en
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org/licenses/by/2.5/deed.en
cc-by-3.0: Creative Commons Attribution 3.0 License. http://creativecommons.
org/licenses/by/3.0/deed.en
GPL: GNU General Public License. http://www.gnu.org/licenses/gpl-2.0.txt
LGPL: GNU Lesser General Public License. http://www.gnu.org/licenses/lgpl.
html
PD: This image is in the public domain.
ATTR: The copyright holder of this file allows anyone to use it for any purpose,
provided that the copyright holder is properly attributed. Redistribution, derivative
work, commercial use, and all other use is permitted.
EURO: This is the common (reverse) face of a euro coin. The copyright on the design
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is reproduction in a format without relief (drawings, paintings, films) provided they
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CFR: Copyright free use.

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EPL: Eclipse Public License. http://www.eclipse.org/org/documents/epl-v10.
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Copies of the GPL, the LGPL as well as a GFDL are included in chapter Licenses238 . Please
note that images in the public domain do not require attribution. You may click on the
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238 Chapter 20 on page 543

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LadyofHats239 (Mariana Ruiz)

Y tambe240
Mariana Ruiz LadyofHats241
Magnus Manske242
user:pschemp243
Katherine Connolly - Dartmouth Electron Microscope Facility

Original uploader was Mikm244 at en.wikipedia245

NHGRI246
US-Gov

Gregory F. Maxwell247 < gmaxwell@gmail.com248 > PGP:

Gregory F. Maxwell249 < gmaxwell@gmail.com250 > PGP:
user:Maksim251
Morning2k252
Persian Poet Gal253

(talk)254

Artwork by Synaptidude255 at en.wikipedia256 |date=200507-05 (original upload date) of Image:Action potential

reloaded.jpg257

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http://en.wikibooks.org/wiki/User%3ALadyofHats
http://en.wikibooks.org/wiki/User%3AY%20tambe
http://en.wikibooks.org/wiki/user%3ALadyofHats
http://en.wikibooks.org/wiki/User%3AMagnus%20Manske
http://en.wikibooks.org/wiki/user%3Apschemp
http://en.wikibooks.org/wiki/%3Aen%3AUser%3AMikm
http://en.wikipedia.org
http://www.genome.gov/12514471
http://en.wikibooks.org/wiki/User%3AGmaxwell
mailto:gmaxwell@gmail.com
http://en.wikibooks.org/wiki/User%3AGmaxwell
mailto:gmaxwell@gmail.com
http://en.wikibooks.org/wiki/user%3AMaksim
http://en.wikibooks.org/wiki/user%3AMorning2k
http://en.wikibooks.org/wiki/%3Aen%3AUser%3APersian%20Poet%20Gal
http://en.wikibooks.org/wiki/%3Aen%3AUser%20talk%3APersian%20Poet%20Gal
http://en.wikibooks.org/wiki/%3Aen%3AUser%3ASynaptidude
http://en.wikipedia.org
http://en.wikibooks.org/wiki/%3AImage%3AAction%20potential%20reloaded.jpg

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Tradimus258
LadyofHats259 Mariana Ruiz Villarreal
User:Primalchaos260

Ralf Stephan (mailto:ralf@ark.in-berlin.de)

After Schwalbe

Original uploader was Kwertii261 at en.wikipedia262

Patrick J. Lynch, medical illustrator

Killfoot263
en:User:Acdx264
User:Dan Pickard265
Original uploader was Oarih266 at en.wikipedia267
B. Welleschik
Patrick J. Lynch, medical illustrator

Gray's Anatomy
Electron Microscopy Facility at The National Cancer Institute at Frederick (NCI-Frederick)

NIDDK

User:Sansculotte268

http://en.wikibooks.org/wiki/User%3ATradimus
http://en.wikibooks.org/wiki/user%3ALadyofHats
http://en.wikibooks.org/wiki/User%3APrimalchaos
http://en.wikibooks.org/wiki/%3Aen%3AUser%3AKwertii
http://en.wikipedia.org
http://en.wikibooks.org/wiki/User%3AKillfoot
http://en.wikibooks.org/wiki/%3Aen%3AUser%3AAcdx
http://en.wikibooks.org/wiki/User%3ADan%20Pickard
http://en.wikibooks.org/wiki/%3Aen%3AUser%3AOarih
http://en.wikipedia.org
http://en.wikibooks.org/wiki/User%3ASansculotte

PD
PD
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List of Figures

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Wapcaplet269 , Reytan270 , Mtcv271

Wapcaplet272 , user:Reytan273 , SVG by user:Sjef274
SKvalen275

Kalumet276
Created by Agateller (Anthony Atkielski)277 , converted to
svg by atom278 .
A. Rad (me) |source={{own
Piotr Micha Jaworski; PioM279

EN280 DE281 PL282

Original uploader was Melensdad283 at en.wikipedia284

Gray's Anatomy
Arcadian285
helix84286

Original uploader was Michaelbladon287 at en.wikipedia288

Mariana Ruiz Villarreal(LadyofHats289 )

GFDL
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http://en.wikibooks.org/wiki/%3Aen%3AUser%3AWapcaplet
http://en.wikibooks.org/wiki/User%3AReytan
http://en.wikibooks.org/wiki/User%3AMtcv
http://en.wikibooks.org/wiki/%3Aen%3AUser%3AWapcaplet
http://en.wikibooks.org/wiki/user%3AReytan
http://en.wikibooks.org/wiki/user%3ASjef
http://en.wikibooks.org/wiki/User%3ASKvalen
http://en.wikibooks.org/wiki/User%3AKalumet
http://en.wikibooks.org/wiki/%3Aen%3AUser%3AAgateller
http://en.wikibooks.org/wiki/%3Acs%3AWikipedista%3Aatom
http://en.wikibooks.org/wiki/%3Apl%3AWikipedysta%3APiom
http://en.wikibooks.org/wiki/%3Apl%3ADyskusja_Wikipedysty%3APiom%23in_English
http://en.wikibooks.org/wiki/%3Apl%3ADyskusja_Wikipedysty%3APiom%23Deutschsprache
http://en.wikibooks.org/wiki/%3Apl%3ADyskusja_Wikipedysty%3APiom%23POLSKI
http://en.wikibooks.org/wiki/%3Aen%3AUser%3AMelensdad
http://en.wikipedia.org
http://en.wikibooks.org/wiki/User%3AArcadian
http://en.wikibooks.org/wiki/user%3Ahelix84
http://en.wikibooks.org/wiki/%3Aen%3AUser%3AMichaelbladon
http://en.wikipedia.org
http://en.wikibooks.org/wiki/User%3ALadyofHats

539

List of Figures

98
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290
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540

Ed Uthman, MD
Ed Uthman, MD
Dungodung290
Lars Aronsson

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CDC, Mysid291
Creator

Mariana Ruiz Villarreal292

LadyofHats293 .

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user:Maksim294
Chris 73
unknown
ekem295 , Courtesy: RWJMS IVF Program
Ed Uthman, MD ( Flickr296 , Wikipedia297 )
X.Compagnion298 (cropd by Hidro299 )

http://en.wikibooks.org/wiki/User%3ADungodung
http://en.wikibooks.org/wiki/User%3AMysid
http://en.wikibooks.org/wiki/user%3ALadyofHats
http://en.wikibooks.org/wiki/User%3ALadyofHats
http://en.wikibooks.org/wiki/user%3AMaksim
http://en.wikibooks.org/wiki/User%3Aekem
http://www.flickr.com/photos/euthman/
http://en.wikibooks.org/wiki/%3Aen%3AUser%3AEuthman
http://en.wikibooks.org/wiki/User%3AMirmillon
http://en.wikibooks.org/wiki/user%3Ahidro

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List of Figures

137

PD
Gray38.png300 :
User Magnus Manske301
en.wikipedia302
derivative work: Amada44303 talk to me304

138
139
140
141
142
143
144
145
146
147
148
149
150

Mike Jones305
brian0918306 307
Mariana Ruiz LadyofHats308
Magnus Manske309
Stephaniegreenwood310
en:User:Cburnett311

on

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Original uploader was Apers0n312 at en.wikipedia313

(Original text : ghr.nlm.nih.gov)

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NIDDK
U.S. Department of Energy Human Genome Program.
Ernest F

J. Finkelstein
Marvin 101

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http://en.wikibooks.org/wiki/%3AFile%3AGray38.png
http://en.wikibooks.org/wiki/%3Aen%3AUser%3AMagnus%20Manske
http://en.wikipedia.org
http://en.wikibooks.org/wiki/User%3AAmada44
http://en.wikibooks.org/wiki/User_talk%3AAmada44
http://en.wikipedia.org/wiki/User%3AAdenosine
http://en.wikibooks.org/wiki/%3Aen%3AUser%3ABrian0918
http://en.wikibooks.org/wiki/%3Aen%3AUser%20talk%3ABrian0918
http://en.wikibooks.org/wiki/user%3ALadyofHats
http://en.wikibooks.org/wiki/User%3AMagnus%20Manske
http://en.wikibooks.org/wiki/User%3AStephaniegreenwood
http://en.wikibooks.org/wiki/%3Aen%3AUser%3ACburnett
http://en.wikibooks.org/wiki/%3Aen%3AUser%3AApers0n
http://en.wikipedia.org

541

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that would be infringed by some manner, permitted by this License, of making, using, or selling its
contributor version, but do not include claims that
would be infringed only as a consequence of further
modification of the contributor version. For purposes of this definition, control includes the right
to grant patent sublicenses in a manner consistent
with the requirements of this License.
Each contributor grants you a non-exclusive, worldwide, royalty-free patent license under the contributors essential patent claims, to make, use, sell, offer for sale, import and otherwise run, modify and
propagate the contents of its contributor version.

In the following three paragraphs, a patent license is any express agreement or commitment,
however denominated, not to enforce a patent (such
as an express permission to practice a patent or
covenant not to sue for patent infringement). To
grant such a patent license to a party means to
make such an agreement or commitment not to enforce a patent against the party.
If you convey a covered work, knowingly relying
on a patent license, and the Corresponding Source
of the work is not available for anyone to copy,
free of charge and under the terms of this License,
through a publicly available network server or other
readily accessible means, then you must either (1)
cause the Corresponding Source to be so available,
or (2) arrange to deprive yourself of the benefit
of the patent license for this particular work, or
(3) arrange, in a manner consistent with the requirements of this License, to extend the patent
license to downstream recipients. Knowingly relying means you have actual knowledge that, but
for the patent license, your conveying the covered
work in a country, or your recipients use of the covered work in a country, would infringe one or more
identifiable patents in that country that you have
reason to believe are valid.
If, pursuant to or in connection with a single transaction or arrangement, you convey, or propagate
by procuring conveyance of, a covered work, and
grant a patent license to some of the parties receiving the covered work authorizing them to use,
propagate, modify or convey a specific copy of the
covered work, then the patent license you grant is
automatically extended to all recipients of the covered work and works based on it.
A patent license is discriminatory if it does not include within the scope of its coverage, prohibits the
exercise of, or is conditioned on the non-exercise
of one or more of the rights that are specifically
granted under this License. You may not convey a
covered work if you are a party to an arrangement
with a third party that is in the business of distributing software, under which you make payment
to the third party based on the extent of your activity of conveying the work, and under which the
third party grants, to any of the parties who would
receive the covered work from you, a discriminatory patent license (a) in connection with copies
of the covered work conveyed by you (or copies
made from those copies), or (b) primarily for and in
connection with specific products or compilations
that contain the covered work, unless you entered
into that arrangement, or that patent license was
granted, prior to 28 March 2007.
Nothing in this License shall be construed as excluding or limiting any implied license or other defenses to infringement that may otherwise be available to you under applicable patent law. 12. No
Surrender of Others Freedom.
If conditions are imposed on you (whether by court
order, agreement or otherwise) that contradict the
conditions of this License, they do not excuse you
from the conditions of this License. If you cannot
convey a covered work so as to satisfy simultaneously your obligations under this License and any
other pertinent obligations, then as a consequence
you may not convey it at all. For example, if you
agree to terms that obligate you to collect a royalty for further conveying from those to whom you
convey the Program, the only way you could satisfy
both those terms and this License would be to refrain entirely from conveying the Program. 13. Use
with the GNU Affero General Public License.

Notwithstanding any other provision of this License, you have permission to link or combine any
covered work with a work licensed under version
3 of the GNU Affero General Public License into
a single combined work, and to convey the resulting work. The terms of this License will continue
to apply to the part which is the covered work, but
the special requirements of the GNU Affero General
Public License, section 13, concerning interaction
through a network will apply to the combination
as such. 14. Revised Versions of this License.
The Free Software Foundation may publish revised
and/or new versions of the GNU General Public License from time to time. Such new versions will be
similar in spirit to the present version, but may differ in detail to address new problems or concerns.
Each version is given a distinguishing version number. If the Program specifies that a certain numbered version of the GNU General Public License
or any later version applies to it, you have the
option of following the terms and conditions either
of that numbered version or of any later version
published by the Free Software Foundation. If the
Program does not specify a version number of the
GNU General Public License, you may choose any
version ever published by the Free Software Foundation.
If the Program specifies that a proxy can decide
which future versions of the GNU General Public
License can be used, that proxys public statement
of acceptance of a version permanently authorizes
you to choose that version for the Program.
Later license versions may give you additional or
different permissions. However, no additional obligations are imposed on any author or copyright
holder as a result of your choosing to follow a later
version. 15. Disclaimer of Warranty.
THERE IS NO WARRANTY FOR THE PROGRAM, TO THE EXTENT PERMITTED BY APPLICABLE LAW. EXCEPT WHEN OTHERWISE
STATED IN WRITING THE COPYRIGHT HOLDERS AND/OR OTHER PARTIES PROVIDE THE
PROGRAM AS IS WITHOUT WARRANTY OF
ANY KIND, EITHER EXPRESSED OR IMPLIED,
INCLUDING, BUT NOT LIMITED TO, THE IMPLIED WARRANTIES OF MERCHANTABILITY
AND FITNESS FOR A PARTICULAR PURPOSE.
THE ENTIRE RISK AS TO THE QUALITY AND
PERFORMANCE OF THE PROGRAM IS WITH
YOU. SHOULD THE PROGRAM PROVE DEFECTIVE, YOU ASSUME THE COST OF ALL NECESSARY SERVICING, REPAIR OR CORRECTION.
16. Limitation of Liability.
IN NO EVENT UNLESS REQUIRED BY APPLICABLE LAW OR AGREED TO IN WRITING
WILL ANY COPYRIGHT HOLDER, OR ANY
OTHER PARTY WHO MODIFIES AND/OR CONVEYS THE PROGRAM AS PERMITTED ABOVE,
BE LIABLE TO YOU FOR DAMAGES, INCLUDING ANY GENERAL, SPECIAL, INCIDENTAL OR CONSEQUENTIAL DAMAGES ARISING
OUT OF THE USE OR INABILITY TO USE
THE PROGRAM (INCLUDING BUT NOT LIMITED TO LOSS OF DATA OR DATA BEING RENDERED INACCURATE OR LOSSES SUSTAINED
BY YOU OR THIRD PARTIES OR A FAILURE
OF THE PROGRAM TO OPERATE WITH ANY
OTHER PROGRAMS), EVEN IF SUCH HOLDER
OR OTHER PARTY HAS BEEN ADVISED OF
THE POSSIBILITY OF SUCH DAMAGES. 17. Interpretation of Sections 15 and 16.
If the disclaimer of warranty and limitation of liability provided above cannot be given local legal ef-

fect according to their terms, reviewing courts shall

apply local law that most closely approximates an
absolute waiver of all civil liability in connection
with the Program, unless a warranty or assumption
of liability accompanies a copy of the Program in
return for a fee.
END OF TERMS AND CONDITIONS How to Apply These Terms to Your New Programs
If you develop a new program, and you want it to
be of the greatest possible use to the public, the
best way to achieve this is to make it free software
which everyone can redistribute and change under
these terms.
To do so, attach the following notices to the program. It is safest to attach them to the start of
each source file to most effectively state the exclusion of warranty; and each file should have at least
the copyright line and a pointer to where the full
notice is found.
<one line to give the programs name and a brief
idea of what it does.> Copyright (C) <year>
<name of author>
This program is free software: you can redistribute
it and/or modify it under the terms of the GNU
General Public License as published by the Free
Software Foundation, either version 3 of the License, or (at your option) any later version.
This program is distributed in the hope that
it will be useful, but WITHOUT ANY WARRANTY; without even the implied warranty of
MERCHANTABILITY or FITNESS FOR A PARTICULAR PURPOSE. See the GNU General Public
License for more details.
You should have received a copy of the GNU General Public License along with this program. If not,
see <http://www.gnu.org/licenses/>.
Also add information on how to contact you by electronic and paper mail.
If the program does terminal interaction, make it
output a short notice like this when it starts in an
interactive mode:
<program> Copyright (C) <year> <name of author> This program comes with ABSOLUTELY
NO WARRANTY; for details type show w. This is
free software, and you are welcome to redistribute it
under certain conditions; type show c for details.
The hypothetical commands show w and show c
should show the appropriate parts of the General
Public License. Of course, your programs commands might be different; for a GUI interface, you
would use an about box.
You should also get your employer (if you work
as a programmer) or school, if any, to sign a
copyright disclaimer for the program, if necessary.
For more information on this, and
how to apply and follow the GNU GPL, see
<http://www.gnu.org/licenses/>.
The GNU General Public License does not permit
incorporating your program into proprietary programs. If your program is a subroutine library, you
may consider it more useful to permit linking proprietary applications with the library. If this is
what you want to do, use the GNU Lesser General
Public License instead of this License. But first,
please read <http://www.gnu.org/philosophy/whynot-lgpl.html>.

20.2 GNU Free Documentation License

Version 1.3, 3 November 2008
Copyright 2000, 2001, 2002, 2007, 2008 Free Software Foundation, Inc. <http://fsf.org/>
Everyone is permitted to copy and distribute verbatim copies of this license document, but changing
it is not allowed. 0. PREAMBLE
The purpose of this License is to make a manual,
textbook, or other functional and useful document
"free" in the sense of freedom: to assure everyone
the effective freedom to copy and redistribute it,
with or without modifying it, either commercially
or noncommercially. Secondarily, this License preserves for the author and publisher a way to get
credit for their work, while not being considered
responsible for modifications made by others.
This License is a kind of "copyleft", which means
that derivative works of the document must themselves be free in the same sense. It complements
the GNU General Public License, which is a copyleft license designed for free software.
We have designed this License in order to use it
for manuals for free software, because free software
needs free documentation: a free program should
come with manuals providing the same freedoms
that the software does. But this License is not limited to software manuals; it can be used for any textual work, regardless of subject matter or whether
it is published as a printed book. We recommend
this License principally for works whose purpose is
instruction or reference. 1. APPLICABILITY AND
DEFINITIONS
This License applies to any manual or other work,
in any medium, that contains a notice placed by the
copyright holder saying it can be distributed under
the terms of this License. Such a notice grants a
world-wide, royalty-free license, unlimited in duration, to use that work under the conditions stated
herein. The "Document", below, refers to any such
manual or work. Any member of the public is a licensee, and is addressed as "you". You accept the
license if you copy, modify or distribute the work
in a way requiring permission under copyright law.
A "Modified Version" of the Document means any
work containing the Document or a portion of it, either copied verbatim, or with modifications and/or
translated into another language.
A "Secondary Section" is a named appendix or a
front-matter section of the Document that deals exclusively with the relationship of the publishers or

authors of the Document to the Documents overall

subject (or to related matters) and contains nothing that could fall directly within that overall subject. (Thus, if the Document is in part a textbook
of mathematics, a Secondary Section may not explain any mathematics.) The relationship could be
a matter of historical connection with the subject
or with related matters, or of legal, commercial,
philosophical, ethical or political position regarding them.
The "Invariant Sections" are certain Secondary Sections whose titles are designated, as being those of
Invariant Sections, in the notice that says that the
Document is released under this License. If a section does not fit the above definition of Secondary
then it is not allowed to be designated as Invariant.
The Document may contain zero Invariant Sections.
If the Document does not identify any Invariant
Sections then there are none.
The "Cover Texts" are certain short passages of text
that are listed, as Front-Cover Texts or Back-Cover
Texts, in the notice that says that the Document is
released under this License. A Front-Cover Text
may be at most 5 words, and a Back-Cover Text
may be at most 25 words.
A "Transparent" copy of the Document means a
machine-readable copy, represented in a format
whose specification is available to the general public, that is suitable for revising the document
straightforwardly with generic text editors or (for
images composed of pixels) generic paint programs
or (for drawings) some widely available drawing editor, and that is suitable for input to text formatters or for automatic translation to a variety of formats suitable for input to text formatters. A copy
made in an otherwise Transparent file format whose
markup, or absence of markup, has been arranged
to thwart or discourage subsequent modification by
readers is not Transparent. An image format is not
Transparent if used for any substantial amount of
text. A copy that is not "Transparent" is called
"Opaque".
Examples of suitable formats for Transparent
copies include plain ASCII without markup, Texinfo input format, LaTeX input format, SGML or
XML using a publicly available DTD, and standardconforming simple HTML, PostScript or PDF designed for human modification. Examples of transparent image formats include PNG, XCF and JPG.
Opaque formats include proprietary formats that
can be read and edited only by proprietary word
processors, SGML or XML for which the DTD
and/or processing tools are not generally available,
and the machine-generated HTML, PostScript or

PDF produced by some word processors for output

purposes only.
The "Title Page" means, for a printed book, the
title page itself, plus such following pages as are
needed to hold, legibly, the material this License
requires to appear in the title page. For works in
formats which do not have any title page as such,
"Title Page" means the text near the most prominent appearance of the works title, preceding the
beginning of the body of the text.
The "publisher" means any person or entity that
distributes copies of the Document to the public.
A section "Entitled XYZ" means a named subunit
of the Document whose title either is precisely XYZ
or contains XYZ in parentheses following text that
translates XYZ in another language. (Here XYZ
stands for a specific section name mentioned below,
such as "Acknowledgements", "Dedications", "Endorsements", or "History".) To "Preserve the Title"
of such a section when you modify the Document
means that it remains a section "Entitled XYZ" according to this definition.
The Document may include Warranty Disclaimers
next to the notice which states that this License
applies to the Document.
These Warranty Disclaimers are considered to be included by reference
in this License, but only as regards disclaiming warranties: any other implication that these Warranty
Disclaimers may have is void and has no effect on
the meaning of this License. 2. VERBATIM COPYING
You may copy and distribute the Document in any
medium, either commercially or noncommercially,
provided that this License, the copyright notices,
and the license notice saying this License applies to
the Document are reproduced in all copies, and that
you add no other conditions whatsoever to those
of this License. You may not use technical measures to obstruct or control the reading or further
copying of the copies you make or distribute. However, you may accept compensation in exchange for
copies. If you distribute a large enough number of
copies you must also follow the conditions in section 3.
You may also lend copies, under the same conditions stated above, and you may publicly display
copies. 3. COPYING IN QUANTITY
If you publish printed copies (or copies in media
that commonly have printed covers) of the Document, numbering more than 100, and the Documents license notice requires Cover Texts, you

must enclose the copies in covers that carry, clearly

and legibly, all these Cover Texts: Front-Cover
Texts on the front cover, and Back-Cover Texts
on the back cover. Both covers must also clearly
and legibly identify you as the publisher of these
copies. The front cover must present the full title
with all words of the title equally prominent and
visible. You may add other material on the covers
in addition. Copying with changes limited to the
covers, as long as they preserve the title of the Document and satisfy these conditions, can be treated
as verbatim copying in other respects.
If the required texts for either cover are too voluminous to fit legibly, you should put the first ones
listed (as many as fit reasonably) on the actual
cover, and continue the rest onto adjacent pages.
If you publish or distribute Opaque copies of the
Document numbering more than 100, you must either include a machine-readable Transparent copy
along with each Opaque copy, or state in or with
each Opaque copy a computer-network location
from which the general network-using public has
access to download using public-standard network
protocols a complete Transparent copy of the Document, free of added material. If you use the latter option, you must take reasonably prudent steps,
when you begin distribution of Opaque copies in
quantity, to ensure that this Transparent copy will
remain thus accessible at the stated location until
at least one year after the last time you distribute
an Opaque copy (directly or through your agents or
retailers) of that edition to the public.
It is requested, but not required, that you contact the authors of the Document well before redistributing any large number of copies, to give them
a chance to provide you with an updated version of
the Document. 4. MODIFICATIONS
You may copy and distribute a Modified Version of
the Document under the conditions of sections 2
and 3 above, provided that you release the Modified Version under precisely this License, with the
Modified Version filling the role of the Document,
thus licensing distribution and modification of the
Modified Version to whoever possesses a copy of it.
In addition, you must do these things in the Modified Version:
* A. Use in the Title Page (and on the covers, if
any) a title distinct from that of the Document,
and from those of previous versions (which should,
if there were any, be listed in the History section
of the Document). You may use the same title as
a previous version if the original publisher of that
version gives permission. * B. List on the Title

Page, as authors, one or more persons or entities

responsible for authorship of the modifications in
the Modified Version, together with at least five of
the principal authors of the Document (all of its
principal authors, if it has fewer than five), unless
they release you from this requirement. * C. State
on the Title page the name of the publisher of the
Modified Version, as the publisher. * D. Preserve
all the copyright notices of the Document. * E. Add
an appropriate copyright notice for your modifications adjacent to the other copyright notices. * F.
Include, immediately after the copyright notices, a
license notice giving the public permission to use
the Modified Version under the terms of this License, in the form shown in the Addendum below. *
G. Preserve in that license notice the full lists of Invariant Sections and required Cover Texts given in
the Documents license notice. * H. Include an unaltered copy of this License. * I. Preserve the section
Entitled "History", Preserve its Title, and add to it
an item stating at least the title, year, new authors,
and publisher of the Modified Version as given on
the Title Page. If there is no section Entitled "History" in the Document, create one stating the title,
year, authors, and publisher of the Document as
given on its Title Page, then add an item describing the Modified Version as stated in the previous
sentence. * J. Preserve the network location, if any,
given in the Document for public access to a Transparent copy of the Document, and likewise the network locations given in the Document for previous
versions it was based on. These may be placed in
the "History" section. You may omit a network location for a work that was published at least four
years before the Document itself, or if the original
publisher of the version it refers to gives permission.
* K. For any section Entitled "Acknowledgements"
or "Dedications", Preserve the Title of the section,
and preserve in the section all the substance and
tone of each of the contributor acknowledgements
and/or dedications given therein. * L. Preserve all
the Invariant Sections of the Document, unaltered
in their text and in their titles. Section numbers or
the equivalent are not considered part of the section
titles. * M. Delete any section Entitled "Endorsements". Such a section may not be included in the
Modified Version. * N. Do not retitle any existing
section to be Entitled "Endorsements" or to conflict
in title with any Invariant Section. * O. Preserve
any Warranty Disclaimers.
If the Modified Version includes new front-matter
sections or appendices that qualify as Secondary
Sections and contain no material copied from the
Document, you may at your option designate some
or all of these sections as invariant. To do this, add
their titles to the list of Invariant Sections in the
Modified Versions license notice. These titles must
be distinct from any other section titles.
You may add a section Entitled "Endorsements",
provided it contains nothing but endorsements of
your Modified Version by various partiesfor example, statements of peer review or that the text
has been approved by an organization as the authoritative definition of a standard.
You may add a passage of up to five words as a
Front-Cover Text, and a passage of up to 25 words
as a Back-Cover Text, to the end of the list of Cover
Texts in the Modified Version. Only one passage of
Front-Cover Text and one of Back-Cover Text may
be added by (or through arrangements made by)
any one entity. If the Document already includes
a cover text for the same cover, previously added
by you or by arrangement made by the same entity
you are acting on behalf of, you may not add an-

other; but you may replace the old one, on explicit

permission from the previous publisher that added
the old one.
The author(s) and publisher(s) of the Document do
not by this License give permission to use their
names for publicity for or to assert or imply endorsement of any Modified Version. 5. COMBINING DOCUMENTS
You may combine the Document with other documents released under this License, under the terms
defined in section 4 above for modified versions,
provided that you include in the combination all
of the Invariant Sections of all of the original documents, unmodified, and list them all as Invariant
Sections of your combined work in its license notice, and that you preserve all their Warranty Disclaimers.
The combined work need only contain one copy of
this License, and multiple identical Invariant Sections may be replaced with a single copy. If there
are multiple Invariant Sections with the same name
but different contents, make the title of each such
section unique by adding at the end of it, in parentheses, the name of the original author or publisher
of that section if known, or else a unique number.
Make the same adjustment to the section titles in
the list of Invariant Sections in the license notice
of the combined work.
In the combination, you must combine any sections
Entitled "History" in the various original documents, forming one section Entitled "History"; likewise combine any sections Entitled "Acknowledgements", and any sections Entitled "Dedications".
You must delete all sections Entitled "Endorsements". 6. COLLECTIONS OF DOCUMENTS
You may make a collection consisting of the Document and other documents released under this License, and replace the individual copies of this License in the various documents with a single copy
that is included in the collection, provided that you
follow the rules of this License for verbatim copying
of each of the documents in all other respects.
You may extract a single document from such a collection, and distribute it individually under this License, provided you insert a copy of this License
into the extracted document, and follow this License in all other respects regarding verbatim copying of that document. 7. AGGREGATION WITH
INDEPENDENT WORKS
A compilation of the Document or its derivatives
with other separate and independent documents or
works, in or on a volume of a storage or distribution
medium, is called an "aggregate" if the copyright resulting from the compilation is not used to limit the
legal rights of the compilations users beyond what
the individual works permit. When the Document
is included in an aggregate, this License does not
apply to the other works in the aggregate which are
not themselves derivative works of the Document.
If the Cover Text requirement of section 3 is applicable to these copies of the Document, then if the
Document is less than one half of the entire aggregate, the Documents Cover Texts may be placed
on covers that bracket the Document within the
aggregate, or the electronic equivalent of covers
if the Document is in electronic form. Otherwise
they must appear on printed covers that bracket
the whole aggregate. 8. TRANSLATION

Translation is considered a kind of modification, so

you may distribute translations of the Document
under the terms of section 4. Replacing Invariant
Sections with translations requires special permission from their copyright holders, but you may include translations of some or all Invariant Sections
in addition to the original versions of these Invariant Sections. You may include a translation of this
License, and all the license notices in the Document,
and any Warranty Disclaimers, provided that you
also include the original English version of this License and the original versions of those notices and
disclaimers. In case of a disagreement between the
translation and the original version of this License
or a notice or disclaimer, the original version will
prevail.
If a section in the Document is Entitled "Acknowledgements", "Dedications", or "History", the requirement (section 4) to Preserve its Title (section
1) will typically require changing the actual title.
9. TERMINATION
You may not copy, modify, sublicense, or distribute
the Document except as expressly provided under
this License. Any attempt otherwise to copy, modify, sublicense, or distribute it is void, and will
automatically terminate your rights under this License.
However, if you cease all violation of this License,
then your license from a particular copyright holder
is reinstated (a) provisionally, unless and until the
copyright holder explicitly and finally terminates
your license, and (b) permanently, if the copyright
holder fails to notify you of the violation by some
reasonable means prior to 60 days after the cessation.
Moreover, your license from a particular copyright
holder is reinstated permanently if the copyright
holder notifies you of the violation by some reasonable means, this is the first time you have received
notice of violation of this License (for any work)
from that copyright holder, and you cure the violation prior to 30 days after your receipt of the
notice.
Termination of your rights under this section does
not terminate the licenses of parties who have received copies or rights from you under this License.
If your rights have been terminated and not permanently reinstated, receipt of a copy of some or all
of the same material does not give you any rights
to use it. 10. FUTURE REVISIONS OF THIS LICENSE
The Free Software Foundation may publish new, revised versions of the GNU Free Documentation License from time to time. Such new versions will be
similar in spirit to the present version, but may differ in detail to address new problems or concerns.
See http://www.gnu.org/copyleft/.
Each version of the License is given a distinguishing version number. If the Document specifies that
a particular numbered version of this License "or
any later version" applies to it, you have the option of following the terms and conditions either of
that specified version or of any later version that
has been published (not as a draft) by the Free Software Foundation. If the Document does not specify
a version number of this License, you may choose
any version ever published (not as a draft) by the
Free Software Foundation. If the Document specifies that a proxy can decide which future versions of

this License can be used, that proxys public statement of acceptance of a version permanently authorizes you to choose that version for the Document.
11. RELICENSING
"Massive Multiauthor Collaboration Site" (or
"MMC Site") means any World Wide Web server
that publishes copyrightable works and also provides prominent facilities for anybody to edit those
works. A public wiki that anybody can edit is
an example of such a server. A "Massive Multiauthor Collaboration" (or "MMC") contained in the
site means any set of copyrightable works thus published on the MMC site.
"CC-BY-SA"
means
the
Creative
Commons
Attribution-Share Alike 3.0 license published by
Creative Commons Corporation, a not-for-profit
corporation with a principal place of business in
San Francisco, California, as well as future copyleft
versions of that license published by that same
organization.
"Incorporate" means to publish or republish a Document, in whole or in part, as part of another Document.
An MMC is "eligible for relicensing" if it is licensed
under this License, and if all works that were first
published under this License somewhere other than
this MMC, and subsequently incorporated in whole
or in part into the MMC, (1) had no cover texts or
invariant sections, and (2) were thus incorporated
prior to November 1, 2008.
The operator of an MMC Site may republish an
MMC contained in the site under CC-BY-SA on the
same site at any time before August 1, 2009, provided the MMC is eligible for relicensing. ADDENDUM: How to use this License for your documents
To use this License in a document you have written,
include a copy of the License in the document and
put the following copyright and license notices just
after the title page:
Copyright (C) YEAR YOUR NAME. Permission is
granted to copy, distribute and/or modify this document under the terms of the GNU Free Documentation License, Version 1.3 or any later version published by the Free Software Foundation; with no
Invariant Sections, no Front-Cover Texts, and no
Back-Cover Texts. A copy of the license is included
in the section entitled "GNU Free Documentation
License".
If you have Invariant Sections, Front-Cover Texts
and Back-Cover Texts, replace the "with . . .
Texts." line with this:
with the Invariant Sections being LIST THEIR TITLES, with the Front-Cover Texts being LIST, and
with the Back-Cover Texts being LIST.
If you have Invariant Sections without Cover Texts,
or some other combination of the three, merge
those two alternatives to suit the situation.
If your document contains nontrivial examples of
program code, we recommend releasing these examples in parallel under your choice of free software
license, such as the GNU General Public License,
to permit their use in free software.

20.3 GNU Lesser General Public License

GNU LESSER GENERAL PUBLIC LICENSE
Version 3, 29 June 2007
Copyright 2007 Free Software Foundation, Inc.
<http://fsf.org/>
Everyone is permitted to copy and distribute verbatim copies of this license document, but changing
it is not allowed.
This version of the GNU Lesser General Public License incorporates the terms and conditions of version 3 of the GNU General Public License, supplemented by the additional permissions listed below.
0. Additional Definitions.
As used herein, this License refers to version 3
of the GNU Lesser General Public License, and the
GNU GPL refers to version 3 of the GNU General
Public License.
The Library refers to a covered work governed by
this License, other than an Application or a Combined Work as defined below.
An Application is any work that makes use of an
interface provided by the Library, but which is not
otherwise based on the Library. Defining a subclass
of a class defined by the Library is deemed a mode
of using an interface provided by the Library.
A Combined Work is a work produced by combining or linking an Application with the Library.
The particular version of the Library with which
the Combined Work was made is also called the
Linked Version.
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