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Picture Galleries

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Gallery Sitemap
Aquaporins

Bakunin, Mikhail
Mikhail Bakunin

Bassler, Bonnie L.


  • Bassler, Bonnie (2010a). Part 1: Bacterial Communication via Quorum Sensing. iBiology - Cell Biology Lectures. Princeton University/HHMI (published March 27, 2010). video (0:28:54)
  • Bassler, Bonnie (2010b). Part 2: Vibrio Cholerae Quorum Sensing and Novel Antibiotics. iBiology - Cell Biology Lectures. Princeton University/HHMI (published March 27, 2010). video (0:19:45)
  • Bassler, Bonnie (2017). Tiny Conspiracies. iBiology - Cell Biology Lectures. Princeton University/HHMI (published November 20, 2017). video (0:26:33)

Cavalier-Smith, Thomas
Thomas Cavalier-Smith






Changeux, Jean-Pierre
Jean-Pierre Changeux

Chomsky, Noam
Noam Chomsky

Darwin, Charles
Charles Darwin

Descartes, René
René Descartes

Dorsal-Ventral Inversion

Doudna, Jennifer A.
Jennifer Doudna

Edelman, Gerald M.
Gerald M. Edelman
The Ubiquity of Degeneracy in Biological Systems

"Degeneracy, the ability of elements that are structurally different to perform the same function or yield the same output, is a well known characteristic of the genetic code and immune systems. Here, we point out that degeneracy is a ubiquitous biological property and argue that it is a feature of complexity at genetic, cellular, system, and population levels. Furthermore, it is both necessary for, and an inevitable outcome of, natural selection."[14]

Gerald M. Edelman & Joseph A, Gally (2001)







Éliade, Mircéa
Mircéa Éliade

Epithelial–Mesenchyme Transitions

Faraday, Michael
Michael Faraday

Fuller, Buckminster
Buckminster Fuller




Golgi, Camillo
Camillo Golgi




HOX Clusters


Kandel, Eric
Eric Kandel

Krishnamurti, Jiddu
Jiddu Krishnamurti

Metchnikoff, Élie
Elie Metchnikoff

Microtubule Organizing Center


Onsager, Lars
Lars Onsager

Please support the courageous people of Ukraine.

Please support the courageous people of Ukraine.


Ramachandran, Vilayanur S.
Vilayanur S Ramachandran

Ramón y Cajal, Santiago
Santiago Ramón y Cajal




Romer, Alfred Sherwood

The Functional Welding of the CNS to the ENS - The Autonomic Nervous System


"To sum up the phylogenetic suggestions gained from a consideration of the structure of the nervous system in living vertebrates, high and low, and of their chordate and protochordate "ancestors," one tends strongly to gain the impression that the remote "visceral" ancestral form had a simple superficial nerve net and, at some early stage, acquired a visceral nerve net as well; that, with the development of the "somatic" animal, there developed the central nervous system, with segmental nerves including a ventral root of somatic motor type and a distinct dorsal root at first composed merely of somatic sensory neurons; but that there was a strong tendency for the somatic animal to attempt neural control over the visceral animal, first perhaps, by a direct connection with the important visceral muscles of the pharynx, later by an attempt to dominate the gut by autonomic fibers, originally by way of dorsal nerve roots, running to the postganglionic neurons, which represent elements of the original gut nerve net. The development of visceral centers in brain and cord was associated with this attempt at domination of the visceral by the somatic animal. But, as we are ourselves aware, the integration of the visceral animal into the dominant nervous system of our somatic being is still far from perfect."[25]

Alfred Sherwood Romer (1972)



The Functional Welding of the CNS to the ENS - Gaining Control


"It is not unreasonable to speculate on the possibility that: The ancestor of the vertebrates may have had, like many invertebrate types, an essentially independent visceral nerve net; that the development of the autonomic system represents an attempt by the central nervous system at gaining control over visceral activity; and that possibly in the peculiar two-neuron system seen here, the post-ganglionic neurons may be representatives of the original visceral nerve net system, the pre-ganglionics representatives of attempts at domination by the central nervous system."[25]

Alfred Sherwood Romer (1972)



Senescence & The Purpose Of The Soma

The Immune System

The Neural Crest

Tunicates

Notes & Commentary

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Notes & Commentary
  1. Subject to major change, revision ,and/or retraction at any moment.
  2. 173-Aquaporin 1fqy
  3. Depicting the six transmembrane alpha-helices and the five interhelical loop regions A-E
  4. Reconstructed by the maximum likelihood method for 78 protein-coding genes. Numbers beside the internal nodes are maximum likelihood bootstrap values obtained from RaxML and Bayesian MCMC posterior probabilities. Black circles indicate 100% bootstrap support and 1.00 posterior probability values.
  5. A: hedgehog and B: Notch homologues. The illustrated domains are some of those found by searches against the Conserved Domain Database. Numbers at the species names are accession numbers, protein IDs from the Joint Genome Institute (JGI) and references where annotation recently have been presented. Domain structure identified in Ministeria is compared with animals - Porifera (Amphimedon and Oscarella), Cnidaria (Nematostella) and Chordata (Homo) - and the choanoflagellate Monosiga. Abbreviations: Hh-signal domain, N-terminal hedgehog domain; Hint cleavage site, cleavage site of the C-terminal hedgehog domain; Hint domain, C-terminal hedgehog domain; Notch(DSL), Notch domain also called Delta Serrate Ligand; EGF, epidermal growth factor domain; NL, domain found in Notch and Lin-12; NOD, NOD region; NODP, NODP region; ANK, ankyrin reapeats; PTP, protein tyrosine phosphatase.
  6. The five choanozoan classes (bold) form at least four distinct clades, one probably related to fungi and the others to animals. Innovations in pseudopod character and their multiple losses with the origin of cell walls during nutritional shifts from engulfing prey (phagotrophy) to saprotrophy or parasitism are indicated by bars. In the common ancestor of animals and choanoflagellates a subset of the filozoan actin-supportd tentacles aggregated as a collar around the cilium (flagellum) for filter feeding. Epithelia and connective tissue made the first animals: the filter-feeding sponges.
  7. Cell structure divergence in phagotrophic non-amoeboid flagellates provided the basis for evolving animals, fungi, plants and chromists. Original description: "Cell structure divergence in phagotrophic non-amoeboid flagellates provided the basis for evolving animals, fungi, plants and chromists.
    Pseudopodia evolved secondarily, myosin II providing the basis for pseudopodia in animals, Amoebozoa (and Percolozoa) and muscles.
    Chloroplasts, originating when the plant ancestor enslaved and modified undigested cyanobacteria, were transferred laterally (red arrow) to make chromists (e.g. brown seaweeds, diatoms, dinoflagellates) whose ancestor modified an enslaved undigested red alga.
    The most basic eukaryote structural dichotomy contrasts Euglenozoa (parallel centrioles; cilia with paraxonemal rods; cytopharynx for feeding) and excavates (Percolozoa, Eolouka, Neolouka: orthogonal centrioles: no paraxonemal rods; feeding by phagocytosing prey drawn into a ventral groove by posterior ciliary currents).
    The pre-animal lineage lost excavate groove-feeding by evolving ventral ciliary gliding locomotion to generate Sulcozoa, protozoa with a dorsal proteinaceous pellicle (blue).
    Irrespective of whether the eukaryote tree is rooted within the protozoan subkingdom Eozoa as shown (most likely) or beside Eolouka-like Reclinomonas with the most primitive mitochondria, the immediate ancestors of animals (Choanozoa) arose by loss of the anterior cilium and sulcozoan dorsal pellicle to make opisthokonts (in red) with a radically simplified, more radially symmetric, microtubular cytoskeleton.
    Long actin-supported filodigits arose in the ancestor of Filosporidia and choanoflagellates and became a circlet of microvilli to make the choanoflagellate/sponge collar for catching bacteria. Filosporidia comprise Filasterea, Ichthyosporea, Corallochytrea.
    The four derived kingdoms (e.g. ANIMALIA, PLANTAE) are shown in upper case; all taxa in lower case belong to the basal eukaryotic kingdom Protozoa." - Of interest to us on our journey towards animals are: myosin, integrins, catenins, cadherins, epithelia, gametes (sperm and egg), and extracellular matrix (ECM).
  8. Taken from Charles Darwin's Notebook B - On the Transmutation of Species (1837).
    This is Darwin's first diagram showing his thoughts on evolutionary diversification. Gerald Edelman's Neural Darwinism would be published 150 years later - a fitting tribute to the enduring power of Darwin's ideas. Although many will claim that this is the first evolutionary tree diagram, it is more of a bush, if anything, and Darwin's initial instincts are prescient.
  9. Wellcome L0051068
  10. Four types of finch: 1: Geospiza magnirostris; 2. Geospiza fortis; 3. Geospiza parvula; 4. Gerthidea olivacea. (Charles Darwin, Journal of Researches... Wellcome_L0026712)
  11. The regional expression of genes associated with the establishment of the dorsal-ventral axis (DV-axis) of the bilaterian body plan during development is inverted in the embryos of chordates (deuterostomes) relative to that of the arthropods (protostomes). Chordates are characterized by a hollow dorsal nerve cord and a ventral heart, while arthropods are characterized by a ventral nerve chord and a dorsal heart.
  12. Protostomes generally, but not always, undergo spiral cleavage followed by formation of the mouth from the blastopore during gastrulation. The protostome coelom and mesoderm are induced at the blastopore end in protostomes to form between the endoderm and ectoderm. Deuterostomes generally undergo radial cleavage followed by formation of the anus from the blastopore during gastrulation. The coelum and mesoderm are derived from invaginations of the archentron on the opposite side from the blastopore.
  13. Description: 1) Degeneracy is the source of Robustness. 2) Degeneracy is positively correlated with Complexity. 3) Degeneracy increases Evolvability. 4) Evolvability is a prerequisite for Complexity. 5) Complexity increases to improve Robustness. 6) Evolvability emerges from Robustness.
  14. The ingenuous 1964 Nirenberg and Leder experiment would identify the mRNA codons, a triplet sequence of ribonucleotides, that coded for each amino acid; thus elucidating the universal genetic code within the DNA when the transcription process was taken into account. Changes in the third position of the codon, the wobble position, often result in the same amino acid, and oftentimes the choice comes down to purine or pyrimidine only when a choice must be made. Similar, but variant, codon sequences tend to yield similar classes of amino acid - polar to polar, non-polar to non-polar, acidic to acidic, and basic to basic residues.
  15. The twenty biological amino acids breakdown into four major classes of biological amino acids - polar (hydrophilic), nonpolar (hydrophobic), acidic, and basic side chain residues. The amino acid backbone is an amino group linked to an α-carbon, on which resides the side chain residue and a hydrogen atom, that is connected to a terminal carboxylate group.
  16. Neuron counts of cerebral cortex and cerebellum - The cerebellum is a key player in integrating the output of the thalamocortical system with the subcortical system. Notice the greater than four-fold abundance of neurons in the cerebellum relative to the neocortex.
  17. Superior-pattern-processing-is-the-essence-of-the-evolved-human-brain-fnins-08-00265-g0002[15] - Structural features of the brains of mammals are conserved from rodents to humans. The upper drawings show the hippocampal formation of an adult human, a kitten and a young mouse. The lower two drawings show the cellular organization of the cerebral cortex of an adult human and an adult mouse, both of which exhibit six cell layers. All of the drawings are adapted from Santiago Ramon y Cajal (DeFelipe and Jones, 1988). CA, cornu ammonis; DG, dentate gyrus; SUB, subiculum.
  18. Lawrence 1960 22.4
  19. Epithelia to mesenchyme (EMT) and Mesenchyme to epithelia (MET) transisitions utilizing CAMs and SAMs to form epethelia; and, growth factors and inducers to mediate the transition to mesenchyme as the CAMs and SAMs are withdrawn or localized on the cell membrane. This figure is from Hill & Wang 2020, The importance of epithelial-mesenchymal transition and autophagy in cancer drug resistance. The connection between the cellular processes of cancer and the cellular processes of embryogenesis are not far fetched. These are the very processes that were undergoing selection at the origin of animals as they transitioned from unicellular organisms to multicellular organisms.[17][18] Cancer is an example of cells that have escaped the developmental constraints of the multicellular organism and reverted to their ancestral pattern of immortal reproduction in the absence of the inhibitory mechanisms on reproduction that proper bodyplan formation requires. One could say that cancer is a problem of morphology.
  20. September 2004
  21. Artist Diego Rivera shown entering the car, carrying coat
  22. Prefabricated bathroom, by Richard Buckminster Fuller, issued 1940
  23. The cytoskeleton is a dynamic structure and microtubules play an important role in determining the architectural state of differentiation for specialized cells. In many ways, the dynamic action of microtubules manifests one of the first, and most easily observable, indications in cells of what we would recognize as life - flagellar motility and/or the amoeboid exploration of the environment through process extension and retraction - all processes determined by the adaptive dynamics of microtubule formation and dissolution.
  24. Multicellular lifecycle diagrams in terms of soma and germ line populations in A.) Plants, B.) Animals, C.) Fungi - (1) Meiosis, leading to the production of germ, (2) Mitosis, leading to production of soma and amplifying germ line populations (3) Sexual Recombination of germ lines within the species population
  25. Histologie du Système Nerveux de l'Homme et des Vertébrés, Vols. 1 and 2. A. Maloine. Paris. 1911
  26. Cajal Institute (CSIC), Madrid
  27. Cajal Institute (CSIC), Madrid
  28. Wellcome L0040799
  29. Wellcome L0040800
  30. Wellcome L0040801
  31. Wellcome L0040802
  32. Wellcome L0002048
  33. Wellcome L0001365
  34. from Estructura de los centros nerviosos de las aves, Madrid, 1905
  35. Instituto Santiago Ramón y Cajal, Madrid, Spain, 1899
  36. a, axon; b, recurrent collateral; c and d, spaces in the dendritic arborization for stellate cells; see Fig. 9 in Texture of the Nervous System of Man and the Vertebrates, Volume 1, Originally published by Springer-Verlag Wien New York in 1999
  37. Cajal Institute (CSIC), Madrid
  38. Cajal Institute (CSIC), Madrid
  39. O - Optic chiasm; C - Visual (and motor) cortex; M, S - Decussating pathways; R, G: Sensory nerves, motor ganglia.
  40. a,b,c: bifurcating optic fibres. c: fibre bifurcating in the two opposite optic tracts. d. Commisure of Gudden. e. Fibres that continue in a different depth. Cajal 1898, Fig6
  41. Artistic grouping of cells and direction of current flow.
  42. from Estructura de los centros nerviosos de las aves, Madrid, 1905
  43. Madrid, 1900
  44. Cajal, 1911
  45. The hallmarks, causes and effects of cellular senescence. (a) The key features of a senescent cell. (b) Senescence occurs in response to multiple contingencies of life (c) Senescence plays a dual role in development and tissue repair/regeneration.
  46. Description: Scanning Electron Microscope (SEM) image of leukocytes, red blood cells platelets circulating in the human bloodstream.
  47. Description: Illustration of disulfide bridges (red) linking the light (L, green) and heavy (H, purple) chains of Immunoglobulin G (IgG) antibody. The variable (V) regions are located at the antigen-binding end; and, the constant (C) domains form the primary frame of the IgG molecule. Another disulfide bridge holds the two symmetrical units made up of a light chain (VL+CL) and a heavy chain (VH+CH1+CH2+CH3) together to form the completed antibody. Work by Rodney Porter with the enzyme papain resulted in cleavage of the antibody into Fab and Fc fragments, while work by Gerald Edelman lead to the reduction of the disulfide bridges so as to separate the molecule into light- and heavy-chain fragments. Together, this work allowed the antibody structure to be sequenced and reconstructed, resulting in the awarding of the Nobel Prize in Physiology or Medicine in 1972.
  48. Description: The immune system has an ancient history within animals. All animals have an innate immune system, but only vertebrates have an "active" antibody-based immune system. The innate (left branch) immune system is ancient and anchored around the phagocytic white blood cells discovered by the pioneering biologist, embryologist, zoologist, immunologist, gerantologist Élie Metchnikoff (May 15, 1845–July 15, 1916).[18]. The antibody-based system (right branch) arose at the origin of vertebrates and is associated with the genome duplication events[27] that provided the duplicate copies of NCAM which eventually resulted in the emergence of genetically recombinant antibodies.[28][29] Paul Ehrlich (March 14, 1854–August 20, 1915)) was the discoverer of antibodies - and, along with Elie Metchnikoff, is considered to be one of the founders of Immunology. In 1908, they would share the first Nobel Prize in Physiology or Medicine. 64 years later, Edelman and Porter would share this very same prize.
  49. Description: Clonal selection theory (CST) - hematopoietic stem cells (1) differentiate and undergo genetic rearrangement to produce a population of cells possessing a wide range of pre-existing diversity with respect to antibody expression (2). Lymphocytes expressing antibodies that would lead to autoimmunity are filtered from the population (3), while the rest of the population represents a degenerate pool of diversity (4) where antigen-selected variants (5) can be differentially amplified in response (6). Once the antigen has been cleared, the responding population will decrease, but not by as much as it was amplified, leaving behind a boosted capacity to respond to future incursions by the antigen - a form of enhanced recognition and memory within the system.
  50. Induction of the Neural crest during neuralation. Once the neural tube has successfully formed and the neural crest cells delaminate from the neural tube and ectoderm by down regulating their CAMs.


Citations

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List of Citations
  1. Cavalier-Smith 2010a.
  2. Cavalier-Smith 2006c.
  3. Cavalier-Smith 2010b.
  4. Cavalier-Smith 2017.
  5. Shalchian-Tabrizi et al. 2008, Fig.1.
  6. Shalchian-Tabrizi et al. 2008, Fig.2.
  7. Shalchian-Tabrizi et al. 2008, Fig.3.
  8. Cavalier-Smith 2017, Fig.1.
  9. Cavalier-Smith 2017, Fig. 2.
  10. Cavalier-Smith 2017, Fig. 3.
  11. Darwin 1837.
  12. Darwin 1859.
  13. Darwin 1872.
  14. Edelman & Gally 2001.
  15. Mattson 2014.
  16. Hill & Wang 2020.
  17. Buss 1987.
  18. 18.0 18.1 Tauber & Chernyak 1991.
  19. 19.0 19.1 Golgi 1885.
  20. Piper 1999.
  21. Akkari 2014.
  22. Hueber 2010.
  23. Lynch 2009.
  24. Chifflet 2012.
  25. 25.0 25.1 Romer 1972.
  26. Elder & Emmerson 2020, Fig. 1.
  27. Dehal & Boore 2005.
  28. Edelman 1987b.
  29. Edelman 1992, p. 206-207.


Sources & References

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