Schizophrenia: Overview and Treatment Options

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Schizophrenia: Overview and Treatment Options

Krishna R. Patel, PharmD, RPh; Jessica Cherian, PharmD, RPh; Kunj Gohil, PharmD, RPh; and Dylan
Atkinson
INTRODUCTION
Schizophrenia is a complex, chronic mental health disorder characterized by an array of symptoms, including delusions,
hallucinations, disorganized speech or behavior, and impaired cognitive ability. The early onset of the disease, along with its
chronic course, make it a disabling disorder for many patients and their families.1 Disability often results from both negative
symptoms (characterized by loss or deficits) and cognitive symptoms, such as impairments in attention, working memory, or
executive function.2 In addition, relapse may occur because of positive symptoms, such as suspiciousness, delusions, and
hallucinations.1,2 The inherent heterogeneity of schizophrenia has resulted in a lack of consensus regarding the disorder’s
diagnostic criteria, etiology, and pathophysiology.1,3
This article provides a concise review of schizophrenia and discusses the available treatment options.
PATHOPHYSIOLOGY
Abnormalities in neurotransmission have provided the basis for theories on the pathophysiology of schizophrenia. Most of
these theories center on either an excess or a deficiency of neurotransmitters, including dopamine, serotonin, and glutamate.
Other theories implicate aspartate, glycine, and gamma-aminobutyric acid (GABA) as part of the neurochemical imbalance of
schizophrenia.1
Abnormal activity at dopamine receptor sites (specifically D
2
) is thought to be associated with many of the symptoms of schizophrenia. Four dopaminergic pathways have been implicated
(Figure 1).4,5 The nigrostriatal pathway originates in the substantia nigra and ends in the caudate nucleus. Low dopamine levels
within this pathway are thought to affect the extrapyramidal system, leading to motor symptoms.1 The mesolimbic pathway,
extending from the ventral tegmental area (VTA) to limbic areas, may play a role in the positive symptoms of schizophrenia in
the presence of excess dopamine.1 The mesocortical pathway extends from the VTA to the cortex. Negative symptoms and
cognitive deficits in schizophrenia are thought to be caused by low mesocortical dopamine levels. The tuberoinfundibular
pathway projects from the hypothalamus to the pituitary gland. A decrease or blockade of tuberoinfundibular dopamine results
in elevated prolactin levels and, as a result, galactorrhea, ammenorrhea, and reduced libido.
The serotonin hypothesis for the development of schizophrenia emerged as a result of the discovery that lysergic acid
diethylamide (LSD) enhanced the effects of serotonin
Dr. Patel is a Clinical Services Manager at MediMedia Managed Markets in Yardley, Pennsylvania. Dr. Cherian is a Clinical
Services Manager at MediMedia Managed Markets as well as a community pharmacist. Dr. Gohil is a Postdoctoral Fellow with
Medical Services at MediMedia Managed Markets. Mr. Atkinson is a candidate for a doctorate in pharmacy at the University of
Pittsburgh School of Pharmacy.
Disclosure: The authors report no commercial or financial relationships in regard to this article.
• September 2014 • Vol. 39 No. 9
in the brain.1 Subsequent research led to the development of drug compounds that blocked both dopamine and serotonin
receptors, in contrast to older medications, which affected only dopamine receptors. The newer compounds were found to be
effective in alleviating both the positive and negative symptoms of schizophrenia.1
Another theory for the symptoms of schizophrenia involves the activity of glutamate, the major excitatory neurotransmitter in
the brain. This theory arose in response to the finding that phenylciclidine and ketamine, two noncompetitive NMDA/ glutamate
antagonists, induce schizophrenia-like symptoms.6 This, in turn, suggested that NMDA receptors are inactive in the normal
regulation of mesocortical dopamine neurons, and pointed to a possible explanation for why patients with schizophrenia exhibit
negative, affective, and cognitive symptoms.7
The brain tissue itself appears to undergo detectable physical changes in patients with schizophrenia. For example, in addition
to an increase in the size of the third and lateral ventricles, individuals at high risk of a schizophrenic episode have a smaller
medial temporal lobe.2
ETIOLOGY
Despite more than a century of research, the precise cause of schizophrenia continues to elude investigators. It is widely
accepted, however, that the various phenotypes of the illness arise from multiple factors, including genetic susceptibility and
environmental influences.2,8
One explanation for the development of schizophrenia is that the disorder begins in utero.6 Obstetric complications, including
bleeding during pregnancy, gestational diabetes, emergency cesarean section, asphyxia, and low birth weight, have been
associated with schizophrenia later in life.2 Fetal disturbances during the second trimester—a key stage in fetal
neurodevelopment—have been of particular interest to researchers.3 Infections and excess stress levels during this period have
been linked to a doubling of the risk of offspring developing schizophrenia.3
Scientific evidence supports the idea that genetic factors play an important role in the causation of schizophrenia; 2 studies
have shown that the risk of illness is approximately 10% for a first-degree relative and 3% for a second-degree relative.9 In the
case of monozygotic twins, the risk of one twin having schizophrenia is 48% if the other has the disorder, whereas the risk is 12%
to 14% in dizygotic twins.9 If both parents have schizophrenia, the risk that they will produce a child with schizophrenia is
approximately 40%.9
Studies of adopted children have been conducted to determine whether the risk of schizophrenia comes from the biological
parents or from the environment in which the child is raised. These investigations have tended to show that changes in the

environment do not affect the risk of developing schizophrenia in children born to biological parents with the illness.3,6 A
genetic basis for schizophrenia is further supported by findings that siblings with schizophrenia often experience onset of the
disorder at the same age.2
Environmental and social factors may also play a role in the development of schizophrenia, especially in individuals who are
vulnerable to the disorder.1 Environmental stressors linked to schizophrenia include childhood trauma, minority ethnicity,
residence in an urban area, and social isolation.1 In addition, social stressors, such as discrimination or economic adversity, may
predispose individuals toward delusional or paranoid thinking.1
EPIDEMIOLOGY
The prevalence of schizophrenia is between 0.6% and 1.9% in the U.S. population.10 Moreover, a claims analysis has
estimated that the annual prevalence of diagnosed schizophrenia in the U.S. is 5.1 per 1,000 lives.11 The prevalence of the
disorder seems to be equal in males and females, although the onset of symptoms occurs at an earlier age in males than in
females.2 Males tend to experience their first episode of schizophrenia in their early 20s, whereas women typically experience
their first episode in their late 20s or early 30s.12
Research into a possible link between the geography of birth and the development of schizophrenia has provided

Figure 1 Pathophysiology of Schizophrenia4,5
Endogenous dopamine
Frontal lobe
Endogenous dopamine
Pituitary gland
Mesocortical pathway
Hypodopaminergic function in the frontal portions of the brain is the cause of
Nigrostriatal pathway
negative symptoms and
Mesolimbic pathway cognitive
impairment in schizophrenia.
Tuberoinfundibular pathway
inconclusive results. A collaborative study by the World Health Organization in 10 countries found that schizophrenia occurred
with comparable frequencies across the various geographi- cally defined populations.13 On the other hand, a more recent review,
which included data from 33 countries, concluded that the incidence of schizophrenia varied by geographic location.14
CLINICAL PRESENTATION
Schizophrenia is the most common functional psychotic disorder, and (as noted previously) individuals with the disorder can
present with a variety of manifestations. Contrary to portrayals of the illness in the media, schizophrenia does not involve a “split
personality.” Rather, it is a chronic psychotic disorder that disrupts the patient’s thoughts and affect. The illness commonly
interferes with a patient’s ability to participate in social events and to foster meaningful relationships.2
Social withdrawal, among other abnormal (schizoid) behaviors, typically precedes a person’s first psychotic episode; however,
some individuals may exhibit no symptoms at all.2 A psychotic episode is characterized by patient-specific signs and symptoms
(psychotic features) that reflect the “false reality” created in the patient’s mind.2,15
As noted earlier, the symptoms of schizophrenia are catego- rized as positive, negative, or cognitive. Each symptom is vitally
important as the clinician attempts to distinguish schizophrenia from other psychotic disorders, such as schizoaffective dis-
Substantia nigra
Vol. 39 No. 9 • September 2014 •
Hyperdopaminergic function in the caudate nucleus is the cause of positive symptoms such as movement disorders in
schizophrenia.
• •
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order, depressive disorder with psychotic features, and bipolar disorder with psychotic features.12
Positive symptoms are the most easily identified and can be classified simply as “psychotic behaviors not seen in healthy
people.”15 Such symptoms include delusions, hallucinations, and abnormal motor behavior in varying degrees of severity.12
Negative symptoms are more difficult to diagnose but are associated with high morbidity as they disturb the patient’s emo- tions
and behavior.12,15 The most common negative symptoms are diminished emotional expression and avolition (decreased
initiation of goal-directed behavior). Patients may also experience alogia and anhedonia. It is important to understand that
negative symptoms may be either primary to a diagnosis of schizophrenia or secondary to a concomitant psychotic diagnosis,
medication, or environmental factor.12,16
Cognitive symptoms are the newest classification in schizophrenia. These symptoms are nonspecific; therefore, they must be
severe enough for another individual to notice them. Cognitive symptoms include disorganized speech, thought, and/or attention,
ultimately impairing the individual’s ability to communicate.12,16
Patients with symptoms of schizophrenia may experience additional limitations and negative conditions. Substance-abuse
disorders occur most often among these patients; these disorders can involve a variety of substances, including alcohol, tobacco,
and prescription medications.12,16 Anxiety, depression, panic, and obsessive-compulsive disorder are also prominent in patients
with schizophrenia and can exacerbate the symptoms of their disorder.12,16 These patients also have a general lack of awareness
of their illness. This mindset has been linked to high rates of nonadherence, relapse, poor psychosocial function, poor hygiene,
and worse disease outcomes.2,12
The primary symptoms and comorbid conditions associated with schizophrenia may ultimately lead to social and occupa-
tional dysfunction.12 Functional consequences include an inadequate or incomplete education, which may affect the patient’s
ability to obtain and hold a stable job. Patients with schizophrenia typically cultivate few social relationships and need daily
support to manage relapses and recurring symptoms.12,16
The prognosis for patients with schizophrenia is generally unpredictable.2 Only 20% of patients report favorable treatment
outcomes.12 The remaining patients experience numerous psychotic episodes, chronic symptoms, and a poor response to
antipsychotics.2
DIAGNOSIS
As described earlier, schizophrenia is a chronic disorder with numerous symptoms, where no single symptom is pathogenic. A
diagnosis of schizophrenia is reached through an assessment of patient-specific signs and symptoms, as described in the
Diagnostic and Statistical Manual of Mental Disorders, Fifth Edition (DSM-5).12 The DSM-5 states that “the diagnostic criteria
[for schizophrenia] include the persistence of two or more of the following active-phase symptoms, each lasting for a significant
portion of at least a one-month period: delusions, hallucinations, disorganized speech, grossly disorganized or catatonic behavior,
and negative symptoms.”12 At least one of the qualifying symptoms must be delusions, hallucinations, or disorganized speech.12

Moreover, the DSM-5 states that, to warrant a diagnosis of schizophrenia, the patient must also exhibit a decreased level of
functioning regarding work, interpersonal relationships, or self-care.12 There must also be continuous signs of schizophrenia
for at least six months, including the one-month period of active-phase symptoms noted above.12
A comprehensive differential diagnosis of schizophrenia is necessary to distinguish the disorder from other mental con-
ditions, such as major depressive disorder with psychotic or catatonic features; schizoaffective disorder; schizophreniform
disorder; obsessive-compulsive disorder; body dysmorphic disorder; and post-traumatic stress disorder. Schizophrenia can be
differentiated from these similar conditions through a careful examination of the duration of the illness, the timing of delusions or
hallucinations, and the severity of depressive or manic symptoms.12 In addition, the clinician must confirm that the presenting
symptoms are not a result of substance abuse or another medical condition.12
TREATMENT OPTIONS Nonpharmacological Therapy
The goals in treating schizophrenia include targeting symptoms, preventing relapse, and increasing adaptive functioning so
that the patient can be integrated back into the community.2 Since patients rarely return to their baseline level of adaptive
functioning, both nonpharmacological and pharmacological treatments must be used to optimize long-term outcomes.2
Pharmacotherapy is the mainstay of schizophrenia management, but residual symptoms may persist. For that reason,
nonpharmacological treatments, such psychotherapy, are also important.17
Psychotherapeutic approaches may be divided into three categories: individual, group, and cognitive behavioral (Figure 2).2
Psychotherapy is a constantly evolving therapeu-
Figure 2 Psychotherapeutic Approaches2
Psychotherapy
Cognitive Behavioral: 1. Cognitive behavioral therapy 2. Compliance therapy
Individual: 1. Supportive/counseling 2. Personal therapy 3. Social skills therapies 4. Vocational sheltered employ- ment
rehabilitation therapies
Group: 1. Interactive/social

tic area. Emerging psychotherapies include meta-cognitive training, narrative therapies, and mindfulness therapy.17
Nonpharmacological treatments should be used as an addition to medications, not as a substitute for them.2
Not only do nonpharmacological therapies fill in gaps in pharmacological treatments; they can help to ensure that patients remain
adherent to their medications.18 Nonadherence rates in schizophrenia range from 37% to 74%, depending on the report.19
Individuals with mental disorders tend to be less adherent for several reasons. They may deny their illness; they may experience
adverse effects that dissuade them from taking more medication; they may not perceive their need for medication; or they may
have grandiose symptoms or paranoia.2 Patients with schizophrenia who stop taking their medication are at increased risk of
relapse, which can lead to hospitalization.18 Therefore, it is important to keep patients informed about their illness and about
the risks and effectiveness of treatment.20 Some psychotherapies can help educate patients about the importance of taking their
medications. These ini- tiatives include cognitive behavioral therapy (CBT), personal therapy, and compliance therapy.17
In addition to focusing on the patient, treatment programs that encourage family support have been shown to decrease
rehospitalization and to improve social functioning.2 Family members can be taught how to monitor the patient and when to
report adverse effects of treatment to the clinician.20 Most psychotherapies promote family involvement.17
Pharmacological Therapy
In most schizophrenia patients, it is difficult to implement effective rehabilitation programs without antipsychotic agents.16
Prompt initiation of drug treatment is vital, especially within five years after the first acute episode, as this is when most
illness-related changes in the brain occur.16,21 Predictors of a poor prognosis include the illicit use of amphetamines and other
central nervous system stimulants,22 as well as alcohol and drug abuse.2 Alcohol, caffeine, and nicotine also have the potential
to cause drug interactions.2
In the event of an acute psychotic episode, drug therapy should be administered immediately. During the first seven days of
treatment, the goal is to decrease hostility and to attempt to return the patient to normal functioning (e.g., sleep- ing and eating).2
At the start of treatment, appropriate dosing should be titrated based on the patient’s response.2
Treatment during the acute phase of schizophrenia is followed by maintenance therapy, which should be aimed at increasing
socialization and at improving self-care and mood.2 Maintenance treatment is necessary to help prevent relapse. The incidence of
relapse among patients receiving maintenance therapy, compared with those not receiving such therapy, is 18% to 32% versus
60% to 80%, respectively.16,23 Drug therapy should be continued for at least 12 months after the remission of the first psychotic
episode.16,24
According to the American Psychiatric Association, second- generation (atypical) antipsychotics (SGAs)—with the exception
of clozapine—are the agents of choice for first-line treatment of schizophrenia.16,25 Clozapine is not recommended because of
its risk of agranulocytosis.2 SGAs are usually preferred over first- generation (typical) antipsychotics (FGAs) because they are

associated with fewer extrapyramidal symptoms.2 However, SGAs tend to have metabolic side effects, such as weight gain,
hyperlipidemia, and diabetes mellitus.26 These adverse effects can contribute to the increased risk of cardiovascular mortality
observed in schizophrenia patients.26
The Texas Medication Algorithm Project (TMAP) has provided a six-stage pharmacotherapeutic algorithm for the treatment
of schizophrenia. Stage 1 is first-line monotherapy with an SGA. If the patient shows little or no response, he or she should
proceed to stage 2, which consists of monotherapy with either another SGA or an FGA. If there is still no response, the patient
should move to stage 3, which consists of clozapine monotherapy with monitoring of the white blood cell (WBC) count.24 If
agranulocytosis occurs, clozapine should be discontinued. If stage-3 therapy fails to elicit a response, the patient should proceed
to stage 4, which combines clozapine with an FGA, an SGA, or electroconvulsive therapy (ECT).24 If the patient still shows no
response to treatment, stage 5 calls for monotherapy with an FGA or an SGA that has not been tried.24 Finally, if stage 5
treatment is unsuccessful, stage 6 consists of combination therapy with an SGA, an FGA, ECT, and/or a mood stabilizer.24
Combination therapy is recommended only in the later stages of the treatment algorithm.27 The routine prescription of two or
more antipsychotics is not recommended because it may increase the risk of drug interactions, nonadherence, and medication
errors.27
Before a new antipsychotic agent is initiated, the patient’s complete medication history should be obtained. Whether the
patient has shown a favorable or unfavorable response to previous antipsychotic treatment will help guide the selection of a new
medication.2
Long-Acting Injectable Antipsychotic Agents Long-acting injectable (LAI) antipsychotic medications offer a viable option for
patients who are nonadherent to an oral medication.2 Clinicians should determine whether the patient’s nonadherence is due to
the adverse effects of treatment. If so, then the clinician should consider an oral medication with a more favorable side-effect
profile.2 Before moving to LAI therapy, a short trial should be conducted with the oral counterpart of the LAI to determine
tolerability.2
A recent meta-analysis of randomized controlled trials (RCTs) concluded that outcomes with LAIs are similar to those with
oral antipsychotics.28 The authors suspected, however, that RCTs might not reflect the “real world” efficacy and safety of
LAIs.29 Therefore, they conducted a meta-analysis of 25 mirror-image studies, in which a total of 5,940 subjects served as their
own controls in naturalistic settings.29 This analysis demonstrated the superiority of LAIs over oral antipsychotics in preventing
hospitalizations (risk ratio [RR] = 0.43) and in reducing the number of hospitalizations (RR = 0.38).29
Treatment-Resistant Schizophrenia Between 10% and 30% of patients with schizophrenia show little symptomatic improvement
after multiple trials of FGAs, and an additional 30% to 60% experience partial or inadequate improvement or unacceptable side
effects during antipsychotic therapy.16
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Clozapine is the most effective antipsychotic in terms of managing treatment-resistant schizophrenia. This drug is
approximately 30% effective in controlling schizophrenic episodes in treatment-resistant patients, compared with a 4% efficacy
rate with the combination of chlorpromazine and benz tropine.30 Clozapine has also been shown to increase serum sodium
concentrations in patients with polydipsia and hyponatremia.31
However, as indicated earlier, clozapine has a problematic safety profile. For example, patients treated with this drug are at
increased risk of developing orthostatic hypotension, which can require close monitoring.2 Moreover, high-dose clozapine has
been associated with serious adverse effects, such as seizures.2
Augmentation and Combination Therapy Both augmentation therapy (with ECT or a mood stabilizer) and combination therapy
(with antipsychotics) may be con- sidered for patients who fail to show an adequate response to clozapine. Clinicians should
observe the following guidelines when administering augmentation therapy:24
• The treatment should be used only in patients with an inadequate response to prior therapy.
• Augmentation agents are rarely effective for schizophrenia symptoms when given alone.
• Patients responding to augmentation treatment usually improve rapidly.
• If an augmentation strategy does not improve the patient’s symptoms, then the agent should be discontinued.
Mood stabilizers are common augmentation agents. Lithium, for example, improves mood and behavior in some patients but
does not have an antipsychotic effect.23
In combination therapy, two antipsychotic drugs—such as an FGA and an SGA, or two different SGAs—are administered
concurrently.2 However, exposure to multiple antipsychotics at the same time may increase the risk of serious side
effects.24,25,32
Mechanism of Action The precise mechanism of action of antipsychotic drugs is unknown, although it has been suggested that
these drugs comprise three main categories: 1) typical, or traditional, antipsychotics, which are associated with high dopamine (D
2
) antagonism and low serotonin (5-HT
2A
) antagonism; 2) atypical antipsychotics that have moderate-to-high D
2
antagonism and high 5-HT
2A
antagonism; and 3) atypical antipsychotics that dem- onstrate low D
2
antagonism and high 5-HT
2A
antagonism.2,33,34 At least 60% to 65% of D
2
receptors must be occupied to decrease the positive symptoms of schizophrenia, whereas a D
2
blockade rate of 77% or more has been associated with extrapyramidal symptoms.33,35
The improvement of negative symptoms and cognition with atypical antipsychotics may be due to 5-HT
2A
antagonism in combination with D
2
blockade, resulting in the release of dopamine into the prefrontal cortex (the area of the brain in which
dopaminergic receptors are hypoactive in untreated individuals with schizophrenia).2 Although atypical antipsychotics appear to
improve negative symptoms, no approved treatment options are specifically indicated for these symptoms.

Adverse Effects
Typical vs. Atypical Antipsychotics The adverse effects of schizophrenia medications can involve several organ systems, as
discussed below.
Table 1 illustrates the risk of two key adverse effects of antipsychotic agents: weight gain and extrapyramidal symptoms.2
SGAs are associated with a greater risk of weight gain, whereas FGAs are associated with a greater risk of extrapyramidal side
effects. SGAs with the lowest risk of extrapyramidal symptoms include aripiprazole, quetiapine, and clozapine.18,36,37,38
Table 1 Comparative Risks of Weight Gain and Extrapyramidal Symptoms With Typical and Atypical
Antipsychotic Agents2
Drug Weight
Extrapyramidal Gain
Symptoms
Typical Antipsychotics (First-Generation Antipsychotics)
Chlorpromazine
++ +++ (Thorazine)
Fluphenazine (Prolixin) + ++++
Haloperidol (Haldol) + ++++
Perphenazine (Trilafon) + ++++
Thioridazine (Mellaril) + +++
Thiothixene (Navane) + ++++
Atypical Antipsychotics (Second-Generation Antipsychotics)
Aripiprazole (Abilify) + +
Asenapine (Saphris) + ++
Clozapine (Clozaril) ++++ +
Iloperidone (Fanapt) ++ ± Lurasidone (Latuda) ± +
Olanzapine (Zyprexa) ++++ ++
Paliperidone (Invega) ++ ++
Quetiapine (Seroquel) ++ +
Risperidone (Risperdal) ++ ++
Ziprasidone (Geodon) + ++
± = negligible risk; + = low risk; ++ = moderate risk; +++ = moderately high risk; ++++ = high risk
Endocrine System Hyperprolactinemia can occur in up to 87% of patients treated with risperidone or paliperidone, possibly
leading to sexual dysfunction, decreased libido, menstrual irregularities, or gynecomastia.2 Aripiprazole or ziprasidone is a
potential treatment option for patients with increased prolactin levels.39
Weight gain is another important side effect in patients receiving antipsychotic drugs.39,40 It can occur in patients treated for
their first psychotic episode2 and may eventually lead to nonadherence.41
Along with hyperprolactinemia and weight gain, anti psychotic drugs also can increase the risks of diabetes mellitus and car-
diovascular-related mortality.39,42 Olanzapine has the greatest

zapine, risk of diabetes, followed by risperidone and quetiapine. The
and quetiapine have the highest sedation
potential.2 latter two agents cause minimal weight gain, however.2
Studies have shown that SGAs offer superior cognitive benefits compared with FGAs, although the CATIE trial found no differ-
Cardiovascular System
ences in cognitive improvement among patients treated with
Orthostatic hypotension can occur in up to 75% of patients
SGAs compared with the FGA perphenazine.2,47 treated
with an antipsychotic agent.43 Patients with diabetes,
All patients treated with antipsychotic agents are at
increased pre-existing cardiovascular disease, or advanced age appear to
risk of seizures. The antipsychotics with the greatest
seizure have the greatest risk, but all patients receiving antipsychotic
risk are clozapine and chlorpromazine.2 Those with the
lowest medications should be counseled to rise slowly from a sitting
risk include risperidone, molindone, thioridazine,
haloperidol, position to avoid a hypotensive episode.2
pimozide, trifluoperazine, and fluphenazine.36
Electrocardiographic changes, especially QTc prolonga-
Poikilothermia (the inability to maintain a constant inter-
tion, can occur in some patients treated with antipsychotics,
nal body temperature independent of external temperatures)
including thioridazine, clozapine, iloperidone, and ziprasidone.
can be a serious side effect of antipsychotic medications.48
In QTc prolongation should be monitored during therapy, and
addition, patients may be at increased risk of heat stroke
dur- treatment should be discontinued if this interval consistently
ing exercise because of an impaired ability to dissipate
excess exceeds 500 msec.2 Antipsychotic medications should be cho-
body heat.2 These side effects most commonly occur
during sen carefully in patients with pre-existing cardiac or cerebro-
treatment with low-potency FGAs, such as chlorpromazine,
but vascular disease, and in those taking diuretics or medications
they have also been associated with the SGAs that have
more that prolong the QTc interval.43
anticholinergic effects, such as clozapine.2 Although some
studies have shown that the risk of sudden
Neuroleptic malignant syndrome (NMS) is a rare but
life- cardiac death in patients treated with FGAs or SGAs is nearly
threatening side effect of antipsychotic drug therapy,
occurring twice that in individuals who do not use antipsychotic medica-
in 0.5% to 1.0% of patients treated with FGAs.2 Since the
introduc- tions, more recent findings suggest that both types of drugs
tion and increased use of SGAs, however, the
treatment-related have similar cardiac mortality risks.43,44
occurrence of this disorder has diminished.2
Psychiatric side effects, such as delirium and psychosis, can
Lipid Changes
occur with higher doses of FGAs or with combination treat-
Patients treated with SGAs or phenothiazines tend to show
ments involving anticholinergics.2 Elderly patients, in
particular, increased concentrations of serum triglycerides and choles-
are at increased risk of chronic confusion and disorientation
terol.2 SGAs with a lower risk in this regard include risperidone,
during treatment with antipsychotic drugs.2 ziprasidone,
and aripiprazole.41,42 In the CATIE trial, olanzapine was shown to have negative effects on cholesterol levels and
Miscellaneous Adverse Effects lipids.45
Schizophrenia medications can cause a variety of other adverse effects, including the following: Central Nervous System
Dystonia is another common side effect of antipsychotic
• Antipsychotic medications with anticholinergic
effects medications. This disorder often results in nonadherence and
have been shown to worsen narrow-angle glaucoma,
can be life-threatening.2 Dystonic reactions typically accompany
and patients should be appropriately monitored.49
treatment with FGAs and are most common in younger male
Chlorpromazine is most commonly associated with
opaque patients.2 Dystonia may be minimized by using SGAs or by
deposits in the cornea and lens.2 Because of the risk of
initiating FGAs at lower doses.2
cataracts, eye examinations are recommended for
patients Akathisia (often accompanied by dysphoria) occurs in 20%
treated with quetiapine.50 Those using thioridazine at
doses to 40% of patients treated with high-potency FGAs, such as
exceeding 800 mg daily are at risk of developing
retinitis haloperidol and fluphenazine.36,46 Quetiapine and clozapine
pigmentosa.2 appear to have the lowest risk for this
side effect.36,37
• Low-potency FGAs and clozapine have been associated
Pseudoparkinsonism has occurred in patients receiving
with urinary hesitancy and retention.2 The incidence
of antipsychotic therapy. The incidence of this disorder has
urinary incontinence among patients taking clozapine
can ranged from 15% to 36% in patients treated with FGAs. It
be as high as 44% and can be persistent in 25% of
patients.2,51 occurs more often in females and in older patients.2 The risk
• FGAs and risperidone have a greater tendency to
cause of pseudoparkinsonism during treatment with SGAs is gener-
sexual dysfunction compared with SGAs.2,52 ally
low, although an increased risk is associated with higher
• Treatment with antipsychotics can cause transient
doses of risperidone.2
leukopenia.2,53 The risk of tardive dyskinesia has
ranged from as low as 0.5%
• The three antipsychotics with the greatest risk for
hema- to as high as 62% during treatment with FGAs and is increased
tological complications are clozapine, chlorpromazine,
in elderly patients.2,37,46 The overall prevalence of the disorder
and olanzapine.54 Clozapine is associated with an
espe- ranges from 20% to 25% among patients receiving long-term
cially high risk for the development of neutropenia or
FGA therapy.2,37 The risk of tardive dyskinesia is significantly
agranulocytosis.54 lower with SGAs, and no cases
have been reported in patients
• On rare occasions, dermatological allergic reactions
have receiving clozapine monotherapy.2,37
occurred at approximately eight weeks after the initiation
Chlorpromazine, thioridazine, mesoridazine, clozapine, olan-
of antipsychotic therapy.2
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• Both FGAs and SGAS can cause photosensitivity, leading to severe sunburn.2
• Clozapine has been reported to cause sialorrhea in approximately 54% of patients with schizophrenia.2 The mechanism of this
effect is unknown.2
The varying safety profiles of antipsychotic medications may be due to their effects on various neuroreceptor systems.
33,34,55
Progress Evaluation
As in other medical specialties, recovery during the treatment of schizophrenia is defined both objectively and subjectively.56
Objective dimensions of recovery include the remission of symptoms and the patient’s return to full-time work or enroll- ment in
college.56 Several tools are available for rating the progress of patients with schizophrenia. The Brief Psychiatric Rating Scale
(BPRS) and the Positive and Negative Syndrome Scale (PANSS), for example, were developed as numerical indicators of
improvement.57 Clinicians also use quicker four- item instruments such as the Positive Symptom Rating Scale and the Brief
Negative Symptom Assessment.24,58
Subjective dimensions of recovery are measured by the patient in terms of his or her life satisfaction, hope, knowledge about
his or her mental illness, and empowerment.56
Despite continued therapeutic advances, the life expectancy of patients with schizophrenia is reduced by approximately 10 to
25 years compared with that of healthy individuals.59 The increased mortality among patients with schizophrenia has been
attributed to unhealthy lifestyles common among this population (i.e., lack of exercise, unhealthy diet, and excessive smoking
and alcohol intake), treatment-related adverse events, the suboptimal treatment of concomitant physical illnesses, and suicide.59
CONCLUSION
Schizophrenia is a complex disorder that requires prompt treatment at the first signs of a psychotic episode. Clinicians must
consider the potential for nonadherence and treatment- related adverse effects when developing a comprehensive treatment
plan. Although patients can increase adaptive functioning through available pharmacological and nonpharmacological treatment
options, it is hoped that future research will address gaps in treatment and potentially a cure for schizophrenia.
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