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Paul E. Keck, Susan L. McElroy: Chapter 54. Treatment of Bipolar Disorder, in The American Psychiatric Publishing
Textbook of Psychopharmacology, 4th Edition. Edited by Alan F. Schatzberg, Charles B. Nemeroff. Copyright ©2009
American Psychiatric Publishing, Inc. DOI: 10.1176/appi.books.9781585623860.443573. Printed 5/10/2009 from
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Chapter 54. Treatment of Bipolar Disorder
TREATMENT OF BIPOLAR DISORDER: INTRODUCTION
Bipolar disorder is a common, recurrent, often severe psychiatric illness that, without adequate
treatment, is associated with high rates of morbidity and mortality (Goodwin and Jamison 2007). In
the Global Burden of Disease survey, bipolar disorder was the sixth leading cause of disability
worldwide in 1990 and, without improved access to treatment, was projected to remain so well into
this century (Murray and Lopez 1996). Morbidity from bipolar disorder often extends well beyond
manic, hypomanic, mixed, and depressive episodes. Full recovery of functioning can lag many
months behind symptomatic improvement, and repeated episodes can lead to lasting functional
impairment (Judd et al. 2005). Recent naturalistic outcome studies indicate that many patients with
bipolar disorder spend protracted periods of time neither well nor syndromally ill but rather
suffering from chronic subsyndromal, especially depressive, symptoms (Judd et al. 2002, 2003).
Bipolar disorder is also among the most heritable of all medical illnesses (Goodwin and Jamison
2007).
The goals of treatment of bipolar disorder are similar to those of management of many chronic
illnesses: rapid, complete remission of acute episodes; prevention of further episodes; suppression
of subsyndromal symptoms; and optimization of functional outcome and quality of life (Keck et al.
2001). However, the treatment of bipolar disorder is often complicated. Although classified as a
mood disorder, bipolar disorder is also characterized by disturbances of behavior, cognition, and
perception. Thus, successful treatment requires that these multiple symptom domains be
addressed. Treatment is further complicated by the diversity of illness presentation (e.g., pattern,
frequency, and severity of episodes; presence of psychosis, comorbid illnesses, acute or chronic
environmental stressors) and course among individuals. Some medications have particular efficacy
in one phase of illness but not in another, and some may actually increase the likelihood of
precipitating a reciprocal mood episode.
The treatment of bipolar disorder has traditionally been divided into the management of acute
manic, mixed, and depressive episodes and the prevention of further episodes and symptoms
(Hirschfeld et al. 2002). Rush (1999) conceptualized a “strategies and tactics” approach to the
management of major depressive disorder, with principles of pharmacotherapy that are readily
applicable to bipolar disorder (Table 54–1). In this chapter we review strategies (i.e., what
treatments to choose) and tactics (i.e., how to implement these strategies once chosen and what
dose and duration of the chosen medication are to be used) for treating bipolar disorder, drawing
primarily on data from randomized, controlled trials. Where such data are lacking, strategies based
on data from open trials, naturalistic studies, and expert consensus guidelines are included. The
treatment of bipolar disorder in children and adolescents is covered elsewhere in this book (see
Chapter 63 in this volume, “Treatment of Child and Adolescent Disorders,” by Wagner and Pliszka).
TABLE 54–1. Treatment principles for bipolar disorder
Individually tailor guidelines.
Use proven treatments first.
Select best medication that is
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Easiest to use (for the patient).
Easiest to manage (for the physician).
Aim for symptom remission, not just response.
Measure symptomatic outcome.
Remember that no medication is a panacea.
Do not give up.
Recognize that psychosocial restoration follows symptom relief.
Interpersonal, family, educational, and social rhythm–targeted psychotherapies can help.
More chronic illness may respond more slowly.
Source. Adapted from Rush AJ: “Strategies and Tactics in the Management of Maintenance Treatment for
Depressed Patients.” Journal of Clinical Psychiatry 60 (Supplement 14):21–26, 1999.
FORMULATION AND IMPLEMENTATION OF A TREATMENT PLAN
Patients with bipolar disorder enter into treatment at various phases of illness. Regardless of
illness phase, treatment begins with a thorough diagnostic assessment (Hirschfeld et al. 2002). In
addition to the clinical features of bipolar disorder described in DSM-IV-TR (American Psychiatric
Association 2000), patients with bipolar disorder also commonly experience symptoms of anxiety,
impulsivity, recklessness, elevated libido, poor insight, inattention, and sensory hyperacuity during
manic or mixed episodes (Keck et al. 2001).
Bipolar disorder frequently presents with depressive episodes. A family history of bipolar disorder
or early age at onset of depression should raise diagnostic questions about bipolar disorder in an
individual presenting for treatment of depression. Studies suggest that 15%–30% of patients
treated for apparent major depressive disorder in outpatient settings subsequently receive a
diagnosis of bipolar I or II disorder (Manning et al. 1997, 1998). The Mood Disorder Questionnaire
(MDQ) is a 13-item self-report screening instrument for bipolar disorder that has been successfully
tested in psychiatric clinics (Hirschfeld et al. 2000) and in the general population (Hirschfeld 2002).
Bipolar disorder is associated with elevated rates of substance use, anxiety, eating,
attention-deficit/hyperactivity, and impulse-control disorders and migraine (Birmaher et al. 2002;
McElroy et al. 2001). Thus, the presence of these illnesses should be assessed in patients with
bipolar disorder, and conversely, bipolar disorder should be assessed in patients presenting with
these other illnesses. Other elements of a complete psychiatric evaluation are summarized in the
American Psychiatric Association’s (1995) “Practice Guideline for Psychiatric Evaluation of Adults.”
The American Psychiatric Association’s revised “Practice Guideline for the Treatment of Patients
With Bipolar Disorder” (Hirschfeld et al. 2002) lists a number of other important elements in the
treatment of patients with bipolar disorder (Table 54–2). Evaluation of safety of the patient and
others and determination of the appropriate treatment setting are essential because of the risks of
suicide, recklessness, and violence associated with mood episodes (Lopez et al. 2001) (Table
54–3). Establishing and maintaining a treatment alliance are early and ongoing goals to facilitate
patient and family education, treatment adherence, and identification of precipitants and prodromal
symptoms. Monitoring treatment response and providing illness education can be enhanced by
using the Life-Chart Method (Denicoff et al. 2002) or other similar longitudinal self-assessments. In
addition, a number of well-validated rating scales exist for monitoring mood symptoms in patients
with bipolar disorder cross-sectionally. These include the Young Mania Rating Scale (R. C. Young et
- 1978) for manic symptoms and the Montgomery-Åsberg Depression Rating Scale (Montgomery
and Åsberg 1979) for depressive symptoms, among others. Because bipolar disorder can lead to
disability and varying degrees of functional impairment in all aspects of life, specific
psychotherapeutic and rehabilitation interventions may be needed.
TABLE 54–2. Clinical components of the management of bipolar disorderPrint: Chapter 54. Treatment of Bipolar Disorder http://www.psychiatryonline.com/popup.aspx?aID=443577&print=yes…
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Perform a diagnostic evaluation.
Evaluate the safety of the patient and others and determine a treatment setting.
Establish and maintain a therapeutic alliance.
Monitor treatment response.
Provide education to the patient and significant others.
Enhance treatment compliance.
Promote awareness of stress and regular patterns of activity and sleep.
Work with the patient to anticipate and address early signs of relapse.
Evaluate and manage functional impairments.
Source. Reprinted from Hirschfeld RMA, Bowden CL, Gitlin MJ, et al.: “Practice Guideline for the Treatment of
Patients With Bipolar Disorder (Revision).” American Journal of Psychiatry 159 (Supplement):1–50, 2002.
Copyright 2002, American Psychiatric Association. Used with permission.
TABLE 54–3. Characteristics to evaluate in an assessment of suicide risk in patients with bipolar
disorder
Presence of suicidal or homicidal ideation, intent, or plans
Access to means for suicide and the lethality of those means
Presence of command hallucinations, other psychotic symptoms, or severe anxiety
Presence of alcohol or substance use
History and seriousness of previous attempts
Family history of or recent exposure to suicide
Source. Adapted from American Psychiatric Association: “Practice Guideline for the Treatment of Patients With
Major Depressive Disorder (Revision).” American Journal of Psychiatry 157 (Supplement):1–45, 2000.
Copyright 2000, American Psychiatric Association; Hirschfeld RMA, Bowden CL, Gitlin MJ, Keck PE, Perlis RH,
Suppes T, Thase ME: “Practice Guideline for the Treatment of Patients With Bipolar Disorder (Revision).”
American Journal of Psychiatry 159 (Supplement):1–50, 2002. Copyright 2002, American Psychiatric
Association. Used with permission.
DEFINITIONS: WHAT IS A MOOD STABILIZER?
The treatment of bipolar disorder is among the most challenging of all treatments for psychiatric
illnesses for a variety of reasons, one of which is that some agents effective in the treatment of one
pole can exacerbate or cause a switch into another pole. Goodwin and Jamison (2007) have defined
mood stabilizer as an agent that demonstrates efficacy in the acute treatment of both mania and
depression, as well as in the prevention of both types of mood episodes (ideal definition) or an
agent that is efficacious in two of these three aspects of treatment (strict definition). In this
chapter, we use the term mood stabilizer according to the strict definition. To date, there is no ideal
agent, although data from randomized, controlled trials suggest that lithium and olanzapine
probably come closest.
TREATMENT OF ACUTE BIPOLAR MANIC AND MIXED EPISODES
Manic and mixed episodes are medical emergencies and frequently require treatment in a hospital
to ensure safety of patients and those around them. The primary goal of treatment of manic and
mixed episodes is rapid symptom reduction, followed by full remission of symptoms and restoration
of psychosocial and vocational functioning (Hirschfeld et al. 2002). These are straightforward goals,
but tailoring treatment to specific patients requires consideration of presenting symptoms and their
severity (e.g., presence or absence of psychosis, manic or mixed episode, proximal frequency of
episodes).Print: Chapter 54. Treatment of Bipolar Disorder http://www.psychiatryonline.com/popup.aspx?aID=443577&print=yes…
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Pharmacotherapy is the cornerstone of treatment of acute manic and mixed episodes and of bipolar
disorder in general. A number of medications have demonstrated efficacy in the treatment of acute
manic and mixed episodes (Table 54–4). Lithium, divalproex, carbamazepine, olanzapine,
risperidone, quetiapine, ziprasidone, aripiprazole, haloperidol, and chlorpromazine have shown
efficacy as monotherapy in the treatment of acute mania in randomized, placebo-controlled trials
(McElroy and Keck 2000; Perlis et al. 2006c). Although these agents typically produce rates of
response (defined as 50% reduction in manic symptoms from baseline to endpoint) of
approximately 50% in short-term (3- to 4-week) trials, relatively few patients (<25%) actually
achieve remission of symptoms within these time intervals while receiving monotherapy with any
of these agents. Thus, use of combination therapy is common in clinical practice to improve
response and remission rates (Suppes et al. 2005). For example, a number of studies comparing
combination treatment with an antipsychotic and lithium or valproate demonstrated superior acute
response rates with combination therapy compared with monotherapy (Scherk et al. 2007).
TABLE 54–4. Evidence-based treatment of acute mania
Treatment Number of positive monotherapy RCTs
Lithium 18
Valproate 9
Carbamazepine 2
Aripiprazole 5
Olanzapine 8
Quetiapine 4
Risperidone 5
Ziprasidone 3
Chlorpromazine 4
Haloperidol 3
ECT 3
Note. ECT = electroconvulsive therapy; RCTs = randomized, controlled trials.
Lithium
Lithium has been a mainstay of treatment for acute mania for more than 50 years, with superior
efficacy compared with placebo (Goodwin et al. 1969; Maggs 1963; Schou et al. 1954; Stokes et al.
1971) and comparable efficacy compared with divalproex (Bowden et al. 1994), carbamazepine
(Lerer et al. 1987; Small et al. 1991), risperidone (Segal et al. 1998), olanzapine (Berk et al. 1999),
quetiapine (Bowden et al. 2005), aripiprazole (Keck et al. 2007), and typical antipsychotics
(Garfinkel et al. 1980; Johnson et al. 1976; Platman 1970; Prien et al. 1972; Shopsin et al. 1975;
Spring et al. 1970; Takahashi et al. 1975). Lithium exerted improvement in psychotic as well as
manic symptoms in these trials. Patients with elated or classic manic symptoms (Bowden 1995)
and relatively few lifetime mood episodes (Swann et al. 1999) appear to have better response rates
to lithium than do patients with mixed episodes, rapid cycling (Dunner and Fieve 1974; McElroy et
- 1992), and numerous prior mood episodes.
Lithium response for acute mania can be maximized by titrating to plasma concentrations at the
upper end of the therapeutic range (1.0–1.4 mmol/L) as tolerated (Stokes et al. 1976). In
randomized, controlled trials, significant clinical improvement usually was reported within 7–14
days among responders (Keck and McElroy 2001). Preliminary data also suggest that the rate of
lithium titration may affect response. Goldberg et al. (1998) found that the rapidity of antimanic
effect of any mood stabilizer (lithium, valproate, carbamazepine) was proportional to the rate of
titration to therapeutic plasma concentrations. Lithium is generally well tolerated during acutePrint: Chapter 54. Treatment of Bipolar Disorder http://www.psychiatryonline.com/popup.aspx?aID=443577&print=yes…
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treatment, and dosages needed to produce acute antimanic effects may be higher than those
needed for maintenance treatment (Bowden 1998). Common side effects associated with acute
treatment with lithium include nausea, vomiting, tremor, somnolence, weight gain, and cognitive
slowing.
Antiepileptics
Divalproex
Divalproex and related formulations of valproic acid had superior efficacy compared with placebo
(Bowden et al. 1994, 2006; Brennan et al. 1984; Emrich et al. 1981; Pope et al. 1991) and
comparable efficacy compared with lithium (Bowden et al. 1994; T. W. Freeman et al. 1992),
haloperidol (McElroy et al. 1996), and olanzapine (Zajecka et al. 2002) in randomized, controlled
acute treatment trials of bipolar manic or mixed episodes. Olanzapine was superior to divalproex in
mean reduction of manic symptoms and in proportion of patients in remission at study completion
in a second head-to-head comparison trial (Tohen et al. 2002a). Muller-Oerlinghausen et al. (2000)
found that the combination of valproate and typical antipsychotics produced significantly lower
mean antipsychotic doses and higher response rates compared with placebo added to typical
antipsychotics in patients with acute mania.
Unlike lithium, valproate has a comparatively wide therapeutic index. Acute antimanic response is
correlated with plasma concentrations between 50 and 125 mg/L, with some evidence of greater
response at the upper end of the therapeutic range (Allen et al. 2006; Zajecka et al. 2002). Some
patients may require plasma concentrations greater than 125 mg/L, but side effects become
progressively more prevalent above this level. Divalproex can be administered at a therapeutic
starting dosage of 20–30 mg/kg/day in inpatients with good tolerability, and some evidence
indicates a more rapid response than with gradual titration from a lower (e.g., 750 mg/day)
starting dose (Hirschfeld et al. 1999; Keck et al. 1993; McElroy et al. 1996; Zajecka et al. 2002).
Divalproex is generally well tolerated during treatment of acute manic or mixed episodes. Common
side effects include somnolence, nausea, vomiting, tremor, weight gain, and cognitive slowing.
Enteric-coated and extended-release formulations (the latter requiring a 20% dosage increase to
yield plasma concentrations equivalent to those with immediate-release formulations) have
improved tolerability compared with valproic acid formulations. Rare serious adverse events
include pancreatitis, thrombocytopenia, significant hepatic transaminase elevation,
hyperammonemic encephalopathy in patients with urea cycle disorders, and hepatic failure.
Carbamazepine and Oxcarbazepine
Until recently, there was a paucity of data from well-designed randomized, controlled trials of
carbamazepine in the treatment of mania. However, an extended-release formulation of
carbamazepine was superior to placebo in two large randomized, placebo-controlled multicenter
trials (Weisler et al. 2004b, 2005). These findings replicated earlier results from a
placebo-controlled crossover trial (Ballenger and Post 1978) and comparison studies against
lithium (Lerer et al. 1987; Small et al. 1991) and chlorpromazine (Grossi et al. 1984; Okuma et al.
1979). In one small comparison study, valproate was more effective than carbamazepine (Vasudev
et al. 2000). Common side effects of carbamazepine include diplopia, blurred vision, ataxia,
somnolence, fatigue, and nausea. Less common side effects include rash, mild leukopenia and
thrombocytopenia, and hyponatremia. Rare serious adverse events include agranulocytosis, aplastic
anemia, thrombocytopenia, hepatic failure, pancreatitis, and exfoliative dermatitis.
Oxcarbazepine, in contrast to carbamazepine, does not induce its own metabolism, has a lower rate
of side effects, and generally has good tolerability (Emrich 1991). Two small randomized, controlled
trials of oxcarbazepine in acute mania found oxcarbazepine to be comparable in efficacy to
haloperidol and lithium (Emrich 1991; Muller and Stoll 1984). However, both trials were
confounded by the use of adjunctive antimanic medications during the trials, and the studies were
too small to detect potential differences in efficacy. In the only large randomized,Print: Chapter 54. Treatment of Bipolar Disorder http://www.psychiatryonline.com/popup.aspx?aID=443577&print=yes…
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placebo-controlled multicenter trial of oxcarbazepine in acute mania to date, a 7-week study in
children and adolescents, oxcarbazepine was not superior to placebo in reduction of manic
symptoms (Wagner et al. 2006). Thus, the use of oxcarbazepine in acute bipolar mania has not
been substantiated based on evidence from clinical studies but rather is based on putative
similarities in mechanism of action with carbamazepine and improved tolerability.
Antipsychotics
Typical (First-Generation) Antipsychotics
Chlorpromazine (Klein 1967) and haloperidol (McIntyre et al. 2005) were superior to placebo in
randomized, controlled trials. Typical antipsychotics bear the burden of neurological and
neuroendocrinological side effects and may increase the risk of postmanic depressive episodes
(Koukopoulos et al. 1980). Thus, typical antipsychotics are commonly regarded as antimanic but
not mood-stabilizing agents.
Atypical (Second-Generation) Antipsychotics
The atypical antipsychotics olanzapine, risperidone, quetiapine, ziprasidone, and aripiprazole all
have demonstrated efficacy in the treatment of acute bipolar mania in at least two randomized,
placebo-controlled trials.
Olanzapine was found to be superior to placebo (Tohen et al. 1999, 2000), superior or equal in
efficacy to divalproex (Tohen et al. 2002a; Zajecka et al. 2002), and comparable to lithium (Berk et
- 1999; Niufan et al. 2007), risperidone (Perlis et al. 2006a), and haloperidol (Tohen et al. 2003a)
in mean reduction of manic and mixed symptoms in 3- to 4-week monotherapy trials. Adjunctive
treatment with olanzapine was superior to placebo in patients who were inadequately responsive to
lithium or divalproex monotherapy (Tohen et al. 2002b).
In the haloperidol comparison trial, olanzapine was significantly more likely to improve depressive
symptoms during the treatment of manic and mixed episodes (Tohen et al. 2003a). In the two
placebo-controlled trials, the rate of response was faster with an initial starting dosage of 15
mg/day (Tohen et al. 2000) compared with 10 mg/day (Tohen et al. 1999). Baker et al. (2003)
reported significant improvement in agitation in manic patients within 24 hours with the use of
rapid initial dosage escalation (20–40 mg/day) compared with usual titration. The intramuscular
formulation of olanzapine has also been studied in the treatment of manic agitation (Meehan et al.
2001). In this study, an intramuscular olanzapine dose of 10 mg produced significant improvement
compared with placebo and numerically greater improvement compared with intramuscular
lorazepam 2 mg at 2 hours following administration. From these studies, it appears that acute
antimanic response to olanzapine may be more rapid in patients treated with higher initial doses,
with dosage administration in proportion to the degree of psychomotor agitation. In short-term
studies, the most common side effects associated with olanzapine were somnolence, constipation,
dry mouth, increased appetite, weight gain, and orthostatic hypotension.
Risperidone was superior to placebo (Hirschfeld et al. 2004; Khanna et al. 2005) and comparable to
olanzapine (Perlis et al. 2006a), haloperidol (Smulevich et al. 2005), and lithium (Segal et al. 1998)
in mean reduction of manic and mixed symptoms as monotherapy in 3- to 4-week trials.
Risperidone was superior to placebo as adjunctive therapy with lithium or divalproex in one
placebo-controlled trial (Sachs et al. 2002), but not in a second placebo-controlled trial in
combination with lithium, divalproex, or carbamazepine (Yatham et al. 2003). However, because
this latter study included patients receiving carbamazepine, it is possible that risperidone plasma
concentrations may have been significantly reduced in these patients, limiting risperidone’s
efficacy. The rate of extrapyramidal side effects associated with risperidone was low when the drug
was administered at average dosages up to 4 mg/day (Hirschfeld et al. 2004; Sachs et al. 2002;
Yatham et al. 2003) but not when administered at average dosages of 6 mg/day or greater (Khanna
et al. 2005; Segal et al. 1998). In short-term trials, other commonly occurring side effects included
prolactin elevation, akathisia, somnolence, dyspepsia, and nausea.Print: Chapter 54. Treatment of Bipolar Disorder http://www.psychiatryonline.com/popup.aspx?aID=443577&print=yes…
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Quetiapine was superior to placebo as monotherapy in two 12-week studies in adult patients
(Bowden et al. 2005; McIntyre et al. 2005) and was comparable to lithium in a 4-week study in
adult patients (Li et al. 2008) and to divalproex in adolescents with bipolar mania (DelBello et al.
2006). Similarly, quetiapine was superior to placebo as adjunctive treatment with lithium or
divalproex (DelBello et al. 2002; Sachs et al. 2004; Yatham et al. 2004). In two placebo-controlled
trials, lithium (Bowden et al. 2005) and haloperidol (McIntyre et al. 2005) were included as active
comparators. There were no significant differences in efficacy among patients receiving quetiapine,
lithium, or haloperidol, although the trials were not powered to detect such a difference if one
existed. The mean modal dose of quetiapine associated with antimanic efficacy in most studies was
approximately 600 mg/day (Vieta et al. 2005b). The most common side effects from quetiapine in
monotherapy trials were headache, dry mouth, constipation, weight gain, somnolence, and
dizziness.
Ziprasidone was superior to placebo (mean dose 120–130 mg/day) in two 3-week monotherapy
trials in adult patients (Keck et al. 2003b; Potkin et al. 2005) and comparable to haloperidol in a
12-week trial (Ramey et al. 2003). Ziprasidone was not superior to placebo as adjunctive treatment
with lithium in a study designed to prove superior onset of action by 2 weeks of treatment (Weisler
et al. 2004a). However, ziprasidone was superior to placebo in reduction of manic symptoms at day
4 in this adjunctive trial. Ziprasidone appears to have dose-related antimanic efficacy within the
therapeutic range of 80–160 mg/day. Ziprasidone-related side effects in monotherapy trials
included headache, somnolence, extrapyramidal signs, akathisia, and dizziness. The intramuscular
(IM) formulation of ziprasidone has also been studied in the treatment of manic agitation (Daniel et
- 2001; Lesem et al. 2001). In these studies, ziprasidone 10–20 mg IM produced significant
improvement compared with ziprasidone 2 mg IM at 0.5–4 hours following administration.
Aripiprazole had significantly greater efficacy in the reduction of manic symptoms compared with
placebo in three 3-week trials (Keck et al. 2003a, 2007; Sachs et al. 2006) and comparable efficacy
with haloperidol (Vieta et al. 2005a) and lithium (Keck et al. 2009) in adequately powered 12-week
comparison trials. Aripiprazole was initiated at 15 or 30 mg/day. Common side effects associated
with aripiprazole in the placebo-controlled trials were headache, nausea, vomiting, constipation,
insomnia, and akathisia.
In the studies of atypical antipsychotics reviewed above, there were no significant differences in
response between patients with or without psychotic features or between patients with manic or
mixed episodes among all agents, with the exception of trials of quetiapine, many of which
excluded mixed patients. Lastly, the prototypical atypical agent clozapine has been reported to
have substantial efficacy in a number of large case series of patients with treatment-refractory
mania (Calabrese et al. 1996; Green et al. 2000) but has not been studied in placebo-controlled
trials in mania.
Electroconvulsive Therapy
Electroconvulsive therapy (ECT) is an important treatment option for manic patients with severe,
psychotic, or catatonic symptoms. ECT was superior in efficacy to lithium (Small et al. 1988) and
the combination of lithium and haloperidol (Mukherjee et al. 1994) in prospective comparison
studies. In the lithium comparison trial (Small et al. 1988), the presence of depressive symptoms at
baseline was the strongest predictor of ECT response. In addition, ECT in combination with
chlorpromazine was superior to sham ECT and chlorpromazine (Sikdar et al. 1994). Although these
were small studies, their findings are consistent with those of other naturalistic studies of ECT in
the treatment of acute mania (Black et al. 1984; Thomas and Reddy 1982). There is a risk of
neurotoxicity in patients receiving ECT while also receiving lithium; thus, lithium should be
discontinued when ECT is administered (Hirschfeld et al. 2002).
Psychotherapy
Psychotherapeutic interventions in patients with acute mania focus on establishing and maintaining
a therapeutic alliance, improving insight, monitoring treatment response, and providing the initialPrint: Chapter 54. Treatment of Bipolar Disorder http://www.psychiatryonline.com/popup.aspx?aID=443577&print=yes…
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elements of education about bipolar disorder and its manifestations to patients and their families
(Hirschfeld et al. 2002). As manic symptoms remit, more attention can be paid to further education,
promoting awareness of stressors and sleep hygiene, identifying harbingers of relapse, and
assessing need for rehabilitation services.
Novel Treatments
The new atypical antipsychotics paliperidone, asenapine, and bifeprunox and new antiepileptics
such as zonisamide, levetiracetam, and acamprosate are being studied as potential antimanic
agents. Among these agents, the only randomized, controlled trial reported to date compared
asenapine (mean dosage = 18 mg/day), olanzapine (mean dosage = 16 mg/day), and placebo over
3 weeks (Hirschfeld et al. 2007). Both treatment groups displayed comparable reductions in manic
symptoms, and both were superior to placebo. By contrast, a number of potential antimanic agents
have not demonstrated convincing efficacy in randomized, controlled trials. These include
gabapentin (Frye et al. 2000; Pande et al. 2000), lamotrigine (Anand et al. 1999; Frye et al. 2000),
topiramate (Kushner et al. 2006), and verapamil (Janicak et al. 1998; Walton et al. 1996).
In two short-term pilot trials, the protein kinase C inhibitor tamoxifen was superior to placebo in
reduction of manic symptoms (Yildiz-Yesiloglu 2007; Zarate et al. 2007). The benzodiazepines
lorazepam and clonazepam have been studied in a number of randomized, controlled trials in acute
mania (Chou et al. 1999) but have not been demonstrated to exert specific antimanic effects.
Nevertheless, adjunctive use of benzodiazepines to treat anxiety, insomnia, and agitation in manic
patients is often therapeutic.
Monotherapy Versus Combination Therapy of Acute Bipolar Manic and
Mixed Episodes
The data reviewed above provide evidence of the efficacy of specific agents administered for
adequate treatment trials at therapeutic doses (Table 54–5). Monotherapy with an antimanic agent
represents one of two initial options, primarily for patients with less severe manic symptoms.
However, combination therapy has generally been demonstrated to have greater and more rapid
efficacy than monotherapy (Scherk et al. 2007). Combination therapy may be a particularly useful
option in patients with severe manic symptoms or psychosis.
TABLE 54–5. Criteria for minimum adequate trials of antimanic agents
Medication Definitive (3-week trial) Probable (2-week trial)
Lithium
0.8 mmol/L
0.7 mmol/L
Valproate
75 g/mL
50 g/mL
Carbamazepine
800 mg/day
600 mg/day
Haloperidol
0.2 mg/kg/day
0.1 mg/kg/day
Chlorpromazine
500 mg/day
300 mg/day
Olanzapine
15 mg/day
10 mg/day
Ziprasidone
120 mg/day
80 mg/day
Risperidone
5 mg/day
4 mg/day
Quetiapine
600 mg/day
400 mg/day
Aripiprazole
30 mg/day
15 mg/day
Source. Adapted from Keck PE Jr, McElroy SL: “Definition, Evaluation, and Management of Treatment
Refractory Mania.” Psychopharmacology Bulletin 35:130–148, 2001. Copyright 2001, MedWorks Media. Used
with permission.
To date, mainly combinations of antipsychotics in conjunction with lithium, valproate, and/or
carbamazepine have been studied. The efficacy of combinations of lithium, valproate, or
carbamazepine versus monotherapy with these agents has not been studied in randomized,Print: Chapter 54. Treatment of Bipolar Disorder http://www.psychiatryonline.com/popup.aspx?aID=443577&print=yes…
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controlled trials, although anecdotal evidence suggests that these combinations may have greater
efficacy than either agent alone (M. P. Freeman and Stoll 1998). Similarly, there are no data to date
to suggest that other than standard therapeutic doses of agents used in combination therapy are
needed.
TREATMENT OF ACUTE BIPOLAR DEPRESSIVE EPISODES
For many patients with bipolar disorder, depressive episodes or chronic waxing and waning
subsyndromal depressive symptoms dominate their course of illness and constitute a major source
of disability (Judd et al. 2002, 2003; Perlis et al. 2006b). In addition, suicide is a substantial risk of
untreated bipolar depression. Thus, the goal of treatment of bipolar depression is full remission of
symptoms (Hirschfeld et al. 2002). This straightforward goal is complicated by the limited efficacy
of many mood stabilizers in bipolar depression (Zornberg and Pope 1993), often requiring the
adjunctive use of unimodal antidepressants with the attendant risk of cycle acceleration or
switching (Table 54–6). Moreover, there are very little data indicating that the addition of
antidepressants to mood stabilizers is more effective than utilization of mood stabilizers alone in
alleviating acute bipolar depressive symptoms (Sachs et al. 2007). To date, only quetiapine and
combination olanzapine–fluoxetine have indications for the treatment of acute bipolar I depression.
TABLE 54–6. Evidence-based treatment of acute bipolar I depression
Treatment Number of positive RCTs
Monotherapy
Quetiapine 2
Lamotrigine 2
Olanzapine 1
Lithium 8
Divalproex 1
Carbamazepine 2
Combination therapy
Olanzapine–fluoxetine 1
Note. RCTs = randomized, controlled trials.
Special Considerations in Bipolar Depression
Antidepressants and the Problem of Switching
The decision to recommend administration or avoidance of antidepressants often means attempting
to walk a therapeutic razor’s edge between alleviating depression and triggering mood switching.
Thus, recent data regarding the protective effect of mood stabilizers against
antidepressant-associated switching and the incidence of switching among antidepressants are
important to weigh in these decisions. Until recently, most treatment guidelines recommended
avoiding antidepressants and relying on mood stabilizers alone in mild to moderate bipolar
depression, and when administering antidepressants for severe or persistent bipolar depression,
they recommended withdrawing them as quickly as possible after remission (Ghaemi et al. 2001;
Sachs et al. 2000). These recommendations were based on reported antidepressant-associated
switch rates, which ranged widely, from 10% to 70% (Thase and Sachs 2000).
Many estimates of the incidence of antidepressant-associated switching were based on naturalistic
studies that did not control for the switch rate associated with the illness itself. The switch rates
reported in recent randomized, controlled acute treatment (i.e., 6–8 weeks) trials of lamotrigine
(Calabrese et al. 1999), quetiapine (Calabrese et al. 2005a; Thase et al. 2006), and olanzapine
monotherapy (Tohen et al. 2003c) and of combinations of paroxetine with lithium (Nemeroff et al.Print: Chapter 54. Treatment of Bipolar Disorder http://www.psychiatryonline.com/popup.aspx?aID=443577&print=yes…
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2001), lithium with valproate (L. T. Young et al. 2000), and fluoxetine with olanzapine (Tohen et al.
2003c) ranged from 3% to 8%. In addition, Post et al. (2001) reported a switch rate of 14% (8%
hypomania, 6% mania) in a 10-week acute treatment trial comparing bupropion, venlafaxine, and
sertraline in combination with mood stabilizers. The switch rate with venlafaxine was significantly
higher than that with the other agents (Post et al. 2006), a finding consistent with an earlier report
by Vieta et al. (2002), who also found a higher switch rate in patients receiving venlafaxine
compared with paroxetine. Thus, with newer antidepressant medications administered in
conjunction with mood stabilizers, switch rates appear to be low (Peet and Peters 1995), although
switch rates may be slightly higher with dual serotonin and norepinephrine reuptake inhibitors such
as venlafaxine. These data are also consistent with the results of several naturalistic studies that
found that concomitant administration of mood stabilizers with antidepressants cut the risk of
switching by about half (Boerlin et al. 1998; Bottlender et al. 2001). The risk of switching appears
to be greater in patients with bipolar I depression than in those with bipolar II depression
(Altshuler et al. 2006).
Mood Stabilizers as Antidepressants
Most randomized, controlled trials of bipolar depression involved patients with bipolar I disorder.
When bipolar II patients were included, their response usually was not reported separately, except
in the quetiapine trials, in which quetiapine was superior to placebo in reduction of depression
symptoms in both bipolar I and II patients (Calabrese et al. 2005a; Thase et al. 2006). It is not
clear whether patients with bipolar II depression require treatment with a mood stabilizer (Thase
and Sachs 2000), although most recommendations suggest that mood stabilizers also form the
cornerstone of treatment for patients with bipolar II disorder. Treatment with a mood-stabilizing
medication, if a patient is not already receiving one, is usually the first-line treatment for bipolar
depression, because the inherent risk of switching is likely to be less with a mood stabilizer alone
than with an antidepressant alone or with a combination of a mood stabilizer and antidepressant.
Lithium
Eight of nine placebo-controlled trials conducted in the 1960s and 1970s in patients with bipolar I
and II disorders found lithium superior to placebo in acute bipolar depression (reviewed in
Zornberg and Pope 1993). In an analysis of five studies in which it was possible to distinguish
“unequivocal” lithium responders from patients who displayed partial but incomplete improvement
in depression, Zornberg and Pope (1993) found that 36% had an unequivocal response, compared
with 79% who had at least partial benefit. The antidepressant efficacy of lithium also was
examined in two studies of paroxetine added to mood stabilizers for bipolar depression (Nemeroff
et al. 2001; L. T. Young et al. 2000). Nemeroff et al. (2001) found that patients receiving lithium at
plasma concentrations greater than 0.8 mEq/L showed no antidepressant benefit from the addition
of paroxetine or imipramine compared with placebo. In contrast, patients receiving lithium at
concentrations less than or equal to 0.8 mEq/L showed significant antidepressant benefit from the
addition of paroxetine compared with placebo. These data confirm earlier impressions that
maximizing lithium levels in patients already receiving lithium, or titrating to levels greater than
0.8 mEq/L when initiating lithium, is important to ensure an adequate trial of lithium for bipolar
depression. L. T. Young et al. (2000) found that adding an alternative mood stabilizer (lithium or
valproate) to the regimen of patients receiving therapeutic doses of a mood stabilizer but
experiencing breakthrough depressive episodes was as effective as adding the antidepressant
paroxetine. Although this study was too small (N = 27) to detect drug–drug differences in efficacy,
the mood stabilizer–mood stabilizer combination was not as well tolerated as the mood
stabilizer–antidepressant combination, and the only patient who switched did so during this
treatment arm.
Atypical Antipsychotics
Quetiapine
Quetiapine (300 mg and 600 mg/day) was superior to placebo in reduction of depressive symptomsPrint: Chapter 54. Treatment of Bipolar Disorder http://www.psychiatryonline.com/popup.aspx?aID=443577&print=yes…
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in two large 8-week multicenter trials involving outpatients with bipolar I and II depression
(Calabrese et al. 2005a; Thase et al. 2006). Patients receiving quetiapine also demonstrated
greater improvement in secondary measures of sleep and anxiety compared with patients receiving
placebo. There was no significant difference in efficacy between the two quetiapine dosage groups.
However, the rate of side effects was lower in the 300 mg/day groups compared with the 600
mg/day groups. Switch rates were low (3%–4%) across all treatment groups and were not
significantly different among the quetiapine and placebo groups.
Olanzapine and Olanzapine–Fluoxetine Combination
Olanzapine and the combination of olanzapine and fluoxetine (OFC) were superior to placebo in
reducing depressive symptoms in an 8-week trial of 833 patients with bipolar I depression (Tohen
et al. 2003c). However, the OFC was superior not only to placebo throughout the trial but also to
olanzapine for weeks 4–8. There were no significant differences in switch rates (6%–7%) among
the three groups. Brown et al. (2006) compared OFC with lamotrigine (titrated to 200 mg/day) in a
7-week comparison trial in outpatients with bipolar I depression. Patients receiving OFC displayed
greater reduction in depressive symptoms compared with patients receiving lamotrigine, although
the lamotrigine group may have had a greater response with a longer trial, given the need for
gradual lamotrigine titration. Switch rates were not significantly different between the two groups.
Antiepileptics
Lamotrigine
In an initial large 7-week randomized, placebo-controlled trial, lamotrigine (at 50 mg/day and 200
mg/day) was superior to placebo in patients with bipolar I depression (Calabrese et al. 1999).
Switch rates (3%–8%) were not significantly different among the three groups. A second large
placebo-controlled, parallel-group, flexible-dose trial involving patients with bipolar I and II
depression did not find a significant advantage for lamotrigine over placebo (Bowden 2001).
However, in a post hoc analysis, lamotrigine was superior to placebo in bipolar I patients. Frye et
- (2000) found lamotrigine superior to placebo in improving depression in a double-blind
crossover trial in patients with treatment-refractory rapid-cycling bipolar I and II disorders.
Lamotrigine was superior to placebo when added to lithium in an 8-week trial in patients with
breakthrough depressive episodes (van der Loos and Nolen 2007). Common side effects of
lamotrigine in these studies included headache, nausea, infection, and xerostomia. The risk of
serious rash from lamotrigine can be reduced by carefully adhering to Physicians’ Desk
Reference–recommended titration schedules, but patients should be warned of the risk of rash and
the need to report it immediately.
Carbamazepine
In two small controlled trials of patients with treatment-refractory bipolar depression, response to
carbamazepine was superior to placebo (Post et al. 1986) and lithium (Small 1990). The results of
these initial intriguing findings have not been followed up by large placebo-controlled,
parallel-group trials.
Divalproex
Two small randomized, placebo-controlled trials of divalproex in the treatment of acute bipolar
depression yielded opposite findings. Sachs and Collins (2001) did not find divalproex to be
superior to placebo in one pilot trial, whereas Davis et al. (2005) found divalproex superior to
placebo in reduction of depressive and anxiety symptoms in a later pilot study. As with
carbamazepine, the results of these initial findings have not been followed up by large
placebo-controlled, parallel-group trials.
Antidepressants
There is a relative dearth of randomized, controlled trials of antidepressants as monotherapy or in
combination with mood stabilizers in bipolar depression (Ghaemi et al. 2001). Thase and SachsPrint: Chapter 54. Treatment of Bipolar Disorder http://www.psychiatryonline.com/popup.aspx?aID=443577&print=yes…
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(2000, p. 558) emphasized that “not a single antidepressant medication, nor even a particular class
of antidepressant, has been demonstrated to be effective in at least two adequately powered,
placebo-controlled clinical trials.” Thus, with a thin evidence base, current recommendations
regarding the use of antidepressants in conjunction with mood stabilizers for acute bipolar I
depression tend toward the conservative (i.e., avoid antidepressants if possible). However, some
general impressions can be gleaned from the available clinical trials. First, switch rates of newer
antidepressants in short-term trials, in general, appear to be lower than those associated with
tricyclic antidepressants (TCAs) in older studies (Thase and Sachs 2000). Second, among all of the
antidepressants studied, the most substantial evidence for efficacy rests with the monoamine
oxidase inhibitor (MAOI) tranylcypromine (Himmelhoch et al. 1991), but safety concerns often
eliminate this agent from first-line therapy choices (Hirschfeld et al. 2002). Bupropion (Sachs et al.
1994) and selective serotonin reuptake inhibitors (SSRIs) (Nemeroff et al. 2001; L. T. Young et al.
2000) are common first-line agents administered in conjunction with mood stabilizers.
Electroconvulsive Therapy
ECT had significantly greater efficacy than MAOIs, TCAs, or placebo in several randomized,
controlled trials in patients with bipolar depression (reviewed in Zornberg and Pope 1993). ECT
may be particularly indicated for patients with severe, psychotic, or catatonic symptoms.
Psychotherapy
There are very few randomized, controlled trials of any form of psychotherapy for patients with
acute bipolar depression. Cognitive-behavioral and interpersonal therapy have demonstrated
efficacy in the treatment of unipolar major depression, but these modalities have been examined
only in very small preliminary studies in patients with bipolar depression, thus far without
conclusive findings (Cole et al. 2002; Zaretsky et al. 1999).
Novel Treatments
As in the treatment of acute bipolar manic and mixed episodes, there is considerable interest in the
potential efficacy of new atypical antipsychotics and antiepileptic agents in the treatment of acute
bipolar depression. With the exceptions of olanzapine, quetiapine, aripiprazole, lamotrigine, and
gabapentin, these agents have not yet been well studied in randomized, controlled trials in the
depressed phase of the illness. In two placebo-controlled trials, aripiprazole-treated patients did
not display significantly greater improvement in depressive symptoms compared with patients
receiving placebo at the 8-week study endpoint (Thase et al. 2008). Shelton and Stahl (2004)
conducted a small pilot study comparing adjunctive treatment with risperidone, paroxetine, or the
combination added to a mood stabilizer in outpatients with bipolar I or bipolar II depression. There
were no significant differences in efficacy among the three treatment groups, but the study was
limited by its small sample size (N = 30). McIntyre et al. (2002) found comparable efficacy for
topiramate (mean dosage = 176 mg/day) and bupropion sustained-release (mean dosage = 250
mg/day) in an 8-week single-blind comparison trial in 36 patients with bipolar depression receiving
mood stabilizers. No switches occurred in either treatment group.
Among other novel treatment approaches, two preliminary placebo-controlled adjunctive trials
examined the efficacy and safety of the dopamine D2/D3 receptor agonist pramipexole in the
treatment of patients with bipolar I and bipolar II depression (Goldberg et al. 2004; Zarate et al.
2004). In both trials, patients receiving pramipexole added to mood stabilizers had significantly
greater reductions in depressive symptoms and significantly greater response rates compared with
those receiving placebo. Switch rates did not differ significantly from those with placebo.
Stoll et al. (1999) reported significant global improvement in depressive symptoms in patients
receiving omega-3 fatty acids compared with placebo. These findings were not replicated in a
second placebo-controlled trial (Keck et al. 2006b).
Monotherapy Versus Combination Therapy of Acute Bipolar Depressive
EpisodesPrint: Chapter 54. Treatment of Bipolar Disorder http://www.psychiatryonline.com/popup.aspx?aID=443577&print=yes…
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The “mood stabilizer first” approach has guided most recommendations regarding the acute
treatment of patients with bipolar I depression (Thase and Sachs 2000). This approach is supported
by at least three lines of evidence: 1) randomized, controlled trials have demonstrated the inherent
antidepressant activity of at least some mood stabilizers (lithium, lamotrigine, olanzapine,
quetiapine); 2) mood stabilizer monotherapy appears to carry a lower switch risk as compared with
mood stabilizer–antidepressant combination therapy; 3) protection against switching can be
implemented if the mood stabilizer alone is not adequate and an antidepressant is needed. Lithium,
lamotrigine, quetiapine, and olanzapine are mood stabilizers with demonstrated efficacy as
monotherapy in acute bipolar depression.
Combination therapy with an antidepressant and a mood stabilizer is an important option in two
clinical groups: patients who do not respond adequately to mood stabilizer monotherapy and
patients who have moderate to severe bipolar depression (Hirschfeld et al. 2002). Among
antidepressant options, paroxetine, fluoxetine, venlafaxine, bupropion, and tranylcypromine are the
most well studied in randomized, controlled trials and appear to have a lower switch risk in
comparison with TCAs. Although no randomized, controlled trials of pharmacotherapy of psychotic
bipolar depression have been conducted, mood stabilizer–antidepressant–antipsychotic and
atypical antipsychotic–antidepressant combinations are common clinical approaches (Keck et al.
2004).
MAINTENANCE TREATMENT
Bipolar disorder is a recurrent lifelong illness in more than 90% of the patients who experience a
manic episode (Goodwin and Jamison 2007). Because of the high risk of recurrence and morbidity
associated with mood episodes and interepisode symptoms, maintenance treatment is usually
recommended after a single manic episode (Hirschfeld et al. 2002). The goals of maintenance
treatment include prevention of syndromal relapse and subsyndromal symptoms, optimization of
functioning, and prevention of suicide. As with bipolar depression, there are a limited number of
randomized, controlled trials of maintenance treatment of bipolar disorder on which to base
treatment recommendations (Table 54–7).
TABLE 54–7. Evidence-based maintenance treatment of bipolar disorder
Treatment Number of positive RCTs
Lithium 8
Lamotrigine 2
Olanzapine 3
Aripiprazole 1
Note. RCTs = randomized, controlled trials.
Lithium
Lithium is the most extensively studied medication in the maintenance treatment of bipolar
disorder. Data from randomized, placebo-controlled trials conducted in the 1960s and 1970s
indicated that lithium protected against relapse, with a fourfold lower risk compared with placebo
at 6-month and 1-year follow-up intervals (Keck et al. 2000). Lithium was superior to placebo in
preventing relapse into mania in two randomized, controlled parallel-group trials lasting 18 months
(Bowden et al. 2003; Calabrese et al. 2003).
Lithium may also reduce the risk of suicide in bipolar disorder beyond that predicted by the
successful prevention of mood episode recurrences (Baldessarini et al. 2003). Moreover, this risk
reduction appears to exceed that of treatment by divalproex (Goodwin et al. 2003).
A number of predictors of poor response to lithium maintenance treatment have been identified.
These include rapid cycling, multiple prior mood episodes, negative family history of mood disorder,
co-occurring alcohol or substance use disorder, and episode sequence ofPrint: Chapter 54. Treatment of Bipolar Disorder http://www.psychiatryonline.com/popup.aspx?aID=443577&print=yes…
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depression–mania–euthymia (Bowden 1995).
The optimal maintenance lithium serum concentration is an important consideration in successful
maintenance treatment. Maintenance lithium serum concentrations usually are lower than those
required to produce acute antimanic efficacy (Bowden 1998). Studies by Gelenberg et al. (1989)
and Keller et al. (1992) found a serum level–response relationship, with levels of 0.4–0.6 mEq/L
being associated with 2.6 times the relapse rate and a significantly greater likelihood of
experiencing subsyndromal symptoms, compared with levels of 0.8 mEq/L or higher. There was
also a serum level–side effect relationship, with patients at higher levels experiencing significantly
higher rates of side effects, often leading to discontinuation. Perlis et al. (2002), in yet another
reanalysis of the Gelenberg et al. (1989) data, reported that an abrupt drop in serum lithium levels,
whether due to random reassignment or to nonadherence, was the most powerful predictor of
relapse. In a comprehensive review of this issue, Baldessarini et al. (2002) concluded that levels of
0.6–0.7 mEq/L appear to provide the best efficacy–tolerability range for most patients. The optimal
lithium level for many patients will be the level that balances relapse prevention and suppression of
subsyndromal symptoms against minimization of bothersome day-to-day side effects.
Antiepileptics
Lamotrigine
Two large 18-month placebo-controlled maintenance trials comparing lamotrigine (200–400
mg/day) with lithium (0.8–1.1 mEq/L) found lamotrigine, but not lithium, superior to placebo in
preventing depressive episodes (Bowden et al. 2003; Calabrese et al. 2003). In contrast, lithium,
but not lamotrigine, was superior to placebo in preventing manic episodes. Taken together, the
results of these two studies suggest that the combination of lithium and lamotrigine might be
especially useful in preventing both manic and depressive episodes, although this remains to be
established in a randomized, controlled trial. Of the nearly 1,200 patients who received lamotrigine
in these trials, 9% had benign rash (morbilliform or exanthematous eruptions), compared with 8%
of the 1,056 patients receiving placebo. When patients who received lamotrigine during the
open-label run-in phase of the studies were included in the analysis, the total incidence of rash was
13%, with two cases of serious rash requiring hospitalization (Calabrese 2002).
Calabrese et al. (2000) conducted a 6-month placebo-controlled relapse prevention study of
lamotrigine (mean dose, 288 mg/day) in 182 patients with rapid-cycling bipolar I and II disorders.
There was no significant difference between the lamotrigine and placebo treatment groups in time
to need for additional medications for recurrent mood symptoms. However, there was a trend in
favor of lamotrigine over placebo specifically in bipolar II patients.
Divalproex
In the only randomized, placebo-controlled maintenance trial of divalproex in bipolar I disorder,
there was no significant difference in the time to development of any mood episode among patients
receiving divalproex, lithium, or placebo (Bowden et al. 2000). A number of unforeseen
methodological limitations in this trial complicated the interpretation of its results. In patients who
received divalproex for treatment of the index manic episode in an open treatment period prior to
randomization, divalproex was superior to placebo in early termination due to any mood episode
(29% vs. 50%) during the subsequent year. This is a clinically relevant observation, since it
supports the efficacy of maintaining patients who respond to divalproex for a manic episode.
Divalproex was also compared with olanzapine in a 47-week blinded maintenance trial (Tohen et al.
2003b) described earlier. Calabrese et al. (2005b) compared divalproex with lithium in a 20-month
study of patients with rapid-cycling bipolar disorder and found comparable relapse rates in both
treatment groups.
There are no data regarding the optimal maintenance valproic acid concentration for bipolar
disorder. Current practice usually consists of titrating to therapeutic serum concentrations (50–125
g/mL) and, as with lithium, balancing relapse and subsyndromal symptom prevention againstPrint: Chapter 54. Treatment of Bipolar Disorder http://www.psychiatryonline.com/popup.aspx?aID=443577&print=yes…
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minimization of side effects (Hirschfeld et al. 2002). Treatment with valproate appears to pose an
increased risk of polycystic ovarian syndrome (PCOS), although the relationship between PCOS and
weight gain as a possible mechanism is unclear (Hirschfeld et al. 2002).
Carbamazepine
Although a number of studies have examined the efficacy of carbamazepine in the maintenance
treatment of bipolar disorder, most of these studies yielded results that were difficult to interpret
on methodological grounds (Dardennes et al. 1995). Two studies compared carbamazepine with
lithium. In the first study, there were no significant differences in relapse rates after 1 year
between lithium (31%) and carbamazepine (37%) (Denicoff et al. 1997). In the second trial,
lithium was superior to carbamazepine on a number of outcome measures at 2.5 years of treatment
(Greil et al. 1997). There are no data regarding serum level–response relationships for
carbamazepine maintenance therapy. Denicoff et al. (1997) found that patients receiving the
combination of carbamazepine and lithium in the third year of their trial had a better response than
patients receiving either agent alone. Greil et al. (1997) found that patients with atypical symptoms
(e.g., psychosis) responded better to carbamazepine than to lithium (Greil et al. 1998).
Therapeutic Monitoring of Lithium, Valproate, and Carbamazepine
Once lithium treatment is established at therapeutic plasma concentrations, recommendations for
monitoring patients receiving lithium maintenance treatment include creatinine level and thyroid
function test, along with a lithium level at least every 6 months initially (Hirschfeld et al. 2002).
Thyroid function testing should be especially considered in patients with rapid cycling. Similarly, in
patients receiving valproate maintenance treatment, recommendations for ongoing monitoring
include obtaining a valproic acid level, hepatic function tests, and complete blood count (CBC) with
platelet count approximately every 6 months (Hirschfeld et al. 2002). For carbamazepine, CBC and
hepatic function tests are recommended approximately every 3 months (Hirschfeld et al. 2002).
Atypical Antipsychotics
Olanzapine
Olanzapine was comparable to divalproex in a 47-week comparison trial (Tohen et al. 2003b) and
to lithium in a 1-year comparison trial (Tohen et al. 2005). Olanzapine received an indication for
maintenance treatment in bipolar disorder based on superiority over placebo in prevention of manic
and depressive episodes over 48 weeks (Tohen et al. 2006). The combination of olanzapine and
lithium or divalproex was superior to placebo and lithium or divalproex in relapse prevention over
18 months in patients who had initially responded to the active combination acutely (Tohen et al.
2002b) and then were rerandomized (Tohen et al. 2004). This is a very clinically relevant finding,
since it suggests that patients who respond acutely to olanzapine in combination with lithium or
divalproex in the treatment of a manic episode have a lower risk of relapse by staying on such a
combination. However, patients in the combination therapy group had twice the weight gain of
patients in the monotherapy group.
Aripiprazole
Aripiprazole was superior to placebo in preventing manic relapse over a 6-month follow-up period
in patients with bipolar disorder who were initially stabilized on aripiprazole monotherapy for an
acute manic or mixed episode (Keck et al. 2006a). There was no significant difference between
treatment with aripiprazole and placebo in relapse into depressive episodes; however, the overall
low relapse rate into depression of this trial may have been due to the inclusion of patients whose
index episodes were manic or mixed, and not depressed.
Electroconvulsive Therapy
The use of ECT in the maintenance treatment of bipolar disorder has never been studied
systematically in a randomized, controlled trial. However, a number of naturalistic studies suggest
that maintenance ECT may be a useful treatment alternative for patients who are inadequatelyPrint: Chapter 54. Treatment of Bipolar Disorder http://www.psychiatryonline.com/popup.aspx?aID=443577&print=yes…
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responsive to pharmacotherapy (Schwartz et al. 1995; Vanelle et al. 1994).
Psychotherapy
Most patients with bipolar disorder experience a common cluster of psychological problems
stemming directly from the illness (Table 54–8). A number of specific psychosocial interventions as
adjuncts to mood stabilizer therapy have been shown to improve the long-term outcome of bipolar
disorder (reviewed in Rizvi and Zaretsky 2007). The best-studied interventions include educational,
interpersonal, family, and cognitive-behavioral therapies. Randomized, controlled trials conducted
over 1- to 2-year follow-up periods support the efficacy of cognitive-behavioral therapy (Lam et al.
2005), family-focused and related forms of therapy (Clarkin et al. 1990, 1998; Miklowitz et al.
2003; Rea et al. 2003), interpersonal and social rhythm therapy (Frank et al. 2005), and group
psychoeducation (Colom et al. 2003) in reducing or delaying mood episode recurrence, increasing
treatment adherence, and improving functioning. Family-focused, interpersonal, and social rhythm
therapy were all associated with delaying time to depressive episode relapse compared with brief
treatment (Miklowitz et al. 2007). Only one study, of cognitive-behavioral therapy, found no
significant benefit overall after 1 year, although post hoc analysis suggested that patients with
fewer than 12 lifetime episodes benefited (Scott et al. 2006).
TABLE 54–8. Common psychological issues associated with bipolar disorder
Emotional consequences of manic, mixed, and depressive episodes
Acceptance of and coping with an often chronic mental illness
Effects of stigmatization
Developmental delays or deviations
Fears of recurrence and resulting inhibitions
Interpersonal challenges: marriage, family, pregnancy, child-rearing
Academic and occupational problems
Legal, social, and emotional problems arising from reckless, impulsive, withdrawn, or violent behavior
Source. Adapted from Hirschfeld RMA, Bowden CL, Gitlin MJ, Keck PE, Perlis RH, Suppes T, Thase ME:
“Practice Guideline for the Treatment of Patients With Bipolar Disorder (Revision).” American Journal of
Psychiatry 159 (Supplement):1–50, 2002. Copyright 2002, American Psychiatric Association. Used with
permission.
Novel Treatments
Quetiapine, ziprasidone, risperidone, and paliperidone, as well as new antiepileptics, may be
potential long-term mood-stabilizing agents but have yet to be studied in randomized, controlled
trials. Clozapine was more effective than “treatment as usual” (combinations of mood stabilizers
and typical antipsychotics) in a 1-year study in patients with treatment-refractory bipolar and
schizoaffective disorder (bipolar subtype) (Suppes et al. 1999) and represents an important
treatment option for patients unresponsive to conventional agents.
TREATMENT CONSIDERATIONS
Monotherapy Versus Combination Therapy
Mood Stabilizers
The optimal pharmacological maintenance treatment of bipolar disorder requires titration of any
single mood-stabilizing medication to eradicate subsyndromal symptoms and prevent relapse.
However, outcome assessments from randomized, controlled trials and naturalistic studies indicate
that only a minority of patients with bipolar disorder experience optimal benefit (no relapse or
recurrences, minimal to no subsyndromal symptoms) from monotherapy with any single mood
stabilizer. Combination therapy is therefore frequently necessary and is commonplace in clinicalPrint: Chapter 54. Treatment of Bipolar Disorder http://www.psychiatryonline.com/popup.aspx?aID=443577&print=yes…
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practice. Unfortunately, very few studies have addressed specific mood stabilizer combinations,
their relative therapeutic advantages, and their tolerability. As described earlier (see “Maintenance
Treatment” section earlier in chapter), the combination of olanzapine with lithium or divalproex
was significantly more likely to prevent relapse compared with lithium or divalproex (with placebo)
in patients initially responsive to the combination (Tohen et al. 2004). In the only other study
reported, Solomon et al. (1997) compared the efficacy of lithium alone versus the combination of
lithium and divalproex for 1 year in 12 patients. The combination significantly reduced the risk of
recurrence of mania or depression but was associated with more side effects. Thus, the clinical
practice of combining mood stabilizers has greatly outstripped the limited data available from
formal studies. Combinations of lithium and divalproex, lithium and carbamazepine, and divalproex
and carbamazepine; triple therapy with all three agents; and lithium and/or divalproex with
atypical antipsychotics, antidepressants, and lamotrigine have all been reported in case series to be
useful maintenance treatment strategies (M. P. Freeman and Stoll 1998).
Mood Stabilizers With Antidepressants
Most recommendations regarding the duration of antidepressant treatment (in conjunction with a
mood stabilizer) in patients with bipolar depression suggest prompt discontinuation of
antidepressants after remission of depression (Ghaemi et al. 2001). Limiting antidepressant
exposure is intended to reduce the risk of switching or cycling. However, discontinuation of
antidepressants during maintenance therapy may also increase the risk of depressive relapse. Two
studies involving different cohorts of bipolar patients treated naturalistically found that termination
of antidepressants was associated with a two- to threefold increased risk of depressive relapse
after 1 year (Altshuler et al. 2001, 2003). In contrast, antidepressant continuation was not
significantly associated with an increased risk of mania. The results of these two studies suggest
that the use of antidepressants in combination with mood stabilizers to prevent recurrence of
bipolar depression may be indicated and necessary for many patients, particularly patients without
a history of or risk factors for rapid cycling (e.g., substance use disorder, thyroid disease). The
optimal duration of antidepressant maintenance treatment and possible predictors of switch versus
depressive relapse require further study.
Rapid Cycling
Rapid cycling, the occurrence of four or more mood episodes within 12 months (Dunner and Fieve
1974), poses a special challenge. Among mood stabilizers, divalproex and atypical antipsychotics
appear to have greater efficacy than lithium in patients with rapid cycling. Lamotrigine is also a
treatment option based on the study by Frye et al. (2000), although its long-term benefit in rapid
cycling may be limited to bipolar II rather than bipolar I disorder (Calabrese et al. 2000). Because
very few randomized, controlled trials are available to inform treatment decisions, most
recommendations are empirical. Combinations of mood stabilizers (e.g., lithium and divalproex,
divalproex and atypical antipsychotics, lithium and lamotrigine) are often recommended (Hirschfeld
et al. 2002).
Co-Occurring Psychiatric Disorders
Among the major psychiatric disorders, bipolar disorder has the highest comorbidity rate (McElroy
et al. 2001). Co-occurring psychiatric disorders can affect treatment recommendations, but to date
very few studies have specifically addressed the acute and long-term treatment of patients with
bipolar disorder and psychiatric comorbidity. In a 6-month placebo-controlled trial in female
patients with bipolar II disorder and borderline personality disorder, divalproex was superior to
placebo in reducing measures of interpersonal sensitivity, anger, hostility, and aggression
(Frankenberg and Zanarini 2002). Lithium was superior to placebo in patients with bipolar
spectrum disorder and co-occurring pathological gambling in a 10-week trial (Hollander et al.
2005). Improvement in gambling severity was correlated with improvement in manic symptoms.
Salloum et al. (2005) conducted a 24-week placebo-controlled trial of adjunctive divalproex in
patients with bipolar I disorder and co-occurring alcohol dependence who were also receiving
lithium and psychosocial treatment. Patients receiving divalproex had significantly fewer days ofPrint: Chapter 54. Treatment of Bipolar Disorder http://www.psychiatryonline.com/popup.aspx?aID=443577&print=yes…
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heavy drinking and showed a trend toward fewer drinks per heavy drinking day compared with
patients receiving placebo. Lastly, Weiss et al. (2007) compared a specifically developed form of
integrated group therapy for patients with bipolar disorder and concurrent substance dependence
with group counseling in patients on mood stabilizers over 20 weeks and found significantly fewer
days of substance use in the integrated therapy group during treatment and at 3-month
posttreatment follow-up.
Mood Stabilizers and Bipolar-Specific Psychotherapy
From the evidence reviewed above regarding the efficacy of several different forms of
psychotherapy specifically developed and operationalized for patients with bipolar disorder, it is
clear that the combination of one of these forms of psychotherapy with maintenance
pharmacotherapy is superior to pharmacotherapy alone in reducing the risk of relapse and
recurrence.
CONCLUSION
There have been substantial advances in the pharmacological treatment of bipolar disorder in the
past decade. A number of medications have demonstrated efficacy in the treatment of acute mania
in placebo-controlled trials, either as monotherapy or as an adjunct to mood stabilizers. In addition,
data are available for the first time indicating that combination therapy with an antipsychotic and a
mood stabilizer is more rapidly effective, with better overall response rates in acute mania, than
either mood stabilizers or antipsychotics alone.
The treatment of bipolar depression remains one of the most understudied aspects of the illness.
The “mood stabilizer first” strategy and combined use of mood stabilizers and antidepressants in
moderate to severe bipolar depression are common approaches.
Most patients with bipolar disorder require treatment with more than one medication during the
course of their illness. The efficacy of combination strategies is only now receiving close scrutiny.
Recent studies suggest that the use of combinations of antidepressants and mood stabilizers as
maintenance treatment for some patients to prevent depressive relapse may be important.
The role and efficacy of different types of psychotherapy at different phases of illness management
in bipolar disorder are now becoming clearly established. These components of treatment are
important in educating patients and families, improving insight and treatment adherence,
enhancing coping skills, and dealing with the sequelae of mood symptoms and episodes—and, it is
hoped, improving functioning and outcome. Treatment advances in bipolar disorder are finally
occurring rapidly. Artfully bringing these treatments to patients with bipolar disorder is both the
challenge and the reward of helping people manage this illness.
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Copyright © 2009 American Psychiatric Publishing, Inc. All Rights Reserved.
Course Content
Introduction to Bipolar Disorder: Understanding the Basics
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Understanding Bipolar Disorder: An Overview
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Causes and Risk Factors of Bipolar Disorder
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Diagnostic Criteria and Assessments
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Quiz: Key Concepts in Bipolar Disorder
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Stigma and Misconceptions About Bipolar Disorder
Diagnosis and Assessment: Tools and Techniques
Pharmacological Interventions: Medications and Management Strategies
Psychotherapeutic Approaches: Cognitive and Behavioral Techniques
Advanced Treatment Planning: Integrative and Holistic Care
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