Treatment of bipolar affective disorder

doi:10.1136/bmj.321.7272.1302

BMJ 2000;321:1302-1303 ( 25 November )

Editorials

Treatment of bipolar affective disorder

New drug treatments are emerging, but more clinical evidence is required

Bipolar affective disorder is a common condition which, among mental illnesses, ranks second only to unipolar depression asa cause of worldwide disability.¹ Classically, it manifestsitself as repeated periods of illness with complete recovery.However, many patients have a poor outcome: a third suffer chronicsymptoms and some 13-24% develop rapid cycling disorder, wherefour or more episodes occur within a year. The lifetime risk ofbipolar disorder is at least 1.2%, with a recognised risk of completedsuicide of 15%. Young men, early in the course of their illness,are at highest risk, especially those with a history of suicideattempts or alcohol abuse and those recently discharged from hospital.Despite its shortcomings, lithium has long been the mainstay oftreatment for bipolar affective disorder. Several newer drugshave emerged over the past 10 years, but evidence of their effectivenessremains disappointinglythin.

Ideally, mood stabilisers should treat both mania and depression and prevent their recurrence. Importantly, treatment itselfshould not precipitate mania or depression or induce rapid cycling.Lithium has been used as a mood stabiliser in bipolar disorderfor 50 years. It continues as a first line treatment in acuteepisodes and in prophylaxis, but doubts remain about its effectivenessin clinical practice. Some patients respond inadequately to lithium,especially those with rapid cycling disorder and those with mixedmania, where manic and depressive symptoms occur together. Itsnarrow therapeutic window necessitates frequent blood monitoring,limiting its use in some countries. Lithium discontinuation mayprecipitate recurrence, a serious problem in the poorlycompliant.

The anticonvulsants carbamazepine and valproate are established alternative and adjunctive treatments to lithium. Valproateis the most frequently prescribed mood stabiliser in the UnitedStates and is increasingly used in Europe. The mechanism of actionof anticonvulsants in bipolar disorder remains unclear. Originallythey were used when lithium was poorly tolerated or ineffective;now they are increasingly used as first line monotherapy, yetthe evidence for their use remains incomplete. The efficacy ofvalproate in treating mania was confirmed in the largest placebocontrolled trial in which it was studied,² but no randomisedcontrolled trials have examined its effects in bipolar depression.Its use in maintenance treatment has been based on open data andone randomised controlled trial in a group of patients with heterogenousaffective disorders.³ Recently, a randomised controlled trialfailed to show that valproate prolonged the time to recurrenceof any mood episode over 12 months, although this result is questionablebecause of the methodological limitations of the study.⁴

The efficacy of carbamazepine in treating mania and bipolar depression and in prophylaxis has been shown in randomised controlledtrials, but evidence for its acute efficacy in bipolar depressionand overall prophylactic efficacy is not strong. Cochrane reviewson the efficacy of carbamazepine and valproate in bipolar disorderare underway.

All the established mood stabilisers appear to be more effective in treating and preventing mania than depression. Lithiumis reported to have specific antisuicidal effects,⁵ but fewdata are available on the antisuicidal effects of carbamazepineand valproate. Although valproate and carbamazepine may be moreeffective than lithium for mixed states and rapid cycling disorder,much treatment resistance remains. New medications for bipolardepression, mixed states, and rapid cycling disorder are urgentlyneeded: new anticonvulsants and atypical antipsychotics are potentialcandidates.

The anticonvulsant lamotrigine has been shown to have acute efficacy in bipolar depression in two randomised controlled trials. ⁶ ⁷ In the first placebo controlled trial conducted in rapid cyclingdisorder, lamotrigine improved the overall relapse rate.⁸ Twoplacebo controlled trials failed to replicate open label evidenceof gabapentin's efficacy in hypomania and mania. ⁷ ⁹ Cochranereviews on both these anticonvulsants in bipolar disorder areinprogress.

Antipsychotics have long been used in bipolar disorder. Typical antipsychotics are effective in acute mania but may exacerbatepostmanic depression. Little evidence supports their prophylacticuse, which risks the induction of tardive dyskinesia. Placebocontrolled studies of olanzapine and risperidone have shown theacute antimanic efficacy of both these atypical antipsychotics,although the effects of prolonged use are not yet clear. The prototypeatypical antipsychotic, clozapine, is reserved for use in highlyrefractory cases of bipolar disorder.¹⁰ Intriguingly, $omega$ -3 fattyacids showed mood stabilising effects in one small randomisedplacebo controlled trial; the underlying mechanism may be theinhibition of signal transduction in neuronal membranes.¹¹

New non-pharmacological treatments such as transcranial magnetic stimulation and vagal nerve stimulation are emerging. Psychologicaltreatments such as cognitive behavioural therapy target recognitionof early warning symptoms and compliance with medication and mayprovide strategies for coping with illness and attendant psychosocialproblems.¹²

The management of this common and often debilitating lifelong illness should be shared between primary care and general psychiatrists.Although many new acute treatments for mania have been evaluatedin placebo controlled studies over the past 10 years, only a fewhave undergone evaluation of their prophylactic efficacy in longterm randomised controlled trials. Clinicians and their patientsneed evidence based treatment strategies that produce completesustained remissions and improve quality oflife.

A H Young, professor of psychiatry.
Karine A N Macritchie, specialist registrar.

Department of Psychiatry, Royal Victoria Infirmary, Newcastle upon Tyne NE1 4LP

J R Calabrese, director, mood disorders programme.

Case Western Reserve University School of Medicine, 11400 Euclid Ave, Suite 200, Cleveland, Ohio 44106, USA

Acknowledgments

AHY is funded by the Stanley Research Foundation and has received consultancy fees from Janssen. JRC is involved in advisoryboards for the following pharmaceutical companies: Abbott, AstraZeneca,Eli Lilly, GlaxoWellcome, Janssen Cilag, Novartis, Parke Davis,Shire, Smith Kline, TAP Holdings, UCB Pharma, andTeva.

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Treating bipolar affective disorder: Max Fink and Allan Young
BMJ 2001 322: 365. [Extract] [Full Text]

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