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Key claims

Strengths:

Well-documented efficacy in acute mania and maintenance therapy – less so for bipolar depression (OFC).
Potential antidepressant effect.
Low EPS risk (compared with conventional antipsychotics, e.g. haloperidol).

Weaknesses:

Key claims:

Efficacy:

Reduced relapse rate: significantly reduces rates of manic and depressive relapse
Increased time to relapse: significantly prolongs the time to relapse into a depressive or manic episode
At least as effective as lithium: olanzapine is at least as effective as lithium in prolonging remission in bipolar disorder and more effective than lithium in preventing relapse into mania
OFC in bipolar depression: OFC is more effective than placebo or olanzapine alone in the treatment of bipolar depression and rapid-cycling depression
No treatment-emergent mania: no risk of treatment-emergent mania with olanzapine or OFC therapy in depressed bipolar patients
Improvements in HR-QoL: olanzapine and OFC improve HR-QoL in depressed bipolar patients

Tolerability:

Fewer drop-outs than lithium: more patients remain on olanzapine therapy compared with lithium in the maintenance of bipolar disorder
No QTc prolongation: olanzapine is not associated with QTc prolongation

General/positioning:

GSK counterclaims:

Olanzapine has never been studied as a maintenance treatment in patients who were initially depressed at study entry.
Olanzapine has been shown to be no more effective than lithium in preventing depressive episodes.
The effect size for olanzapine in the treatment of acute bipolar depression is modest and smaller than that of lamotrigine.
Both olanzapine and OFC caused significant weight gain after only 8 weeks of treatment.
Depression and somnolence are consistently among the most frequently side effects observed with olanzapine maintenance treatment.
Weight gain has been a significant issue in olanzapine treatment observed in every clinical trial presented to date.