Efficacy of Olanzapine in Combination With Valproate or Lithium in the Treatment of Mania in Patients Partially Nonresponsive to Valproate or Lithium Monotherapy

Mauricio Tohen; K. N. Roy Chengappa; Trisha Suppes; Carlos A. Zarate; Joseph R. Calabrese; Charles L. Bowden; Gary S. Sachs; David J. Kupfer; Robert W. Baker; Richard C. Risser; Elisabeth L. Keeter; Peter D. Feldman; Gary D. Tollefson; Alan Breier

doi:10.1001/archpsyc.59.1.62

Efficacy of Olanzapine in Combination With Valproate or Lithium in the Treatment of Mania in Patients Partially Nonresponsive to Valproate or Lithium Monotherapy

Mauricio Tohen(Eli Lilly (United States)), K. N. Roy Chengappa(University of Pittsburgh), Trisha Suppes(The University of Texas at Austin), Carlos A. Zarate(National Institutes of Health), Joseph R. Calabrese(Case Western Reserve University), Charles L. Bowden(The University of Texas at San Antonio), Gary S. Sachs(Harvard University Press), David J. Kupfer(University of Pittsburgh), Robert W. Baker(Eli Lilly (United States)), Richard C. Risser(Eli Lilly (United States)), Elisabeth L. Keeter(Eli Lilly (United States)), Peter D. Feldman(Eli Lilly (United States)), Gary D. Tollefson(Eli Lilly (United States)), Alan Breier(Eli Lilly (United States))

Archives of General Psychiatry

January 1, 2002

10.1001/archpsyc.59.1.62

Cited by 439

Abstract

BACKGROUND: A 6-week double-blind, randomized, placebo-controlled trial was conducted to determine the efficacy of combined therapy with olanzapine and either valproate or lithium compared with valproate or lithium alone in treating acute manic or mixed bipolar episodes. METHODS: The primary objective was to evaluate the efficacy of olanzapine (5-20 mg/d) vs placebo when added to ongoing mood-stabilizer therapy as measured by reductions in Young Mania Rating Scale (YMRS) scores. Patients with bipolar disorder (n = 344), manic or mixed episode, who were inadequately responsive to more than 2 weeks of lithium or valproate therapy, were randomized to receive cotherapy (olanzapine + mood-stabilizer) or monotherapy (placebo + mood-stabilizer). RESULTS: Olanzapine cotherapy improved patients' YMRS total scores significantly more than monotherapy (-13.11 vs -9.10; P = .003). Clinical response rates (> or = 50% improvement on YMRS) were significantly higher with cotherapy (67.7% vs 44.7%; P< .001). Olanzapine cotherapy improved 21-item Hamilton Depression Rating Scale (HAMD-21) total scores significantly more than monotherapy (4.98 vs 0.89 points; P< .001). In patients with mixed-episodes with moderate to severe depressive symptoms (DSM-IV mixed episode; HAMD-21 score of > or = 20 at baseline), olanzapine cotherapy improved HAMD-21 scores by 10.31 points compared with 1.57 for monotherapy (P< .001). Extrapyramidal symptoms (Simpson-Angus Scale, Barnes Akathisia Scale, Abnormal Involuntary Movement Scale) were not significantly changed from baseline to end point in either treatment group. Treatment-emergent symptoms that were significantly higher for the olanzapine cotherapy group included somnolence, dry mouth, weight gain, increased appetite, tremor, and slurred speech. CONCLUSION: Compared with the use of valproate or lithium alone, the addition of olanzapine provided superior efficacy in the treatment of manic and mixed bipolar episodes.

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