Title: Once-Daily Quetiapine XR Monotherapy Effective and Well Tolerated in Bipolar Depression: Presented at EPA
|
|
To print: Select File and then Print from your browser's menu Title: Once-Daily Quetiapine XR Monotherapy Effective and Well Tolerated in Bipolar Depression: Presented at EPA |
|
"Once-Daily Quetiapine XR Monotherapy Effective and Well Tolerated in Bipolar Depression: Presented at EPA" By Chris Berrie LISBON, Portugal -- January 27, 2009 -- An extended-release (XR) formulation of the atypical antipsychotic quetiapine is well tolerated and more effective than placebo in the treatment of acute depressive episodes in patients with bipolar I and II disorder, according to results of a multicentre, randomised, double-blind, parallel-group, placebo-controlled, phase 3 study. Björn Paulsson, MD, AstraZeneca Pharmaceuticals LP, Wilmington, Delaware, discussed the results in a presentation on January 25 on behalf of the study authors here at the European Psychiatry Association (EPA) 17th Annual Meeting. The researchers enrolled outpatients aged 18 to 65 years with a clinical diagnosis of bipolar I or II disorder with or without rapidly cycling disease, who had an acute episode of depression. Further criteria included a total score of 20 or greater on the 17-item Hamilton Rating Scale for Depression (HAM-D17), an item 1 score of 2 or greater on the HAM-D17, and total score no greater than 12 on the Young Mania Rating Scale (YMRS). The primary outcome was change from baseline to week 8 on total score of the Montgomery-Äsberg Depression Rating Scale (MADRS). The secondary outcomes included primary outcome subgroups, rates of response, and changes in Clinical Global Impression-Bipolar Disorder-Severity of Illness (CGI-BP-S) score. Patient baseline demographics showed no differences between the placebo and quetiapine XR groups for bipolar I disorder (80.3% vs 80.5%, respectively), rapid cycling (27.7% vs 27.1%), mean MADRS score (30.1 vs 29.8), HAM-D17 score (24.6 vs 24.8), and CGI-BP-S score (4.4 vs 4.5). After a washout period of up to 28 days, 137 patients were randomised to placebo and 133 to quetiapine XR 300 mg QD for 8 weeks. Quetiapine XR dosing was tapered through 50, 100, 200, and 300 mg over the first 4 days and then was maintained. Concomitant psychoactive drugs allowed were lorazepam, zolpidem tartrate, zaleplon, zopicione, and chloral hydrate. Mean ages were 39.9 years in the quetiapine group and 39.0 years in the placebo group; men made up 37.2% and 33.8%, respectively, of each group. Quetiapine XR treatment was significantly more effective than placebo for reduction in mean MADRS scores from week 1 through week 8. At week 8, reductions in mean MADRS scores were 17.4 for quetiapine XR and 11.9 for placebo ([P < .001) and were similar for the bipolar I (P < .001) and 2 (P < .05) analyses and for patients without (P < .001) and with (P < .01) rapid cycling. For individual MADRS items, 8 of 10 were significantly reduced with quetiapine XR over placebo (P < .05 to P < .001), with no effects on "lassitude" and "suicidal thoughts." These benefits for quetiapine XR over placebo were also reflected in the remaining secondary outcomes. |
|
Copyright © 2009 P\S\L Consulting Group Inc. All rights reserved. Republication or redistribution of P\S\L content is expressly prohibited without the prior written consent of P\S\L. P\S\L shall not be liable for any errors, omissions or delays in this content or any other content on its sites, newsletters or other publications, nor for any decisions or actions taken in reliance on such content. Go back This site is maintained by webmaster@pslgroup.com Please contact us with any comments, problems or bugs. All contents Copyright (c) 2009 P\S\L Consulting Group Inc. All rights reserved. |