University of Toronto, Toronto, Ontario, Canada.
Accelerated Enrollment Solutions, Atlanta, Georgia, USA.
Bipolar Disord. 2024 Aug;26(5):442-453. doi: 10.1111/bdi.13421. Epub 2024 Apr 12.
Cariprazine treats acute manic and depressive episodes in bipolar I disorder (BP-I), but its efficacy in preventing relapse of mood episode remains unknown.
In this phase 3b, double-blind, placebo-controlled study, patients with BP-I with acute manic or depressive episodes (each with/without mixed features), were treated with cariprazine 3.0 mg/day during a 16-week open-label treatment period; those who achieved stable remission within 8 weeks and remained stable for at least another 8 weeks were randomized to receive cariprazine 1.5 or 3.0 mg per day or placebo in the double-blind treatment period for up to 39 weeks. The primary efficacy endpoint was time to relapse of any mood episode. Adverse events (AEs) were assessed.
Patients (440/896) enrolled in the open-label treatment period achieved stability criteria and were randomized to receive cariprazine 3.0 mg/day (n = 148), cariprazine 1.5 mg/day (n = 147), or placebo (n = 145) in the double-blind treatment period. Relapse rates were 17.9%, 16.8%, and 19.7% in the cariprazine 3.0 mg/day, cariprazine 1.5 mg/day, and placebo groups, respectively. Neither dose of cariprazine was more effective than placebo on the primary outcome (3.0 mg/day: HR = 0.89, [95% CI: 0.5, 1.5]; 1.5 mg/day: HR = 0.83, 95% CI [0.5, 1.4]). The most frequently reported AEs (≥5%) were akathisia, headache, insomnia, and nausea in the open-label treatment period and increased weight and insomnia in the double-blind treatment period. In the open-label and double-blind treatment periods, 7.5% and 1.6% of patients experienced an AE leading to discontinuation.
Cariprazine was not superior to placebo in the prevention of relapses in this study. Relapse rates were unusually low in the placebo group. Cariprazine was well-tolerated.
卡利拉嗪可治疗双相情感障碍 I 型(BP-I)的急性躁狂和抑郁发作,但预防情绪发作复发的疗效尚不清楚。
在这项 3b 期、双盲、安慰剂对照研究中,患有急性躁狂或抑郁发作(各有/无混合特征)的 BP-I 患者在 16 周的开放标签治疗期内接受卡利拉嗪 3.0mg/天治疗;在 8 周内达到稳定缓解且至少再稳定 8 周的患者,在双盲治疗期内随机接受卡利拉嗪 1.5 或 3.0mg/天或安慰剂治疗,最长 39 周。主要疗效终点是任何情绪发作的复发时间。评估不良事件(AE)。
进入开放标签治疗期的患者(440/896)达到稳定标准,并在双盲治疗期内随机接受卡利拉嗪 3.0mg/天(n=148)、卡利拉嗪 1.5mg/天(n=147)或安慰剂(n=145)治疗。卡利拉嗪 3.0mg/天、卡利拉嗪 1.5mg/天和安慰剂组的复发率分别为 17.9%、16.8%和 19.7%。卡利拉嗪的两个剂量在主要结局上均不比安慰剂更有效(3.0mg/天:HR=0.89,[95%CI:0.5,1.5];1.5mg/天:HR=0.83,95%CI [0.5,1.4])。在开放标签治疗期内报告的最常见不良事件(≥5%)为静坐不能、头痛、失眠和恶心,在双盲治疗期内为体重增加和失眠。在开放标签和双盲治疗期内,分别有 7.5%和 1.6%的患者因不良事件而停药。
在这项研究中,卡利拉嗪在预防复发方面并不优于安慰剂。安慰剂组的复发率异常低。卡利拉嗪耐受良好。
