托吡酯长期预防偏头痛：关键试验的开放标签扩展研究

Long-term migraine prevention with topiramate: open-label extension of pivotal trials.

作者信息

Rapoport Alan, Mauskop Alexander, Diener Hans-Christoph, Schwalen Susanne, Pfeil Joop

机构信息

The New England Center for Headache, PC, Stamford, CT 06902, USA.

出版信息

Headache. 2006 Jul-Aug;46(7):1151-60. doi: 10.1111/j.1526-4610.2006.00506.x.

DOI:10.1111/j.1526-4610.2006.00506.x

PMID:16866719

Abstract

OBJECTIVE

To demonstrate that topiramate is an effective and generally well-tolerated migraine preventive therapy when used for up to 14 months.

BACKGROUND

Topiramate 100 and 200 mg/d significantly reduced mean monthly migraine frequency during 2 large, 26-week, randomized, placebo-controlled trials. Only a small number of clinical trials have examined the long-term (> or =1 year) effectiveness and safety of migraine preventive therapies.

METHODS

Five hundred sixty-seven patients with an established history of migraine with or without aura were enrolled in this 8-month, open-label extension of 2 large (49 US and 52 US and Canadian medical centers), randomized, double-blind, placebo-controlled, parallel group, 26-week trials of identical design. To be eligible for the open-label extension, patients were required to have either completed the double-blind phase of the 2 pivotal migraine prevention trials or withdrew after 4 weeks due to lack of efficacy. All eligible patients, regardless of type or dose of study medication (topiramate or placebo) received in the double-blind phase, were titrated to a clinically effective dose of open-label topiramate based on physician judgment of patient response. Efficacy of topiramate was measured as the change in mean monthly migraine frequency.

RESULTS

The mean topiramate dose during the open-label extension phase was 124.7 mg/d and 150.3 mg/d for patients on placebo (n = 159) or topiramate (n = 408), respectively, during the double-blind phase (N = 567, 91% female, mean age 39.4 years). Patients on topiramate for up to 14 months had 2.2 +/- 2.4 (mean +/- SD) migraines per month after completion of the open-label extension phase (3.4 +/- 2.6 at double-blind endpoint). Patients on topiramate during the open-label extension phase only (placebo during the double-blind phase) had 3.0 +/- 2.9 migraines per month at open-label extension endpoint (4.9 +/- 3.0 migraines per month at double-blind endpoint). Discontinuation rates due to adverse events during the double-blind phase were 22.2% for patients on topiramate and 11.0% for patients on placebo. Discontinuation rates due to adverse events during the open-label extension phase were 8.6% for those patients who had already received topiramate during the double-blind phase and 20.9% for those patients who had previously received placebo.

CONCLUSIONS

Patients receiving topiramate experienced a sustained reduction in migraine frequency for up to 14 months. The effectiveness and safety of topiramate was consistent with that observed during 2 26-week pivotal trials.

摘要

目的

证明托吡酯用于长达14个月时是一种有效且总体耐受性良好的偏头痛预防性治疗药物。

背景

在两项大型、为期26周、随机、安慰剂对照试验中，托吡酯100和200mg/天显著降低了平均每月偏头痛发作频率。仅有少数临床试验研究了偏头痛预防性治疗的长期（≥1年）有效性和安全性。

方法

567例有或无先兆偏头痛确诊病史的患者参与了这项为期8个月的开放标签扩展试验，该试验是对两项大型（49家美国和52家美国及加拿大医疗中心）、设计相同的随机、双盲、安慰剂对照、平行组、为期26周试验的扩展。要符合开放标签扩展试验的条件，患者需完成两项关键偏头痛预防试验的双盲阶段，或因缺乏疗效在4周后退出。所有符合条件的患者，无论在双盲阶段接受的研究药物（托吡酯或安慰剂）类型或剂量如何，均根据医生对患者反应的判断滴定至开放标签托吡酯的临床有效剂量。托吡酯的疗效通过平均每月偏头痛发作频率的变化来衡量。

结果

在开放标签扩展阶段，安慰剂组（n = 159）和托吡酯组（n = 408）患者在双盲阶段（N = 567，91%为女性，平均年龄39.4岁）的托吡酯平均剂量分别为124.7mg/天和150.3mg/天。接受托吡酯治疗长达14个月的患者在开放标签扩展阶段结束后每月有2.2±2.4（均值±标准差）次偏头痛发作（双盲终点时为3.4±2.6次）。仅在开放标签扩展阶段接受托吡酯治疗（双盲阶段接受安慰剂）的患者在开放标签扩展终点时每月有3.0±2.9次偏头痛发作（双盲终点时为每月4.9±3.0次）。双盲阶段因不良事件导致的停药率，托吡酯组患者为22.2%，安慰剂组患者为11.0%。开放标签扩展阶段因不良事件导致的停药率，双盲阶段已接受托吡酯治疗的患者为8.6%，先前接受安慰剂治疗的患者为20.9%。