依泊格帕坦基于先前暴露和对曲坦类药物反应的疗效:一项事后分析。
Efficacy of ubrogepant based on prior exposure and response to triptans: A post hoc analysis.
机构信息
The Neurology Center, Headache Center of Southern California, Carlsbad, CA, USA.
NIHR-Wellcome Trust King's Clinical Research Facility, King's College, London, UK.
出版信息
Headache. 2021 Mar;61(3):422-429. doi: 10.1111/head.14089. Epub 2021 Mar 22.
OBJECTIVE
To determine the potential efficacy of ubrogepant for acute treatment of migraine based on historical experience with triptans.
BACKGROUND
Although triptans have improved migraine treatment, their efficacy and tolerability may limit their utility in some individuals. Ubrogepant is a small-molecule, oral calcitonin gene-related peptide receptor antagonist approved by the Food and Drug Administration for acute treatment of migraine in adults.
METHODS
This post hoc analysis of pooled data from the pivotal trials ACHIEVE I and II, identically designed, randomized, double-blind, phase 3, single-attack trials of ubrogepant in adults with a history of migraine with/without aura, examined the efficacy and tolerability of ubrogepant 50 mg versus placebo based on participants' historical experience with triptans: triptan responder, triptan-insufficient responder, and triptan naïve. Co-primary efficacy endpoints were pain freedom and absence of most bothersome migraine-associated symptom (MBS) 2 h post initial dose. Adverse events (AEs) within historical triptan experience subgroups were evaluated.
RESULTS
In the pooled analysis population (n = 1799), 682 (placebo, n = 350; ubrogepant 50 mg, n = 332), 451 (placebo, n = 223; ubrogepant, n = 228), and 666 (placebo, n = 339; ubrogepant, n = 327) participants were triptan responders, triptan-insufficient responders, and triptan-naïve, respectively. Response rates on co-primary efficacy endpoints were higher for ubrogepant versus placebo across all groups. Treatment-by-subgroup interaction p values based on odds ratios for pain freedom (p = 0.290) and absence of MBS (p = 0.705) indicated no significant impact of historical triptan experience on ubrogepant efficacy. AE incidence for ubrogepant did not differ appreciably across historical triptan experience subgroups.
CONCLUSIONS
Ubrogepant efficacy and tolerability did not differ for the acute treatment of migraine in participants classified as triptan responders, triptan-insufficient responders, and triptan-naïve based on their historical experience with triptans.
目的
基于曲坦类药物的历史经验,确定ubrogepant 治疗偏头痛急性发作的潜在疗效。
背景
尽管曲坦类药物改善了偏头痛的治疗效果,但它们的疗效和耐受性可能限制了其在某些人群中的应用。ubrogepant 是一种小分子、口服降钙素基因相关肽受体拮抗剂,已获美国食品药品监督管理局批准用于治疗成人偏头痛急性发作。
方法
本研究为一项基于历史经验的事后分析,对患有有先兆/无先兆偏头痛成人的两项关键性、设计相同的、随机、双盲、3 期单发作临床试验(ACHIEVE I 和 II)的数据进行了汇总分析,这些患者均有偏头痛的病史,研究比较了 ubrogepant 50mg 与安慰剂的疗效和耐受性,根据参与者使用曲坦类药物的历史经验,将参与者分为曲坦类药物应答者、曲坦类药物应答不足者和曲坦类药物初治者。主要疗效终点为初始给药后 2 小时疼痛无缓解和最困扰的偏头痛相关症状(MBS)无缓解。评估了历史曲坦类药物经验亚组中的不良事件(AE)。
结果
在汇总分析人群中(n=1799),682 名参与者(安慰剂组,n=350;ubrogepant 50mg 组,n=332)、451 名参与者(安慰剂组,n=223;ubrogepant 组,n=228)和 666 名参与者(安慰剂组,n=339;ubrogepant 组,n=327)分别为曲坦类药物应答者、曲坦类药物应答不足者和曲坦类药物初治者。与安慰剂相比,ubrogepant 在所有组中的主要疗效终点的应答率均更高。基于比值比的疼痛无缓解(p=0.290)和 MBS 无缓解(p=0.705)的治疗-亚组交互 p 值表明,历史曲坦类药物经验对 ubrogepant 的疗效无显著影响。ubrogepant 的不良事件发生率在不同历史曲坦类药物经验亚组中无明显差异。
结论
基于曲坦类药物的历史经验,将参与者分为曲坦类药物应答者、曲坦类药物应答不足者和曲坦类药物初治者,在偏头痛的急性治疗中,ubrogepant 的疗效和耐受性无差异。
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