Danish Headache Center, Rigshospitalet Glostrup, University of Copenhagen, Copenhagen, Denmark.
Pain Department and FHU InovPain, Centre Hospitalier Universitaire de Nice, Nice, France; INSERM U1107 Migraine and Trigeminal Pain, Auvergne University, Clermont-Ferrand, France.
Lancet Neurol. 2022 Jul;21(7):597-607. doi: 10.1016/S1474-4422(22)00185-5.
The monoclonal antibody eptinezumab, which targets calcitonin gene-related peptide, has shown migraine preventive effects starting the day following infusion and acceptable safety and tolerability in phase 3 trials, but benefits in the subpopulations of patients with previous preventive treatment failures were not examined. We aimed to investigate the safety and efficacy of eptinezumab for migraine prevention in adults with migraine and two-to-four previous preventive treatment failures.
DELIVER was a multicentre, multi-arm, phase 3b trial comprising a 24-week double-blind, placebo-controlled period and a 48-week dose-blinded extension. We recruited adults with episodic or chronic migraine with at least 4 monthly migraine days (as per International Headache Society guidelines) and documented evidence of two-to-four previous preventive treatment failures within the past 10 years, from 96 study locations across Europe (n=93) and the USA (n=3). Patients were randomly assigned (1:1:1) via a centralised randomisation system, stratified by baseline monthly headache days and country, to eptinezumab 100 mg, eptinezumab 300 mg, or placebo. The primary efficacy endpoint was the change from baseline in mean monthly migraine days (captured using a daily electronic diary) in weeks 1-12, assessed in the full analysis set. All participants and study personnel were masked to study drug assignments. The dose-blinded extension period is ongoing. The trial is registered with ClinicalTrials.gov, NCT04418765, and EudraCT, 2019-004497-25.
Between June 1, 2020, and Oct 7, 2021, 891 individuals were randomly assigned and received at least one dose of study drug (safety population; eptinezumab 100 mg n=299 [34%], eptinezumab 300 mg n=294 [33%], placebo n=298 [33%]). 865 patients completed the placebo-controlled period. The change from baseline to weeks 1-12 in mean monthly migraine days was -4·8 (SE 0·37) with eptinezumab 100 mg, -5·3 (0·37) with eptinezumab 300 mg, and -2·1 (0·38) with placebo. The difference from placebo in change in mean monthly migraine days from baseline was significant with eptinezumab 100 mg (-2·7 [95% CI -3·4 to -2·0]; p<0·0001) and eptinezumab 300 mg (-3·2 [-3·9 to -2·5]; p<0·0001). Treatment-emergent adverse events occurred in 127 (42%) of 299 patients in the eptinezumab 100 mg group, in 120 (41%) of 294 in the eptinezumab 300 mg group, and in 119 (40%) of 298 in the placebo group. The most common treatment-emergent adverse event was COVID-19 (20 [7%] of 299 patients in the eptinezumab 100 mg group, 17 [6%] of 294 in the eptinezumab 300 mg group, and 16 [5%] of 298 in the placebo group). Serious adverse events were uncommon (five [2%] of 299 in the eptinezumab 100 mg group, seven [2%] of 294 in the eptinezumab 300 mg group, four [1%] of 298 in the placebo group) and included anaphylactic reaction (eptinezumab 300 mg n=2) and COVID-19 (eptinezumab 100 mg n=1 and eptinezumab 300 mg n=1).
In adults with migraine and two-to-four previous preventive treatment failures, eptinezumab provided significant migraine preventive effects compared with placebo, with acceptable safety and tolerability, indicating that eptinezumab might be an effective treatment option for this patient population. The dose-blinded extension period will provide additional long-term safety data in patients with migraine and previous preventive treatment failures.
H Lundbeck.
靶向降钙素基因相关肽的单克隆抗体依普替扎umab 在输注后次日即显示出偏头痛预防作用,并且在 3 期试验中具有可接受的安全性和耐受性,但先前预防治疗失败的患者亚组的获益情况尚未进行研究。我们旨在研究依普替扎umab 对偏头痛预防的安全性和有效性,该研究纳入了偏头痛且过去 10 年内有 2 至 4 次预防治疗失败的成年人。
DELIVER 是一项多中心、多臂、3b 期试验,包括 24 周的双盲、安慰剂对照期和 48 周的剂量盲扩展期。我们从欧洲(n=93)和美国(n=3)的 96 个研究地点招募了偏头痛发作频率至少为 4 次/月(根据国际头痛协会指南)且过去 10 年内有 2 至 4 次预防治疗失败记录的偏头痛成年患者。患者通过中央随机化系统以 1:1:1 的比例随机分配至依普替扎umab 100mg、依普替扎umab 300mg 或安慰剂组,分层因素为基线每月头痛天数和国家。主要疗效终点是在第 1-12 周内使用每日电子日记记录的平均每月偏头痛天数的变化,在全分析集(full analysis set)中进行评估。所有参与者和研究人员对研究药物的分配均设盲。剂量盲扩展期正在进行中。该试验在 ClinicalTrials.gov 注册,NCT04418765,和 EudraCT,2019-004497-25。
在 2020 年 6 月 1 日至 2021 年 10 月 7 日期间,891 名患者被随机分配并接受了至少一剂研究药物(安全性人群;依普替扎umab 100mg 组 n=299 [34%],依普替扎umab 300mg 组 n=294 [33%],安慰剂组 n=298 [33%])。865 名患者完成了安慰剂对照期。依普替扎umab 100mg 组的平均每月偏头痛天数从基线到第 1-12 周的变化为-4·8(SE 0·37),依普替扎umab 300mg 组为-5·3(0·37),安慰剂组为-2·1(0·38)。依普替扎umab 100mg 组和依普替扎umab 300mg 组的平均每月偏头痛天数与安慰剂组相比,从基线的变化差异均有统计学意义(依普替扎umab 100mg 组-2·7 [95%CI -3·4 至 -2·0];p<0·0001;依普替扎umab 300mg 组-3·2 [-3·9 至 -2·5];p<0·0001)。依普替扎umab 100mg 组 299 名患者中有 127 名(42%)和依普替扎umab 300mg 组 294 名患者中有 120 名(41%)发生了治疗出现的不良事件,安慰剂组 298 名患者中有 119 名(40%)发生了治疗出现的不良事件。最常见的治疗出现的不良事件是 COVID-19(依普替扎umab 100mg 组 299 名患者中有 20 名[7%],依普替扎umab 300mg 组 294 名患者中有 17 名[6%],安慰剂组 298 名患者中有 16 名[5%])。严重不良事件少见(依普替扎umab 100mg 组 5 名[2%],依普替扎umab 300mg 组 7 名[2%],安慰剂组 4 名[1%]),包括过敏反应(依普替扎umab 300mg 组 2 例)和 COVID-19(依普替扎umab 100mg 组 1 例和依普替扎umab 300mg 组 1 例)。
在偏头痛且过去 10 年内有 2 至 4 次预防治疗失败的成年人中,与安慰剂相比,依普替扎umab 提供了显著的偏头痛预防效果,具有可接受的安全性和耐受性,表明依普替扎umab 可能是该患者人群的有效治疗选择。在过去有预防治疗失败的偏头痛患者中,剂量盲扩展期将提供额外的长期安全性数据。
H Lundbeck。
