Institute for Medical Informatics, Biometry and Epidemiology, Medical Faculty of the University of Duisburg-Essen, Essen, Germany.
Jefferson Headache Center, Thomas Jefferson University Hospitals, Philadelphia, PA, USA.
Headache. 2021 Jan;61(1):125-136. doi: 10.1111/head.14036. Epub 2020 Dec 13.
To evaluate the efficacy, tolerability, and safety of eptinezumab 100 and 300 mg compared with placebo in patients with the dual diagnosis of chronic migraine (CM) and medication-overuse headache (MOH).
Eptinezumab, a humanized monoclonal antibody targeting calcitonin gene-related peptide, may be effective for treating patients with a dual diagnosis of CM and MOH.
PROMISE-2 (NCT02974153) was a double-blind, randomized, placebo-controlled, phase 3 study that comprised a screening visit, a 28-day pretreatment period, and a 32-week study duration. Patients in this exploratory analysis of a prespecified subgroup had confirmed diagnoses of both CM and MOH at screening. Patients were randomly assigned to receive intravenous eptinezumab 100, 300 mg, or placebo every 12 weeks. Efficacy outcomes included mean changes from baseline in monthly migraine days (MMDs) during weeks 1-12, migraine responder rates at week 12, and percentages of patients below International Classification of Headache Disorders thresholds for CM and MOH over weeks 1-24.
There were 431 patients who were diagnosed with CM and MOH as specified in the protocol and received eptinezumab 100 mg (n = 139), 300 mg (n = 147), or placebo (n = 145). During the baseline period, these patients experienced an average of 16.7 migraine days across treatment arms. Over weeks 1-12, eptinezumab-treated patients experienced greater reductions from baseline in MMDs than placebo patients (100 mg, change from baseline = -8.4, difference from placebo [95% confidence interval (CI)] = -3.0 [-4.56, -1.52], p < 0.0001 vs. placebo; 300 mg, change from baseline = -8.6, difference from placebo [95% CI] = -3.2 [-4.66, -1.78], p < 0.0001 vs. placebo; placebo, -5.4). Compared with placebo, more eptinezumab-treated patients were ≥50% migraine responders (100 mg, 84/139 [60.4%]; 300 mg, 91/147 [61.9%]; placebo, 50/145 [34.5%]) or ≥75% responders (100 mg, 38/139 [27.3%]; 300 mg, 44/147 [29.9%]; placebo, 21/145 [14.5%]) over weeks 1-12. Therapeutic benefits with eptinezumab were observed from day 1 after dosing, and improvements were sustained with an additional dose. For the full 24-week treatment period, 71/139 (51.1%), 80/147 (54.4%), and 47/145 (32.4%) of 100, 300 mg, and placebo-treated patients, respectively, were below CM thresholds, and of the patients who provided sufficient acute medication data, 47/93 (50.5%), 53/107 (49.5%), and 26/96 (27.1%), respectively, were below medication-overuse thresholds.
In patients diagnosed with both CM and MOH, eptinezumab treatment resulted in greater reductions in MMDs, higher responder rates, and fewer patients meeting CM and MOH criteria, thus demonstrating the efficacy and clinical utility of eptinezumab in this patient population.
评估依普替扎umab 100mg 和 300mg 与安慰剂相比在慢性偏头痛(CM)和药物过度使用性头痛(MOH)双重诊断患者中的疗效、耐受性和安全性。
依普替扎umab 是一种针对降钙素基因相关肽的人源化单克隆抗体,可能对治疗 CM 和 MOH 双重诊断患者有效。
PROMISE-2(NCT02974153)是一项双盲、随机、安慰剂对照、3 期研究,包括筛选访问、28 天预处理期和 32 周研究期。本探索性亚组预设分析中的患者在筛选时均确诊为 CM 和 MOH。患者被随机分配接受每 12 周静脉注射依普替扎umab 100mg、300mg 或安慰剂。疗效结局包括从基线到第 1-12 周的每月偏头痛天数(MMD)的平均变化、第 12 周的偏头痛缓解率以及第 1-24 周 CM 和 MOH 国际头痛疾病分类阈值以下的患者百分比。
根据方案规定诊断为 CM 和 MOH 的 431 例患者接受了依普替扎umab 100mg(n=139)、300mg(n=147)或安慰剂(n=145)治疗。在基线期,这些患者在治疗臂中平均经历了 16.7 次偏头痛发作。在第 1-12 周期间,与安慰剂组相比,依普替扎umab 治疗患者的 MMD 从基线的下降幅度更大(100mg,从基线的变化= -8.4,与安慰剂的差异[95%置信区间(CI)]= -3.0 [-4.56,-1.52],p<0.0001;300mg,从基线的变化= -8.6,与安慰剂的差异[95%CI]= -3.2 [-4.66,-1.78],p<0.0001;安慰剂,-5.4)。与安慰剂相比,更多的依普替扎umab 治疗患者为≥50%偏头痛缓解者(100mg,84/139 [60.4%];300mg,91/147 [61.9%];安慰剂,50/145 [34.5%])或≥75%缓解者(100mg,38/139 [27.3%];300mg,44/147 [29.9%];安慰剂,21/145 [14.5%])。在第 1-12 周期间,依普替扎umab 治疗从给药后第 1 天开始出现治疗益处,并且随着额外剂量的给药,改善得以持续。在整个 24 周治疗期间,分别有 71/139(51.1%)、80/147(54.4%)和 47/145(32.4%)的 100、300mg 和安慰剂治疗患者低于 CM 阈值,在提供足够急性药物数据的患者中,分别有 47/93(50.5%)、53/107(49.5%)和 26/96(27.1%)低于药物过度使用阈值。
在诊断为 CM 和 MOH 的患者中,依普替扎umab 治疗可导致 MMD 更大幅度降低、缓解率更高、符合 CM 和 MOH 标准的患者更少,从而证明了依普替扎umab 在这一患者人群中的疗效和临床实用性。
