在接受加奈珠单抗治疗的患者中,从高频阵发性偏头痛转为低频阵发性偏头痛:两项全球随机临床试验结果。
Shift from high-frequency to low-frequency episodic migraine in patients treated with Galcanezumab: results from two global randomized clinical trials.
机构信息
Eli Lilly and Company, Indianapolis, IN, 46285, USA.
Phoenix Headache Institute, Scottsdale, USA.
出版信息
J Headache Pain. 2021 May 28;22(1):48. doi: 10.1186/s10194-021-01222-w.
BACKGROUND
Patients with episodic migraine (EM) with a higher-frequency of migraine headache days (HFEM: 8-14 migraine headache days/month) have a greater disease burden and a higher risk of progressing to chronic migraine (CM) with associated acute treatment overuse versus those with low-frequency EM (LFEM: 4-7 migraine headache days/month). In this post hoc analysis, we assessed the proportions of patients who shifted from HFEM to LFEM and to very low-frequency EM (VLFEM: 0-3 migraine headache days/month) status following treatment with galcanezumab versus placebo.
METHODS
EVOLVE-1 and EVOLVE-2 were double-blind, Phase 3 studies in patients with EM. Patients (18-65 years) were randomized (2:1:1) to subcutaneous monthly injections of placebo, galcanezumab 120 mg (240 mg loading dose) or 240 mg, for up to 6 months. Data were pooled and endpoints were change from baseline in number of migraine headache days/month and patients who shifted from HFEM to LFEM or VLFEM status. Impact of change in HFEM status on migraine headache days/month, quality of life and disability was also assessed.
RESULTS
A total of 66% (1176/1773) patients from EVOLVE studies had HFEM status at baseline and were included in this analysis; placebo: 592, galcanezumab 120 mg: 294 and galcanezumab 240 mg: 290. At each month, both doses of galcanezumab resulted in a higher proportion of patients who shifted to 0-7 monthly headache days/month (VLFEM or LFEM status). Patients who shifted from HFEM at baseline to VLFEM status at Month 3, a relatively larger proportion of patients on galcanezumab 120 mg versus placebo remained at VLFEM status at Months 4-6; Months 4-5 for galcanezumab 240 mg versus placebo. Among the galcanezumab-treated patients who did-not-shift or shifted to LFEM or VLFEM status for ≥3 consecutive months until the end of the study, patients who shifted from HFEM to VLFEM status experienced the largest reduction in migraine headache days/month and the largest clinically meaningful improvements in daily functioning (MSQ-RFR) and disability (MIDAS).
CONCLUSIONS
In patients with HFEM, treatment with galcanezumab (120 mg and 240 mg) significantly reduced migraine headache days/month, maintained remission status at subsequent months until the end of the study, and improved patients' quality of life versus placebo.
TRIAL REGISTRATION
ClinicalTrials.gov Identifier: EVOLVE-1, NCT02614183 ; EVOLVE-2, NCT02614196 .
背景
与低频偏头痛发作天数(EM:每月 4-7 偏头痛发作天数)相比,发作性偏头痛(EM)患者偏头痛发作天数较高(HFEM:每月 8-14 偏头痛发作天数),疾病负担更大,进展为慢性偏头痛(CM)的风险更高,且伴随急性治疗过度使用。在这项事后分析中,我们评估了加奈珠单抗治疗后,从 HFEM 转为 LFEM(每月 4-7 偏头痛发作天数)和极低频偏头痛发作天数(VLFEM:每月 0-3 偏头痛发作天数)的患者比例。
方法
EVOLVE-1 和 EVOLVE-2 是两项双盲、III 期临床试验,研究对象为 EM 患者。患者(18-65 岁)随机分为皮下每月注射安慰剂、加奈珠单抗 120mg(240mg 负荷剂量)或 240mg,治疗时间最长为 6 个月。对数据进行了汇总,并对从基线开始偏头痛发作天数每月的变化和从 HFEM 转为 LFEM 或 VLFEM 状态的患者进行了终点评估。还评估了 HFEM 状态变化对偏头痛发作天数/月、生活质量和残疾的影响。
结果
共有 66%(1773 例中的 1176 例)来自 EVOLVE 研究的患者基线时为 HFEM 状态,包括 1176 例患者(安慰剂:592 例,加奈珠单抗 120mg:294 例,加奈珠单抗 240mg:290 例)。在每个月,加奈珠单抗的两种剂量都导致更多的患者转为每月头痛发作天数为 0-7 天/月(VLFEM 或 LFEM 状态)。基线时从 HFEM 转为 VLFEM 状态的患者,在第 3 个月,加奈珠单抗组中相对较大比例的患者在第 4-6 个月仍保持 VLFEM 状态,而安慰剂组在第 4-5 个月保持 VLFEM 状态;在第 240mg 加奈珠单抗组中为第 4 个月和第 5 个月。在加奈珠单抗治疗的患者中,至少连续 3 个月转为 LFEM 或 VLFEM 状态直至研究结束的患者中,从 HFEM 转为 VLFEM 状态的患者偏头痛发作天数/月减少最多,日常生活功能(MSQ-RFR)和残疾(MIDAS)的临床意义改善最大。
结论
在 HFEM 患者中,加奈珠单抗(120mg 和 240mg)治疗可显著减少偏头痛发作天数/月,维持随后几个月的缓解状态,直至研究结束,并改善患者的生活质量,优于安慰剂。
临床试验注册
EVOLVE-1,NCT02614183;EVOLVE-2,NCT02614196。
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