加巴喷丁治疗患者与安慰剂治疗患者的治疗结局:发作性丛集性头痛患者 3 期随机研究的事后分析。
Treatment Outcomes in Patients Treated With Galcanezumab vs Placebo: Post Hoc Analyses From a Phase 3 Randomized Study in Patients With Episodic Cluster Headache.
机构信息
California Medical Clinic for Headache, Santa Monica, CA, USA.
Eli Lilly and Company, Indianapolis, IN, USA.
出版信息
Headache. 2020 Nov;60(10):2254-2264. doi: 10.1111/head.14011. Epub 2020 Nov 11.
BACKGROUND
Cluster headache (CH) is a highly disabling primary headache disorder. To date, characterization of outcomes in the preventive treatment of episodic CH, including precise definitions of clinically meaningful attack frequency reduction and impact on acute treatment management, is lacking.
METHODS
This was a Phase 3, randomized, double-blind, placebo-controlled study in patients (men or women aged 18-65 years) diagnosed with episodic CH as defined by the International Classification of Headache Disorders-3 beta criteria. In this post hoc analysis, we evaluated the median time-to-first occurrence of ≥50, ≥75, or 100% reduction from baseline in CH attack frequency, and impact on acute medication use. An anchor-based assessment of clinically relevant attack frequency reduction using the Patient Global Impression of Improvement (PGI-I) scores at Week 4 was also assessed.
RESULTS
The median time-to-first occurrence of ≥50, ≥75, or 100% reduction from baseline in CH attacks was consistently shorter (9-10 days sooner) with galcanezumab vs placebo (median [95% confidence interval, 95% CI]: ≥50%, 5 days [4.0 to 7.0] vs 14 days [6.0 to 19.0]; ≥75%, 11 days [7.0 to 16.0] vs 21 days [13.0 to 26.0]; 100%, 22 days [16.0 to 37.0] vs 32 days [23.0 to 34.0]). Mean reduction from baseline in the overall frequency of weekly pooled acute medication use across Weeks 1-3 was significantly greater with galcanezumab vs placebo (11.0 vs 5.5; odds ratio, OR [95% CI]: 5.52 [1.02, 10.01]; P value = .017). Patients reporting "much better" on the PGI-I experienced a median weekly CH attack reduction of approximately 43% from baseline across Weeks 1-3. The overall odds of achieving an attack reduction threshold of 43% across Weeks 1-3 was significantly higher with galcanezumab vs placebo (Weeks 1-3: OR [95% CI], 2.60 [1.3 to 5.3]).
CONCLUSIONS
Faster median time-to-first occurrence of response rates, lower frequency of pooled acute medications use, and a greater proportion of patients achieving a response anchored by patient-reported improvement were observed for galcanezumab vs placebo.
背景
丛集性头痛(CH)是一种高度致残的原发性头痛疾病。迄今为止,在预防性治疗发作性 CH 中,包括对临床有意义的发作频率降低的精确定义以及对急性治疗管理的影响,尚缺乏描述。
方法
这是一项 3 期、随机、双盲、安慰剂对照研究,纳入了符合国际头痛疾病分类第 3 版β标准的发作性 CH 诊断的患者(年龄 18-65 岁的男性或女性)。在本事后分析中,我们评估了从基线开始 CH 发作频率降低≥50%、≥75%或 100%的中位数首次出现时间,以及对急性药物使用的影响。还评估了第 4 周时使用患者总体印象改善(PGI-I)评分的基于锚定的临床相关发作频率降低的评估。
结果
与安慰剂相比,加奈珠单抗治疗后首次出现≥50%、≥75%或 100%发作频率降低的中位数时间更短(提前 9-10 天)(≥50%,5 天[4.0 至 7.0] vs 14 天[6.0 至 19.0];≥75%,11 天[7.0 至 16.0] vs 21 天[13.0 至 26.0];100%,22 天[16.0 至 37.0] vs 32 天[23.0 至 34.0])。第 1-3 周每周汇总急性药物使用频率的基线平均降低幅度在加奈珠单抗治疗组显著大于安慰剂组(11.0 与 5.5;比值比[95%置信区间]:5.52[1.02,10.01];P 值=0.017)。在 PGI-I 上报告“好得多”的患者,在第 1-3 周内,每周 CH 发作的中位数基线降低幅度约为 43%。在第 1-3 周,与安慰剂相比,加奈珠单抗组达到 43%发作频率降低阈值的总体可能性显著更高(第 1-3 周:比值比[95%置信区间],2.60[1.3 至 5.3])。
结论
与安慰剂相比,加奈珠单抗治疗更快出现首次反应率中位数,更低的急性药物联合使用频率,以及更高比例的患者达到患者报告改善为锚定的反应。
Zotero 插件