ALLEGRO脱发症2b/3期和3期长期临床研究显示,利特西替尼的长期疗效可达第24个月

Melissa Piliang, J. Soung, B. King, Jerry Shapiro, Lidia Rudnicka, Paul Farrant, Nina Magnolo, Bianca Piraccini, Xin Luo, Deborah Woodworth, G. Schaefer, A. Lejeune, Robert Wolk
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Data are reported for patients who received: 1) daily ritlecitinib 50-mg with a 4-week 200-mg daily loading dose (“200/50-mg”); 2) daily ritlecitinib 50-mg with no loading dose (“50-mg”). Outcomes include the proportions of patients with response (based on Severity of Alopecia Tool [SALT] score ≤20, SALT ≤10, and Patients’ Global Impression of Change [PGI-C] score of “moderately improved” or “greatly improved”) through Month 24, and the proportions of patients sustaining SALT ≤20 response from Month 12 through Month 24. Observed and imputed (modified last observation carried forward [mLOCF]) data, to account for missing values, are reported (data cutoff: December 9, 2022). \nResults: The 200/50-mg and 50-mg groups included 194 and 191 patients; 127 (65.5%) and 111 (58.1%) were ongoing at the data cutoff. 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引用次数: 1

摘要

简介在ALLEGRO-2b/3(NCT03732807)研究中,利特西替尼对年龄≥12岁的斑秃(AA)患者的疗效和安全性均达到了第48周。ALLEGRO-LT(NCT04006457)是一项正在进行的3期开放标签研究,旨在调查利特西替尼治疗AA的长期安全性和疗效。我们报告了ALLEGRO-2b/3和ALLEGRO-LT截至第24个月的最新中期疗效结果。研究方法纳入年龄≥12岁、头皮脱发≥50%且从ALLEGRO-2b/3转入ALLEGRO-LT的AA患者。报告了接受以下治疗的患者的数据1)每日服用瑞替西替尼 50 毫克,同时服用为期 4 周的每日 200 毫克负荷剂量("200/50-毫克");2)每日服用瑞替西替尼 50 毫克,同时不服用负荷剂量("50-毫克")。研究结果包括:到第24个月出现应答的患者比例(基于脱发严重程度工具[SALT]评分≤20分、SALT≤10分和患者总体变化印象[PGI-C]评分 "中度改善 "或 "大幅改善"),以及从第12个月到第24个月保持SALT≤20分应答的患者比例。报告了观察数据和估算数据(修改后的最后观察结转数据 [mLOCF]),以考虑缺失值(数据截止日期:2022 年 12 月 9 日)。结果:200/50毫克组和50毫克组分别有194名和191名患者;数据截止时,127名(65.5%)和111名(58.1%)患者仍在接受治疗。200/50毫克组和50毫克组的SALT≤20应答率从第12个月(45.9%和45.1% [观察值];41.8%和40.3% [mLOCF])上升到第24个月(63.1%和60.8% [观察值];50.8%和46.1% [mLOCF])。在第 12 个月至第 24 个月期间,200/50 毫克组(39.4% 至 51.1% [观察值];35.6% 至 40.9% [毫升有机碳])和 50 毫克组(34.2% 至 50.8% [观察值];30.9% 至 37.7% [毫升有机碳])的 SALT ≤10 反应率有所上升。在第 12 个月 SALT ≤20 的应答者中,92.8%(200/50 毫克)和 79.7%(50 毫克)(观察组)在第 24 个月保持了这种应答。PGI-C 反应率从第 12 个月开始保持不变(200/50 毫克:69.4% [观察],50 毫克:79.7% [观察]):69.4%[观察],65.3%[mLOCF];50 毫克:61.6%[观察],57.7%[mLOCF])至第 24 个月(200/50 毫克:76.4%[观察],57.7%[mLOCF]):76.4%[观察],65.4%[mLOCF];50 毫克:70.0%[观察],57.7%[mLOCF70.0%[观察],56.6%[mLOCF])。结论利特西替尼50毫克(无论是否服用200毫克负荷剂量)在第24个月时显示出了有临床意义的、持续的临床医生和患者报告疗效,支持在年龄≥12岁的重症AA患者中长期使用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Long-Term Efficacy of Ritlecitinib up to Month 24 From the ALLEGRO Phase 2b/3 and Long-Term Phase 3 Clinical Studies in Alopecia Areata
Introduction: Ritlecitinib demonstrated efficacy and safety to Week 48 in patients aged ≥12 years with alopecia areata (AA) in ALLEGRO-2b/3 (NCT03732807). ALLEGRO-LT (NCT04006457) is an ongoing, phase 3, open-label study investigating the long-term safety and efficacy of ritlecitinib in AA. We report updated interim efficacy results of ritlecitinib up to Month 24 from ALLEGRO-2b/3 and ALLEGRO-LT. Methods: Patients aged ≥12 years with AA and ≥50% scalp hair loss who rolled-over to ALLEGRO-LT from ALLEGRO-2b/3 were included. Data are reported for patients who received: 1) daily ritlecitinib 50-mg with a 4-week 200-mg daily loading dose (“200/50-mg”); 2) daily ritlecitinib 50-mg with no loading dose (“50-mg”). Outcomes include the proportions of patients with response (based on Severity of Alopecia Tool [SALT] score ≤20, SALT ≤10, and Patients’ Global Impression of Change [PGI-C] score of “moderately improved” or “greatly improved”) through Month 24, and the proportions of patients sustaining SALT ≤20 response from Month 12 through Month 24. Observed and imputed (modified last observation carried forward [mLOCF]) data, to account for missing values, are reported (data cutoff: December 9, 2022). Results: The 200/50-mg and 50-mg groups included 194 and 191 patients; 127 (65.5%) and 111 (58.1%) were ongoing at the data cutoff. SALT ≤20 response rates in the 200/50-mg and 50-mg groups increased from Month 12 (45.9% and 45.1% [observed]; 41.8% and 40.3% [mLOCF]) to Month 24 (63.1% and 60.8% [observed]; 50.8% and 46.1% [mLOCF]). SALT ≤10 response rates increased between Months 12 and 24 for the 200/50-mg group (39.4% to 51.1% [observed]; 35.6% to 40.9% [mLOCF]) and 50-mg group (34.2% to 50.8% [observed]; 30.9% to 37.7% [mLOCF]). Of SALT ≤20 responders at Month 12, 92.8% (200/50-mg) and 79.7% (50-mg) (observed) sustained this response through Month 24. PGI-C response rates were maintained from Month 12 (200/50-mg: 69.4% [observed], 65.3% [mLOCF]; 50-mg: 61.6% [observed], 57.7% [mLOCF]) to Month 24 (200/50-mg: 76.4% [observed], 65.4% [mLOCF]; 50-mg: 70.0% [observed], 56.6% [mLOCF]). Conclusion: Ritlecitinib 50-mg (with or without a 200-mg loading dose) demonstrated clinically meaningful and sustained clinician- and patient-reported efficacy through Month 24, which supports its long-term use in patients aged ≥12 years with severe AA.
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