用Janus激酶抑制剂托法替布的软膏制剂治疗斑块状银屑病:一项2b期随机临床试验。
Treatment of plaque psoriasis with an ointment formulation of the Janus kinase inhibitor, tofacitinib: a Phase 2b randomized clinical trial.
作者信息
Papp Kim A, Bissonnette Robert, Gooderham Melinda, Feldman Steven R, Iversen Lars, Soung Jennifer, Draelos Zoe, Mamolo Carla, Purohit Vivek, Wang Cunshan, Ports William C
机构信息
K Papp Clinical Research and Probity Medical Research Inc, Waterloo, ON, Canada.
Innovaderm Research, Montreal, QC, Canada.
出版信息
BMC Dermatol. 2016 Oct 3;16(1):15. doi: 10.1186/s12895-016-0051-4.
BACKGROUND
Most psoriasis patients have mild to moderate disease, commonly treated topically. Current topical agents have limited efficacy and undesirable side effects associated with long-term use. Tofacitinib is a small molecule Janus kinase inhibitor investigated for the topical treatment of psoriasis.
METHODS
This was a 12-week, randomized, double-blind, parallel-group, vehicle-controlled Phase 2b study of tofacitinib ointment (2 % and 1 %) applied once (QD) or twice (BID) daily in adults with mild to moderate plaque psoriasis. Primary endpoint: proportion of patients with Calculated Physician's Global Assessment (PGA-C) clear or almost clear and ≥2 grade improvement from baseline at Weeks 8 and 12. Secondary endpoints: proportion of patients with PGA-C clear or almost clear; proportion achieving Psoriasis Area and Severity Index 75 (PASI75) response; percent change from baseline in PASI and body surface area; change from baseline in Itch Severity Item (ISI). Adverse events (AEs) were monitored and clinical laboratory parameters measured.
RESULTS
Overall, 435 patients were randomized and 430 patients received treatment. The proportion of patients with PGA-C clear or almost clear and ≥2 grade improvement from baseline at Week 8 was 18.6 % for 2 % tofacitinib QD (80 % confidence interval [CI] for difference from vehicle: 3.8, 18.2 %) and 22.5 % for 2 % tofacitinib BID (80 % CI: 3.1, 18.5 %); this was significantly higher vs vehicle for both dosage regimens. No significant difference vs vehicle was seen at Week 12. Significantly more patients achieved PGA-C clear or almost clear with 2 % tofacitinib QD and BID and 1 % tofacitinib QD (not BID) at Week 8, and with 2 % tofacitinib BID at Week 12. Pruritus was significantly reduced vs vehicle with 2 % and 1 % tofacitinib BID (starting Day 2), and 2 % tofacitinib QD (starting Day 3). Overall, 44.2 % of patients experienced AEs, 8.1 % experienced application site AEs, and 2.3 % experienced serious AEs. The highest incidence of AEs (including application site AEs) was in the vehicle QD group.
CONCLUSIONS
In adults with mild to moderate plaque psoriasis, 2 % tofacitinib ointment QD and BID showed greater efficacy than vehicle at Week 8, but not Week 12, with an acceptable safety and local tolerability profile.
TRIAL REGISTRATION
NCT01831466 registered March 28, 2013.
背景
大多数银屑病患者病情为轻度至中度,通常采用局部治疗。目前的局部用药疗效有限,且长期使用会产生不良副作用。托法替布是一种小分子Janus激酶抑制剂,正在研究用于银屑病的局部治疗。
方法
这是一项为期12周的随机、双盲、平行组、赋形剂对照的2b期研究,在患有轻度至中度斑块状银屑病的成人中,每日一次(QD)或两次(BID)应用2%和1%的托法替布软膏。主要终点:在第8周和第12周时,计算得出的医生整体评估(PGA-C)为清除或几乎清除且较基线改善≥2级的患者比例。次要终点:PGA-C为清除或几乎清除的患者比例;达到银屑病面积和严重程度指数改善75%(PASI75)反应的患者比例;PASI和体表面积较基线的变化百分比;瘙痒严重程度项目(ISI)较基线的变化。监测不良事件(AE)并测量临床实验室参数。
结果
总体而言,435例患者被随机分组,430例患者接受治疗。2%托法替布QD组在第8周时PGA-C为清除或几乎清除且较基线改善≥2级的患者比例为18.6%(与赋形剂相比差异的80%置信区间[CI]:3.8,18.2%),2%托法替布BID组为22.5%(80%CI:3.1,18.5%);两种给药方案与赋形剂相比均显著更高。在第12周时与赋形剂相比无显著差异。在第8周时,2%托法替布QD和BID组以及1%托法替布QD组(而非BID组)达到PGA-C清除或几乎清除的患者显著更多,在第12周时2%托法替布BID组达到该标准的患者显著更多。与赋形剂相比,2%和1%托法替布BID组(从第2天开始)以及2%托法替布QD组(从第3天开始)的瘙痒显著减轻。总体而言,44.2%的患者发生AE,8.1%的患者发生用药部位AE,2.3%的患者发生严重AE。AE(包括用药部位AE)发生率最高的是赋形剂QD组。
结论
在患有轻度至中度斑块状银屑病的成人中,2%托法替布软膏QD和BID在第8周时显示出比赋形剂更高的疗效,但在第12周时未显示出此优势,且安全性和局部耐受性可接受。
试验注册
NCT01831466,于20l3年3月28日注册。
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