阿普米拉斯、依那西普和安慰剂治疗中重度斑块状银屑病患者的疗效和安全性:一项IIIb期随机安慰剂对照试验(LIBERATE)的52周结果
The efficacy and safety of apremilast, etanercept and placebo in patients with moderate-to-severe plaque psoriasis: 52-week results from a phase IIIb, randomized, placebo-controlled trial (LIBERATE).
作者信息
Reich K, Gooderham M, Green L, Bewley A, Zhang Z, Khanskaya I, Day R M, Goncalves J, Shah K, Piguet V, Soung J
机构信息
SCIderm Research Institute and Dermatologikum Hamburg, Hamburg, Germany.
SKiN Centre for Dermatology and Probity Medical Research, Peterborough, ON, Canada.
出版信息
J Eur Acad Dermatol Venereol. 2017 Mar;31(3):507-517. doi: 10.1111/jdv.14015. Epub 2016 Dec 19.
BACKGROUND
Apremilast, an oral, small-molecule phosphodiesterase 4 inhibitor, has demonstrated efficacy in patients with moderate-to-severe psoriasis.
OBJECTIVE
Evaluate efficacy and safety of apremilast vs. placebo in biologic-naive patients with moderate-to-severe plaque psoriasis and safety of switching from etanercept to apremilast in a phase IIIb, randomized, double-blind, placebo-controlled study (NCT01690299).
METHODS
Two hundred and fifty patients were randomized to placebo (n = 84), apremilast 30 mg BID (n = 83) or etanercept 50 mg QW (n = 83) through Week 16; thereafter, all patients continued or switched to apremilast through Week 104. The primary efficacy endpoint was achievement of PASI-75 at Week 16 with apremilast vs. placebo. Secondary endpoints included achievement of PASI-75 at Week 16 with etanercept vs. placebo and improvements in other clinical endpoints vs. placebo at Week 16. Outcomes were assessed through Week 52. This study was not designed for apremilast vs. etanercept comparisons.
RESULTS
At Week 16, PASI-75 achievement was greater with apremilast (39.8%) vs. placebo (11.9%; P < 0.0001); 48.2% of patients achieved PASI-75 with etanercept (P < 0.0001 vs. placebo). PASI-75 response was maintained in 47.3% (apremilast/apremilast), 49.4% (etanercept/apremilast) and 47.9% (placebo/apremilast) of patients at Week 52. Most common adverse events (≥5%) with apremilast, including nausea, diarrhoea, upper respiratory tract infection, nasopharyngitis, tension headache and headache, were mild or moderate in severity; diarrhoea and nausea generally resolved in the first month. No new safety or tolerability issues were observed through Week 52 with apremilast.
CONCLUSION
Apremilast demonstrated significant efficacy vs. placebo at Week 16 in biologic-naive patients with psoriasis, which was sustained over 52 weeks, and demonstrated safety consistent with the known safety profile of apremilast. Switching from etanercept to apremilast did not result in any new or clinically significant safety findings, and efficacy was maintained with apremilast through Week 52.
背景
阿普米司特是一种口服小分子磷酸二酯酶4抑制剂,已在中重度银屑病患者中显示出疗效。
目的
在一项IIIb期随机、双盲、安慰剂对照研究(NCT01690299)中,评估阿普米司特对比安慰剂在初治中重度斑块状银屑病患者中的疗效和安全性,以及从依那西普转换为阿普米司特的安全性。
方法
250例患者随机分为安慰剂组(n = 84)、阿普米司特30 mg每日两次组(n = 83)或依那西普50 mg每周一次组(n = 83),治疗16周;此后,所有患者继续使用或转换为阿普米司特治疗至104周。主要疗效终点是第16周时阿普米司特对比安慰剂达到银屑病面积和严重程度指数改善75%(PASI-75)。次要终点包括第16周时依那西普对比安慰剂达到PASI-75,以及第16周时其他临床终点对比安慰剂的改善情况。疗效评估至第52周。本研究未设计用于阿普米司特对比依那西普的比较。
结果
在第16周时,阿普米司特组达到PASI-75的比例(39.8%)高于安慰剂组(11.9%;P < 0.0001);依那西普组48.2%的患者达到PASI-75(对比安慰剂,P < 0.0001)。在第52周时,47.3%(阿普米司特/阿普米司特组)、49.4%(依那西普/阿普米司特组)和47.9%(安慰剂/阿普米司特组)的患者维持了PASI-75反应。阿普米司特最常见的不良事件(≥5%)包括恶心、腹泻、上呼吸道感染、鼻咽炎、紧张性头痛和头痛,严重程度为轻度或中度;腹泻和恶心通常在第一个月内缓解。至第52周,未观察到阿普米司特新的安全性或耐受性问题。
结论
在初治银屑病患者中,阿普米司特在第16周时对比安慰剂显示出显著疗效,并在52周内持续存在,且安全性与阿普米司特已知的安全性特征一致。从依那西普转换为阿普米司特未导致任何新的或具有临床意义的安全性发现,且至第52周阿普米司特维持了疗效。
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