Nash Peter, Behrens Frank, Orbai Ana-Maria, Rathmann Suchitrita S, Adams David H, Benichou Olivier, Deodhar Atul
Department of Medicine, University of Queensland, Brisbane, Queensland, Australia.
Center for Innovative Diagnostics and Therapy in Rheumatology/Immunology (CIRI), Goethe University Frankfurt and Fraunhofer IME Project Group Translational Medicine and Pharmacology TMP, Frankfurt, Germany.
RMD Open. 2018 Sep 7;4(2):e000692. doi: 10.1136/rmdopen-2018-000692. eCollection 2018.
To conduct subset analyses of SPIRIT-P2 (Standard Protocol Items: Recommendations for Interventional Trials, NCT02349295) to investigate the efficacy and safety of ixekizumab versus placebo in three subgroups of patients with active psoriatic arthritis (PsA) according to the concomitant conventional synthetic disease-modifying antirheumatic drug (cDMARD) received: any background cDMARDs (including methotrexate), background methotrexate only.
Patients were randomised to receive placebo, ixekizumab 80 mg every 4 weeks (IXEQ4W) or every 2 weeks (IXEQ2W). Efficacy and safety were assessed when patients were subdivided according to cDMARD use at baseline. Efficacy was evaluated versus placebo at week 24 by the American College of Rheumatology criteria (ACR20/50), achievement of minimal disease activity (MDA) state, DiseaseActivityIndex for PsA (DAPSA), 28-joint DiseaseActivityScore using C reactive protein (DAS28-CRP), HealthAssessmentQuestionnaire-Disability Index and the 36-item Short-Form health survey physical functioning domain.
Regardless of background cDMARD status, ACR20, ACR50 and MDA response rates were significantly higher than placebo with IXEQ4W or IXEQ2W treatment. Similarly, significant improvements were observed relative to placebo for DAS28-CRP and DAPSA across subgroups. Physical function also significantly improved relative to placebo with IXEQ4W treatment regardless of background cDMARD status and with IXEQ2W alone. Percentages of reported treatment emergent adverse events (AEs), serious AEs (including serious infections) and discontinuations due to AEs in each subgroup were comparable to the overall SPIRIT-P2 population.
Ixekizumab was efficacious in patients with active PsA and previous tumour necrosis factor inhibitor (TNFi)inadequate response or TNFi intolerance treated with ixekizumab alone or when added to cDMARDswith subgroup safety profiles that were consistent with that observed in the overall SPIRIT-P2 population.
对SPIRIT-P2(标准方案项目:干预性试验建议,NCT02349295)进行亚组分析,以研究在根据所接受的传统合成抗风湿药物(cDMARD)划分的三个活动性银屑病关节炎(PsA)患者亚组中,司库奇尤单抗对比安慰剂的疗效和安全性:任何背景cDMARD(包括甲氨蝶呤)、仅背景甲氨蝶呤。
患者被随机分为接受安慰剂、每4周一次80mg司库奇尤单抗(IXEQ4W)或每2周一次(IXEQ2W)。根据基线时cDMARD的使用情况对患者进行细分后评估疗效和安全性。在第24周时,依据美国风湿病学会标准(ACR20/50)、达到最小疾病活动(MDA)状态、银屑病关节炎疾病活动指数(DAPSA)、使用C反应蛋白的28关节疾病活动评分(DAS28-CRP)、健康评估问卷残疾指数以及36项简明健康调查身体功能领域,与安慰剂对比评估疗效。
无论背景cDMARD状态如何,使用IXEQ4W或IXEQ2W治疗时,ACR20、ACR50和MDA缓解率均显著高于安慰剂。同样,各亚组中DAS28-CRP和DAPSA相对于安慰剂均观察到显著改善。无论背景cDMARD状态如何,使用IXEQ4W治疗以及单独使用IXEQ2W时,身体功能相对于安慰剂也有显著改善。各亚组中报告的治疗中出现的不良事件(AE)、严重AE(包括严重感染)以及因AE导致停药的百分比与SPIRIT-P2总体人群相当。
对于活动性PsA且既往肿瘤坏死因子抑制剂(TNFi)反应不足或TNFi不耐受的患者,单独使用司库奇尤单抗或添加到cDMARD时,司库奇尤单抗有效,且亚组安全性特征与SPIRIT-P2总体人群中观察到的一致。
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