Institute of Rheumatology and Department of Rheumatology, 1st Faculty of Medicine, Charles University, Prague, Czech Republic.
Altoona Center for Clinical Research, Duncansville, PA, USA.
Arthritis Res Ther. 2017 Dec 22;19(1):285. doi: 10.1186/s13075-017-1490-y.
Secukinumab, an anti-interleukin-17A monoclonal antibody, improved the signs and symptoms of ankylosing spondylitis (AS) in two phase 3 studies (MEASURE 1 and MEASURE 2). Here, we present 52-week results from the MEASURE 3 study assessing the efficacy and safety of secukinumab 300 and 150 mg subcutaneous maintenance dosing, following an intravenous loading regimen.
A total of 226 patients were randomized to intravenous secukinumab 10 mg/kg (baseline, weeks 2 and 4) followed by subcutaneous secukinumab 300 mg (IV-300 mg) or 150 mg (IV-150 mg) every 4 weeks, or matched placebo. Patients in the placebo group were re-randomized to subcutaneous secukinumab at a dose of 300 or 150 mg at week 16. The primary endpoint was the Assessment of SpondyloArthritis international Society criteria for 20% improvement (ASAS20) response rate at week 16 in the IV-300 mg or IV-150 mg versus placebo. Other endpoints assessed through week 52 included improvements in ASAS40, ASAS 5/6, Bath Ankylosing Spondylitis Disease Activity Index, and ASAS partial remission responses, as well as the change from baseline in high-sensitivity C-reactive protein levels. Statistical analyses followed a predefined hierarchical hypothesis testing strategy to adjust for multiplicity of testing, with non-responder imputation used for binary variables and mixed-model repeated measures for continuous variables.
The primary efficacy endpoint was met; the ASAS20 response rate was significantly greater at week 16 in the IV-300 mg (60.5%; P < 0.01) and IV-150 mg (58.1%; P < 0.05) groups versus placebo (36.8%). All secondary endpoints were met at week 16, except ASAS partial remission in the IV-150 mg group. Improvements achieved with secukinumab in all clinical endpoints at week 16 were also sustained at week 52. Infections, including candidiasis, were more common with secukinumab than with placebo during the placebo-controlled period. During the entire treatment period, pooled incidence rates of Candida infections and grade 3-4 neutropenia were 1.8% for both of these adverse events in secukinumab-treated patients.
Secukinumab (300 mg and 150 mg dose groups) provided rapid, significant and sustained improvement through 52 weeks in the signs and symptoms of patients with AS. The safety profile was consistent with previous reports, with no new or unexpected findings.
ClinicalTrials.gov, NCT02008916 . Registered on 8 December 2013. EUDRACT 2013-001090-24. Registered on 24 October 2013). The study was not retrospectively registered.
司库奇尤单抗是一种抗白细胞介素-17A 的单克隆抗体,在两项 3 期研究(MEASURE 1 和 MEASURE 2)中改善了强直性脊柱炎(AS)的体征和症状。在这里,我们报告了 MEASURE 3 研究的 52 周结果,该研究评估了皮下维持剂量为 300mg 和 150mg 的司库奇尤单抗在静脉注射负荷方案后的疗效和安全性。
共有 226 名患者被随机分配至静脉注射司库奇尤单抗 10mg/kg(基线,第 2 周和第 4 周),随后每 4 周皮下注射司库奇尤单抗 300mg(IV-300mg)或 150mg(IV-150mg),或匹配的安慰剂。安慰剂组的患者在第 16 周时重新随机分配至皮下司库奇尤单抗 300mg 或 150mg 剂量。主要终点是 IV-300mg 或 IV-150mg 组与安慰剂组在第 16 周时达到强直性脊柱炎国际学会 20%改善标准(ASAS20)应答率。其他通过第 52 周评估的终点包括 ASAS40、ASAS5/6、巴斯强直性脊柱炎疾病活动指数和 ASAS 部分缓解反应的改善,以及从基线到第 52 周的高敏 C 反应蛋白水平的变化。统计分析遵循预先确定的分层假设检验策略,以调整检验的多重性,使用非应答者插补用于二项变量,混合模型重复测量用于连续变量。
主要疗效终点得到满足;在第 16 周,IV-300mg(60.5%;P<0.01)和 IV-150mg(58.1%;P<0.05)组与安慰剂(36.8%)相比,ASAS20 应答率显著更高。所有次要终点均在第 16 周达到,除了 IV-150mg 组的 ASAS 部分缓解。在第 16 周时,司库奇尤单抗在所有临床终点的改善在第 52 周时也得到了维持。在安慰剂对照期间,司库奇尤单抗比安慰剂更常见感染,包括念珠菌感染。在整个治疗期间,司库奇尤单抗治疗患者的念珠菌感染和 3-4 级中性粒细胞减少症的累积发生率均为 1.8%。
司库奇尤单抗(300mg 和 150mg 剂量组)通过 52 周的治疗显著改善了 AS 患者的体征和症状,且改善效果迅速且持久。安全性特征与之前的报告一致,没有新的或意外的发现。
ClinicalTrials.gov,NCT02008916。于 2013 年 12 月 8 日注册。EUDRACT 2013-001090-24。于 2013 年 10 月 24 日注册。该研究未进行回顾性注册。
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