Rheumatology Department, Cochin Hospital, Paris Descartes University, Paris, France
Sanofi R&D, Bridgewater, New Jersey, USA.
Ann Rheum Dis. 2020 Dec;79(12):1600-1607. doi: 10.1136/annrheumdis-2020-218447. Epub 2020 Sep 22.
Recent advances in systemic sclerosis (SSc) show that it involves a T-helper type-2-oriented immune response with interleukin (IL)-4 and IL-13. Romilkimab is an engineered, humanised, bispecific immunoglobulin-G4 antibody that binds and neutralises IL-4/IL-13 making it ideal for exploration in fibrosis.
Patients aged ≥18 years diagnosed with diffuse cutaneous SSc (dcSSc), and with or without immunosuppressive background therapy, were randomised (1:1) to subcutaneous romilkimab 200 mg or placebo one time per week for 24 weeks in this double-blind, proof-of-concept, phase II study. The primary endpoint was change in modified Rodnan skin score (mRSS) from baseline to week 24.
Ninety-seven patients were randomised to romilkimab (n=48) or placebo (n=49) for 24 weeks. Least-squares mean (SE) change in mRSS was -4.76 (0.86) for romilkimab versus -2.45 (0.85) for placebo yielding a mean (SE) (90% CI) difference of -2.31 (1.21) (-4.32 to -0.31; p=0.0291, one-sided). Treatment-emergent AEs were balanced between placebo (n=41; 84%) and romilkimab (n=40; 80%). Most were mild-to-moderate and discontinuations were low (three overall). There were two deaths (one scleroderma renal crisis (romilkimab) and one cardiomyopathy (placebo)), neither were considered treatment related. Two patients in the placebo group had a cardiovascular treatment-emergent SAE (one cardiac failure, one cardiomyopathy), but there were no cardiac safety signals with romilkimab.
This study demonstrated significant effects on skin changes with romilkimab in early dcSSc that require confirmation with a longer and more comprehensive phase III study to determine clinical relevance.
NCT02921971.
最近系统性硬化症 (SSc) 的研究进展表明,它涉及到 Th2 型免疫反应,伴有白细胞介素 (IL)-4 和 IL-13。Romilkimab 是一种工程化的、人源化的双特异性免疫球蛋白 G4 抗体,可结合并中和 IL-4/IL-13,非常适合探索纤维化。
这项双盲、概念验证性、Ⅱ期研究共纳入了年龄≥18 岁、诊断为弥漫性皮肤型 SSc(dcSSc)且无论是否接受免疫抑制背景治疗的患者,按 1:1 比例随机分配接受皮下注射 Romilkimab 200mg 或安慰剂,每周 1 次,共 24 周。主要终点为从基线到 24 周时改良 Rodnan 皮肤评分 (mRSS) 的变化。
97 例患者被随机分为 Romilkimab 组(n=48)或安慰剂组(n=49),接受 24 周治疗。Romilkimab 组的 mRSS 最小二乘均数(SE)变化为-4.76(0.86),安慰剂组为-2.45(0.85),两组间的平均(SE)(90%CI)差值为-2.31(1.21)(-4.32 至 -0.31;p=0.0291,单侧)。Romilkimab 组(n=40;80%)和安慰剂组(n=41;84%)的治疗中出现的不良事件发生率相近。大多数为轻中度,停药率较低(共 3 例)。共有 2 例死亡(1 例为硬皮病肾危象(Romilkimab),1 例为心肌病(安慰剂)),均与治疗无关。安慰剂组有 2 例心血管治疗中出现的不良事件(1 例心力衰竭,1 例心肌病),但 Romilkimab 组没有心脏安全性信号。
这项研究表明 Romilkimab 对早期 dcSSc 的皮肤变化有显著影响,需要进行更长时间和更全面的Ⅲ期研究来确定其临床相关性。
NCT02921971。
