Manchon Eric, Laplaud David, Vukusic Sandra, Labauge Pierre, Moreau Thibault, Kobelt Gisela, Grouin Jean-Marie, Lotz Marie, Pau David, Christine Lebrun Frenay
Centre Hospitalier de Gonesse, Service de Neurologie, Gonesse, France.
Nantes Université, Service de Neurologie, Centre Hospitalier Universitaire de Nantes, CIC INSERM 1413, Center for Research in Transplantation and Translational Immunology, INSERM UMR 1064, Nantes, France.
Mult Scler Relat Disord. 2022 Dec;68:104109. doi: 10.1016/j.msard.2022.104109. Epub 2022 Aug 13.
Ocrelizumab, a humanized anti-CD20 monoclonal antibody, has been approved in Europe for the treatment of adult patients with active relapsing multiple sclerosis (RMS) and primary progressive multiple sclerosis (PPMS), on the basis of previous phase III studies. However, limited data were available on ocrelizumab efficacy in RMS according to the Lublin definition of activity (clinical and/or imaging features) used in the current drug label. The PRO-MSACTIVE study was thus designed to provide additional data on ocrelizumab efficacy according to this definition, and also on safety and patient reported outcomes (PROs).
PRO-MSACTIVE is a national, multicenter, open-label, single-arm phase IV French study, conducted in patients with active RMS (relapsing-remitting multiple sclerosis, RRMS, or secondary progressive multiple sclerosis, SPMS). The primary endpoint, which was assessed at week (W) 48, was defined as the proportion of patients free of disease activity (defined by no relapses and no T1 gadolinium-enhancing nor new and/or enlarging T2 lesions using brain MRI). Disease activity, disability and PROs using 6 questionnaires for disease severity, quality of life, impact on work productivity, and treatment satisfaction were described at W24 and W48. Adverse events were described until W72.
Among the 422 analyzed patients (RRMS: 376, SPMS: 46), 63.3% (95% CI [58.5%; 67.9%]) were free of disease activity at W48 (RRMS: 62.2% [57.1%; 67.2%], SPMS: 71.7% [56.5%; 84.0%]). A total of 358 patients (84.8%; RRMS: 84.6%, SPMS: 87.0%) were relapse-free up to W48, and the overall adjusted annualized relapse rate was 0.14 (RRMS: 0.15, SPMS: 0.09). Overall, 67.8% of patients (RRMS: 66.8%, SPMS: 76.1%) had no evidence of MRI activity (no T1 gadolinium-enhancing lesions [83.4%] and no new/enlarging T2 lesions [75.1%]); 58.5% of patients (RRMS: 57.7%, SPMS: 65.2%) achieved No Evidence of Disease Activity (NEDA: no relapses, no confirmed disability progression, and no MRI activity) at W48. All PRO scores were stable between the first dose of ocrelizumab and W48 and better outcomes were seen for patients having an EDSS score ≥4. Overall, 89.3% of patients reported adverse events, 62.3% adverse events assessed as related to ocrelizumab, and 8.5% serious adverse events. No serious infusion-related reactions, opportunistic infections, progressive multifocal leukoencephalopathy, nor deaths were reported. No new safety signal was identified.
These data confirm the efficacy of ocrelizumab in a pragmatic setting and its favorable benefit-risk profile in patients with RMS. (ClinicalTrials.gov identifier: NCT03589105; EudraCT identifier: 2018-000780-91).
奥瑞珠单抗是一种人源化抗CD20单克隆抗体,基于之前的III期研究,已在欧洲获批用于治疗成年复发型多发性硬化(RMS)和原发性进展型多发性硬化(PPMS)患者。然而,根据当前药品标签中使用的卢布林活动定义(临床和/或影像学特征),关于奥瑞珠单抗在RMS中的疗效数据有限。因此,PRO-MSACTIVE研究旨在根据该定义提供关于奥瑞珠单抗疗效、安全性及患者报告结局(PRO)的更多数据。
PRO-MSACTIVE是一项法国全国性、多中心、开放标签、单臂IV期研究,纳入活动性RMS患者(复发缓解型多发性硬化,RRMS,或继发进展型多发性硬化,SPMS)。在第48周(W48)评估的主要终点定义为无疾病活动的患者比例(定义为无复发,且脑MRI未显示T1加权像钆增强或新的和/或扩大的T2病灶)。在W24和W48描述疾病活动、残疾情况以及使用6份问卷评估的疾病严重程度、生活质量、对工作生产力的影响和治疗满意度等PRO。记录至W72的不良事件。
在422例分析患者中(RRMS:376例,SPMS:46例),63.3%(95%CI[58.5%;67.9%])在W48时无疾病活动(RRMS:62.2%[57.1%;67.2%],SPMS:71.7%[56.5%;84.0%])。共有358例患者(84.8%;RRMS:84.6%,SPMS:87.0%)至W48时无复发,总体调整年化复发率为0.14(RRMS:0.15,SPMS:0.09)。总体而言,67.8%的患者(RRMS:66.8%,SPMS:76.1%)无MRI活动证据(无T1加权像钆增强病灶[83.4%]且无新的/扩大的T2病灶[75.1%]);58.5%的患者(RRMS:57.7%,SPMS:65.2%)在W48时达到无疾病活动证据(NEDA:无复发、无确认的残疾进展且无MRI活动)。所有PRO评分在首次给予奥瑞珠单抗至W48期间保持稳定,且扩展残疾状态量表(EDSS)评分≥4的患者结局更佳。总体而言,89.3%的患者报告了不良事件,62.3%的不良事件被评估为与奥瑞珠单抗相关,8.5%为严重不良事件。未报告严重的输液相关反应、机会性感染、进行性多灶性白质脑病或死亡。未发现新的安全信号。
这些数据证实了奥瑞珠单抗在实际应用中的疗效及其在RMS患者中良好的效益风险比。(ClinicalTrials.gov标识符:NCT03589105;EudraCT标识符:2018-000780-91)
