多发性硬化症患者之前接受芬戈莫德治疗对利妥昔单抗/奥曲昔单抗早期和晚期反应的影响

IF 7.8 1区 医学 Q1 CLINICAL NEUROLOGY
Lisa Graille-Avy, Clemence Boutiere, Camille Rigollet, Marine Perriguey, Audrey Rico, Sarah Demortiere, Pierre Durozard, Frederic Hilezian, Frederic Vely, Pierre Bertault-Peres, Jean Pelletier, Adil Maarouf, Bertrand Audoin
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引用次数: 0

摘要

背景和目的:现实生活中的研究表明,多发性硬化症(MS)患者在改用利妥昔单抗(RTX)或奥克利珠单抗(OCR)后出现疾病活动的风险可能会因之前的疾病改变疗法(DMT)而不同,芬戈莫德(FING)的风险更高:我们对结构化前瞻性数据收集进行了回顾性分析,其中包括马赛多发性硬化症中心开具RTX/OCR处方的所有连续复发性多发性硬化症患者。对临床和磁共振成像结果采用了Cox比例危险模型:我们共纳入了 321 名患者,其中位数(四分位数间距 [IQR])随访时间为 RTX/OCR 开始后的 3.5 年(1.5-5 年)。首次输注RTX/OCR时,患者的平均(标清)年龄为37(10)岁,中位(IQR)病程为8年(3-15):68 名患者在 RTX/OCR 之前未接受过治疗,108 名患者从 FING 改用其他疗法,47 名患者从低效疗法改用其他疗法,98 名患者从纳他珠单抗改用其他疗法。在统计分析中,"FING "组根据该组冲洗期的中位值(27 天)分为 "短FING "组和 "长FING "组。根据考克斯比例危险度分析,仅 "长FING "组患者在接受RTX/OCR治疗的前6个月内复发的风险高于既往未接受过DMT治疗的患者(危险度比[HR]:8.78;95% CI 1.72-44.86;P < 0.01)。既往 DMT 和 FING 冲洗期对 6 个月时的 B 细胞水平没有影响。在RTX/OCR的前6个月之后,年龄(P = 0.01)、男性会增加新发T2病变的风险(HR:2.26;95% CI 1.08-4.74;P = 0.03),EDSS≥2会增加残疾累积的风险(HR:3.01;95% CI 1.34-6.74;P < 0.01)。在开始使用 RTX/OCR 6 个月后,之前的 DMT 对其疗效没有影响:讨论:对于从FING转为RTX/OCR的患者,与使用其他DMT或未使用过DMT的患者相比,只有当冲洗期超过26天时,在治疗的前6个月内疾病再激活的风险才会增加。在治疗的头 6 个月之后,FING 或之前的其他 DMT 均不会降低 RTX/OCR 的疗效。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Effect of Prior Treatment With Fingolimod on Early and Late Response to Rituximab/Ocrelizumab in Patients With Multiple Sclerosis.

Background and objectives: Real-life studies noted that the risk of disease activity in multiple sclerosis (MS) after switching to rituximab (RTX) or ocrelizumab (OCR) may be unequal depending on prior disease-modifying therapy (DMT), with a higher risk associated with fingolimod (FING).

Methods: We performed a retrospective analysis of a structured prospective data collection including all consecutive patients with relapsing MS who were prescribed RTX/OCR in the MS center of Marseille. Cox proportional hazards models were applied to clinical and MRI outcomes.

Results: We included 321 patients with a median (interquartile range [IQR]) follow-up of 3.5 years (1.5-5) after RTX/OCR initiation. At the first RTX/OCR infusion, the mean (SD) age of patients was 37 (10) years, and the median (IQR) disease duration was 8 years (3-15): 68 patients did not receive treatment before RTX/OCR and 108 switched from FING, 47 from low efficacy therapy, and 98 from natalizumab. For statistical analysis, the group "FING" was divided into "short-FING" and "long-FING" groups according to the median value of the group's washout period (27 days). On Cox proportional hazards analysis, for only the "long-FING" group, the risk of relapse within the first 6 months of RTX/OCR was increased as compared with patients without previous DMT (hazard ratio [HR]: 8.78; 95% CI 1.72-44.86; p < 0.01). Previous DMT and washout period duration of FING had no effect on B-cell levels at 6 months. Beyond the first 6 months of RTX/OCR, age <40 years was associated with increased risk of relapse (HR: 3.93; 95% CI 1.30-11.89; p = 0.01), male sex with increased risk of new T2 lesions (HR: 2.26; 95% CI 1.08-4.74; p = 0.03), and EDSS ≥2 with increased risk of disability accumulation (HR: 3.01; 95% CI 1.34-6.74; p < 0.01). Previous DMT had no effect on the effectiveness of RTX/OCR beyond 6 months after initiation.

Discussion: For patients switching from FING to RTX/OCR, the risk of disease reactivation within the first 6 months of treatment was increased as compared with patients with other DMT or no previous DMT only when the washout period exceeded 26 days. Neither FING nor other previous DMT reduced the effectiveness of RTX/OCR beyond the first 6 months of treatment.

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来源期刊
CiteScore
15.60
自引率
2.30%
发文量
219
审稿时长
8 weeks
期刊介绍: Neurology Neuroimmunology & Neuroinflammation is an official journal of the American Academy of Neurology. Neurology: Neuroimmunology & Neuroinflammation will be the premier peer-reviewed journal in neuroimmunology and neuroinflammation. This journal publishes rigorously peer-reviewed open-access reports of original research and in-depth reviews of topics in neuroimmunology & neuroinflammation, affecting the full range of neurologic diseases including (but not limited to) Alzheimer's disease, Parkinson's disease, ALS, tauopathy, and stroke; multiple sclerosis and NMO; inflammatory peripheral nerve and muscle disease, Guillain-Barré and myasthenia gravis; nervous system infection; paraneoplastic syndromes, noninfectious encephalitides and other antibody-mediated disorders; and psychiatric and neurodevelopmental disorders. Clinical trials, instructive case reports, and small case series will also be featured.
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