Md Yusof Md Yuzaiful, Shaw Daniel, El-Sherbiny Yasser M, Dunn Emma, Rawstron Andy C, Emery Paul, Vital Edward M
Leeds Institute of Rheumatic and Musculoskeletal Medicine, University of Leeds, Chapel Allerton Hospital, Chapeltown Road, Leeds, UK.
NIHR Leeds Biomedical Research Centre, Leeds Teaching Hospitals NHS Trust, Leeds, UK.
Ann Rheum Dis. 2017 Nov;76(11):1829-1836. doi: 10.1136/annrheumdis-2017-211191. Epub 2017 Jul 6.
To assess factors associated with primary and secondary non-response to rituximab in systemic lupus erythematosus (SLE) and evaluate management of secondary non-depletion non-response (2NDNR).
125 patients with SLE treated with rituximab over 12 years were studied prospectively. A major clinical response was defined as improvement of all active British Isles Lupus Assessment Group (BILAG)-2004 domains to grade C/better and no A/B flare. Partial responders were defined by one persistent BILAG B. B-cell subsets were measured using highly sensitive flow cytometry. Patients with 2NDNR, defined by infusion reaction and defective depletion, were treated with ocrelizumab or ofatumumab.
117 patients had evaluable data. In cycle 1 (C1), 96/117 (82%) achieved BILAG response (major=50%, partial=32%). In multivariable analysis, younger age (OR 0.97, 95% CI 0.94 to 1.00) and B-cell depletion at 6 weeks (OR 3.22, 95% CI 1.24 to 8.33) increased the odds of major response. Complete depletion was predicted by normal complement and lower pre-rituximab plasmablasts and was not associated with increased serious infection post-rituximab. Seventy-seven (with data on 72) C1 responders were retreated on clinical relapse. Of these, 61/72 (85%) responded in cycle 2 (C2). Of the 11 C2 non-responders, nine met 2NDNR criteria (incidence=12%) and tested positive for anti-rituximab antibodies. Lack of concomitant immunosuppressant and higher pre-rituximab plasmablasts predicted 2NDNR. Five were switched to ocrelizumab/ofatumumab, and all depleted and responded.
Treatment with anti-CD20 agents can be guided by B-cell monitoring and should aim to achieve complete depletion. 2NDNR is associated with anti-rituximab antibodies, and switching to humanised agents restores depletion and response. In SLE, alternative anti-CD20 antibodies may be more consistently effective.
评估系统性红斑狼疮(SLE)患者对利妥昔单抗原发性和继发性无反应的相关因素,并评估继发性非耗竭性无反应(2NDNR)的管理。
对125例在12年期间接受利妥昔单抗治疗的SLE患者进行前瞻性研究。主要临床反应定义为所有活跃的不列颠群岛狼疮评估组(BILAG)-2004领域改善至C级或更好且无A/B级复发。部分反应者定义为存在一个持续的BILAG B级。使用高灵敏度流式细胞术检测B细胞亚群。由输注反应和耗竭缺陷定义的2NDNR患者接受奥瑞珠单抗或奥法妥单抗治疗。
117例患者有可评估数据。在第1周期(C1),96/117(82%)达到BILAG反应(主要反应=50%,部分反应=32%)。多变量分析显示,年龄较小(比值比[OR]0.97,95%置信区间[CI]0.94至1.00)和6周时B细胞耗竭(OR 3.22,95%CI 1.24至8.33)增加了主要反应的几率。正常补体、利妥昔单抗治疗前较低的浆母细胞可预测完全耗竭,且与利妥昔单抗治疗后严重感染增加无关。77例(72例有数据)C1反应者在临床复发时再次接受治疗。其中,61/72(85%)在第2周期(C2)有反应。11例C2无反应者中,9例符合2NDNR标准(发生率=12%)且抗利妥昔单抗抗体检测呈阳性。未同时使用免疫抑制剂和利妥昔单抗治疗前较高的浆母细胞可预测2NDNR。5例改用奥瑞珠单抗/奥法妥单抗,均实现耗竭且有反应。
抗CD20药物治疗可通过B细胞监测来指导,且应旨在实现完全耗竭。2NDNR与抗利妥昔单抗抗体相关,并改用人源化药物可恢复耗竭及反应情况。在SLE中,替代抗CD20抗体可能更具持续有效性。
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