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[利妥昔单抗在抗中性粒细胞胞浆抗体相关性系统性血管炎治疗中的作用]

[The role of rituximab in the treatment of ANCA-associated systemic vasculitis].

作者信息

Roccatello Dario, Vangelista Alba, Pani Antonello

机构信息

Centro di Ricerche di Immunopatologia e Documentazione su Malattie Rare, Ospedale G. Bosco e Universita di Torino, Torino, Italy.

出版信息

G Ital Nefrol. 2011 Sep-Oct;28(5):474-88.

PMID:22028261
Abstract

A considerable minority of patients with ANCA-associated small-vessel vasculitis are refractory to conventional therapy or experience dose-limiting side effects. Novel therapeutic approaches include rituximab, a genetically engineered chimeric murine-human monoclonal antibody that binds to CD20, which is expressed on human B cells. It was approved in 1997 for the treatment of CD20-positive B-cell non-Hodgkin lymphoma and in 2006 for the treatment of rheumatoid arthritis. The multiple mechanisms proposed for rituximab-mediated B-cell depletion are discussed in this paper. Cumulative data from several open studies on the treatment of microscopic ANCA-associated polyangiitis suggest that in the vast majority of cases rituximab has a beneficial effect. Two randomized controlled trials confirmed these promising results, suggesting that rituximab might be considered as an option for first-line therapy of induction of remission of ANCA-associated vasculitis, and providing an additional tool for treating patients with disease relapse after previous therapy. While rituximab is very effective in the depletion of B cells, current research suggests it could also influence other immune system cells and reestablish immune homeostasis and tolerance. The safety profile of rituximab reveals that most reactions are infusion-related and that the incidence of serious side effects is low. Systemic infection remains a major concern and may result in death. A small number of cases of progressive multifocal leukoencephalopathy reported in patients receiving rituximab in off-label use (albeit none with ANCA-associated vasculitis) highlights the importance of pharmacovigilance.

摘要

相当一部分抗中性粒细胞胞浆抗体(ANCA)相关小血管炎患者对传统治疗无效或出现剂量限制性副作用。新型治疗方法包括利妥昔单抗,它是一种基因工程嵌合型鼠源-人源单克隆抗体,可与人类B细胞上表达的CD20结合。1997年它被批准用于治疗CD20阳性B细胞非霍奇金淋巴瘤,2006年被批准用于治疗类风湿关节炎。本文讨论了利妥昔单抗介导的B细胞耗竭的多种机制。多项关于显微镜下ANCA相关多血管炎治疗的开放性研究的累积数据表明,在绝大多数情况下利妥昔单抗具有有益作用。两项随机对照试验证实了这些有前景的结果,表明利妥昔单抗可被视为诱导ANCA相关血管炎缓解的一线治疗选择,并为治疗先前治疗后疾病复发的患者提供了额外手段。虽然利妥昔单抗在耗竭B细胞方面非常有效,但目前的研究表明它也可能影响其他免疫系统细胞并重建免疫稳态和耐受性。利妥昔单抗的安全性表明,大多数反应与输液相关,严重副作用的发生率较低。全身感染仍然是一个主要问题,可能导致死亡。少数接受利妥昔单抗超适应证使用的患者报告了进行性多灶性白质脑病病例(尽管没有ANCA相关血管炎患者),这突出了药物警戒的重要性。

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