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炎症性肌病的免疫治疗:实用方法和未来前景。

Immunotherapy of inflammatory myopathies: practical approach and future prospects.

机构信息

Neuroimmunology Unit, Department of Pathophysiology, University of Athens Medical School, Athens, Greece,

出版信息

Curr Treat Options Neurol. 2011 Jun;13(3):311-23. doi: 10.1007/s11940-011-0119-8.

Abstract

The inflammatory myopathies, a group of chronic myopathic conditions, are potentially treatable, so proper diagnosis and early initiation of therapy are necessary. The most common types are polymyositis (PM), dermatomyositis (DM), necrotizing autoimmune myopathy (NAM), and inclusion body myositis (IBM). This review provides practical advice on treatment and identifies emerging new therapies. Although IBM is difficult to treat, PM, DM, and NAM respond to appropriate immunotherapies, if diagnosed early and treated aggressively. In uncontrolled studies, PM and DM respond to prednisone to some degree and for a period of time. The commonly used immunosuppressive drugs (azathioprine, cyclosporine, mycophenolate, or methotrexate) may offer some non-evidence-based "steroid-sparing" effect but provide minimal benefit on their own. As a result, the second-line therapy is intravenous immunoglobulin (IVIg), which a controlled study has shown to be effective in DM and which appears to be effective in PM and NAM; it offers minimal and transient benefit to only a small number of IBM patients, however. Uncontrolled series have suggested that rituximab and tacrolimus may offer additional benefit to some patients not adequately controlled with the aforementioned therapies. IBM is usually resistant to most therapies, but early initiation of therapy may be helpful at times. Emerging agents against T cells, B cells, transmigration, or transduction molecules are discussed as potential new treatment options.

摘要

炎性肌病是一组慢性肌病,有潜在的治疗可能,因此正确诊断和早期开始治疗是必要的。最常见的类型包括多发性肌炎(PM)、皮肌炎(DM)、坏死性自身免疫性肌病(NAM)和包涵体肌炎(IBM)。本综述提供了治疗的实用建议,并确定了新兴的新疗法。尽管 IBM 难以治疗,但如果及早诊断和积极治疗,PM、DM 和 NAM 会对适当的免疫疗法有反应。在未受控制的研究中,PM 和 DM 在一定程度上和一定时间内对泼尼松有反应。常用的免疫抑制剂(硫唑嘌呤、环孢素、霉酚酸酯或甲氨蝶呤)可能具有一定的非基于证据的“激素节省”作用,但自身益处有限。因此,二线治疗是静脉注射免疫球蛋白(IVIg),一项对照研究表明其对 DM 有效,且似乎对 PM 和 NAM 有效;然而,它仅对少数 IBM 患者有最小且短暂的益处。未受控制的系列研究表明,利妥昔单抗和他克莫司可能对上述治疗方法未能充分控制的某些患者提供额外的益处。IBM 通常对大多数治疗方法有抗性,但有时早期开始治疗可能会有所帮助。针对 T 细胞、B 细胞、迁移或转导分子的新兴药物被讨论为潜在的新治疗选择。

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