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[多发性硬化症进展型的治疗]

[Treatment of progressive forms of multiple sclerosis].

作者信息

Edan G

机构信息

Service de Neurologie, CHU Rennes.

出版信息

Rev Neurol (Paris). 2001 Sep;157(8-9 Pt 2):1008-13.

PMID:11787331
Abstract

There is not a standardized definition of rapidly worsening Multiple Sclerosis (MS). Arbitrary, we have designed under this term patients having a very active MS (patients having more than 2 relapses within the last 12 months) or rapid progression of handicap (more than 2 points EDSS progression within the last 12 months). The design of most previous studies using azathioprine, cyclophosphamide, methotrexate do not fulfill criteria to draw final conclusions as to the efficacy of these drugs as an immunoprophylactic agent in Multiple Sclerosis (MS). During the last five years, efficacy of immunomodulatory and immunosuppressive agents was provided by some well-designed randomized control clinical trials: among the immunosuppressors, mitoxantrone deserves special consideration as there were three controlled trials in Europe during the two last years that demonstrated strong efficacy both on clinical and MRI criteria. Due to its potentially cardiotoxicity, related to total cumulative dose, mitoxantrone should presently only be used in selected patients with a very high relapse rate and incomplete remission or in those who do not respond to INF beta treatment. The immunomodulatory agents (interferon beta 1a or 1b, copolymer 1) demonstrated a significant effect on the reduction of relapse rate (about 30 p. cent reduction), on progression of handicap and on MRI. In secondary progressive MS, an effect on progression is demonstrated only on patients still having relapses. No trial devoted to worsening patients as defined above have been yet designed with immunomodulatory agents.

摘要

目前尚无快速进展型多发性硬化症(MS)的标准化定义。我们自行设定,该术语涵盖具有非常活跃的MS患者(过去12个月内复发超过2次)或残疾进展迅速的患者(过去12个月内扩展残疾状态量表(EDSS)进展超过2分)。以往大多数使用硫唑嘌呤、环磷酰胺、甲氨蝶呤的研究设计,不符合就这些药物作为多发性硬化症(MS)免疫预防剂的疗效得出最终结论的标准。在过去五年中,一些精心设计的随机对照临床试验证实了免疫调节和免疫抑制药物的疗效:在免疫抑制剂中,米托蒽醌值得特别关注,因为在过去两年欧洲有三项对照试验表明,其在临床和磁共振成像(MRI)标准方面均显示出强大疗效。由于其潜在的心脏毒性与总累积剂量有关,目前米托蒽醌仅应在复发率非常高且缓解不完全的特定患者或对干扰素β治疗无反应的患者中使用。免疫调节药物(干扰素β-1a或-1b、共聚肽1)对降低复发率(降低约30%)、残疾进展和MRI表现均有显著效果。在继发进展型MS中,仅对仍有复发的患者显示出对疾病进展的影响。尚未设计专门针对上述定义的病情恶化患者的免疫调节药物试验。

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