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药物诱导的亚急性皮肤型狼疮的系统性综述。

A systematic review of drug-induced subacute cutaneous lupus erythematosus.

机构信息

University of Utah School of Medicine, Salt Lake City, USA.

出版信息

Br J Dermatol. 2011 Mar;164(3):465-72. doi: 10.1111/j.1365-2133.2010.10110.x. Epub 2011 Feb 17.

Abstract

The initial appearance of subacute cutaneous lupus erythematosus (SCLE) skin lesions in conjunction with Ro/SS-A autoantibodies occurring as an adverse reaction to hydrochlorothiazide [i.e. drug-induced SCLE (DI-SCLE)] was first reported in 1985. Over the past decade an increasing number of drugs in different classes has been implicated as triggers for DI-SCLE. The management of DI-SCLE can be especially challenging in patients taking multiple medications capable of triggering DI-SCLE. Our objectives were to review the published English language literature on DI-SCLE and use the resulting summary data pool to address questions surrounding drug-induced SCLE and to develop guidelines that might be of value to clinicians in the diagnosis and management of DI-SCLE. A systematic review of the Medline/PubMed-cited literature on DI-SCLE up to August 2009 was performed. Our data collection and analysis strategies were prospectively designed to answer a series of questions related to the clinical, prognostic and pathogenetic significance of DI-SCLE. One hundred and seventeen cases of DI-SCLE were identified and reviewed. White women made up the large majority of cases, and the mean overall age was 58·0 years. Triggering drugs fell into a number of different classes, highlighted by antihypertensives and antifungals. Time intervals ('incubation period') between drug exposure and appearance of DI-SCLE varied greatly and were drug class dependent. Most cases of DI-SCLE spontaneously resolved within weeks of drug withdrawal. Ro/SS-A autoantibodies were present in 80% of the cases in which such data were reported and most remained positive after resolution of SCLE skin disease activity. No significant differences in the clinical, histopathological or immunopathological features between DI-SCLE and idiopathic SCLE were detected. There is now adequate published experience to suggest that DI-SCLE does not differ clinically, histopathologically or immunologically from idiopathic SCLE. It should be recognized as a distinct clinical constellation differing clinically and immunologically from the classical form of drug-induced systemic lupus erythematosus.

摘要

药物诱导的亚急性皮肤型狼疮(DI-SCLE)最初于 1985 年被报道,表现为与 Ro/SS-A 自身抗体相关的亚急性皮肤型狼疮(SCLE)皮肤损害,同时伴有氢氯噻嗪的不良反应(即药物诱导的 SCLE)。在过去十年中,越来越多的不同种类的药物被认为是 DI-SCLE 的触发因素。在服用多种可能引发 DI-SCLE 的药物的患者中,DI-SCLE 的治疗可能极具挑战性。我们的目标是回顾已发表的有关 DI-SCLE 的英文文献,并使用由此产生的汇总数据来解决与药物诱导的 SCLE 相关的问题,并制定可能对临床医生诊断和治疗 DI-SCLE 有价值的指南。对截至 2009 年 8 月的 Medline/PubMed 文献进行了系统回顾。我们的数据收集和分析策略是前瞻性设计的,旨在回答一系列与 DI-SCLE 的临床、预后和发病机制意义相关的问题。共鉴定并回顾了 117 例 DI-SCLE 病例。白人女性占绝大多数,平均年龄为 58.0 岁。触发药物来自多个不同的类别,以降压药和抗真菌药为主。从接触药物到出现 DI-SCLE 的时间间隔(“潜伏期”)差异很大,并且取决于药物类别。大多数 DI-SCLE 病例在停药后数周内自发缓解。在报告此类数据的病例中,80%的病例存在 Ro/SS-A 自身抗体,并且在 SCLE 皮肤疾病活动缓解后大多数仍为阳性。在 DI-SCLE 和特发性 SCLE 之间,未检测到临床、组织病理学或免疫病理学特征的显著差异。目前已有足够的经验表明,DI-SCLE 在临床、组织病理学或免疫学方面与特发性 SCLE 没有区别。应将其视为一种与经典药物诱导的系统性红斑狼疮在临床上和免疫学上均不同的独特临床综合征。

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