Atypical haemolytic uraemic syndrome and mutations in complement regulator genes.

Springer seminars in immunopathology Pub Date : 2005-11-01 Epub Date: 2005-11-11 DOI:10.1007/s00281-005-0003-2
Marie-Agnès Dragon-Durey, Véronique Frémeaux-Bacchi
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引用次数: 89

Abstract

Haemolytic uraemic syndrome (HUS) is a thrombotic microangiopathy (TMA) disorder characterised by the association of haemolytic anaemia, thrombocytopenia and acute renal failure. Atypical forms (non-related to shigatoxin) may be familial or sporadic, with frequent recurrences and most of them lead to end stage renal failure. During the last years, different groups have demonstrated genetic predisposition of atypical HUS involving complement components factor H (FH), CD46 [or membrane co-factor protein (MCP)] and factor I. These three proteins are involved in the regulation of the alternative pathway of the complement system. Several series have reported mutations in the FH gene (called HF1) in between 10 and 22% of atypical HUS patients. At this time, four pedigrees corresponding to 13 cases have been reported with an MCP mutation and four cases with a sporadic disease presented factor I mutation. Whereas FH mutations were reported in both familial and sporadic forms of HUS, CD46 mutations were restricted to familial HUS, and factor I mutations were only observed in cases of sporadic HUS. We speculate that the penetrance of the disease may be variable regarding the identified susceptibility factors. Recently, the analysis of single nucleotide polymorphisms in both HF1 and MCP in three large cohorts of HUS patients identified significant association between atypical HUS and HF1 and MCP particular alleles. All these results, together with the finding of anti-FH antibodies in some atypical HUS patients, strongly suggest that an abnormality in the regulation of the alternative pathway participates in the patho-physiological mechanisms of atypical HUS. The recent progress made in the determination of susceptibility factors for atypical HUS has permitted the development of new diagnostic tests and may eventually lead to new specific treatments to block the pathological process.

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非典型溶血性尿毒综合征和补体调节基因突变。
溶血性尿毒综合征(HUS)是一种以溶血性贫血、血小板减少症和急性肾衰竭为特征的血栓性微血管病(TMA)疾病。非典型形式(与志贺毒素无关)可能是家族性或散发的,经常复发,大多数导致终末期肾功能衰竭。在过去的几年里,不同的群体已经表现出非典型溶血性尿毒综合征的遗传易感,涉及补体成分因子H (FH)、CD46[或膜辅助因子蛋白(MCP)]和因子i。这三种蛋白参与补体系统替代途径的调节。有几个系列报告在10%至22%的非典型溶血性尿毒综合征患者中发生了FH基因(称为HF1)突变。目前,已经报道了4个谱系对应13例MCP突变和4例散发疾病呈现因子I突变。家族性和散发性溶血性尿毒综合征均报道了FH突变,而CD46突变仅限于家族性溶血性尿毒综合征,而因子I突变仅在散发性溶血性尿毒综合征病例中观察到。我们推测,疾病的外显率可能是可变的关于确定的易感性因素。最近,对三个大型溶血性尿毒综合征患者的HF1和MCP单核苷酸多态性分析发现,非典型溶血性尿毒综合征与HF1和MCP特定等位基因之间存在显著关联。这些结果,再加上在部分非典型溶血性尿毒综合征患者中发现抗fh抗体,强烈提示该替代通路调控异常参与了非典型溶血性尿毒综合征的病理生理机制。最近在确定非典型溶血性尿毒综合征的易感因素方面取得的进展,使新的诊断测试得以发展,并可能最终导致新的特异性治疗方法来阻断病理过程。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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