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典型(肠病性)溶血尿毒综合征的治疗。

Treatment of typical (enteropathic) hemolytic uremic syndrome.

机构信息

Department of Pediatrics, Division of Nephrology, McGill University, Montreal Children's Hospital, Montreal, Quebec, Canada.

出版信息

Semin Thromb Hemost. 2010 Sep;36(6):594-610. doi: 10.1055/s-0030-1262881. Epub 2010 Sep 23.

DOI:10.1055/s-0030-1262881
PMID:20865636
Abstract

Typical enteropathic HUS (eHUS) is triggered by Shiga toxin (Stx)-producing bacteria (STPB), predominantly Stx-producing ESCHERICHIA COLI O157. The cell biological aspects of Stx have been well defined, but host factors potentially predisposing to the development or severity of HUS remain elusive. Treatment of eHUS includes supportive measures and invasive extracorporeal therapies. Thirty to 60% of children with eHUS require dialysis. Peritoneal and hemodialysis appear equally effective. Patient age, center experience, and equipment availability determine the choice of the modality; circulatory instability may require continuous renal replacement therapies. At present, no evidence indicates that plasma infusion or exchange therapies improve outcome of Stx-induced HUS. However, the traditional separation between diarrhea-positive (D (+)) and negative (D (-)) HUS, implying two entirely different pathological pathways, requires a fresh look: Atypical HUS may follow nonspecific diarrhea, and, conversely, STPB and fecal Stx may not be detected anymore at the time of the diagnosis of HUS. Recently, Stx has been found to directly interfere with the alternative complement pathway regulator factor H in vitro, whereas some patients with Stx-HUS demonstrate evidence of complement activation. Among newer treatments for eHUS, development of Stx-neutralizing monoclonal antibodies is the most advanced. This review concludes with a discussion of the rationale, mode of action, and status of presently available therapeutic antibodies against Stx2 and Stx1.

摘要

典型的肠病相关性溶血尿毒综合征(eHUS)由志贺毒素(Stx)产生细菌(STPB)触发,主要是产志贺毒素的大肠杆菌 O157。Stx 的细胞生物学方面已经得到了很好的定义,但宿主因素可能导致 HUS 的发生或严重程度仍不清楚。eHUS 的治疗包括支持性措施和侵入性体外治疗。30%至 60%的 eHUS 患儿需要透析。腹膜透析和血液透析同样有效。患者年龄、中心经验和设备可用性决定了治疗方式的选择;循环不稳定可能需要连续肾脏替代治疗。目前,没有证据表明血浆输注或交换疗法能改善 Stx 诱导的 HUS 的预后。然而,传统上将腹泻阳性(D (+))和阴性(D (-))HUS 分开,暗示两种完全不同的病理途径,需要重新审视:非典型 HUS 可能继发于非特异性腹泻,反之,在 HUS 诊断时可能不再检测到 STPB 和粪便 Stx。最近,Stx 已被发现可直接干扰体外替代补体途径调节剂因子 H,而一些 Stx-HUS 患者表现出补体激活的证据。在 eHUS 的新治疗方法中,开发 Stx 中和单克隆抗体是最先进的。本文最后讨论了目前针对 Stx2 和 Stx1 的治疗性抗体的作用机制、作用模式和现有治疗性抗体的状态。

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