C1 inhibitor: molecular and clinical aspects.

Springer seminars in immunopathology Pub Date : 2005-11-01 Epub Date: 2005-11-11 DOI:10.1007/s00281-005-0001-4
Marco Cicardi, Lorenza Zingale, Andrea Zanichelli, Emanuela Pappalardo, Benedetta Cicardi
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引用次数: 93

Abstract

C1 inhibitor (C1-INH) is a serine protease inhibitor (serpins) that inactivates several different proteases in the complement, contact, coagulation, and fibrinolytic systems. By its C-terminal part (serpin domain), characterized by three beta-sheets and an exposed mobile reactive loop, C1-INH binds, and blocks the activity of its target proteases. The N-terminal end (nonserpin domain) confers to C1-INH the capacity to bind lipopolysaccharides and E-selectin. Owing to this moiety, C1-INH intervenes in regulation of the inflammatory reaction. The heterozygous deficiency of C1-INH results in hereditary angioedema (HAE). The clinical picture of HAE is characterized by bouts of local increase in vascular permeability. Depending on the affected site, patients suffer from disfiguring subcutaneous edema, abdominal pain, vomiting and/or diarrhoea for edema of the gastrointestinal mucosa, dysphagia, and dysphonia up to asphyxia for edema of the pharynx and larynx. Apart from its genetic deficiency, there are several pathological conditions such as ischemia-reperfusion, septic shock, capillary leak syndrome, and pancreatitis, in which C1-INH has been reported to either play a pathogenic role or be a potential therapeutic tool. These potential applications were identified long ago, but controlled studies have not been performed to confirm pilot experiences. Recombinant C1-INH, produced in transgenic animals, has recently been produced for treatment of HAE, and clinical trials are in progress. We can expect that the introduction of this new product, along with the existing plasma derivative, will renew interest in exploiting C1-INH as a therapeutic agent.

C1抑制剂:分子和临床方面。
C1抑制剂(C1- inh)是一种丝氨酸蛋白酶抑制剂(丝氨酸蛋白酶抑制剂),在补体、接触、凝血和纤溶系统中失活几种不同的蛋白酶。C1-INH通过其c端部分(serpin结构域),以三个β -sheet和一个暴露的移动反应环为特征,结合并阻断其靶蛋白酶的活性。n端(非丝氨酸蛋白结构域)赋予C1-INH结合脂多糖和e -选择素的能力。由于这部分,C1-INH干预炎症反应的调节。C1-INH杂合缺乏导致遗传性血管性水肿(HAE)。HAE的临床表现以局部血管通透性增加为特征。根据受累部位的不同,患者可出现毁容性皮下水肿、腹痛、胃肠道粘膜水肿的呕吐和/或腹泻、咽喉部水肿的吞咽困难和发音困难直至窒息。除了遗传缺陷外,C1-INH在缺血再灌注、感染性休克、毛细血管渗漏综合征和胰腺炎等病理情况下也有报道,在这些情况下C1-INH要么起致病作用,要么是潜在的治疗工具。这些潜在的应用在很久以前就被发现了,但还没有进行对照研究来证实试点经验。在转基因动物中生产的重组C1-INH最近被用于治疗HAE,临床试验正在进行中。我们可以预期,这种新产品的推出,以及现有的血浆衍生物,将重新引起人们对开发C1-INH作为治疗剂的兴趣。
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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