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外源性 inter-α 抑制剂蛋白可预防细胞死亡并改善小鼠的缺血性脑卒中结局。

Exogenous inter-α inhibitor proteins prevent cell death and improve ischemic stroke outcomes in mice.

机构信息

Department of Neurology, McGovern Medical School at University of Texas Health Science Center at Houston, Houston, Texas, USA.

Genomic and RNA Profiling Core, Baylor College of Medicine, Houston, Texas, USA.

出版信息

J Clin Invest. 2021 Sep 1;131(17). doi: 10.1172/JCI144898.

Abstract

Inter-α inhibitor proteins (IAIPs) are a family of endogenous plasma and extracellular matrix molecules. IAIPs suppress proinflammatory cytokines, limit excess complement activation, and bind extracellular histones to form IAIP-histone complexes, leading to neutralization of histone-associated cytotoxicity in models of sepsis. Many of these detrimental processes also play critical roles in the pathophysiology of ischemic stroke. In this study, we first assessed the clinical relevance of IAIPs in stroke and then tested the therapeutic efficacy of exogenous IAIPs in several experimental stroke models. IAIP levels were reduced in both ischemic stroke patients and in mice subjected to experimental ischemic stroke when compared with controls. Post-stroke administration of IAIP significantly improved stroke outcomes across multiple stroke models, even when given 6 hours after stroke onset. Importantly, the beneficial effects of delayed IAIP treatment were observed in both young and aged mice. Using targeted gene expression analysis, we identified a receptor for complement activation, C5aR1, that was highly suppressed in both the blood and brain of IAIP-treated animals. Subsequent experiments using C5aR1-knockout mice demonstrated that the beneficial effects of IAIPs are mediated in part by C5aR1. These results indicate that IAIP is a potential therapeutic candidate for the treatment of ischemic stroke.

摘要

抑制素 α 蛋白(IAIPs)是一类内源性血浆和细胞外基质分子。IAIPs 可抑制促炎细胞因子,限制补体过度激活,并与细胞外组蛋白结合形成 IAIP-组蛋白复合物,从而中和脓毒症模型中组蛋白相关的细胞毒性。这些有害过程中的许多在缺血性中风的病理生理学中也起着关键作用。在这项研究中,我们首先评估了 IAIP 在中风中的临床相关性,然后在几种实验性中风模型中测试了外源性 IAIP 的治疗效果。与对照组相比,缺血性中风患者和实验性缺血性中风小鼠的 IAIP 水平降低。与对照组相比,中风后给予 IAIP 可显著改善多种中风模型的中风结局,即使在中风发作后 6 小时给予。重要的是,在年轻和年老的小鼠中均观察到延迟给予 IAIP 的有益效果。通过靶向基因表达分析,我们鉴定了补体激活受体 C5aR1,IAIP 处理的动物的血液和大脑中该受体的表达均受到高度抑制。随后使用 C5aR1 基因敲除小鼠的实验表明,IAIP 的有益作用部分是通过 C5aR1 介导的。这些结果表明,IAIP 是治疗缺血性中风的潜在治疗候选物。

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