吞噬细胞的 NADPH 依赖性氧化酶。

W M Nauseef
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引用次数: 98

摘要

多形核白细胞(PMNs)是先天性免疫系统中的一个重要细胞元素,可摄取外源颗粒和微生物,并杀死被吞噬的微生物。PMNs 的杀微生物活性取决于一系列强效系统的相互作用,包括相对稳定的降解蛋白和易变的活性自由基。这些系统可分为氧依赖机制和非氧化机制,但生理上的相对活性取决于这两种系统之间精确协调的相互作用。负责氧依赖系统活性的酶复合物是呼吸爆发氧化酶,它对宿主防御的重要贡献体现在 PMN 缺乏氧化酶活性的个体(即慢性肉芽肿病(CGD)患者)中频繁出现的严重感染。过去十年中,在了解呼吸爆发氧化酶的蛋白质成分、它们在静息 PMN 中的亚细胞分布以及它们在吞噬体和质膜上组装成一个功能系统的激动剂依赖性方面取得了重大进展。与此同时,人们对 CGD 的分子基础也有了实质性的了解。尽管如此,我们对该系统特定成分的精确功能贡献、调节其协调组装的分子机制以及相关蛋白在非吞噬细胞中的作用的认识仍存在很大差距。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The NADPH-dependent oxidase of phagocytes.

Polymorphonuclear leukocytes (PMNs) represent a prominent cellular element in the innate immune system, serving to ingest exogenous particles and microbes and to kill phagocytosed microorganisms. The microbicidal activity of PMNs depends on the interactions of a broad array of potent systems, including relatively stable degradative proteins as well as labile reactive radicals. These systems can be categorized as oxygen-dependent and nonoxidative mechanisms, although the physiologically relative activity depends on the precisely orchestrated interplay between both systems. The enzyme complex responsible for the activity of the oxygen-dependent system is the respiratory burst oxidase and its important contribution to host defense is best illustrated by the frequent and severe infections seen in individuals whose PMNs lack oxidase activity, namely patients with chronic granulomatous disease (CGD). Multiple elements comprise the oxygen-dependent system, and significant advances have been made in the past decade in understanding the protein components of the respiratory burst oxidase, their subcellular distribution in resting PMNs, and their agonist-dependent assembly into a functional system at phagosomal and plasma membranes. In parallel, substantial insights into the molecular bases of CGD have likewise been made. Nonetheless there remain significant gaps in our understanding of the precise functional contributions of particular components of the system, the molecular mechanisms that regulate their coordinated assembly, and the role of related proteins in nonphagocytic cells.

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