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FIC 蛋白:从细菌到人,再回到细菌。

FIC proteins: from bacteria to humans and back again.

机构信息

CNRS and Ecole normale supérieure Paris-Saclay, 94235 Cachan, France.

出版信息

Pathog Dis. 2018 Mar 1;76(2). doi: 10.1093/femspd/fty012.

Abstract

During the last decade, FIC proteins have emerged as a large family comprised of a variety of bacterial enzymes and a single member in animals. The air de famille of FIC proteins stems from a domain of conserved structure, which catalyzes the post-translational modification of proteins (PTM) by a phosphate-containing compound. In bacteria, examples of FIC proteins include the toxin component of toxin/antitoxin modules, such as Doc-Phd and VbhT-VbhA, toxins secreted by pathogenic bacteria to divert host cell processes, such as VopS, IbpA and AnkX, and a vast majority of proteins of unknown functions. FIC proteins catalyze primarily the transfer of AMP (AMPylation), but they are not restricted to this PTM and also carry out other modifications, for example by phosphocholine or phosphate. In a recent twist, animal FICD/HYPE was shown to catalyze both AMPylation and de-AMPylation of the endoplasmic reticulum BIP chaperone to regulate the unfolded protein response. FICD shares structural features with some bacterial FIC proteins, raising the possibility that bacteria also encode such dual activities. In this review, we discuss how structural, biochemical and cellular approaches have fertilized each other to understand the mechanism, regulation and function of FIC proteins from bacterial pathogens to humans.

摘要

在过去的十年中,FIC 蛋白已成为一个庞大的家族,其中包括各种细菌酶和动物中的一个单一成员。FIC 蛋白的家族特征源于结构保守的结构域,该结构域通过含有磷酸的化合物催化蛋白质的翻译后修饰(PTM)。在细菌中,FIC 蛋白的例子包括毒素/抗毒素模块的毒素成分,例如 Doc-Phd 和 VbhT-VbhA,以及分泌到宿主细胞中以改变宿主细胞过程的致病细菌毒素,例如 VopS、IbpA 和 AnkX,以及绝大多数具有未知功能的蛋白质。FIC 蛋白主要催化 AMP 的转移(AMPylation),但它们不仅限于这种 PTM,还进行其他修饰,例如磷酸胆碱或磷酸。最近的一项研究表明,动物 FICD/HYPE 可以催化内质网 BIP 伴侣蛋白的 AMPylation 和去 AMPylation,以调节未折叠蛋白反应。FICD 与一些细菌 FIC 蛋白具有结构特征,这增加了细菌也编码这种双重活性的可能性。在这篇综述中,我们讨论了结构、生化和细胞方法如何相互促进,以了解从细菌病原体到人类的 FIC 蛋白的机制、调节和功能。

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