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靶向宿主染色质功能的病毒编码酶。

Viral-encoded enzymes that target host chromatin functions.

作者信息

Wei Hua, Zhou Ming-Ming

机构信息

Department of Structural and Chemical Biology, Mount Sinai School of Medicine, New York University, One Gustave L. Levy Place, New York, NY 10029, USA.

出版信息

Biochim Biophys Acta. 2010 Mar-Apr;1799(3-4):296-301. doi: 10.1016/j.bbagrm.2009.08.007. Epub 2009 Aug 27.

Abstract

Ever since their existence, there has been an everlasting arms race between viruses and their host cells. Host cells have developed numerous strategies to silence viral gene expression whereas viruses always find their ways to overcome these obstacles. Recent studies show that viruses have also evolved to take full advantage of existing cellular chromatin components to activate or repress its own genes when needed. While in most cases viruses encode certain proteins to recruit or inhibit cellular factors through physical interactions, growing examples show that viral-encoded enzymes affect host chromatin structure through post-translationally modifying histones or other cellular proteins important for chromatin function. The most well-studied example is vSET encoded by paramecium bursaria chlorella virus 1. vSET specifically methylates histone H3 at lysine 27, causing genome-wide silencing of Polycomb target genes upon infection, thus mimicking the function of Polycomb repressive complex 2 (PRC2) in eukaryotes. Other examples include BGLF4 from Epstein-Barr virus that affects both condensin and topoisomerase II activity and Us3 from Herpes Simplex virus 1 that inhibits HDAC1 function through phosphorylation.

摘要

自从病毒存在以来,病毒与其宿主细胞之间就一直存在着一场永不停歇的军备竞赛。宿主细胞已经发展出多种策略来沉默病毒基因表达,而病毒总能找到克服这些障碍的方法。最近的研究表明,病毒也已经进化到能够充分利用现有的细胞染色质成分,在需要时激活或抑制自身基因。虽然在大多数情况下,病毒编码某些蛋白质,通过物理相互作用招募或抑制细胞因子,但越来越多的例子表明,病毒编码的酶通过对组蛋白或其他对染色质功能重要的细胞蛋白质进行翻译后修饰,来影响宿主染色质结构。研究最深入的例子是草履虫小球藻病毒1编码的vSET。vSET特异性地使组蛋白H3的赖氨酸27甲基化,在感染时导致全基因组范围的多梳靶基因沉默,从而模拟真核生物中多梳抑制复合物2(PRC2)的功能。其他例子包括爱泼斯坦-巴尔病毒的BGLF4,它影响凝缩蛋白和拓扑异构酶II的活性,以及单纯疱疹病毒1的Us3,它通过磷酸化抑制HDAC1的功能。

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