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痘病毒进入过程中的膜融合

Membrane fusion during poxvirus entry.

作者信息

Moss Bernard

机构信息

Laboratory of Viral Diseases, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

Semin Cell Dev Biol. 2016 Dec;60:89-96. doi: 10.1016/j.semcdb.2016.07.015. Epub 2016 Jul 14.

Abstract

Poxviruses comprise a large family of enveloped DNA viruses that infect vertebrates and invertebrates. Poxviruses, unlike most DNA viruses, replicate in the cytoplasm and encode enzymes and other proteins that enable entry, gene expression, genome replication, virion assembly and resistance to host defenses. Entry of vaccinia virus, the prototype member of the family, can occur at the plasma membrane or following endocytosis. Whereas many viruses encode one or two proteins for attachment and membrane fusion, vaccinia virus encodes four proteins for attachment and eleven more for membrane fusion and core entry. The entry-fusion proteins are conserved in all poxviruses and form a complex, known as the Entry Fusion Complex (EFC), which is embedded in the membrane of the mature virion. An additional membrane that encloses the mature virion and is discarded prior to entry is present on an extracellular form of the virus. The EFC is held together by multiple interactions that depend on nine of the eleven proteins. The entry process can be divided into attachment, hemifusion and core entry. All eleven EFC proteins are required for core entry and at least eight for hemifusion. To mediate fusion the virus particle is activated by low pH, which removes one or more fusion repressors that interact with EFC components. Additional EFC-interacting fusion repressors insert into cell membranes and prevent secondary infection. The absence of detailed structural information, except for two attachment proteins and one EFC protein, is delaying efforts to determine the fusion mechanism.

摘要

痘病毒是一个包含包膜DNA病毒的大家族,可感染脊椎动物和无脊椎动物。与大多数DNA病毒不同,痘病毒在细胞质中复制,并编码能实现病毒进入、基因表达、基因组复制、病毒粒子组装以及抵抗宿主防御的酶和其他蛋白质。该病毒家族的原型成员痘苗病毒可以在质膜处进入,也可以在胞吞作用后进入。许多病毒编码一两种用于附着和膜融合的蛋白质,而痘苗病毒则编码四种用于附着的蛋白质和另外十一种用于膜融合及核心进入的蛋白质。进入融合蛋白在所有痘病毒中都是保守的,并形成一个复合体,称为进入融合复合体(EFC),它嵌入成熟病毒粒子的膜中。病毒的细胞外形式存在一层额外的膜,该膜包裹着成熟病毒粒子,并在进入之前被丢弃。EFC通过多种相互作用结合在一起,这些相互作用依赖于十一种蛋白质中的九种。进入过程可分为附着、半融合和核心进入。核心进入需要所有十一种EFC蛋白,半融合至少需要八种。为了介导融合,病毒粒子在低pH值下被激活,这会去除一种或多种与EFC成分相互作用的融合抑制因子。其他与EFC相互作用的融合抑制因子插入细胞膜,防止二次感染。除了两种附着蛋白和一种EFC蛋白外,缺乏详细的结构信息,这延缓了确定融合机制的研究工作。

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Vaccinia virus immune evasion: mechanisms, virulence and immunogenicity.牛痘病毒免疫逃避:机制、毒力和免疫原性。
J Gen Virol. 2013 Nov;94(Pt 11):2367-2392. doi: 10.1099/vir.0.055921-0. Epub 2013 Sep 2.
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Orthopoxvirus species and strain differences in cell entry.正痘病毒属种和株在细胞进入方面的差异。
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Poxvirus cell entry: how many proteins does it take?痘病毒细胞进入:需要多少种蛋白?
Viruses. 2012 May;4(5):688-707. doi: 10.3390/v4050688. Epub 2012 Apr 27.

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