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巨型潘多拉病毒的一种主要病毒粒子蛋白由失活的细菌糖苷水解酶演变而来。

Evolution of a major virion protein of the giant pandoraviruses from an inactivated bacterial glycoside hydrolase.

作者信息

Krupovic Mart, Yutin Natalya, Koonin Eugene

机构信息

Department of Microbiology, Archaeal Virology Unit, Institut Pasteur, Paris 75015, France.

National Library of Medicine, National Center for Biotechnology Information, National Institutes of Health, Bethesda, MD 20894, USA.

出版信息

Virus Evol. 2020 Nov 30;6(2):veaa059. doi: 10.1093/ve/veaa059. eCollection 2020 Jul.

Abstract

The diverse viruses in the phylum (also known as NLCDVs, Nucleo-cytoplasmic Large DNA Viruses) typically possess large icosahedral virions. However, in several families of , the icosahedral capsid was replaced by irregular particle shapes, most notably, the amphora-like virions of pandoraviruses and pithoviruses, the largest known virus particles in the entire virosphere. Pandoraviruses appear to be the most highly derived viruses in this phylum because their evolution involved not only the change in the virion shape, but also, the actual loss of the gene encoding double-jelly roll major capsid protein (DJR MCP), the main building block of icosahedral capsids in this virus assemblage. Instead, pandoravirus virions are built of unrelated abundant proteins. Here we show that the second most abundant virion protein of pandoraviruses, major virion protein 2 (MVP2), evolved from an inactivated derivative of a bacterial glycoside hydrolase of the GH16 family. The ancestral form of MVP2 was apparently acquired early in the evolution of the , to become a minor virion protein. After a duplication in the common ancestor of pandoraviruses and molliviruses, one of the paralogs displaces DJR MCP in pandoraviruses, conceivably, opening the way for a major increase in the size of the virion and the genome. Exaptation of a carbohydrate-binding protein for the function of the MVP is a general trend in virus evolution and might underlie the transformation of the virion shape in other groups of the as well.

摘要

在核质大DNA病毒门(也称为NLCDVs)中的多种病毒通常具有大型二十面体病毒粒子。然而,在该门的几个科中,二十面体衣壳被不规则的粒子形状所取代,最显著的是潘多拉病毒和髓病毒的瓮状病毒粒子,它们是整个病毒圈中已知最大的病毒粒子。潘多拉病毒似乎是该门中衍生程度最高的病毒,因为它们的进化不仅涉及病毒粒子形状的变化,还涉及编码双果冻卷主要衣壳蛋白(DJR MCP)的基因的实际丢失,DJR MCP是该病毒组合中二十面体衣壳的主要组成部分。相反,潘多拉病毒粒子由不相关的丰富蛋白质构成。在这里,我们表明潘多拉病毒的第二丰富的病毒粒子蛋白,主要病毒粒子蛋白2(MVP2),是从GH16家族细菌糖苷水解酶的失活衍生物进化而来的。MVP2的祖先形式显然是在核质大DNA病毒门进化的早期获得的,成为一种次要的病毒粒子蛋白。在潘多拉病毒和软体病毒的共同祖先中发生一次复制后,其中一个旁系同源物在潘多拉病毒中取代了DJR MCP,可以想象,这为病毒粒子和基因组大小的大幅增加开辟了道路。将一种碳水化合物结合蛋白适应性用于MVP的功能是病毒进化中的一个普遍趋势,也可能是核质大DNA病毒门其他类群中病毒粒子形状转变的基础。

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