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具有不同 M1 蛋白的甲型 H1N1 WSN33 病毒的体外和体内复制。

In vitro and in vivo replication of influenza A H1N1 WSN33 viruses with different M1 proteins.

机构信息

Veterinary Diagnostic Division, Chongqing Municipal Center for Animal Disease Control and Prevention, Chongqing 401120, PR China.

Department of Veterinary and Biomedical Sciences, South Dakota State University, Brookings, SD, USA.

出版信息

J Gen Virol. 2013 Apr;94(Pt 4):884-895. doi: 10.1099/vir.0.046219-0. Epub 2012 Dec 19.

Abstract

The M1 protein is a major structural protein that has multiple functions in various steps within the life cycle of the influenza A virus (IAV). However, little is currently known about the role of M1 in IAV replication in vivo and the associated pathogenesis. In this study, six isogenic H1N1 WSN33 viruses, constructed to express unique M1 proteins derived from various strains, subtypes or WSN33 itself, were tested to determine in vitro and in vivo functional exchangeability of M1 proteins in the replication and pathogenesis of the WSN33 virus. Despite five chimeric M1 viruses replicating to levels similar to those of the parental WSN33 virus in cell cultures, all M1 chimeras exhibited improved replication and enhanced virulence in mice when compared with the WSN33 virus. Interestingly, M1 proteins derived from swine viruses caused more severe clinical diseases than those from human or quail. These data indicate that the M1 protein is an important determinant of viral replication and pathogenic properties in mice, although the functions of M1 observed in vivo are not adequately reflected in simple infections of cultured cells. Chimeric M1 viruses that are variable in their clinical manifestations described here will aid future understanding of the role of M1 in IAV pathogenesis.

摘要

M1 蛋白是一种主要的结构蛋白,在甲型流感病毒(IAV)的生命周期的多个步骤中具有多种功能。然而,目前对于 M1 在 IAV 体内复制中的作用以及相关发病机制知之甚少。在这项研究中,构建了六个具有独特 M1 蛋白的同基因 H1N1 WSN33 病毒,这些 M1 蛋白源自不同的株、亚型或 WSN33 本身,以确定 M1 蛋白在 WSN33 病毒复制和发病机制中的体外和体内功能可交换性。尽管五个嵌合 M1 病毒在细胞培养中复制到与亲本 WSN33 病毒相似的水平,但与 WSN33 病毒相比,所有 M1 嵌合体在小鼠中均表现出增强的复制和增强的毒力。有趣的是,源自猪的病毒的 M1 蛋白引起的临床疾病比源自人类或鹌鹑的病毒更严重。这些数据表明,M1 蛋白是决定病毒在小鼠中复制和致病特性的重要因素,尽管在体内观察到的 M1 功能不能充分反映在简单的细胞培养感染中。本文描述的在临床表现上具有变异性的嵌合 M1 病毒将有助于未来理解 M1 在 IAV 发病机制中的作用。

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