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风疹病毒对线粒体功能改变中 p32 和微管的作用。

Involvement of p32 and microtubules in alteration of mitochondrial functions by rubella virus.

机构信息

Institute of Virology, University of Leipzig, Johannisallee 30, Leipzig D-04103, Germany.

出版信息

J Virol. 2011 Apr;85(8):3881-92. doi: 10.1128/JVI.02492-10. Epub 2011 Jan 19.

Abstract

The interaction of the rubella virus (RV) capsid (C) protein and the mitochondrial p32 protein is believed to participate in virus replication. In this study, the physiological significance of the association of RV with mitochondria was investigated by silencing p32 through RNA interference. It was demonstrated that downregulation of p32 interferes with microtubule-directed redistribution of mitochondria in RV-infected cells. However, the association of the viral C protein with mitochondria was not affected. When cell lines either pretreated with respiratory chain inhibitors or cultivated under (mild) hypoxic conditions were infected with RV, viral replication was reduced in a time-dependent fashion. Additionally, RV infection induces increased activity of mitochondrial electron transport chain complex III, which was associated with an increase in the mitochondrial membrane potential. These effects are outstanding among the examples of mitochondrial alterations caused by viruses. In contrast to the preferential localization of p32 to the mitochondrial matrix in most cell lines, RV-permissive cell lines were characterized by an almost exclusive membrane association of p32. Conceivably, this contributes to p32 function(s) during RV replication. The data presented suggest that p32 fulfills an essential function for RV replication in directing trafficking of mitochondria near sites of viral replication to meet the energy demands of the virus.

摘要

风疹病毒(RV)衣壳(C)蛋白与线粒体 p32 蛋白的相互作用被认为参与病毒复制。在这项研究中,通过 RNA 干扰沉默 p32 来研究 RV 与线粒体结合的生理意义。结果表明,下调 p32 会干扰 RV 感染细胞中线粒体的微管定向重分布。然而,病毒 C 蛋白与线粒体的结合不受影响。当用呼吸链抑制剂预处理或在(轻度)低氧条件下培养的细胞系感染 RV 时,病毒复制呈时间依赖性减少。此外,RV 感染诱导线粒体电子传递链复合物 III 活性增加,这与线粒体膜电位增加有关。这些作用在病毒引起的线粒体改变的例子中是突出的。与大多数细胞系中 p32 优先定位于线粒体基质相反,RV 允许的细胞系的 p32 几乎完全与膜结合。可以想象,这有助于 p32 在 RV 复制过程中的功能。所提供的数据表明,p32 通过指导线粒体在病毒复制部位附近的运输,以满足病毒的能量需求,从而为 RV 复制完成了一项重要功能。

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