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麻疹病毒核糖核蛋白复合物的细胞内运输是由 Rab11A 阳性再循环内体介导的,从而驱动病毒从极化上皮细胞的顶膜释放。

Intracellular transport of the measles virus ribonucleoprotein complex is mediated by Rab11A-positive recycling endosomes and drives virus release from the apical membrane of polarized epithelial cells.

机构信息

Department of Virology 3, National Institute of Infectious Diseases, Tokyo, Japan.

出版信息

J Virol. 2013 Apr;87(8):4683-93. doi: 10.1128/JVI.02189-12. Epub 2013 Feb 13.

Abstract

Many viruses use the host trafficking system at a variety of their replication steps. Measles virus (MV) possesses a nonsegmented negative-strand RNA genome that encodes three components of the ribonucleoprotein (RNP) complex (N, P, and L), two surface glycoproteins, a matrix protein, and two nonstructural proteins. A subset of immune cells and polarized epithelial cells are in vivo targets of MV, and MV is selectively released from the apical membrane of polarized epithelial cells. However, the molecular mechanisms for the apical release of MV remain largely unknown. In the present study, the localization and trafficking mechanisms of the RNP complex of MV were analyzed in detail using recombinant MVs expressing fluorescent protein-tagged L proteins. Live cell imaging analyses demonstrated that the MV RNP complex was transported in a manner dependent on the microtubule network and together with Rab11A-containing recycling endosomes. The RNP complex was accumulated at the apical membrane and the apical recycling compartment. The accumulation and shedding of infectious virions were severely impaired by expression of a dominant negative form of Rab11A. On the other hand, recycling endosome-mediated RNP transport was totally dispensable for virus production in nonpolarized cells. These data provide the first demonstration of the regulated intracellular trafficking events of the MV RNP complex that define the directional viral release from polarized epithelial cells.

摘要

许多病毒在其复制的多个步骤中利用宿主运输系统。麻疹病毒(MV)具有非分段负链 RNA 基因组,编码核蛋白(RNP)复合物的三个成分(N、P 和 L)、两种表面糖蛋白、一种基质蛋白和两种非结构蛋白。免疫细胞和极化上皮细胞亚群是 MV 的体内靶标,MV 从极化上皮细胞的顶膜选择性释放。然而,MV 顶膜释放的分子机制在很大程度上仍不清楚。在本研究中,使用表达荧光蛋白标记 L 蛋白的重组 MV 详细分析了 MV 的 RNP 复合物的定位和运输机制。活细胞成像分析表明,MV RNP 复合物的运输方式依赖于微管网络,并与含有 Rab11A 的再循环内体一起运输。RNP 复合物在顶膜和顶膜再循环隔室中积累。表达显性负形式的 Rab11A 严重损害了感染性病毒颗粒的积累和脱落。另一方面,再循环内体介导的 RNP 运输对于非极化细胞中的病毒产生是完全不需要的。这些数据首次证明了 MV RNP 复合物的受调控的细胞内运输事件,这些事件定义了从极化上皮细胞的定向病毒释放。

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