首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Ebola virus proteins NP VP35 and VP24 are essential and sufficient to mediate nucleocapsid transport
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Ebola virus proteins NP VP35 and VP24 are essential and sufficient to mediate nucleocapsid transport

机译:埃博拉病毒蛋白NPVP35和VP24对介导核衣壳转运至关重要且足够

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摘要

The intracytoplasmic movement of nucleocapsids is a crucial step in the life cycle of enveloped viruses. Determination of the viral components necessary for viral nucleocapsid transport competency is complicated by the dynamic and complex nature of nucleocapsid assembly and the lack of appropriate model systems. Here, we established a live-cell imaging system based on the ectopic expression of fluorescent Ebola virus (EBOV) fusion proteins, allowing the visualization and analysis of the movement of EBOV nucleocapsid-like structures with different protein compositions. Only three of the five EBOV nucleocapsid proteins—nucleoprotein, VP35, and VP24—were necessary and sufficient to form transport-competent nucleocapsid-like structures. The transport of these structures was found to be dependent on actin polymerization and to have dynamics that were undistinguishable from those of nucleocapsids in EBOV-infected cells. The intracytoplasmic movement of nucleocapsid-like structures was completely independent of the viral matrix protein VP40 and the viral surface glycoprotein GP. However, VP40 greatly enhanced the efficiency of nucleocapsid recruitment into filopodia, the sites of EBOV budding.
机译:核衣壳的胞质内移动是包膜病毒生命周期中的关键步骤。核衣壳装配的动态和复杂性质以及缺乏适当的模型系统,使确定病毒核衣壳转运能力所需的病毒成分变得复杂。在这里,我们基于荧光埃博拉病毒(EBOV)融合蛋白的异位表达建立了活细胞成像系统,从而可以可视化和分析具有不同蛋白组成的EBOV核衣壳样结构的运动。五个EBOV核衣壳蛋白中只有三个-核蛋白,VP35和VP24-足以形成具有运输能力的核衣壳样结构。发现这些结构的运输取决于肌动蛋白的聚合反应,并具有与EBOV感染的细胞中的核衣壳动力学没有区别的动力学。核衣壳样结构的胞质内运动完全独立于病毒基质蛋白VP40和病毒表面糖蛋白GP。但是,VP40大大提高了将核衣壳募集到丝状伪足(EBOV出芽部位)的效率。

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