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通过网格蛋白介导的内吞作用将狂犬病毒摄入上皮细胞取决于肌动蛋白。

Uptake of rabies virus into epithelial cells by clathrin-mediated endocytosis depends upon actin.

机构信息

Department of Microbiology and Immunobiology.

出版信息

J Virol. 2013 Nov;87(21):11637-47. doi: 10.1128/JVI.01648-13. Epub 2013 Aug 21.

Abstract

Rabies virus (RABV) causes a fatal zoonotic encephalitis. Disease symptoms require replication and spread of the virus within neuronal cells; however, in infected animals as well as in cell culture the virus replicates in a broad range of cell types. Here we use a single-cycle RABV and a recombinant vesicular stomatitis virus (rVSV) in which the glycoprotein (G) was replaced with that of RABV (rVSV RABV G) to examine RABV uptake into the African green monkey kidney cell line BS-C-1. Combining biochemical studies and real-time spinning-disk confocal fluorescence microscopy, we show that the predominant entry pathway of RABV particles into BS-C-1 cells is clathrin dependent. Viral particles enter cells in pits with elongated structures and incomplete clathrin coats which depend upon actin to complete the internalization process. By measuring the time of internalization and the abundance of the clathrin adaptor protein AP2, we further show that the pits that internalize RABV particles are similar to those that internalize VSV particles. Pharmacological perturbations of dynamin or of actin polymerization inhibit productive infection, linking our observations on particle uptake with viral infectivity. This work extends to RABV particles the finding that clathrin-mediated endocytosis of rhabdoviruses proceeds through incompletely coated pits which depend upon actin.

摘要

狂犬病病毒(RABV)会引起致命的人畜共患脑炎。疾病症状需要病毒在神经元细胞内复制和传播;然而,在受感染的动物和细胞培养中,病毒在广泛的细胞类型中复制。在这里,我们使用单周期 RABV 和一种重组的水疱性口炎病毒(rVSV),其中糖蛋白(G)被 RABV 的糖蛋白取代(rVSV RABV G),以研究 RABV 进入非洲绿猴肾细胞系 BS-C-1 的摄取情况。结合生化研究和实时旋转盘共聚焦荧光显微镜,我们表明 RABV 颗粒进入 BS-C-1 细胞的主要进入途径是网格蛋白依赖性的。病毒颗粒进入细胞时会形成带有细长结构和不完全网格蛋白包被的凹陷,这些凹陷依赖于肌动蛋白来完成内化过程。通过测量内化时间和网格蛋白衔接蛋白 AP2 的丰度,我们进一步表明,内化 RABV 颗粒的凹陷与内化 VSV 颗粒的凹陷相似。肌球蛋白或肌动蛋白聚合的药理学干扰会抑制病毒的有效感染,将我们对颗粒摄取的观察与病毒感染力联系起来。这项工作将网格蛋白介导的 RABV 颗粒内吞作用通过不完全包被的凹陷进行,该过程依赖于肌动蛋白,这一发现扩展到了 RABV 颗粒。

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