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丙型肝炎病毒核心蛋白以微管和动力蛋白依赖性方式诱导脂滴重新分布。

Hepatitis C virus core protein induces lipid droplet redistribution in a microtubule- and dynein-dependent manner.

作者信息

Boulant Steeve, Douglas Mark W, Moody Laura, Budkowska Agata, Targett-Adams Paul, McLauchlan John

机构信息

MRC Virology Unit, Institute of Virology, Church Street, Glasgow G11 5JR, UK.

出版信息

Traffic. 2008 Aug;9(8):1268-82. doi: 10.1111/j.1600-0854.2008.00767.x. Epub 2008 May 17.

Abstract

Attachment of hepatitis C virus (HCV) core protein to lipid droplets (LDs) is linked to release of infectious progeny from infected cells. Core progressively coats the entire LD surface from a unique site on the organelle, and this process coincides with LD aggregation around the nucleus. We demonstrate that LD redistribution requires only core protein and is accompanied by reduced abundance of adipocyte differentiation-related protein (ADRP) on LD surfaces. Using small hairpin RNA technology, we show that knock down of ADRP has a similar phenotypic effect on LD redistribution. Hence, ADRP is crucial to maintain a disperse intracellular distribution of LDs. From additional experimental evidence, LDs are associated with microtubules and aggregate principally around the microtubule-organizing centre in HCV-infected cells. Disrupting the microtubule network or microinjecting anti-dynein antibody prevented core-mediated LD redistribution. Moreover, microtubule disruption reduced virus titres, implicating transport networks in virus assembly and release. We propose that the presence of core on LDs favours their movement towards the nucleus, possibly to increase the probability of interaction between sites of HCV RNA replication and virion assembly.

摘要

丙型肝炎病毒(HCV)核心蛋白与脂滴(LDs)的附着与感染性子代病毒从受感染细胞中的释放有关。核心蛋白从细胞器上的一个独特位点开始逐渐覆盖整个脂滴表面,这一过程与脂滴在细胞核周围的聚集同时发生。我们证明脂滴重新分布仅需要核心蛋白,并且伴随着脂滴表面脂肪细胞分化相关蛋白(ADRP)丰度的降低。使用小发夹RNA技术,我们表明敲低ADRP对脂滴重新分布具有类似的表型效应。因此,ADRP对于维持脂滴在细胞内的分散分布至关重要。从其他实验证据来看,脂滴与微管相关,并且在HCV感染的细胞中主要聚集在微管组织中心周围。破坏微管网络或显微注射抗动力蛋白抗体可阻止核心蛋白介导的脂滴重新分布。此外,微管破坏降低了病毒滴度,这表明运输网络参与病毒组装和释放。我们提出脂滴上核心蛋白的存在有利于它们向细胞核移动,可能是为了增加HCV RNA复制位点与病毒粒子组装位点之间相互作用的概率。

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