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痘苗病毒的组装:利福平对病毒蛋白p65细胞内分布的影响

Assembly of vaccinia virus: effects of rifampin on the intracellular distribution of viral protein p65.

作者信息

Sodeik B, Griffiths G, Ericsson M, Moss B, Doms R W

机构信息

Cell Biology Program, European Molecular Biology Laboratory, Heidelberg, Germany.

出版信息

J Virol. 1994 Feb;68(2):1103-14. doi: 10.1128/JVI.68.2.1103-1114.1994.

Abstract

The cytoplasmic assembly of vaccinia virus is reversibly blocked by the antibiotic rifampin, leading to the accumulation of partially membrane-delineated rifampin bodies in infected cells. Rifampin-resistant vaccinia virus mutants have point mutations in the D13L gene, which is controlled by a late promoter and expresses a 65-kDa protein, designated p65. To further characterize the mechanism of rifampin inhibition and the function of p65 in virus assembly, we raised antibodies to this protein. Immunoreactive p65 was expressed at late times of infection, and neither its expression nor its turnover was affected by rifampin. Virus-associated p65 could be extracted only with denaturing detergents from purified virions, suggesting that it is an integral viral component. Immunofluorescence studies showed that p65 is localized to the sites of virus assembly. Also, immunoelectron microscopy showed p65 to be associated with viral crescents as well as spherical, immature virions, in both cases predominantly on the inner or concave surface. In the presence of rifampin, p65 was found in large, cytoplasmic inclusion bodies that were distinct from rifampin bodies. The rifampin bodies themselves were labeled with p65 antibodies only after reversal of the rifampin block, predominantly on the viral crescents which rapidly formed following removal of the drug. We propose that p65 functions as an internal scaffold in the formation of viral crescents and immature virions, analogously to the matrix proteins of other viruses.

摘要

痘苗病毒的胞质组装被抗生素利福平可逆性阻断,导致感染细胞中出现部分被膜界定的利福平体。利福平抗性痘苗病毒突变体在D13L基因中有点突变,该基因由晚期启动子控制并表达一种65 kDa的蛋白,命名为p65。为了进一步阐明利福平抑制机制以及p65在病毒组装中的功能,我们制备了针对该蛋白的抗体。免疫反应性p65在感染后期表达,其表达和周转均不受利福平影响。仅用变性去污剂才能从纯化的病毒粒子中提取与病毒相关的p65,这表明它是病毒的一个组成成分。免疫荧光研究表明,p65定位于病毒组装位点。此外,免疫电子显微镜显示p65与病毒新月体以及球形未成熟病毒粒子相关,在这两种情况下主要位于内表面或凹面。在有利福平存在的情况下,p65存在于大型胞质包涵体中,这些包涵体与利福平体不同。只有在利福平阻断作用逆转后,利福平体本身才被p65抗体标记,主要在去除药物后迅速形成的病毒新月体上。我们提出,p65在病毒新月体和未成熟病毒粒子形成过程中起内部支架的作用,类似于其他病毒的基质蛋白。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8bc0/236549/fbca6ce235d8/jvirol00011-0537-a.jpg

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