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乳头多瘤空泡病毒DNA复制起始蛋白,即牛乳头瘤病毒1型E1和猿猴病毒40大T抗原,与人复制蛋白A的相互作用。

Interactions of the papovavirus DNA replication initiator proteins, bovine papillomavirus type 1 E1 and simian virus 40 large T antigen, with human replication protein A.

作者信息

Han Y, Loo Y M, Militello K T, Melendy T

机构信息

Department of Microbiology and Center for Microbial Pathogenesis, School of Medicine and Biomedical Sciences, State University of New York at Buffalo, New York, USA.

出版信息

J Virol. 1999 Jun;73(6):4899-907. doi: 10.1128/JVI.73.6.4899-4907.1999.

Abstract

Papovaviruses utilize predominantly cellular DNA replication proteins to replicate their own viral genomes. To appropriate the cellular DNA replication machinery, simian virus 40 (SV40) large T antigen (Tag) binds to three different cellular replication proteins, the DNA polymerase alpha-primase complex, the replication protein A (RPA) complex, and topoisomerase I. The functionally similar papillomavirus E1 protein has also been shown to bind to the DNA polymerase alpha-primase complex. Enzyme-linked immunoassay-based protein interaction assays and protein affinity pull-down assays were used to show that the papillomavirus E1 protein also binds to the cellular RPA complex in vitro. Furthermore, SV40 Tag was able to compete with bovine papillomavirus type 1 E1 for binding to RPA. Each of the three RPA subunits was individually overexpressed in Escherichia coli as a soluble fusion protein. These fusion proteins were used to show that the E1-RPA and Tag-RPA interactions are primarily mediated through the 70-kDa subunit of RPA. These results suggest that different viruses have evolved similar mechanisms for taking control of the cellular DNA replication machinery.

摘要

乳头瘤多瘤空泡病毒主要利用细胞DNA复制蛋白来复制其自身的病毒基因组。为了利用细胞DNA复制机制,猴病毒40(SV40)大T抗原(Tag)与三种不同的细胞复制蛋白结合,即DNA聚合酶α-引发酶复合物、复制蛋白A(RPA)复合物和拓扑异构酶I。功能相似的乳头瘤病毒E1蛋白也已被证明能与DNA聚合酶α-引发酶复合物结合。基于酶联免疫吸附测定的蛋白质相互作用分析和蛋白质亲和下拉分析表明,乳头瘤病毒E1蛋白在体外也能与细胞RPA复合物结合。此外,SV40 Tag能够与1型牛乳头瘤病毒E1竞争结合RPA。RPA的三个亚基分别在大肠杆菌中作为可溶性融合蛋白单独过表达。这些融合蛋白用于表明E1-RPA和Tag-RPA相互作用主要通过RPA的70 kDa亚基介导。这些结果表明,不同病毒已经进化出类似的机制来控制细胞DNA复制机制。

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