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脊髓灰质炎病毒RNA依赖性RNA聚合酶介导的分子内和分子间尿苷酸化作用

Intramolecular and intermolecular uridylylation by poliovirus RNA-dependent RNA polymerase.

作者信息

Richards Oliver C, Spagnolo Jeannie F, Lyle John M, Vleck Susan E, Kuchta Robert D, Kirkegaard Karla

机构信息

Department of Microbiology and Immunology, Stanford University School of Medicine, 299 Campus Drive, Stanford, CA 94305-5402, USA.

出版信息

J Virol. 2006 Aug;80(15):7405-15. doi: 10.1128/JVI.02533-05.

Abstract

The 22-amino-acid protein VPg can be uridylylated in solution by purified poliovirus 3D polymerase in a template-dependent reaction thought to mimic primer formation during RNA amplification in infected cells. In the cell, the template used for the reaction is a hairpin RNA termed 2C-cre and, possibly, the poly(A) at the 3' end of the viral genome. Here, we identify several additional substrates for uridylylation by poliovirus 3D polymerase. In the presence of a 15-nucleotide (nt) RNA template, the poliovirus polymerase uridylylates other polymerase molecules in an intermolecular reaction that occurs in a single step, as judged by the chirality of the resulting phosphodiester linkage. Phosphate chirality experiments also showed that VPg uridylylation can occur by a single step; therefore, there is no obligatory uridylylated intermediate in the formation of uridylylated VPg. Other poliovirus proteins that could be uridylylated by 3D polymerase in solution were viral 3CD and 3AB proteins. Strong effects of both RNA and protein ligands on the efficiency and the specificity of the uridylylation reaction were observed: uridylylation of 3D polymerase and 3CD protein was stimulated by the addition of viral protein 3AB, and, when the template was poly(A) instead of the 15-nt RNA, the uridylylation of 3D polymerase itself became intramolecular instead of intermolecular. Finally, an antiuridine antibody identified uridylylated viral 3D polymerase and 3CD protein, as well as a 65- to 70-kDa host protein, in lysates of virus-infected human cells.

摘要

22个氨基酸的蛋白质VPg可在溶液中被纯化的脊髓灰质炎病毒3D聚合酶在模板依赖性反应中尿苷酸化,该反应被认为模拟了感染细胞中RNA扩增过程中的引物形成。在细胞中,用于该反应的模板是一种称为2C-cre的发夹RNA,可能还有病毒基因组3'端的聚腺苷酸(poly(A))。在这里,我们鉴定出脊髓灰质炎病毒3D聚合酶尿苷酸化的几种其他底物。在存在15个核苷酸(nt)的RNA模板的情况下,脊髓灰质炎病毒聚合酶在分子间反应中使其他聚合酶分子尿苷酸化,该反应一步发生,这可通过所得磷酸二酯键的手性来判断。磷酸手性实验还表明,VPg尿苷酸化可一步发生;因此,在尿苷酸化的VPg形成过程中不存在必需的尿苷酸化中间体。在溶液中可被3D聚合酶尿苷酸化的其他脊髓灰质炎病毒蛋白是病毒3CD和3AB蛋白。观察到RNA和蛋白质配体对尿苷酸化反应的效率和特异性都有强烈影响:添加病毒蛋白3AB可刺激3D聚合酶和3CD蛋白的尿苷酸化,并且当模板是聚腺苷酸(poly(A))而不是15-nt RNA时,3D聚合酶本身的尿苷酸化变成分子内而不是分子间的。最后,一种抗尿苷抗体在病毒感染的人类细胞裂解物中鉴定出尿苷酸化的病毒3D聚合酶和3CD蛋白,以及一种65至70 kDa的宿主蛋白。

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