Teterina N L, Zhou W D, Cho M W, Ehrenfeld E
Department of Molecular Biology and Biochemistry, School of Biological Sciences, University of California, Irvine 92717, USA.
J Virol. 1995 Jul;69(7):4245-54. doi: 10.1128/JVI.69.7.4245-4254.1995.
Poliovirus (PV) 2C protein is a nonstructural polypeptide involved in viral RNA replication, whose biochemical activity(ies) in this process has not been defined. By using site-directed mutagenesis, it was shown previously that disruption of nucleotide-binding motifs present in this protein abolished viral RNA synthesis (C. Mirzayan and E. Wimmer, Virology 189:547-555, 1992; N. L. Teterina, K. M. Kean, E. Gorbalenya, V. I. Agol, and M. Girard, J. Gen. Virol. 73:1977-1986, 1992). We have tested whether PV 2C or 2BC protein provided in trans could rescue the replication of these mutated genomes. Rescuing proteins were provided either by cotransfection with helper chimeric PV-coxsackievirus genomes or by expression in cells with a vaccinia virus-T7 RNA polymerase transient-expression system. We report here that replication of mutated RNAs genomes was poorly supported in trans both by helper genomes and by expressed 2C or 2BC proteins. Similarly, very inefficient complementation was observed for two mutated genomes with lethal lesions in 3D polymerase coding sequence. Our results indicate that poliovirus RNA replication shows marked preference for proteins contributed in cis.
脊髓灰质炎病毒(PV)2C蛋白是一种参与病毒RNA复制的非结构多肽,其在此过程中的生化活性尚未明确。通过定点诱变,先前已表明破坏该蛋白中存在的核苷酸结合基序会消除病毒RNA合成(C.米尔扎扬和E.维默,《病毒学》189:547 - 555,1992;N.L.捷捷里娜、K.M.基恩、E.戈尔巴列尼亚、V.I.阿戈尔和M.吉拉德,《普通病毒学杂志》73:1977 - 1986,1992)。我们测试了反式提供的PV 2C或2BC蛋白是否能挽救这些突变基因组的复制。挽救蛋白通过与辅助嵌合PV - 柯萨奇病毒基因组共转染或通过痘苗病毒 - T7 RNA聚合酶瞬时表达系统在细胞中表达来提供。我们在此报告,辅助基因组以及表达的2C或2BC蛋白对突变RNA基因组的反式复制支持不佳。同样,对于在3D聚合酶编码序列中具有致死性损伤的两个突变基因组,观察到非常低效的互补作用。我们的结果表明,脊髓灰质炎病毒RNA复制对顺式提供的蛋白表现出明显的偏好。
