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能够在哺乳动物细胞中进行持续非细胞病变性复制的RNA复制子的筛选。

Selection of RNA replicons capable of persistent noncytopathic replication in mammalian cells.

作者信息

Frolov I, Agapov E, Hoffman T A, Prágai B M, Lippa M, Schlesinger S, Rice C M

机构信息

Department of Molecular Microbiology, Washington University School of Medicine, St. Louis, Missouri 63110-1093, USA.

出版信息

J Virol. 1999 May;73(5):3854-65. doi: 10.1128/JVI.73.5.3854-3865.1999.

Abstract

The natural life cycle of alphaviruses, a group of plus-strand RNA viruses, involves transmission to vertebrate hosts via mosquitoes. Chronic infections are established in mosquitoes (and usually in mosquito cell cultures), but infection of susceptible vertebrate cells typically results in rapid shutoff of host mRNA translation and cell death. Using engineered Sindbis virus RNA replicons expressing puromycin acetyltransferase as a dominant selectable marker, we identified mutations allowing persistent, noncytopathic replication in BHK-21 cells. Two of these adaptive mutations involved single-amino-acid substitutions in the C-terminal portion of nsP2, the viral helicase-protease. At one of these loci, nsP2 position 726, numerous substitution mutations were created and characterized in the context of RNA replicons and infectious virus. Our results suggest a direct correlation between the level of viral RNA replication and cytopathogenicity. This work also provides a series of alphavirus replicons for noncytopathic gene expression studies (E. V. Agapov, I. Frolov, B. D. Lindenbach, B. M. Prágai, S. Schlesinger, and C. M. Rice, Proc. Natl. Acad. Sci. USA 95:12989-12994, 1998) and a general strategy for selecting RNA viral mutants adapted to different cellular environments.

摘要

甲病毒是一类正链RNA病毒,其天然生命周期包括通过蚊子传播给脊椎动物宿主。甲病毒能在蚊子(通常也能在蚊子细胞培养物中)建立慢性感染,但易感脊椎动物细胞感染甲病毒通常会导致宿主mRNA翻译迅速停止和细胞死亡。我们利用表达嘌呤霉素乙酰转移酶作为显性选择标记的工程化辛德毕斯病毒RNA复制子,鉴定出了能在BHK - 21细胞中持续、非细胞病变性复制的突变。其中两个适应性突变涉及病毒解旋酶 - 蛋白酶nsP2 C末端部分的单氨基酸替换。在其中一个位点,即nsP2的726位,在RNA复制子和感染性病毒的背景下创建并表征了许多替换突变。我们的结果表明病毒RNA复制水平与细胞致病性之间存在直接关联。这项工作还为非细胞病变性基因表达研究提供了一系列甲病毒复制子(E. V. 阿加波夫、I. 弗罗洛夫、B. D. 林登巴赫、B. M. 普拉盖、S. 施莱辛格和C. M. 赖斯,《美国国家科学院院刊》95:12989 - 12994,1998年),以及一种选择适应不同细胞环境的RNA病毒突变体的通用策略。

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