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感染早期的冠状病毒转录

Coronavirus transcription early in infection.

作者信息

An S, Maeda A, Makino S

机构信息

Department of Microbiology and Institute for Cellular and Molecular Biology, The University of Texas at Austin, Austin, Texas 78712-1095, USA.

出版信息

J Virol. 1998 Nov;72(11):8517-24. doi: 10.1128/JVI.72.11.8517-8524.1998.

Abstract

We studied the accumulation kinetics of murine coronavirus mouse hepatitis virus (MHV) RNAs early in infection by using cloned MHV defective interfering (DI) RNA that contained an intergenic sequence from which subgenomic DI RNA is synthesized in MHV-infected cells. Genomic DI RNA and subgenomic DI RNA accumulated at a constant ratio from 3 to 11 h postinfection (p.i.) in the cells infected with MHV-containing DI particles. Earlier, at 1 h p.i., this ratio was not constant; only genomic DI RNA accumulated, indicating that MHV RNA replication, but not MHV RNA transcription, was active during the first hour of MHV infection. Negative-strand genomic DI RNA and negative-strand subgenomic DI RNA were first detectable at 1 and 3 h p.i., respectively, and the amounts of both RNAs increased gradually until 6 h p.i. These data showed that at 2 h p.i., subgenomic DI RNA was undergoing synthesis in the cells in which negative-strand subgenomic DI RNA was undetectable. These data, therefore, signify that negative-strand genomic DI RNA, but not negative-strand subgenomic DI RNA, was an active template for subgenomic DI RNA synthesis early in infection.

摘要

我们通过使用克隆的鼠冠状病毒小鼠肝炎病毒(MHV)缺陷干扰(DI)RNA研究了感染早期鼠冠状病毒小鼠肝炎病毒(MHV)RNA的积累动力学,该DI RNA包含一个基因间序列,在MHV感染的细胞中可从该序列合成亚基因组DI RNA。在感染含MHV DI颗粒的细胞中,基因组DI RNA和亚基因组DI RNA在感染后3至11小时(p.i.)以恒定比例积累。更早的时候,在感染后1小时,这个比例并不恒定;只有基因组DI RNA积累,这表明在MHV感染后的第一个小时,MHV RNA复制活跃,但MHV RNA转录不活跃。负链基因组DI RNA和负链亚基因组DI RNA分别在感染后1小时和3小时首次被检测到,并且两种RNA的量在感染后6小时之前逐渐增加。这些数据表明,在感染后2小时,亚基因组DI RNA正在负链亚基因组DI RNA未被检测到的细胞中进行合成。因此,这些数据表明,负链基因组DI RNA而非负链亚基因组DI RNA是感染早期亚基因组DI RNA合成的活性模板。

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Coronavirus transcription early in infection.感染早期的冠状病毒转录
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