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小鼠冠状病毒中前导mRNA融合的异常异质性:对RNA转录和重组机制的启示

Unusual heterogeneity of leader-mRNA fusion in a murine coronavirus: implications for the mechanism of RNA transcription and recombination.

作者信息

Zhang X, Lai M M

机构信息

Howard Hughes Medical Institute, University of Southern California School of Medicine, Los Angeles 90033-1054.

出版信息

J Virol. 1994 Oct;68(10):6626-33. doi: 10.1128/JVI.68.10.6626-6633.1994.

Abstract

Coronavirus mRNA transcription was thought to be regulated by the interaction between the leader RNA and the intergenic sequence (IS), probably involving direct RNA-RNA interactions between complementary sequences. In this study, we found that a particular strain of mouse hepatitis virus, JHM2c, which has a deletion of a 9-nucleotide (nt) sequence (UUUAUAAAC) immediately downstream of the leader RNA, transcribed subgenomic mRNA species containing a whole array of heterogeneous leader fusion sites. Using a transfected defective interfering RNA which contains an IS and a reporter (chloramphenicol acetyltransferase) gene and JHM2c as a helper virus, we demonstrated that subgenomic mRNAs transcribed from the defective interfering RNAs were extremely heterogeneous. The leader-mRNA fusion sites in this virus can be grouped into five types. In type I, the leader is fused with the consensus IS of the template RNA at a site within the UCUAA repeats, consistent with the classical model of discontinuous transcription. In type II, the leader is fused with the consensus IS as in type I, but the leader of mRNA contains some nucleotide substitutions within the UCUAA repeats. In type III, the leader is fused with mRNAs at a site either upstream or downstream of the consensus IS. The sequences around the fusion sites bear little or no homology to the leader. As a result, mRNAs contain sequences complementary to the template sequences upstream of the IS or have sequence deletions downstream of the IS. In type IV, the leader is fused to the IS at the 9-nt sequence immediately downstream of the UCUAA repeats. In type V, the leader-mRNA fusion site contains a duplication of a portion of the leader sequence or an insertion of nontemplated sequences which are not present in either leader or template RNA. These patterns of leader-mRNA fusion resemble the aberrant homologous recombination frequently seen in other RNA viruses. The degree of heterogeneity of leader fusion sites is dependent on the sequences of both the leader RNA and IS. These results suggest that leader-mRNA fusion in coronavirus transcription does not require direct RNA-RNA interaction between complementary sequences. A modified model of RNA transcription and recombination based on protein-RNA and protein-protein interactions is proposed. This study also provides a paradigm for aberrant homologous recombination.

摘要

冠状病毒的mRNA转录被认为是由前导RNA与基因间序列(IS)之间的相互作用调控的,可能涉及互补序列之间直接的RNA-RNA相互作用。在本研究中,我们发现一种特定的小鼠肝炎病毒株JHM2c,其在前导RNA下游紧邻处缺失了一个9核苷酸(nt)序列(UUUAUAAAC),转录出的亚基因组mRNA种类包含一系列异质的前导融合位点。使用一种转染的缺陷干扰RNA,其包含一个IS和一个报告基因(氯霉素乙酰转移酶)以及JHM2c作为辅助病毒,我们证明从缺陷干扰RNA转录出的亚基因组mRNA极其异质。该病毒中的前导-mRNA融合位点可分为五种类型。在I型中,前导序列在UCUAA重复序列内的一个位点与模板RNA的共有IS融合,这与经典的不连续转录模型一致。在II型中,前导序列与I型一样与共有IS融合,但mRNA的前导序列在UCUAA重复序列内含有一些核苷酸替换。在III型中,前导序列在共有IS的上游或下游位点与mRNA融合。融合位点周围的序列与前导序列几乎没有同源性。结果,mRNA包含与IS上游模板序列互补的序列或在IS下游有序列缺失。在IV型中,前导序列在UCUAA重复序列下游紧邻的9核苷酸序列处与IS融合。在V型中,前导-mRNA融合位点包含前导序列一部分的重复或非模板序列的插入,这些序列在前导RNA或模板RNA中均不存在。这些前导-mRNA融合模式类似于在其他RNA病毒中常见的异常同源重组。前导融合位点的异质程度取决于前导RNA和IS的序列。这些结果表明,冠状病毒转录中的前导-mRNA融合不需要互补序列之间直接的RNA-RNA相互作用。基于蛋白质-RNA和蛋白质-蛋白质相互作用,提出了一种RNA转录和重组的改进模型。本研究还为异常同源重组提供了一个范例。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5cf1/237083/e3a14dc4a012/jvirol00019-0504-a.jpg

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