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一种用于冠状病毒mRNA前导引物转录的体外系统。

An in vitro system for the leader-primed transcription of coronavirus mRNAs.

作者信息

Baker S C, Lai M M

机构信息

Howard Hughes Medical Institute, Department of Microbiology, University of Southern California School of Medicine, Los Angeles 90033.

出版信息

EMBO J. 1990 Dec;9(12):4173-9. doi: 10.1002/j.1460-2075.1990.tb07641.x.

Abstract

We have developed an in vitro transcription system which can utilize exogenous leader RNA for mouse hepatitis virus (MHV) 'leader-primed' mRNA transcription. Cytoplasmic extracts containing viral proteins and template RNA were prepared by lysolecithin permeabilization of MHV-infected cells. Synthetic leader RNA which differed in sequence from the endogenous leader RNA was added to the extracts and demonstrated to be incorporated into MHV mRNAs. Irrespective of the size of leader RNAs added, the exogenous leader RNA was joined to the endogenous mRNA at the same site, which corresponds to a UCUAA pentanucleotide repeat region. Only leader RNAs containing the pentanucleotide sequences could be utilized for transcription. Mismatches between the intergenic site and the exogenous leader sequence within the pentanucleotide repeat region were corrected in the in vitro system. This in vitro system thus established a novel mechanism of leader-primed transcription using exogenous RNA in trans, and suggests the involvement of a specific ribonuclease activity during coronavirus mRNA synthesis.

摘要

我们开发了一种体外转录系统,该系统可利用外源性前导RNA进行小鼠肝炎病毒(MHV)的“前导引物”mRNA转录。通过用溶血卵磷脂通透MHV感染的细胞来制备含有病毒蛋白和模板RNA的细胞质提取物。将与内源性前导RNA序列不同的合成前导RNA添加到提取物中,并证明其被整合到MHV mRNA中。无论添加的前导RNA大小如何,外源性前导RNA都在同一位点与内源性mRNA连接,该位点对应于一个UCUAA五核苷酸重复区域。只有含有五核苷酸序列的前导RNA可用于转录。在体外系统中,五核苷酸重复区域内基因间位点与外源性前导序列之间的错配得到了校正。因此,该体外系统建立了一种利用反式外源性RNA进行前导引物转录的新机制,并提示在冠状病毒mRNA合成过程中涉及一种特定的核糖核酸酶活性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/37c0/552193/2d7306603fee/emboj00239-0365-a.jpg

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