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转录差异过早终止作为冠状病毒基因表达调控的一种推测机制。

Differential premature termination of transcription as a proposed mechanism for the regulation of coronavirus gene expression.

作者信息

Konings D A, Bredenbeek P J, Noten J F, Hogeweg P, Spaan W J

机构信息

European Molecular Biology Laboratory, Heidelberg, FRG.

出版信息

Nucleic Acids Res. 1988 Nov 25;16(22):10849-60. doi: 10.1093/nar/16.22.10849.

Abstract

We propose that the different subgenomic mRNA levels of coronaviruses are controlled through differential premature termination of transcription, and are modulated by the relative strength of transcriptional initiation/blockage events. We present the complete set of sequences covering the leader encoding and intergenic regions of the MHV-A59 strain. A computer-assisted analysis of the two now complete sets of these sequences of strain IBV-M42 and MHV-A59 shows that, in contrast to the previous theory, differences amongst stabilities of intermolecular base-pairings between the leader and the intergenic regions are not sufficient to determine the mRNA gradients in both MHV and IBV infected cells. Neither can the accessibility of the interacting regions on the leader and the negative stranded genome, as revealed by secondary structure analysis, explain the mRNA levels. The nested gene organisation itself, on the other hand, could be responsible for observed mRNA levels gradually increasing with gene order. Relatively slow new initiation events at intergenic regions are proposed to block elongation of passing transcripts which, via temporary pausing, can cause premature termination of transcription. This effects longer transcripts more than shorter ones.

摘要

我们提出,冠状病毒不同亚基因组mRNA水平是通过转录的差异过早终止来控制的,并受转录起始/阻断事件相对强度的调节。我们展示了覆盖MHV-A59株前导编码区和基因间隔区的完整序列集。对IBV-M42株和MHV-A59株这两组现已完整的序列进行计算机辅助分析表明,与先前的理论相反,前导区和基因间隔区之间分子间碱基配对稳定性的差异不足以确定MHV和IBV感染细胞中的mRNA梯度。二级结构分析显示,前导区与负链基因组上相互作用区域的可及性也无法解释mRNA水平。另一方面,嵌套基因组织本身可能是观察到的mRNA水平随基因顺序逐渐增加的原因。有人提出,基因间隔区相对缓慢的新起始事件会阻断通过的转录本的延伸,这些转录本通过暂时停顿会导致转录过早终止。这对较长转录本的影响大于较短转录本。

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