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三磷酸溴尿苷抑制痘苗病毒的转录终止和mRNA释放。

Bromouridine triphosphate inhibits transcription termination and mRNA release by vaccinia virions.

作者信息

Shuman S, Moss B

机构信息

Program in Molecular Biology, Sloan-Kettering Institute, New York, New York 10021.

出版信息

J Biol Chem. 1989 Dec 15;264(35):21356-60.

PMID:2592381
Abstract

Termination of transcription in vitro by purified vaccinia virus RNA polymerase occurs downstream of a cis-acting signal UUUUUNU in the nascent RNA strand and requires a trans-acting termination factor, VTF, that is associated with the viral mRNA capping enzyme. Factor-dependent termination can be inhibited specifically by incorporation of BrUMP (from BrUTP) into nascent RNA in place of UMP. The relevance of VTF action to early vaccinia mRNA biogenesis was demonstrated in the present study of the effects of BrUTP on mRNA synthesis and release by permeabilized vaccinia virions. BrUMP incorporation inhibited the release of newly made transcripts from the virus particle, resulting in the accumulation of transcripts within virus cores. This effect was observed also with IUMP, but not with BrCMP or IMP incorporation. Transcripts synthesized in the presence of BrUTP were heterogeneous in size and severalfold larger than transcripts made in the presence of UTP. The progressive increase in the size of the core-associated, BrUMP-containing transcripts indicated that they were still engaged by elongating RNA polymerase. These results are consistent with a predominant pathway of mRNA 3'-end formation by virions that involves VTF-dependent transcription termination. These data do not support an alternative model of 3'-end formation by endonucleolytic cleavage of larger RNA precursors.

摘要

纯化的痘苗病毒RNA聚合酶在体外转录的终止发生在新生RNA链中顺式作用信号UUUUUNU的下游,并且需要一种反式作用终止因子VTF,它与病毒mRNA加帽酶相关。通过将BrUMP(来自BrUTP)掺入新生RNA中取代UMP,可以特异性抑制因子依赖性终止。在本研究中,通过BrUTP对通透化痘苗病毒粒子的mRNA合成和释放的影响,证明了VTF作用与早期痘苗mRNA生物合成的相关性。掺入BrUMP抑制了新合成的转录本从病毒颗粒中的释放,导致转录本在病毒核心内积累。用IUMP掺入也观察到这种效果,但用BrCMP或IMP掺入则未观察到。在BrUTP存在下合成的转录本大小不均一,比在UTP存在下合成的转录本大几倍。与核心相关的、含BrUMP的转录本大小的逐渐增加表明它们仍与延伸的RNA聚合酶结合。这些结果与病毒粒子形成mRNA 3'末端的主要途径一致,该途径涉及VTF依赖性转录终止。这些数据不支持通过较大RNA前体的内切核酸酶切割形成3'末端的替代模型。

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