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通过另一种蛋白质与新生RNA相连的HIV-1 Tat蛋白激活转录。

Activation of transcription by HIV-1 Tat protein tethered to nascent RNA through another protein.

作者信息

Southgate C, Zapp M L, Green M R

机构信息

Department of Biochemistry and Molecular Biology, Harvard University, Cambridge, Massachusetts 02138.

出版信息

Nature. 1990 Jun 14;345(6276):640-2. doi: 10.1038/345640a0.

Abstract

The human immunodeficiency virus type I (HIV-1) nuclear protein Tat is a potent activator of viral gene transcription. Activation by Tat requires a cis-acting element, the transactivation response (TAR) site, located immediately downstream of the transcription start site. Several observations suggest that TAR functions as the nascent RNA product of the HIV long-terminal-repeat promoter (for a review, see ref. 6). Indeed, Tat protein and several cellular proteins bind directly to nascent TAR RNA in vitro. The significance of these in vitro interactions remains to be established. Here we report that Tat can activate transcription when bound to nascent RNA through the RNA-binding domain of another HIV-1 protein, Rev. Rev is a sequence-specific RNA-binding protein, which interacts with the viral RNA element RRE (refs 11-15). A Tat-Rev fusion protein efficiently activates transcription from an HIV-1 promoter derivative, in which TAR has been replaced by the RRE. We conclude that activation of transcription by Tat can occur by direct binding to nascent RNA, and that the sole function of TAR may be to provide a Tat-binding site. Our results further suggest that cellular proteins that bind specifically to TAR RNA or TAR DNA may not be essential for Tat-responsiveness.

摘要

I型人类免疫缺陷病毒(HIV-1)的核蛋白Tat是病毒基因转录的有效激活剂。Tat的激活需要一个顺式作用元件,即位于转录起始位点下游紧邻处的反式激活应答(TAR)位点。多项观察结果表明,TAR作为HIV长末端重复启动子的新生RNA产物发挥作用(综述见参考文献6)。实际上,Tat蛋白和几种细胞蛋白在体外可直接与新生的TAR RNA结合。这些体外相互作用的意义尚待确定。在此我们报告,当Tat通过另一种HIV-1蛋白Rev的RNA结合结构域与新生RNA结合时,它能够激活转录。Rev是一种序列特异性RNA结合蛋白,它与病毒RNA元件RRE相互作用(参考文献11 - 15)。一种Tat-Rev融合蛋白能有效激活HIV-1启动子衍生物的转录,在该衍生物中TAR已被RRE取代。我们得出结论,Tat对转录的激活可通过与新生RNA直接结合来实现,并且TAR的唯一功能可能是提供一个Tat结合位点。我们的结果进一步表明,与TAR RNA或TAR DNA特异性结合的细胞蛋白对于Tat反应性可能并非必不可少。

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