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通过对TFIIE-α的结构-功能研究分析TFIIE在基础转录和TFIIH介导的羧基末端结构域磷酸化中的作用。

Analysis of the role of TFIIE in basal transcription and TFIIH-mediated carboxy-terminal domain phosphorylation through structure-function studies of TFIIE-alpha.

作者信息

Ohkuma Y, Hashimoto S, Wang C K, Horikoshi M, Roeder R G

机构信息

Laboratory of Biochemistry and Molecular Biology, Rockefeller University, New York, New York 10021, USA.

出版信息

Mol Cell Biol. 1995 Sep;15(9):4856-66. doi: 10.1128/MCB.15.9.4856.

DOI:10.1128/MCB.15.9.4856
PMID:7651404
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC230731/
Abstract

The general transcription factor TFIIE recruits TFIIH at a late stage of transcription initiation complex formation and markedly stimulates TFIIH-dependent phosphorylation of the carboxy-terminal domain (CTD) of RNA polymerase II. To study this function of TFIIE in more detail, systematic deletion mutations were introduced into the large subunit of TFIIE (TFIIE-alpha) and were analyzed with regard to their effects on TFIIH-dependent CTD phosphorylation, TFIIE-dependent basal and enhancer-dependent transcription, and interactions of TFIIE-alpha with both TFIIE-beta and TFIIH. The amino (N)-terminal half of TFIIE-alpha, which possesses several putative structural motifs, was sufficient for the phosphorylation and transcription activities and for TFIIE-beta interactions, whereas a site effecting both strong interactions with TFIIH and large stimulatory effects on transcription and CTD phosphorylation was localized to an acidic region near the carboxy (C) terminus. The fact that these activities appear to be tightly linked supports the idea that TFIIE interacts physically and functionally with TFIIH and that CTD phosphorylation is essential for transcription under normal conditions. The present results suggest that TFIIE, via its effect on TFIIH, may act as a checkpoint for formation of a preinitiation complex.

摘要

通用转录因子TFIIE在转录起始复合物形成的后期招募TFIIH,并显著刺激RNA聚合酶II羧基末端结构域(CTD)的TFIIH依赖性磷酸化。为了更详细地研究TFIIE的这一功能,将系统性缺失突变引入TFIIE的大亚基(TFIIE-α),并分析其对TFIIH依赖性CTD磷酸化、TFIIE依赖性基础转录和增强子依赖性转录以及TFIIE-α与TFIIE-β和TFIIH相互作用的影响。TFIIE-α的氨基(N)末端一半具有几个假定的结构基序,足以支持磷酸化和转录活性以及与TFIIE-β的相互作用,而一个对与TFIIH的强相互作用以及对转录和CTD磷酸化有巨大刺激作用的位点位于羧基(C)末端附近的一个酸性区域。这些活性似乎紧密相连,这一事实支持了TFIIE在物理和功能上与TFIIH相互作用以及CTD磷酸化在正常条件下对转录至关重要的观点。目前的结果表明,TFIIE可能通过其对TFIIH的作用,作为起始前复合物形成的一个检查点。

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本文引用的文献

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