人TFIIF中RAP30/RAP74以1.7埃分辨率呈现的新型二聚化折叠结构。

Novel dimerization fold of RAP30/RAP74 in human TFIIF at 1.7 A resolution.

作者信息

Gaiser F, Tan S, Richmond T J

机构信息

ETH Zürich, Institut fr Molekularbiologie und Biophysik, Zürich, Switzerland.

出版信息

J Mol Biol. 2000 Oct 6;302(5):1119-27. doi: 10.1006/jmbi.2000.4110.

DOI:10.1006/jmbi.2000.4110

PMID:11183778

Abstract

General transcription factor IIF (TFIIF) is required for transcription by RNA polymerase II; it consists minimally of a heterodimer of RNA polymerase-associated proteins RAP30 and RAP74. According to solution and mutagenesis studies, the multiple domains of RAP30 and RAP74 bind PolII, TFIIB, TAF250 and DNA in interactions that are essential for transcription initiation and elongation. The X-ray structure of the RAP30/RAP74 interaction domains at 1.7 A resolution reveals a novel "triple barrel" dimerization fold and suggests with mutant data that interactions with the transcription apparatus are mediated not only by this tripartite beta-barrel, but also via flexible loops and alpha and beta-structures extending from it.

摘要

通用转录因子IIF（TFIIF）是RNA聚合酶II转录所必需的；它至少由与RNA聚合酶相关的蛋白质RAP30和RAP74的异二聚体组成。根据溶液和诱变研究，RAP30和RAP74的多个结构域在转录起始和延伸所必需的相互作用中与PolII、TFIIB、TAF250和DNA结合。RAP30/RAP74相互作用结构域在1.7埃分辨率下的X射线结构揭示了一种新型的“三桶”二聚化折叠，并通过突变数据表明与转录装置的相互作用不仅由这种三方β桶介导，还通过从其延伸的柔性环以及α和β结构介导。

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人TFIIF中RAP30/RAP74以1.7埃分辨率呈现的新型二聚化折叠结构。

Novel dimerization fold of RAP30/RAP74 in human TFIIF at 1.7 A resolution.

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