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CCG1/TAF(II)250相互作用因子B(CIB)的晶体结构

The crystal structure of CCG1/TAF(II)250-interacting factor B (CIB).

作者信息

Padmanabhan Balasundaram, Kuzuhara Takashi, Adachi Naruhiko, Horikoshi Masami

机构信息

Horikoshi Gene Selector Project, Exploratory Research for Advanced Technology, Japan Science and Technology Corporation, 5-9-6 Tokodai, Tsukuba, Ibaraki 300-2635, Japan.

出版信息

J Biol Chem. 2004 Mar 5;279(10):9615-24. doi: 10.1074/jbc.M312165200. Epub 2003 Dec 11.

Abstract

The general transcription initiation factor TFIID and its interactors play critical roles in regulating the transcription from both naked and chromatin DNA. We have isolated a novel TFIID interactor that we denoted as CCG1/TAF(II)250-interacting factor B (CIB). We show here that CIB activates transcription. To further understand the function of this protein, we determined its crystal structure at 2.2-Angstroms resolution. The tertiary structure of CIB reveals an alpha/beta-hydrolase fold that resembles structures in the prokaryotic alpha/beta-hydrolase family proteins. It is not similar in structure or primary sequence to any eukaryotic transcription or chromatin factors that have been reported to date. CIB possesses a conserved catalytic triad that is found in other alpha/beta-hydrolases, and our in vitro studies confirmed that it bears hydrolase activity. However, CIB differs from other alpha/beta-hydrolases in that it lacks a binding site excursion, which facilitates the substrate selectivity of the other alpha/beta-hydrolases. Further functional characterization of CIB based on its tertiary structure and through biochemical studies may provide novel insights into the mechanisms that regulate eukaryotic transcription.

摘要

通用转录起始因子TFIID及其相互作用蛋白在调控裸露DNA和染色质DNA的转录过程中发挥着关键作用。我们分离出了一种新型的TFIID相互作用蛋白,将其命名为CCG1/TAF(II)250相互作用因子B(CIB)。我们在此表明CIB可激活转录。为了进一步了解该蛋白的功能,我们测定了其分辨率为2.2埃的晶体结构。CIB的三级结构揭示了一种α/β水解酶折叠,类似于原核α/β水解酶家族蛋白中的结构。其结构和一级序列与迄今为止报道的任何真核转录或染色质因子均不相似。CIB拥有一个在其他α/β水解酶中发现的保守催化三联体,我们的体外研究证实它具有水解酶活性。然而,CIB与其他α/β水解酶的不同之处在于它缺乏一个结合位点偏移,而结合位点偏移有助于其他α/β水解酶的底物选择性。基于其三级结构并通过生化研究对CIB进行进一步的功能表征,可能会为调控真核转录的机制提供新的见解。

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