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TIF2,一种160千道尔顿的转录调节因子,参与核受体配体依赖性激活功能AF-2的调节。

TIF2, a 160 kDa transcriptional mediator for the ligand-dependent activation function AF-2 of nuclear receptors.

作者信息

Voegel J J, Heine M J, Zechel C, Chambon P, Gronemeyer H

机构信息

Institut de Génétique et de Biologie Moléculaire et Cellulaire (IGBMC), CNRS/INSERM/ULP/Collége de France, Illkrich, Strasbourg, France.

出版信息

EMBO J. 1996 Jul 15;15(14):3667-75.

Abstract

Nuclear receptors (NRs) act as ligand-inducible transcription factors which regulate the expression of target genes upon binding to cognate response elements. The ligand-dependent activity of the NR activation function AF-2 is believed to be mediated to the transcription machinery through transcriptional mediators/intermediary factors (TIFs). We report here the cloning of the 160 kDa human nuclear protein TIF2, which exhibits all properties expected for a mediator of AF-2: (i) it interacts in vivo with NRs in an agonist-dependent manner; (ii) it binds directly to the ligand-binding domains (LBDs) of NRs in an agonist- and AF-2-integrity-dependent manner in vitro; (iii) it harbours an autonomous transcriptional activation function; (iv) it relieves nuclear receptor autosquelching; and (v) it enhances the activity of some nuclear receptor AF-2s when overexpressed in mammalian cells. TIF2 exhibits partial sequence homology with the recently isolated steroid receptor coactivator SRC-1, indicating the existence of a novel gene family of nuclear receptor transcriptional mediators.

摘要

核受体(NRs)作为配体诱导型转录因子,在与同源反应元件结合后调节靶基因的表达。NR激活功能AF-2的配体依赖性活性被认为是通过转录介质/中介因子(TIFs)介导至转录机制的。我们在此报告160 kDa人核蛋白TIF2的克隆,其表现出作为AF-2介质所预期的所有特性:(i)它在体内以激动剂依赖性方式与NRs相互作用;(ii)它在体外以激动剂和AF-2完整性依赖性方式直接结合NRs的配体结合域(LBDs);(iii)它具有自主转录激活功能;(iv)它解除核受体自身抑制;以及(v)当在哺乳动物细胞中过表达时,它增强一些核受体AF-2的活性。TIF2与最近分离的类固醇受体共激活因子SRC-1表现出部分序列同源性,表明存在核受体转录介质的一个新基因家族。

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