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核受体共激活因子:多种酶、多种复合物、多种功能。

Nuclear receptor coactivators: multiple enzymes, multiple complexes, multiple functions.

作者信息

McKenna N J, Xu J, Nawaz Z, Tsai S Y, Tsai M J, O'Malley B W

机构信息

Department of Cell Biology, Baylor College of Medicine, Houston, TX 77030, USA.

出版信息

J Steroid Biochem Mol Biol. 1999 Apr-Jun;69(1-6):3-12. doi: 10.1016/s0960-0760(98)00144-7.

Abstract

Nuclear receptors are ligand-inducible transcription factors which mediate the physiological effects of steroid, thyroid and retinoid hormones. By regulating the assembly of a transcriptional preinitiation complex at the promoter of target genes, they enhance the expression of these genes in response to hormone. Recent evidence suggests that nuclear receptors act in part by recruiting multiple coregulator proteins which may have specific functions during transcriptional initiation. Liganded receptors recruit members of the SRC family, a group of structurally and functionally related transcriptional coactivators. Receptors also interact with the transcriptional cointegrators p300 and CBP, which are proposed to integrate diverse afferent signals at hormone-regulated promoters. p300/CBP and members of the SRC coactivator family have intrinsic histone acetyltransferase activity which is believed to disrupt the nucleosomal structure at these promoters. Other nuclear receptor coactivators include a member of the SWI/SNF complex, BRG-1, which couples ATP hydrolysis to chromatin remodelling, and the E3 ubiquitin-protein ligases E6-AP and RPF-1. Finally, nuclear receptor coactivators appear to be organized into preformed subcomplexes, an arrangement that may facilitate their efficient assembly into diverse higher order configurations.

摘要

核受体是配体诱导型转录因子,介导类固醇、甲状腺激素和视黄酸的生理效应。通过调节靶基因启动子处转录起始前复合物的组装,它们响应激素增强这些基因的表达。最近的证据表明,核受体部分通过招募多种共调节蛋白发挥作用,这些共调节蛋白在转录起始过程中可能具有特定功能。配体结合的受体招募SRC家族成员,这是一组结构和功能相关的转录共激活因子。受体还与转录共整合因子p300和CBP相互作用,它们被认为在激素调节的启动子处整合各种传入信号。p300/CBP和SRC共激活因子家族成员具有内在的组蛋白乙酰转移酶活性,据信这种活性会破坏这些启动子处的核小体结构。其他核受体共激活因子包括SWI/SNF复合物的一个成员BRG-1,它将ATP水解与染色质重塑偶联,以及E3泛素蛋白连接酶E6-AP和RPF-1。最后,核受体共激活因子似乎被组织成预先形成的亚复合物,这种排列可能有助于它们有效地组装成各种更高阶的结构。

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