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Rb增强核受体的p160/SRC共激活因子依赖性活性及激素反应性。

Rb enhances p160/SRC coactivator-dependent activity of nuclear receptors and hormone responsiveness.

作者信息

Batsché Eric, Desroches Julien, Bilodeau Steve, Gauthier Yves, Drouin Jacques

机构信息

Laboratoire de Génétique Moléculaire, Institut de Recherches Cliniques de Montréal, Quebec, Canada.

出版信息

J Biol Chem. 2005 May 20;280(20):19746-56. doi: 10.1074/jbc.M413428200. Epub 2005 Mar 14.

Abstract

The retinoblastoma tumor suppressor protein (Rb) is best known as a repressor of genes involved in cell cycle progression. Rb has also been implicated in activation of transcription, in particular by nuclear receptors (NRs) and by differentiation-related transcription factors, but the relevance of this activity is unclear. We show that Rb and the related proteins p107 and p130 enhance the activity of NRs related to NGFI-B (Nur factors) through direct interactions with NGFI-B and SRC-2. Although recruitment of SRC/p160 coactivators to the NGFI-B AF1 domain is independent of Rb, its presence enhances SRC-dependent transcription. Rb potentiation of SRC coactivators is exerted on a subset (Nur factors, hepatocyte nuclear factor-4 (HNF-4), SF-1, and ER) but not all NRs. The levels of Rb-related proteins modulate hormone responsiveness of the NGFI-B-dependent pituitary proopiomelanocortin gene and HNF-4-dependent transcription during enterocyte differentiation. Increased Rb expression upon cell differentiation may promote differentiated functions, at least in part, by potentiation of NR activity.

摘要

视网膜母细胞瘤肿瘤抑制蛋白(Rb)最为人所知的是作为参与细胞周期进程的基因的阻遏物。Rb还与转录激活有关,特别是通过核受体(NRs)和与分化相关的转录因子,但这种活性的相关性尚不清楚。我们发现,Rb以及相关蛋白p107和p130通过与NGFI-B和SRC-2直接相互作用,增强了与NGFI-B相关的NRs(Nur因子)的活性。虽然将SRC/p160共激活因子募集到NGFI-B的AF1结构域与Rb无关,但其存在增强了SRC依赖的转录。Rb对SRC共激活因子的增强作用作用于一部分(Nur因子、肝细胞核因子-4(HNF-4)、SF-1和雌激素受体(ER))而非所有的NRs。Rb相关蛋白的水平在肠细胞分化过程中调节NGFI-B依赖的垂体促肾上腺皮质激素原基因的激素反应性和HNF-4依赖的转录。细胞分化时Rb表达增加可能至少部分地通过增强NR活性来促进分化功能。

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