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选择性共调节因子对雌激素受体活性的调控

Modulation of estrogen receptor activity by selective coregulators.

作者信息

Martini Paolo G V, Katzenellenbogen Benita S

机构信息

Department of Molecular and Integrative Physiology, College of Medicine, University of Illinois, 524 Burrill Hall, 407 South Goodwin Avenue, Urbana, IL 61801, USA.

出版信息

J Steroid Biochem Mol Biol. 2003 Jun;85(2-5):117-22. doi: 10.1016/s0960-0760(03)00207-3.

Abstract

The estrogen receptor (ER), a member of the nuclear hormone receptor superfamily, is a hormone-regulated transcription factor that mediates the effects of estrogens and antiestrogens in breast cancer and other estrogen target cells. Because of the role of estrogens in promoting the growth and progression of breast cancer, there is great interest in exploring ways to functionally inactivate the ER, thereby suppressing ER-mediated gene expression and cell proliferation. These approaches have involved the use of antiestrogens such as tamoxifen, dominant negative ERs and, more recently, the use of corepressors. Through the use of two-hybrid screening, we have recently identified a selective repressor of estrogen receptor activity (REA). This protein is recruited to the hormone-occupied ER and selectively represses its transcriptional activity but not the other steroid and non-steroid nuclear receptors. REA also interacts with a protein, prothymosin-alpha (PTalpha), that selectively enhances ER transcriptional activity by recruiting the repressive REA protein away from ER. Analysis of the mechanisms underlying the activities of these two proteins highlights a new role for REA and PTalpha as activity-modulating proteins that confer receptor specificity.

摘要

雌激素受体(ER)是核激素受体超家族的成员,是一种激素调节的转录因子,介导雌激素和抗雌激素在乳腺癌及其他雌激素靶细胞中的作用。由于雌激素在促进乳腺癌生长和进展中的作用,人们对探索使ER功能失活的方法非常感兴趣,从而抑制ER介导的基因表达和细胞增殖。这些方法包括使用抗雌激素如他莫昔芬、显性负性ER,以及最近使用的共抑制因子。通过双杂交筛选,我们最近鉴定出一种雌激素受体活性的选择性抑制因子(REA)。这种蛋白质被募集到与激素结合的ER上,并选择性地抑制其转录活性,但不影响其他类固醇和非类固醇核受体。REA还与一种蛋白质,即前胸腺素α(PTα)相互作用,PTα通过将抑制性的REA蛋白从ER上募集走,从而选择性地增强ER的转录活性。对这两种蛋白质活性潜在机制的分析突出了REA和PTα作为赋予受体特异性的活性调节蛋白的新作用。

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