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The G-protein-coupled estrogen receptor GPER in health and disease.

机译:G蛋白偶联雌激素受体GPER在健康和疾病中的作用。

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摘要

Estrogens mediate profound effects throughout the body and regulate physiological and pathological processes in both women and men. The low prevalence of many diseases in premenopausal women is attributed to the presence of 17beta-estradiol, the predominant and most potent endogenous estrogen. In addition to endogenous estrogens, several man-made and plant-derived molecules, such as bisphenol A and genistein, also exhibit estrogenic activity. Traditionally, the actions of 17beta-estradiol are ascribed to two nuclear estrogen receptors (ERs), ERalpha and ERbeta, which function as ligand-activated transcription factors. However, 17beta-estradiol also mediates rapid signaling events via pathways that involve transmembrane ERs, such as G-protein-coupled ER 1 (GPER; formerly known as GPR30). In the past 10 years, GPER has been implicated in both rapid signaling and transcriptional regulation. With the discovery of GPER-selective ligands that can selectively modulate GPER function in vitro and in preclinical studies and with the use of Gper knockout mice, many more potential roles for GPER are being elucidated. This Review highlights the physiological roles of GPER in the reproductive, nervous, endocrine, immune and cardiovascular systems, as well as its pathological roles in a diverse array of disorders including cancer, for which GPER is emerging as a novel therapeutic target and prognostic indicator.
机译:雌激素介导整个人体的深远影响,并调节男女的生理和病理过程。绝经前女性中许多疾病的低患病率归因于17β-雌二醇的存在,这是最主要和最有效的内源性雌激素。除内源性雌激素外,几种人造和植物来源的分子,例如双酚A和染料木黄酮,也具有雌激素活性。传统上,17β-雌二醇的作用归因于两个核雌激素受体(ER),ERalpha和ERbeta,它们起配体激活的转录因子的作用。但是,17β-雌二醇还通过涉及跨膜ER的途径(例如G蛋白偶联的ER 1(GPER;以前称为GPR30))介导快速信号事件。在过去的十年中,GPER参与了快速信号传导和转录调控。随着能够在体外和临床前研究中选择性调节GPER功能的GPER选择性配体的发现,以及使用Gper基因敲除小鼠,人们正在阐明GPER的许多潜在作用。这篇综述着重介绍了GPER在生殖,神经,内分泌,免疫和心血管系统中的生理作用,以及其在包括癌症在内的各种疾病中的病理作用,GPER已成为一种新型的治疗靶点和预后指标。

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