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从雌激素受体的体内基因靶向到绝经后雌激素调节的优化。

From in vivo gene targeting of oestrogen receptors to optimization of their modulation in menopause.

机构信息

INSERM U1048-I2MC, Faculté de Médecine, Université de Toulouse et CHU de Toulouse, Toulouse, France.

出版信息

Br J Pharmacol. 2012 Jan;165(1):57-66. doi: 10.1111/j.1476-5381.2011.01538.x.

Abstract

The ancestral status of oestrogen receptor (ER) in the family of the steroid receptors has probably contributed to the pleiotropic actions of oestrogens, and in particular, that of 17β-oestradiol (E2). Indeed, in addition to their well-described role in sexual development and reproduction, they influence most of the physiological processes. The pathophysiological counterpart of these actions includes prevention of osteoporosis, atheroma and type 2 diabetes, and also the promotion of uterus and breast cancer growth. Thus, the major challenge consists in uncoupling some beneficial actions from other deleterious ones, that is, selective ER modulation. Tamoxifen and raloxifene are already used, as they prevent the recurrence of breast cancer and mimic oestrogen action mainly on bone. Both E2 and tamoxifen exhibit a proliferative and, thus, a protumoural action on the endometrium. Activation of ERα and ERβ regulates target gene transcription (genomic action) through two independent activation functions, AF-1 and AF-2, but can also elicit rapid membrane-initiated steroid signals. In the present review, we attempted to summarize recent advances provided by the in vivo molecular 'dissection' of ERα, allowing the uncoupling of some of its actions and potentially paving the way to optimized selective ER modulators.

摘要

甾体激素受体家族中雌激素受体(ER)的祖先进化地位可能促成了雌激素的多效性作用,特别是 17β-雌二醇(E2)的作用。事实上,除了其在性发育和生殖方面的明确作用外,它们还影响着大多数生理过程。这些作用的病理生理学对应物包括预防骨质疏松症、动脉粥样硬化和 2 型糖尿病,以及促进子宫和乳腺癌的生长。因此,主要的挑战在于将一些有益的作用与其他有害的作用分离,即选择性 ER 调节。他莫昔芬和雷洛昔芬已经被使用,因为它们可以预防乳腺癌的复发,并主要在骨骼上模拟雌激素的作用。E2 和他莫昔芬都对子宫内膜表现出增殖作用,从而具有促肿瘤作用。ERα 和 ERβ 的激活通过两个独立的激活功能区 AF-1 和 AF-2 调节靶基因转录(基因组作用),但也可以引发快速的膜起始甾体信号。在本综述中,我们试图总结通过体内分子“剖析”ERα 所提供的最新进展,从而实现了对其部分作用的分离,并有可能为优化的选择性 ER 调节剂铺平道路。

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本文引用的文献

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