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在表达核受体共激活因子的雌性小鼠下丘脑中,雌二醇优先诱导孕激素受体-A(PR-A)而不是 PR-B。

Estradiol Preferentially Induces Progestin Receptor-A (PR-A) Over PR-B in Cells Expressing Nuclear Receptor Coactivators in the Female Mouse Hypothalamus.

机构信息

Neuroscience Program, Wellesley College , Wellesley, Massachusetts 02481.

Department of Molecular and Cellular Biology, Baylor College of Medicine , Houston, Texas 77030.

出版信息

eNeuro. 2015 Aug 13;2(4). doi: 10.1523/ENEURO.0012-15.2015. eCollection 2015 Jul-Aug.

Abstract

Estrogens act in brain to profoundly influence neurogenesis, sexual differentiation, neuroprotection, cognition, energy homeostasis, and female reproductive behavior and physiology through a variety of mechanisms, including the induction of progestin receptors (PRs). PRs are expressed as two isoforms, PR-A and PR-B, that have distinct functions in physiology and behavior. Because these PR isoforms cannot be distinguished using cellular resolution techniques, the present study used isoform-specific null mutant mice that lack PR-A or PR-B for the first time to investigate whether 17β-estradiol benzoate (EB) regulates the differential expression of the PR isoforms in the ventromedial nucleus of the hypothalamus (VMN), arcuate nucleus, and medial preoptic area, brain regions that are rich in EB-induced PRs. Interestingly, EB induced more PR-A than PR-B in all three brain regions, suggesting that PR-A is the predominant isoform in these regions. Given that steroid receptor coactivator (SRC)-1 and SRC-2 are important in estrogen receptor (ER)-dependent transcription in brain, including PR induction, we tested whether the expression of these coactivators was correlated with PR isoform expression. The majority of EB-induced PR cells expressed both SRC-1 and SRC-2 in the three brain regions of all genotypes. Interestingly, the intensity of PR-A immunoreactivity correlated with SRC-2 expression in the VMN, providing a potential mechanism for selective ER-mediated transactivation of PR-A over PR-B in a brain region-specific manner. In summary, these novel findings indicate that estrogens differentially regulate PR-A and PR-B expression in the female hypothalamus, and provide a mechanism by which steroid action in brain can selectively modulate behavior and physiology.

摘要

雌激素通过多种机制在大脑中发挥作用,深刻影响神经发生、性分化、神经保护、认知、能量平衡以及女性生殖行为和生理,包括诱导孕激素受体(PR)。PR 以两种同工型表达,即 PR-A 和 PR-B,它们在生理和行为中具有不同的功能。由于这些 PR 同工型不能使用细胞分辨率技术区分,本研究首次使用同工型特异性缺失突变小鼠,缺乏 PR-A 或 PR-B,首次研究 17β-雌二醇苯甲酸酯(EB)是否调节下丘脑腹内侧核(VMN)、弓状核和中脑前脑区中 PR 同工型的差异表达,这些脑区富含 EB 诱导的 PR。有趣的是,EB 在所有三个脑区诱导的 PR-A 多于 PR-B,表明 PR-A 是这些区域的主要同工型。鉴于类固醇受体共激活剂(SRC)-1 和 SRC-2 在脑内雌激素受体(ER)依赖性转录中很重要,包括 PR 诱导,我们测试了这些共激活剂的表达是否与 PR 同工型表达相关。在所有基因型的三个脑区中,大多数 EB 诱导的 PR 细胞均表达 SRC-1 和 SRC-2。有趣的是,PR-A 免疫反应性的强度与 VMN 中 SRC-2 的表达相关,为 ER 介导的 PR-A 选择性反式激活提供了一种潜在的机制,这种选择性反式激活以脑区特异性的方式发生。总之,这些新发现表明雌激素在女性下丘脑以不同的方式调节 PR-A 和 PR-B 的表达,并提供了一种机制,说明类固醇在脑内的作用可以选择性地调节行为和生理。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ed76/4596027/c81dedd8ebbb/enu0041500980001.jpg

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