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雌激素受体α、G 蛋白偶联雌激素受体 1 和芳香化酶:在大鼠尾壳核、伏隔核核心和壳区的发育、性别和区域特异性差异。

Estrogen receptor alpha, G-protein coupled estrogen receptor 1, and aromatase: Developmental, sex, and region-specific differences across the rat caudate-putamen, nucleus accumbens core and shell.

机构信息

Department of Biological Sciences, North Carolina State University, Raleigh, North Carolina, USA.

W.M. Keck Center for Behavioral Biology, North Carolina State University, Raleigh, North Carolina, USA.

出版信息

J Comp Neurol. 2021 Mar;529(4):786-801. doi: 10.1002/cne.24978. Epub 2020 Aug 3.

Abstract

Sex steroid hormones such as 17β-estradiol (estradiol) regulate neuronal function by binding to estrogen receptors (ERs), including ERα and GPER1, and through differential production via the enzyme aromatase. ERs and aromatase are expressed across the nervous system, including in the striatal brain regions. These regions, comprising the nucleus accumbens core, shell, and caudate-putamen, are instrumental for a wide-range of functions and disorders that show sex differences in phenotype and/or incidence. Sex-specific estrogen action is an integral component for generating these sex differences. A distinctive feature of the striatal regions is that in adulthood neurons exclusively express membrane but not nuclear ERs. This long-standing finding dominates models of estrogen action in striatal regions. However, the developmental etiology of ER and aromatase cellular expression in female and male striatum is unknown. This omission in knowledge is important to address, as developmental stage influences cellular estrogenic mechanisms. Thus, ERα, GPER1, and aromatase cellular immunoreactivity was assessed in perinatal, prepubertal, and adult female and male rats. We tested the hypothesis that ERα, GPER1, and aromatase exhibits sex, region, and age-specific differences, including nuclear expression. ERα exhibits nuclear expression in all three striatal regions before adulthood and disappears in a region- and sex-specific time-course. Cellular GPER1 expression decreases during development in a region- but not sex-specific time-course, resulting in extranuclear expression by adulthood. Somatic aromatase expression presents at prepuberty and increases by adulthood in a region- but not sex-specific time-course. These data indicate that developmental period exerts critical sex-specific influences on striatal cellular estrogenic mechanisms.

摘要

甾体性激素,如 17β-雌二醇(雌二醇),通过与雌激素受体(ERs)结合,包括 ERα 和 GPER1,并通过芳香化酶的差异产生来调节神经元功能。ERs 和芳香化酶在神经系统中表达,包括纹状体脑区。这些区域包括伏隔核核心、壳和尾壳核,对广泛的功能和障碍至关重要,这些功能和障碍在表型和/或发病率方面存在性别差异。雌激素的性别特异性作用是产生这些性别差异的一个组成部分。纹状体区域的一个显著特征是,在成年期神经元仅表达膜但不表达核 ERs。这一长期存在的发现主导了纹状体区域中雌激素作用的模型。然而,雌性和雄性纹状体中 ER 和芳香化酶细胞表达的发育病因尚不清楚。这一知识上的遗漏很重要,因为发育阶段会影响细胞雌激素机制。因此,评估了围产期、青春期前和成年雌性和雄性大鼠纹状体中 ERα、GPER1 和芳香化酶的细胞免疫反应性。我们检验了以下假设:ERα、GPER1 和芳香化酶表现出性别、区域和年龄特异性差异,包括核表达。ERα 在成年前的所有三个纹状体区域均表现出核表达,并在区域和性别特异性的时间过程中消失。细胞 GPER1 表达在发育过程中呈区域但非性别特异性时间过程下降,导致成年后出现核外表达。体细胞芳香化酶在青春期前出现,并在区域但非性别特异性时间过程中增加到成年期。这些数据表明,发育时期对纹状体细胞雌激素机制具有关键的性别特异性影响。

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