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Evidence of direct estrogenic regulation of human corticotropin-releasing hormone gene expression. Potential implications for the sexual dimophism of the stress response and immune/inflammatory reaction.

机译:人类促肾上腺皮质激素释放激素基因表达的直接雌激素调节的证据。对应激反应和免疫/炎症反应的性二态性的潜在影响。

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摘要

Corticotropin-releasing hormone (CRH) plays major roles in coordination of the stress response and regulation of the immune/inflammatory reaction, two important functions associated with sexual dimorphism. Two overlapping segments of the 5' flanking region of the human (h) CRH gene, the proximal 0.9 kb (containing two perfect half-palindromic estrogen-responsive elements [EREs]) and the 2.4 kb (including the former and containing two additional perfect half-palindromic EREs), were examined for their ability to confer estrogen-mediated transcriptional enhancement to a homologous or heterologous promoter. The level of estrogen-induced transactivation by the 0.9- and 2.4-kb segments was determined by chloramphenicol acetyltransferase analysis in CV-1 cells cotransfected with estrogen receptor (ER) cDNA expression plasmids, and found to be respectively approximately 10% and 20% of that of the strongly estrogen-responsive Xenopus vitellogenin A2 enhancer. Gel retardation and immunoprecipitation demonstrated specific association between the perfect half-palindromic EREs of hCRH gene and the DNA binding domain of hER in vitro. These findings may constitute the basis of sexual dimorphism in the expression of the CRH gene in the central nervous system and periphery, and might shed light in existing gender differences in stress response and immune regulation.
机译:促肾上腺皮质激素释放激素(CRH)在应激反应的协调和免疫/炎症反应的调节中起主要作用,这是与性二态性相关的两个重要功能。人(h)CRH基因5'侧翼区的两个重叠部分,近端0.9 kb(包含两个完美的半回文雌激素反应元件[ERE])和2.4 kb(包括前者并且包含两个额外的完美检查了半回文的ERE)将雌激素介导的转录增强作用赋予同源或异源启动子的能力。通过氯霉素乙酰转移酶分析确定了用雌激素受体(ER)cDNA表达质粒共转染的CV-1细胞中0.9-kb和2.4-kb片段引起的雌激素诱导的反式激活水平,发现分别约占10%和20%强烈雌激素反应的非洲爪蟾卵黄蛋白原A2增强剂。凝胶阻滞和免疫沉淀表明,hCRH基因的完美半回文ERE与hER的DNA结合结构域之间存在特异性联系。这些发现可能构成了CRH基因在中枢神经系统和周围组织中性二态性的基础,并可能揭示了应激反应和免疫调节中的性别差异。

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