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通过 C/EBPα 部分束缚雄激素受体,雄激素激活叶酸受体α 基因。

Androgen activation of the folate receptor α gene through partial tethering of the androgen receptor by C/EBPα.

机构信息

Department of Biochemistry and Cancer Biology, Medical University of Ohio, 3000 Arlington Avenue, Toledo, OH 43614, United States.

出版信息

J Steroid Biochem Mol Biol. 2010 Nov;122(5):333-40. doi: 10.1016/j.jsbmb.2010.08.008. Epub 2010 Sep 15.

Abstract

The folate receptor α (FRα) is critical for normal embryonic and fetal development. The receptor has a relatively narrow tissue specificity which includes the visceral endoderm and the placenta and mediates delivery of folate, inadequacy of which results in termination of pregnancy or developmental defects. We have previously reported that the FRα gene is negatively and directly regulated by estrogen and positively but indirectly by progesterone and glucocorticoid. To further investigate hormonal control of this gene and in view of the growing evidence for the importance of the androgen receptor (AR) in endometrial and placental functions, we examined the response of the FRα gene to androgen. Here we demonstrate that the FRα gene is directly activated by androgen. The P4 promoter of the FRα gene is the target of hormone-dependent activation by the androgen receptor (AR) in a manner that is co-activator-dependent. The site of functional association of AR in the FRα gene maps to a 35bp region occurring ∼1500bp upstream of the target promoter. The functional elements within this region are an androgen response element (ARE) half-site and a non-canonical C/EBP element that cooperate to recruit AR in a manner that is dependent on the DNA-bound C/EBPα. Since the placenta is rich in C/EBPα, the findings underscore the multiplicity of mechanisms by which the FRα gene is under the exquisite control of steroid hormones.

摘要

叶酸受体 α(FRα)对于正常的胚胎和胎儿发育至关重要。该受体具有相对狭窄的组织特异性,包括内脏内胚层和胎盘,并介导叶酸的输送,叶酸不足会导致妊娠终止或发育缺陷。我们之前曾报道过,FRα 基因受到雌激素的负向和直接调控,受到孕激素和糖皮质激素的正向但间接调控。为了进一步研究该基因的激素调控,并且鉴于雄激素受体(AR)在子宫内膜和胎盘功能中的重要性的证据不断增加,我们研究了雄激素对 FRα 基因的反应。在这里,我们证明雄激素可以直接激活 FRα 基因。FRα 基因的 P4 启动子是雄激素受体(AR)依赖激素激活的靶标,这种激活方式依赖共激活因子。AR 在 FRα 基因中的功能结合位点定位于靶启动子上游约 1500bp 的 35bp 区域。该区域内的功能元件是雄激素反应元件(ARE)半位点和非典型 C/EBP 元件,以依赖于 DNA 结合的 C/EBPα 的方式募集 AR。由于胎盘富含 C/EBPα,这些发现强调了 FRα 基因受类固醇激素精细调控的多种机制。

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