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Sp1结合位点和雌激素反应元件半位点参与人孕激素受体A启动子的调控。

Sp1 binding sites and an estrogen response element half-site are involved in regulation of the human progesterone receptor A promoter.

作者信息

Petz L N, Nardulli A M

机构信息

Department of Molecular and Integrative Physiology, University of Illinois, Urbana, 61801, USA.

出版信息

Mol Endocrinol. 2000 Jul;14(7):972-85. doi: 10.1210/mend.14.7.0493.

Abstract

Progesterone receptor gene expression is induced by estrogen in MCF-7 human breast cancer cells. Although it is generally thought that estrogen responsiveness is mediated through estrogen response elements (EREs), the progesterone receptor gene lacks an identifiable ERE. The progesterone receptor A promoter does, however, contain a half-ERE/Sp1 binding site comprised of an ERE half-site upstream of two Sp1 binding sites. We have used in vivo deoxyribonuclease I (DNase I) footprinting to demonstrate that the half-ERE/Sp1 binding site is more protected when MCF-7 cells are treated with estrogen than when cells are not exposed to hormone, suggesting that this region is involved in estrogen-regulated gene expression. The ability of the half-ERE/Sp1 binding site to confer estrogen responsiveness to a simple heterologous promoter was confirmed in transient cotransfection assays. In vitro DNase I footprinting and gel mobility shift assays demonstrated that Sp1 present in MCF-7 nuclear extracts and purified Sp1 protein bound to the two Sp1 sites and that the estrogen receptor enhanced Sp1 binding. In addition to its effects on Sp1 binding, the estrogen receptor also bound directly to the ERE half-site. Taken together, these findings suggest that the estrogen receptor and Sp1 play a role in activation of the human progesterone receptor A promoter.

摘要

在MCF-7人乳腺癌细胞中,雌激素可诱导孕激素受体基因表达。虽然一般认为雌激素反应性是通过雌激素反应元件(ERE)介导的,但孕激素受体基因缺乏可识别的ERE。然而,孕激素受体A启动子确实包含一个由两个Sp1结合位点上游的ERE半位点组成的半ERE/Sp1结合位点。我们利用体内脱氧核糖核酸酶I(DNase I)足迹法证明,与未暴露于激素的细胞相比,用雌激素处理MCF-7细胞时,半ERE/Sp1结合位点受到的保护更多,这表明该区域参与雌激素调节的基因表达。在瞬时共转染实验中证实了半ERE/Sp1结合位点赋予简单异源启动子雌激素反应性的能力。体外DNase I足迹法和凝胶迁移率变动分析表明,MCF-7核提取物中的Sp1和纯化的Sp1蛋白与两个Sp1位点结合,雌激素受体增强了Sp1的结合。除了对Sp1结合的影响外,雌激素受体还直接与ERE半位点结合。综上所述,这些发现表明雌激素受体和Sp1在人孕激素受体A启动子的激活中发挥作用。

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