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人催产素基因近端启动子中多重激素反应元件的亲和力和活性。

The affinity and activity of the multiple hormone response element in the proximal promoter of the human oxytocin gene.

作者信息

Stedronsky K, Telgmann R, Tillmann G, Walther N, Ivell R

机构信息

Institute for Hormone and Fertility Research, University of Hamburg, Hamburg, Germany.

出版信息

J Neuroendocrinol. 2002 Jun;14(6):472-85. doi: 10.1046/j.1365-2826.2002.00799.x.

DOI:10.1046/j.1365-2826.2002.00799.x
PMID:12047722
Abstract

In vivo there appears to be a marked association between oestrogen levels and the expression of the oxytocin (OT) gene in most tissues. Transfection and DNA-protein binding experiments using high levels of either oestrogen receptor (ER)alpha or ERbeta imply a direct interaction of these transcription factors with the multiple hormone response element (HRE) at approximately -160 from the transcription start site of the OT gene in most species. In an extensive set of experiments, we show, using both transfection and protein-DNA binding, that low to moderate amounts of either oestrogen receptor, while being able to interact directly with a classic oestrogen response element (ERE) fail to interact with the human OT -160 HRE. Instead, this element, similar to its bovine counterpart, has a high affinity for the orphan receptors steroidogenic factor 1 and chicken ovalbumin upstream promoter transcription factor. Second, the human and bovine OT promoter can be made artificially responsive towards oestrogen in a cotransfection system over-expressing ERalpha or ERbeta, but not in cells expressing natural levels of these steroid receptors. Interestingly, nuclear extracts from both ERalpha-positive MCF7 cells and ERalpha-negative MDA-MB231 cells both contain a transcription factor which binds specifically to both the hOT-HRE element and to a classic ERE, and which has orphan receptor-like binding properties rather than those of an oestrogen receptor. Together, these and other results suggest that oestrogen action in vivo on the OT gene in all species is more likely to involve a DNA-independent mechanism than classic direct interactions with dimeric oestrogen receptors.

摘要

在体内,雌激素水平与大多数组织中催产素(OT)基因的表达之间似乎存在显著关联。使用高水平的雌激素受体(ER)α或ERβ进行的转染和DNA-蛋白质结合实验表明,在大多数物种中,这些转录因子与OT基因转录起始位点约-160处的多个激素反应元件(HRE)直接相互作用。在一系列广泛的实验中,我们通过转染和蛋白质-DNA结合表明,低至中等量的任何一种雌激素受体虽然能够与经典的雌激素反应元件(ERE)直接相互作用,但却无法与人类OT -160 HRE相互作用。相反,该元件与其牛对应物相似,对孤儿受体类固醇生成因子1和鸡卵清蛋白上游启动子转录因子具有高亲和力。其次,在过表达ERα或ERβ的共转染系统中,人类和牛的OT启动子可以被人为地诱导对雌激素产生反应,但在表达这些类固醇受体天然水平的细胞中则不能。有趣的是,ERα阳性的MCF7细胞和ERα阴性的MDA-MB231细胞的核提取物都含有一种转录因子,该转录因子与hOT-HRE元件和经典ERE都能特异性结合,并且具有类似孤儿受体的结合特性而非雌激素受体的结合特性。总之,这些结果以及其他结果表明,在体内所有物种中,雌激素对OT基因的作用更可能涉及一种不依赖DNA的机制,而不是与二聚体雌激素受体的经典直接相互作用。

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