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核孤儿受体COUP-TF和ARP-1通过增强自身调节作用正向调控鳟鱼雌激素受体基因。

The nuclear orphan receptors COUP-TF and ARP-1 positively regulate the trout estrogen receptor gene through enhancing autoregulation.

作者信息

Lazennec G, Kern L, Valotaire Y, Salbert G

机构信息

UPRES-A CNRS 6026, Equipe Associée d'Endocrinologie Moléculaire des Poissons, INRA, Université de Rennes I, France.

出版信息

Mol Cell Biol. 1997 Sep;17(9):5053-66. doi: 10.1128/MCB.17.9.5053.

Abstract

The rainbow trout estrogen receptor (rtER) is a positively autoregulated gene in liver cells. In a previous report, we showed that upregulation is mediated by an estrogen response element (ERE) located in the proximal promoter of the gene and that a half binding site for nuclear receptors (5'-TGACCT-3') located 15 bp upstream of the ERE is involved in the magnitude of the estrogen response. We now report that the human orphan receptor COUP-TF and a COUP-TF-like protein from trout liver are able to bind to the consensus half-site. When cotransfected with the rtER gene proximal promoter, COUP-TF had no regulatory functions on its own. Interestingly, COUP-TF enhanced rtER transactivation properties in the presence of estradiol in a dose-dependent manner when cotransfected with the rtER gene promoter. Unliganded retinoid receptor heterodimers had the same helper function as COUP-TF in the presence of estradiol but were switched to repressors when the ligand all-trans-retinoic acid was added. Mutation of the consensus half-site only slightly reduced COUP-TF helper function, suggesting that it actually results from a complex mechanism that probably involves both DNA binding of COUP-TF to the promoter and protein-protein interaction with another transcription factor bound to the promoter. Nevertheless, a DNA-binding-defective mutant of COUP-TF was also defective in ER helper function. Competition footprinting analysis suggested that COUP-TF actually establishes contacts with the consensus upstream half-site and the downstream ERE half-site that would form a DR-24-like response element. Interaction of COUP-TF with the DR-24 element was confirmed in footprinting assays by using nuclear extracts from Saccharomyces cerevisiae expressing COUP-TF. Finally, interaction of COUP-TF with mutants of the rtER gene promoter showed that COUP-TF recognizes the ERE when the upstream half-site is mutated. These data show that COUP-TF may activate transcription through interaction with other nuclear receptors. This cross-talk between liganded nuclear receptors and orphan receptors is likely to modulate the spectrum of action of a particular ligand-receptor complex and may participate in the cell-type specificity of the ligand effect.

摘要

虹鳟鱼雌激素受体(rtER)是肝细胞中一个正向自调节基因。在之前的一份报告中,我们表明上调是由位于该基因近端启动子中的雌激素反应元件(ERE)介导的,并且位于ERE上游15 bp处的核受体半结合位点(5'-TGACCT-3')参与了雌激素反应的强度。我们现在报告,人类孤儿受体COUP-TF和来自鳟鱼肝脏的一种COUP-TF样蛋白能够结合到共有半位点。当与rtER基因近端启动子共转染时,COUP-TF自身没有调节功能。有趣的是,当与rtER基因启动子共转染时,COUP-TF在雌二醇存在的情况下以剂量依赖的方式增强了rtER的反式激活特性。未结合配体的类视黄醇受体异二聚体在雌二醇存在时具有与COUP-TF相同的辅助功能,但当添加配体全反式维甲酸时则转变为抑制剂。共有半位点的突变仅略微降低了COUP-TF的辅助功能,这表明它实际上是由一种复杂机制导致的,该机制可能既涉及COUP-TF与启动子的DNA结合,也涉及与结合在启动子上的另一种转录因子的蛋白质-蛋白质相互作用。然而,COUP-TF的一个DNA结合缺陷突变体在ER辅助功能方面也存在缺陷。竞争足迹分析表明,COUP-TF实际上与上游共有半位点和下游ERE半位点建立了接触,这些位点将形成一个类似DR-24的反应元件。通过使用表达COUP-TF的酿酒酵母核提取物进行足迹分析,证实了COUP-TF与DR-24元件的相互作用。最后,COUP-TF与rtER基因启动子突变体的相互作用表明,当上游半位点突变时,COUP-TF能够识别ERE。这些数据表明,COUP-TF可能通过与其他核受体相互作用来激活转录。配体结合的核受体与孤儿受体之间的这种相互作用可能会调节特定配体-受体复合物的作用谱,并可能参与配体效应的细胞类型特异性。

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