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雄激素选择性增强子中特异性突变的变化。雄激素受体差异DNA结合作用的证据。

Change of specificity mutations in androgen-selective enhancers. Evidence for a role of differential DNA binding by the androgen receptor.

作者信息

Verrijdt G, Schoenmakers E, Haelens A, Peeters B, Verhoeven G, Rombauts W, Claessens F

机构信息

Division of Biochemistry, Faculty of Medicine, Campus Gasthuisberg, University of Leuven, Herestraat 49, B-3000 Leuven, Belgium.

出版信息

J Biol Chem. 2000 Apr 21;275(16):12298-305. doi: 10.1074/jbc.275.16.12298.

Abstract

The androgen and glucocorticoid receptors recognize identical DNA motifs, leaving unanswered the question of how steroid specificity of transcriptional regulation is established in cells containing both receptors. Here, we provide evidence that subtle differences in low affinity DNA recognition might be a crucial element in the generation of steroid-specific responses. Here we identify simple hormone response elements in the mouse sex-limited protein enhancer and the human secretory component androgen response unit to be essential for the androgen specificity of both enhancers. We describe specific in vitro binding to these motifs by the DNA-binding domain of the androgen but not the glucocorticoid receptor. Both elements can be considered partial direct repeats of the 5'-TGTTCT-3' core binding motif. In addition, we show that specific point mutations in their left half-sites, essentially changing the nature of the repeats, strongly enhance the glucocorticoid sensitivity of the respective enhancers, whereas they have no effect on their androgen responsiveness. Accordingly, these mutations allow specific binding of the glucocorticoid receptor DNA-binding domain to both elements in vitro. With these experiments, we demonstrate that differential recognition by the androgen receptor of nonconventional steroid response elements is, at least in some cases, an important mechanism in androgen-specific transcriptional regulation.

摘要

雄激素受体和糖皮质激素受体识别相同的DNA基序,这使得在同时含有这两种受体的细胞中如何建立转录调控的类固醇特异性这一问题仍未得到解答。在此,我们提供证据表明,低亲和力DNA识别中的细微差异可能是产生类固醇特异性反应的关键因素。我们在此确定,小鼠性别限制蛋白增强子和人类分泌成分雄激素反应单元中的简单激素反应元件对于这两种增强子的雄激素特异性至关重要。我们描述了雄激素而非糖皮质激素受体的DNA结合结构域与这些基序的特异性体外结合。这两个元件均可视为5'-TGTTCT-3'核心结合基序的部分直接重复序列。此外,我们表明,其左半位点的特定点突变,本质上改变了重复序列的性质,强烈增强了相应增强子的糖皮质激素敏感性,而对其雄激素反应性没有影响。因此,这些突变使得糖皮质激素受体DNA结合结构域在体外能与这两个元件特异性结合。通过这些实验,我们证明,雄激素受体对非常规类固醇反应元件的差异识别,至少在某些情况下,是雄激素特异性转录调控中的一个重要机制。

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