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Differential DNA binding by the androgen and glucocorticoid receptors involves the second Zn-finger and a C-terminal extension of the DNA-binding domains.

机译:雄激素和糖皮质激素受体的差异DNA结合涉及DNA结合域的第二个Zn指和C端延伸。

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摘要

The androgen and glucocorticoid hormones evoke specific in vivo responses by activating different sets of responsive genes. Although the consensus sequences of the glucocorticoid and androgen response elements are very similar, this in vivo specificity can in some cases be explained by differences in DNA recognition between both receptors. This has clearly been demonstrated for the androgen response element PB-ARE-2 described in the promoter of the rat probasin gene. Swapping of different fragments between the androgen- and glucocorticoid-receptor DNA-binding domains demonstrates that (i) the first Zn-finger module is not involved in this sequence selectivity and (ii) that residues in the second Zn-finger as well as a C-terminal extension of the DNA-binding domain from the androgen receptor are required. For specific and high-affinity binding to response elements, the DNA-binding domains of the androgen and glucocorticoid receptors need a different C-terminal extension. The glucocorticoid receptor requires 12 C-terminal amino acids for high affinity DNA binding, while the androgen receptor only involves four residues. However, for specific recognition of the PB-ARE-2, the androgen receptor also requires 12 C-terminal residues. Our data demonstrate that the mechanism by which the androgen receptor binds selectively to the PB-ARE-2 is different from that used by the glucocorticoid receptor to bind a consensus response element. We would like to suggest that the androgen receptor recognizes response elements as a direct repeat rather than the classical inverted repeat.
机译:雄激素和糖皮质激素通过激活不同组的反应基因来引起特定的体内反应。尽管糖皮质激素和雄激素应答元件的共有序列非常相似,但是在某些情况下,这种体内特异性可以通过两种受体之间的DNA识别差异来解释。对于大鼠probasin基因的启动子中描述的雄激素响应元件PB-ARE-2,这已得到明确证明。雄激素和糖皮质激素受体DNA结合域之间不同片段的交换表明(i)第一个锌指模块不参与此序列选择性;(ii)第二个锌指中的残基以及需要从雄激素受体的DNA结合结构域的C末端延伸。为了与反应元件特异性和高亲和力结合,雄激素和糖皮质激素受体的DNA结合结构域需要不同的C端延伸。糖皮质激素受体需要12个C末端氨基酸才能实现高亲和力DNA结合,而雄激素受体仅涉及四个残基。但是,为了特异性识别PB-ARE-2,雄激素受体也需要12个C端残基。我们的数据表明,雄激素受体选择性结合至PB-ARE-2的机制不同于糖皮质激素受体结合共有应答元件的机制。我们想建议雄激素受体将反应元件识别为直接重复,而不是经典的反向重复。

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