首页> 外文OA文献 >DAX-1 (Dosage-Sensitive Sex Reversal-Adrenal Hypoplasia Congenita Critical Region on the X-Chromosome, Gene 1) Selectively Inhibits Transactivation But Not Transrepression Mediated by the Glucocorticoid Receptor in a LXXLL-Dependent Manner
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DAX-1 (Dosage-Sensitive Sex Reversal-Adrenal Hypoplasia Congenita Critical Region on the X-Chromosome, Gene 1) Selectively Inhibits Transactivation But Not Transrepression Mediated by the Glucocorticoid Receptor in a LXXLL-Dependent Manner

机译:DAX-1(X染色体上剂量敏感的性逆转-肾上腺皮质功能减退先天性关键区域,基因1)以LXXLL依赖性方式选择性抑制糖皮质激素受体介导的反式激活,但不抑制反式激活

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摘要

The glucocorticoid receptor (GR) mediates virtually all actions of glucocorticoids, and the nature and magnitude of a cell’s response to these steroids are determined primarily by hormone concentration and GR signaling capacity. DAX-1 (dosagesensitive sex reversal-adrenal hypoplasia congenita critical region on the X-chromosome, gene 1) is an orphan nuclear receptor that functions as a corepressor, and deletion or mutation of DAX-1 causes a decrease in glucocorticoid production. However it is unclear whether DAX-1 also alters GR function as a transcription factor. Here, we demonstrate that DAX-1 acts as a novel selective GR modulator. It specifically inhibits ligand-dependent GR transactivation with little effect on GR-mediated transrepression. As demonstrated by coimmunoprecipitation and glutathione- S-transferase pull-down assays, DAX-1 physically interacts with GR, but this interaction does not influence either ligand-induced GR nuclear translocation or subsequent GR association with glucocorticoid-responsive elements. Instead, DAX-1 competes with coactivators such as GR-interacting protein 1 for binding to the receptor. Specifically, suppression of GR transactivation is mediated by the N-terminal half of DAX-1, and in particular the LXXLL motifs. Thus we demonstrate that DAX-1 directly modulates GR signaling in addition to affecting glucocorticoid hormone levels.
机译:糖皮质激素受体(GR)实际上介导了糖皮质激素的所有作用,细胞对这些类固醇的反应的性质和大小主要由激素浓度和GR信号传导能力决定。 DAX-1(X染色体基因1上的剂量敏感性性逆转-肾上腺皮质发育不全先天性关键区域)是一种孤儿核受体,它起着核心抑制剂的作用,而DAX-1的缺失或突变会导致糖皮质激素生成减少。但是,不清楚DAX-1是否也改变GR功能作为转录因子。在这里,我们证明DAX-1充当新型选择性GR调节剂。它特异性抑制配体依赖性GR反式激活,而对GR介导的反式抑制作用很小。如共免疫沉淀法和谷胱甘肽-S-转移酶下拉试验所证明,DAX-1与GR发生物理相互作用,但这种相互作用既不影响配体诱导的GR核易位,也不影响随后的GR与糖皮质激素反应性元素的结合。相反,DAX-1与诸如GR相互作用蛋白1的共激活因子竞争结合受体。具体而言,GR反式激活的抑制是由DAX-1的N端(尤其是LXXLL基序)介导的。因此,我们证明DAX-1除了影响糖皮质激素水平外,还直接调节GR信号传导。

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