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首页> 外文期刊>Molecular and Cellular Endocrinology >Modulation of transcription parameters in glucocorticoid receptor-mediated repression.
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Modulation of transcription parameters in glucocorticoid receptor-mediated repression.

机译:糖皮质激素受体介导的抑制中转录参数的调节。

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摘要

Glucocorticoid receptors (GRs) affect both gene induction and gene repression. The disparities of receptor binding to DNA and increased vs. decreased gene expression have suggested significant mechanistic differences between GR-mediated induction and repression. Numerous transcription factors are known to modulate three parameters of gene induction: the total activity (Vmax) and position of the dose-response curve with glucocorticoids (EC50) and the percent partial agonist activity with antiglucocorticoids. We have examined the effects on GR-mediated repression of five modulators (coactivators TIF2 [GRIP1, SRC-2] and SRC-1, corepressor SMRT, and comodulators STAMP and Ubc9), a glucocorticoid steroid (deacylcortivazol [DAC]) of very different structure, and an inhibitor of histone deacetylation (trichostatin A [TSA]). These factors interact with different domains of GR and thus are sensitive topological probes of GR action. These agents altered the Vmax, EC50, and percent partial agonist activity of endogenous and exogenous repressed genes similarly to that previously observed for GR-regulated gene induction. Collectively, these results suggest that GR-mediated induction and repression share many of the same molecular interactions and that the causes for different levels of gene transcription arise from more distal downstream steps.
机译:糖皮质激素受体(GRs)影响基因诱导和基因抑制。受体与DNA结合的差异以及基因表达的增加与减少之间的差异表明GR介导的诱导和抑制之间存在显着的机理差异。已知许多转录因子可调节基因诱导的三个参数:使用糖皮质激素的总活性(Vmax)和剂量反应曲线的位置(EC50),以及使用抗糖皮质激素的部分激动剂活性的百分比。我们已经研究了五个调节剂(糖皮质激素类固醇(去酰基化皮质醇[DAC])对五个调节剂(共激活剂TIF2 [GRIP1,SRC-2]和SRC-1,共抑制物SMRT以及共调节剂STAMP和Ubc9)对GR介导的阻遏作用的影响。结构和组蛋白去乙酰化抑制剂(曲古抑菌素A [TSA])。这些因素与GR的不同域相互作用,因此是GR作用的敏感拓扑探针。这些试剂改变了内源性和外源性阻抑基因的Vmax,EC50和部分激动剂活性百分比,类似于先前观察到的GR调控基因诱导。总体而言,这些结果表明,GR介导的诱导和抑制共有许多相同的分子相互作用,而基因转录水平不同的原因则来自更远的下游步骤。

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