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定位核小体对孕酮受体与孕酮反应元件结合的调控。

Modulation of progesterone receptor binding to progesterone response elements by positioned nucleosomes.

作者信息

Pham T A, McDonnell D P, Tsai M J, O'Malley B W

机构信息

Department of Cell Biology, Baylor College of Medicine, Houston, Texas 77030.

出版信息

Biochemistry. 1992 Feb 11;31(5):1570-8. doi: 10.1021/bi00120a039.

Abstract

In cells, steroid hormone receptors interact with target enhancer elements on nucleosomes to regulate transcription of genes. To elucidate how nucleosomes can potentially regulate the interactions of steroid receptors with steroid response elements, we have examined the effects of nucleosome positioning and histone source on the binding of the progesterone receptor to DNA elements on nucleosomes reconstituted in vitro. We find that the affinity of the receptor for its response element is dependent on the position of the element within the nucleosome, but not on the histone source, active or inactive chromatin. Our results suggest that the strength of DNA-histone interactions within the nucleosome modulates the binding of progesterone receptor to response elements. Thus, nucleosome positioning is likely to influence the function of steroid receptors in vivo.

摘要

在细胞中,类固醇激素受体与核小体上的靶增强子元件相互作用以调节基因转录。为了阐明核小体如何潜在地调节类固醇受体与类固醇反应元件的相互作用,我们研究了核小体定位和组蛋白来源对孕酮受体与体外重构核小体上的DNA元件结合的影响。我们发现,受体对其反应元件的亲和力取决于该元件在核小体内的位置,而不取决于组蛋白来源,即活性或非活性染色质。我们的结果表明,核小体内DNA-组蛋白相互作用的强度调节孕酮受体与反应元件的结合。因此,核小体定位可能会影响体内类固醇受体的功能。

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