Modulation of the Glucocorticoid Receptor Activity by Post-Translational Modifications

A. Liberman, María Antunica-Noguerol, E. Arzt
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引用次数: 11

Abstract

Glucocorticoids (GCs) regulate numerous physiologic processes in order to maintain homeostasis. Most of their actions are mediated by an intracellular GC receptor (GR). The dysregulation of the GR function has been associated with different pathologies such as stress-related disorders and inflammatory and autoimmune diseases. The final outcome of GC actions is regulated at multiple levels and has been extensively reported. Nowadays, novel insights into the modulation of the GR activity arise from the study of the multiprotein chaperone/cochaperone machinery, the nuclear receptor cofactors (coactivators and corepressors), and chromatin regulation and their concomitant impact on GR-mediated gene transcription. Nevertheless, the complexity of GR-mediated gene regulation cannot be explained by a finite number of chaperones and cofactors. A further level in the regulation of GR activity is achieved by posttranslational modifications (PTMs) in response to external stimuli. PTMs can regulate protein stability, structure, function, activity, intracellular localization, and interaction with other proteins during cellular processes. Therefore, dynamic regulation of the molecular properties of these proteins by PTMs allows for further understanding the complexity of GR-dependent gene expression and its impact on GR-mediated pathophysiological processes.
翻译后修饰对糖皮质激素受体活性的调节
糖皮质激素(GCs)调节许多生理过程以维持体内平衡。它们的大部分作用是由细胞内GC受体(GR)介导的。GR功能失调与应激相关疾病、炎症和自身免疫性疾病等不同病理有关。GC作用的最终结果在多个层面受到调节,并已被广泛报道。目前,对GR活性调控的新见解来自多蛋白伴侣/伴侣机制、核受体辅助因子(共激活因子和辅抑制因子)、染色质调控及其对GR介导的基因转录的伴随影响的研究。然而,gr介导的基因调控的复杂性不能用有限数量的伴侣和辅助因子来解释。GR活性的进一步调控是通过响应外部刺激的翻译后修饰(PTMs)实现的。在细胞过程中,PTMs可以调节蛋白质的稳定性、结构、功能、活性、细胞内定位以及与其他蛋白质的相互作用。因此,通过PTMs对这些蛋白分子特性的动态调控,可以进一步了解gr依赖基因表达的复杂性及其对gr介导的病理生理过程的影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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