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首页> 外文期刊>Biochimica et biophysica acta. Molecular cell research >Regulation of mitochondrial respiratory chain biogenesis by estrogens/estrogen receptors and physiological, pathological and pharmacological implications.
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Regulation of mitochondrial respiratory chain biogenesis by estrogens/estrogen receptors and physiological, pathological and pharmacological implications.

机译:雌激素/雌激素受体对线粒体呼吸链生物发生的调控及其生理,病理和药理学意义。

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摘要

There has been increasing evidence pointing to the mitochondrial respiratory chain (MRC) as a novel and important target for the actions of 17beta-estradiol (E(2)) and estrogen receptors (ER) in a number of cell types and tissues that have high demands for mitochondrial energy metabolism. This novel E(2)-mediated mitochondrial pathway involves the cooperation of both nuclear and mitochondrial ERalpha and ERbeta and their co-activators on the coordinate regulation of both nuclear DNA- and mitochondrial DNA-encoded genes for MRC proteins. In this paper, we have: 1) comprehensively reviewed studies that reveal a novel role of estrogens and ERs in the regulation of MRC biogenesis; 2) discussed their physiological, pathological and pharmacological implications in the control of cell proliferation and apoptosis in relation to estrogen-mediated carcinogenesis, anti-cancer drug resistance in human breast cancer cells, neuroprotection for Alzheimer's disease and Parkinson's disease in brain, cardiovascular protection in human heart and their beneficial effects in lens physiology related to cataract in the eye; and 3) pointed out new research directions to address the key questions in this important and newly emerging area. We also suggest a novel conceptual approach that will contribute to innovative regimens for the prevention or treatment of a wide variety of medical complications based on E(2)/ER-mediated MRC biogenesis pathway.
机译:越来越多的证据表明线粒体呼吸链(MRC)是17β-雌二醇(E(2))和雌激素受体(ER)在许多细胞类型和组织高度活跃的组织中的作用的新的重要靶标线粒体能量代谢的需求。这种新颖的E(2)介导的线粒体途径涉及核和线粒体ERalpha和ERbeta及其共激活因子对MRC蛋白的核DNA和线粒体DNA编码基因的协调调控的合作。在本文中,我们有:1)全面审查的研究揭示了雌激素和内质网在MRC生物发生调控中的新作用; 2)讨论了它们在控制细胞增殖和凋亡方面的生理,病理和药理学意义,涉及雌激素介导的致癌作用,人类乳腺癌细胞的抗癌药耐药性,脑部阿尔茨海默氏病和帕金森氏病的神经保护作用,人的心脏及其对与白内障有关的晶状体生理的有益作用; 3)指出了新的研究方向,以解决这一重要且新兴领域中的关键问题。我们还建议一种新颖的概念方法,将有助于基于E(2)/ ER介导的MRC生物发生途径预防或治疗多种医学并发症的创新方案。

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