首页> 外文期刊>Journal of pharmacological sciences. >Pathophysiological response to hypoxia - from the molecular mechanisms of malady to drug discovery: epigenetic regulation of the hypoxic response via hypoxia-inducible factor and histone modifying enzymes.
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Pathophysiological response to hypoxia - from the molecular mechanisms of malady to drug discovery: epigenetic regulation of the hypoxic response via hypoxia-inducible factor and histone modifying enzymes.

机译:对缺氧的病理生理反应-从疾病的分子机制到药物发现:通过缺氧诱导因子和组蛋白修饰酶对缺氧反应进行表观遗传调控。

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摘要

The hypoxia response regulated primarily by hypoxia-inducible factor (HIF) influences metabolism, cell survival, and angiogenesis to maintain biological homeostasis. In addition to the traditional transcriptional regulation by HIF, recent studies have shown that epigenetic modulation such as histone methylation, acetylation, and DNA methylation could change the regulation of the response to hypoxia. Eukaryotic chromatin is known to be modified by multiple post-translational histone methylation and demethylation, which result in the chromatin conformation change to adapt to hypoxic stimuli. Interestingly, some of the histone demethylase enzymes, which have the Jumonji domain-containing family, require oxygen to function and are induced by hypoxia in an HIF-1-dependent manner. Recent studies have demonstrated that histone modifiers play important roles in the hypoxic environment such as that in cancer cells and that they may become new therapeutic targets for cancer patients. It may lead to finding a new therapy for cancer to clarify a new epigenetic mechanism by HIF and histone demethylase such as JMJD1A (KDM3A) under hypoxia.
机译:主要由缺氧诱导因子(HIF)调节的缺氧反应影响代谢,细胞存活和血管生成,以维持生物稳态。除了通过HIF进行传统的转录调控外,最近的研究表明,表观遗传调控(例如组蛋白甲基化,乙酰化和DNA甲基化)可以改变对缺氧反应的调控。已知真核染色质会被多个翻译后的组蛋白甲基化和去甲基化修饰,从而导致染色质构象变化,以适应缺氧刺激。有趣的是,一些具有包含Jumonji域的家族的组蛋白脱甲基酶需要氧气才能发挥功能,并通过缺氧以HIF-1依赖的方式被诱导。最近的研究表明,组蛋白修饰剂在低氧环境(如癌细胞)中起着重要作用,它们可能成为癌症患者的新治疗靶标。它可能导致寻找一种新的癌症治疗方法,以阐明缺氧条件下HIF和组蛋白脱甲基酶(例如JMJD1A(KDM3A))的新表观遗传机制。

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