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Post-translational modification of proteins during intermittent hypoxia.

机译:间歇性缺氧期间蛋白质的翻译后修饰。

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Post-translational modification (PTM) is one of the mechanisms by which protein function is regulated by chronic hypoxia. This article presents an overview of recent findings on PTM of proteins induced by chronic intermittent hypoxia (CIH) which is experienced by humans with sleep disordered breathing resulting in autonomic abnormalities. The analysis of PTM of proteins involves electrophoretic separation of tissue or cellular proteins followed by immunolabeling using antibodies specific to native and post-translationally modified forms. Recent results demonstrate that CIH, depending on the pattern, duration and severity of hypoxia, alters the state of phosphorylation of a subset of proteins associated with transcriptional factor activation, signaling pathways and neurotransmitter synthesis via activation of appropriate enzymatic machinery that catalyzes specific phosphorylation reactions. Investigation pertaining to PTMs associated with CIH is at its infant stage and future application of high throughput proteomics techniques are necessary to unravel other important PTMs associated with various critical metabolic and signaling pathways that are activated by intermittent hypoxia.
机译:翻译后修饰(PTM)是慢性缺氧调节蛋白质功能的机制之一。本文概述了由慢性间歇性缺氧(CIH)诱导的蛋白PTM的最新发现,该现象被呼吸紊乱的人类经历过,导致自主神经异常。蛋白质PTM的分析涉及组织或细胞蛋白质的电泳分离,然后使用对天然和翻译后修饰形式具有特异性的抗体进行免疫标记。最近的结果表明,CIH取决于缺氧的方式,持续时间和严重程度,可通过激活催化特定磷酸化反应的适当酶促机制来改变与转录因子激活,信号传导途径和神经递质合成相关的蛋白质子集的磷酸化状态。与CIH相关的PTM的研究尚处于婴儿阶段,高通量蛋白质组学技术的未来应用对于揭示与间歇性低氧激活的各种关键代谢和信号通路相关的其他重要PTM是必要的。

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