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The nonepigenetic role for small molecule histone deacetylase inhibitors in the regulation of cardiac function

机译:小分子组蛋白脱乙酰酶抑制剂在心脏功能调节中的非对致病作用

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摘要

Eight million US adults are projected to suffer from heart failure (HF) by 2030. Of concern, 5-year mortality rates following HF diagnosis approximate 40%. Small molecule histone deacetylase (HDAC) inhibitors have demonstrated efficacy for the treatment and reversal of HF. Historically, HDACs were studied as regulators of nucleosomal histones, in which lysine deacetylation on histone tails changed DNA-histone protein electrostatic interactions, leading to chromatin condensation and changes in gene expression. However, recent proteomics studies have demonstrated that approximately 4500 proteins can be acetylated in various tissues; the function of most of these remains unknown. This Review will focus on the nonepigenetic role for lysine acetylation in the heart, with a focus on nonepigenetic actions for HDAC inhibitors on cardiac function.
机译:预计百万美国成年人将患有2030年的心力衰竭(HF)。关注,5年的死亡率,后诊断额外40%。 小分子组蛋白脱乙酰化酶(HDAC)抑制剂已经证明了HF治疗和逆转的功效。 从历史上看,HDAC被研究了作为核致组蛋白的调节剂,其中组蛋白尾部的赖氨酸脱乙酰化改变了DNA-组蛋白静电相互作用,导致染色质缩合和基因表达的变化。 然而,最近的蛋白质组学研究表明,在各种组织中可以乙酰化约4500种蛋白质; 大多数这些仍然是未知的。 本综述将专注于心脏中赖氨酸乙酰化的非聚糖作用,重点关注心脏功能对HDAC抑制剂的非对接动作。

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