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Niacin: an old lipid drug in a new NAD(+) dress

机译:烟酸:新的nad(+)连衣裙中的旧脂质药物

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Niacin, the first antidyslipidemic drug, has been at the center stage of lipid research for many decades before the discovery of statins. However, to date, despite its remarkable effects on lipid profiles, the clinical outcomes of niacin treatment on cardiac events is still debated. In addition to its historically well-defined interactions with central players of lipid metabolism, niacin can be processed by eukaryotic cells to synthesize a crucial cofactor, NAD(+). NAD(+) acts as a cofactor in key cellular processes, including oxidative phosphorylation, glycolysis, and DNA repair. More recently, evidence has emerged that NAD(+) also is an essential cosubstrate for the sirtuin family of protein deacylases and thereby has an impact on a wide range of cellular processes, most notably mitochondrial homeostasis, energy homeostasis, and lipid metabolism. NAD(+) achieves these remarkable effects through sirtuin-mediated deacetylation of key transcriptional regulators, such as peroxisome proliferator-activated receptor gamma coactivator 1-alpha, LXR, and SREBPs, that control these cellular processes. Here, we present an alternative point of view to explain niacin's mechanism of action, with a strong focus on the importance of how this old drug acts as a control switch of NAD(+)/sirtuin-mediated control of metabolism.
机译:第一次防药脂质药物烟酸已经在发现他汀类药物之前几十年前在脂质研究的中心阶段。然而,迄今为止,尽管对脂质概况产生了显着影响,但仍讨论了烟酸治疗烟酸治疗的临床结果。除了与脂质代谢中央球员的历史明确定义的相互作用之外,烟酸可以通过真核细胞加工,以合成关键的辅因子NAD(+)。 NAD(+)在关键细胞过程中用作辅助因子,包括氧化磷酸化,糖酵解和DNA修复。最近,证据表明,NAD(+)也是SIRTUIN系列蛋白质脱酰基酶的必要宇烷体,从而对各种细胞过程产生影响,最典型的线粒体稳态,能量稳态和脂质代谢。 NAD(+)通过SIRTUIN介导的关键转录调节剂的脱乙酰化,例如过氧化物酶促增殖物激活的受体γ1-α,LXR和SREBP来实现这些显着的效果,可控制这些细胞过程。在这里,我们展示了另一种观点来解释烟酸的行动机制,强烈关注该旧药物如何作为NAD(+)/ sirtuin的控制切换的重要性的重要性。

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