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The First Quantitative Acetylome Analysis In Response to a Regulatory Enzyme Identified 4623 Kac Sites and Diverse Sirt1-regulated Pathways

机译:响应于调节酶的第一定量乙酰胺分析鉴定了4623个KAC位点和不同的SIRT1调节途径

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Despite of the progress in identifying many Lys acetylation (Kac) proteins, Kac substrates for Kac-regulatory enzymes remain largely unknown, presenting a major knowledge gap in Kac biology. Here we identified and quantified 4623 Kac sites in 1800 Kac proteins in SIRT1~(+/+) and SIRT1~(-/-) MEF cells, representing the first study to reveal an enzyme-regulated Kac subproteome and the largest Lys acetylome reported to date from a single study. Four hundred eighty-five Kac sites were enhanced by more than 100% after SIRT1 knockout. Our results indicate that SIRT1 regulates the Kac states of diverse cellular pathways. Interestingly, we found that a number of acetyltransferases and major acetyltransferase complexes are targeted by SIRT1. Moreover, we showed that the activities of the acetyltransferases are regulated by SIRT1-mediated deacetylation. Taken together, our results reveal the Lys acetylome in response to SIRT1, provide new insights into mechanisms of SIRT1 function, and offer biomarker candidates for the clinical evaluation of SIRT1-activator compounds.
机译:尽管在确定许多赖氨酸乙酰化(卡克)蛋白的进展,为KAC-调节酶底物卡克仍是未知,呈现在卡克生物学的主要知识差距。在这里,我们确定和量化在1800个卡克蛋白4623个卡克网站中SIRT1〜(+ / +)和SIRT1〜( - / - )MEF细胞,代表研究首次揭示了一种酶调节卡克subproteome和最大的赖氨酸acetylome报日期从单一的研究。四百85卡克位点超过100%增强SIRT1基因敲除后。我们的研究结果表明,SIRT1调节不同的细胞通路的科航。有趣的是,我们发现,一些乙酰转移酶和乙酰基转移酶的主要复合物由SIRT1的目标。此外,我们发现,乙酰转移酶的活动由SIRT1介导的脱乙酰化调控。总之,我们的研究结果显示响应SIRT1利斯acetylome,提供新的见解为SIRT1激活剂化合物的临床评估SIRT1功能的机制,并提供潜在生物标志物。

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