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Quantitative Analysis of the Whole-Body Metabolic Fate of Branched-Chain Amino Acids

机译:支链氨基酸全身代谢命运的定量分析

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Elevations in branched-chain amino acids (BCAAs) associate with numerous systemic diseases, including cancer, diabetes, and heart failure. However, an integrated understanding of whole-body BCAA metabolism remains lacking. Here, we employ in vivo isotopic tracing to systemically quantify BCAA oxidation in healthy and insulin-resistant mice. We find that most tissues rapidly oxidize BCAAs into the tricarboxylic acid (TCA) cycle, with the greatest quantity occurring in muscle, brown fat, liver, kidneys, and heart. Notably, pancreas supplies 20% of its TCA carbons from BCAAs. Genetic and pharmacologic suppression of branched-chain alpha-ketoacid dehydrogenase kinase, a clinically targeted regulatory kinase, induces BCAA oxidation primarily in skeletal muscle of healthy mice. While insulin acutely increases BCAA oxidation in cardiac and skeletal muscle, chronically insulin-resistant mice show blunted BCAA oxidation in adipose tissues and liver, shifting BCAA oxidation toward muscle. Together, this work provides a quantitative framework for understanding systemic BCAA oxidation in health and insulin resistance.
机译:分枝链氨基酸(BCAAs)升级与众多全身疾病联系,包括癌症,糖尿病和心力衰竭。然而,对全身BCAA新陈代谢的综合了解仍然缺乏。这里,我们在体内同位素追踪中,以系统地定量健康和胰岛素抗性小鼠的BCAA氧化。我们发现大多数组织迅速将BCAAs迅速氧化成三羧酸(TCA)循环,最大数量发生在肌肉,棕色脂肪,肝细胞,肾脏和心脏中。值得注意的是,胰腺从BCAAS提供20%的TCA碳。支链α-酮酸脱氢酶激酶的遗传和药理学抑制,临床靶向调节激酶,主要诱导BCAA氧化在健康小鼠的骨骼肌中。胰岛素急性增加心脏和骨骼肌中的BCAA氧化,慢性胰岛素抗性小鼠在脂肪组织和肝脏中显示出BCAA氧化,使BCAA氧化朝向肌肉。在一起,这项工作提供了了解健康和胰岛素抵抗力的系统性BCAA氧化的定量框架。

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