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轻度代谢扰动改变线粒体蛋白的琥珀酰化。

Mild metabolic perturbations alter succinylation of mitochondrial proteins.

机构信息

Burke Medical Research Institute, Brain and Mind Research Institute, Weill Cornell Medicine, White Plains, New York.

Brain and Mind Research Institute, Weill Cornell Medicine, White Plains, New York.

出版信息

J Neurosci Res. 2017 Nov;95(11):2244-2252. doi: 10.1002/jnr.24103. Epub 2017 Jun 20.

Abstract

Succinylation of proteins is widespread, modifies both the charge and size of the molecules, and can alter their function. For example, liver mitochondrial proteins have 1,190 unique succinylation sites representing multiple metabolic pathways. Succinylation is sensitive to both increases and decreases of the NAD -dependent desuccinylase, SIRT5. Although the succinyl group for succinylation is derived from metabolism, the effects of systematic variation of metabolism on mitochondrial succinylation are not known. Changes in succinylation of mitochondrial proteins following variations in metabolism were compared against the mitochondrial redox state as estimated by the mitochondrial NAD /NADH ratio using fluorescent probes. The ratio was decreased by reduced glycolysis and/or glutathione depletion (iodoacetic acid; 2-deoxyglucose), depressed tricarboxylic acid cycle activity (carboxyethyl ester of succinyl phosphonate), and impairment of electron transport (antimycin) or ATP synthase (oligomycin), while uncouplers of oxidative phosphorylation (carbonyl cyanide m-chlorophenyl hydrazine or tyrphostin) increased the NAD /NADH ratio. All of the conditions decreased succinylation. In contrast, reducing the oxygen from 20% to 2.4% increased succinylation. The results demonstrate that succinylation varies with metabolic states, is not correlated to the mitochondrial NAD /NADH ratio, and may help coordinate the response to metabolic challenge.

摘要

蛋白质的琥珀酰化作用广泛存在,既改变了分子的电荷和大小,又改变了其功能。例如,肝线粒体蛋白有 1190 个独特的琥珀酰化位点,代表了多种代谢途径。琥珀酰化作用对 NAD 依赖性脱琥珀酰酶 SIRT5 的增加和减少都很敏感。尽管琥珀酰基用于琥珀酰化,但系统代谢变化对线粒体琥珀酰化的影响尚不清楚。使用荧光探针,通过线粒体 NAD/NADH 比率估计线粒体氧化还原状态,比较了代谢变化后线粒体蛋白琥珀酰化的变化。糖酵解和/或谷胱甘肽耗竭(碘乙酸;2-脱氧葡萄糖)降低了 NAD/NADH 比率,三羧酸循环活性降低(琥珀酰磷酸羧乙基酯),电子传递受损(抗霉素)或 ATP 合酶(寡霉素),而氧化磷酸化的解偶联剂(氰基氯苯腙或 tyrphostin)增加了 NAD/NADH 比率。所有条件均降低了琥珀酰化作用。相比之下,将氧气从 20%降低到 2.4%会增加琥珀酰化作用。结果表明,琥珀酰化作用随代谢状态而变化,与线粒体 NAD/NADH 比率无关,可能有助于协调对代谢挑战的反应。

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