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小鼠肝细胞中与年龄相关的线粒体质子泄漏增加及ATP周转反应减少。

Age-related increase in mitochondrial proton leak and decrease in ATP turnover reactions in mouse hepatocytes.

作者信息

Harper M E, Monemdjou S, Ramsey J J, Weindruch R

机构信息

Department of Biochemistry, Microbiology and Immunology, Faculty of Medicine, University of Ottawa, Ottawa, Ontario, Canada K1H 8M5.

出版信息

Am J Physiol. 1998 Aug;275(2):E197-206. doi: 10.1152/ajpendo.1998.275.2.E197.

Abstract

Age-related changes in mitochondria, including decreased respiratory control ratios and altered mitochondrial inner membrane lipid composition, led us to study oxidative phosphorylation in hepatocytes from old (30 mo) and young (3 mo) male C57BL/J mice. Top-down metabolic control analysis and its extension, elasticity analysis, were used to identify changes in the control and regulation of the three blocks of reactions constituting the oxidative phosphorylation system: substrate oxidation, mitochondrial proton leak, and the ATP turnover reactions. Resting oxygen consumption of cells from old mice was 15% lower (P < 0.05) than in young cells. This is explained entirely by a decrease in oxygen consumption supporting ATP turnover reactions. At all values of mitochondrial membrane potential assessed, the proportion of total oxygen consumption used to balance the leak was greater in the old cells than in the young cells. Metabolic control coefficients indicate a shift in control over respiration and phosphorylation away from substrate oxidation toward increased control by leak and by ATP turnover reactions. Control of the actual number of ATP molecules synthesized by mitochondria for each oxygen atom consumed by the ATP turnover and leak reactions was greater in old than in young cells, showing that efficiency in older cells is more sensitive to changes in these two blocks of reactions than in young cells.

摘要

线粒体与年龄相关的变化,包括呼吸控制率降低和线粒体内膜脂质组成改变,促使我们研究老年(30月龄)和年轻(3月龄)雄性C57BL/J小鼠肝细胞中的氧化磷酸化过程。采用自上而下的代谢控制分析及其扩展形式——弹性分析,来确定构成氧化磷酸化系统的三个反应模块(底物氧化、线粒体质子泄漏和ATP周转反应)在控制和调节方面的变化。老年小鼠细胞的静息氧消耗量比年轻细胞低15%(P<0.05)。这完全是由于支持ATP周转反应的氧消耗量减少所致。在评估的所有线粒体膜电位值下,老年细胞中用于平衡泄漏的总氧消耗量所占比例高于年轻细胞。代谢控制系数表明,呼吸和磷酸化的控制从底物氧化向泄漏和ATP周转反应的控制增加发生了转变。老年细胞中线粒体为ATP周转和泄漏反应消耗的每个氧原子合成的实际ATP分子数的控制比年轻细胞更强,这表明老年细胞的效率对这两个反应模块变化的敏感性高于年轻细胞。

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