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Modulation of oxidative phosphorylation machinery signifies a prime mode of anti-ageing mechanism of calorie restriction in male rat liver mitochondria

机译:氧化磷酸化机制的调节标志着雄性大鼠肝线粒体卡路里限制的抗衰老机制的主要模式

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Mitochondria being the major source and target of reactive oxygen species (ROS) play a crucial role during ageing. We analyzed ageing and calorie restriction (CR)-induced changes in abundance of rat liver mitochondrial proteins to understand key aspects behind the age-retarding mechanism of CR. The combination of blue-native (BN) gel system with fluorescence Difference Gel Electrophoresis (DIGE) facilitated an efficient analysis of soluble and membrane proteins, existing as monomers or multi-protein assemblies. Changes in abundance of specific key subunits of respiratory chain complexes I, IV and V, critical for activity and/or assembly of the complexes were identified. CR lowered complex I assembly and complex IV activity, which is discussed as a molecular mechanism to minimize ROS production at mitochondria. Notably, the antioxidant system was found to be least affected. The GSH:GSSG couple could be depicted as a rapid mean to handle the fluctuations in ROS levels led by reversible metabolic shifts. We evaluated the relative significance of ROS generation against quenching. We also observed parallel and unidirectional changes as effect of ageing and CR, in subunits of ATP synthase, cytochrome P450 and glutathione S-transferase. This is the first report on such 'putatively hormetic' ageing-analogous effects of CR, besides the age-retarding ones.
机译:线粒体是活性氧(ROS)的主要来源和目标,在衰老过程中起着至关重要的作用。我们分析了衰老和卡路里限制(CR)诱导的大鼠肝线粒体蛋白丰度变化,以了解CR延缓年龄机制的关键方面。蓝原色(BN)凝胶系统与荧光差异凝胶电泳(DIGE)的结合有助于有效分析以单体或多蛋白组合物形式存在的可溶性和膜蛋白。确定了呼吸链复合物I,IV和V的特定关键亚基的丰度变化,这对于复合物的活性和/或组装至关重要。 CR降低了复杂的I装配和复杂的IV活性,这被认为是将线粒体中ROS产生最小化的分子机制。值得注意的是,发现抗氧化剂系统受影响最小。 GSH:GSSG对可以描述为一种快速的方法,可以应对由可逆的代谢变化导致的ROS水平波动。我们评估了相对于淬灭活性氧生成的相对重要性。我们还观察到了衰老和CR的平行和单向变化,它们是ATP合酶,细胞色素P450和谷胱甘肽S-转移酶的亚基。这是关于CR的这种“可能是令人发指的”衰老类似效应的首份报告,除了具有延缓衰老的效应。

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