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线粒体氧化磷酸化的生理多样性

Physiological diversity of mitochondrial oxidative phosphorylation.

作者信息

Benard G, Faustin B, Passerieux E, Galinier A, Rocher C, Bellance N, Delage J-P, Casteilla L, Letellier T, Rossignol R

机构信息

INSERM U688, Physiopathologie mitochondriale, Université Victor Segalen-Bordeaux 2, Bordeaux, France.

出版信息

Am J Physiol Cell Physiol. 2006 Dec;291(6):C1172-82. doi: 10.1152/ajpcell.00195.2006. Epub 2006 Jun 28.

Abstract

To investigate the physiological diversity in the regulation and control of mitochondrial oxidative phosphorylation, we determined the composition and functional features of the respiratory chain in muscle, heart, liver, kidney, and brain. First, we observed important variations in mitochondrial content and infrastructure via electron micrographs of the different tissue sections. Analyses of respiratory chain enzyme content by Western blot also showed large differences between tissues, in good correlation with the expression level of mitochondrial transcription factor A and the activity of citrate synthase. On the isolated mitochondria, we observed a conserved molar ratio between the respiratory chain complexes and a variable stoichiometry for coenzyme Q and cytochrome c, with typical values of [1-1.5]:[30-135]:[3]:[9-35]:[6.5-7.5] for complex II:coenzyme Q:complex III:cytochrome c:complex IV in the different tissues. The functional analysis revealed important differences in maximal velocities of respiratory chain complexes, with higher values in heart. However, calculation of the catalytic constants showed that brain contained the more active enzyme complexes. Hence, our study demonstrates that, in tissues, oxidative phosphorylation capacity is highly variable and diverse, as determined by different combinations of 1) the mitochondrial content, 2) the amount of respiratory chain complexes, and 3) their intrinsic activity. In all tissues, there was a large excess of enzyme capacity and intermediate substrate concentration, compared with what is required for state 3 respiration. To conclude, we submitted our data to a principal component analysis that revealed three groups of tissues: muscle and heart, brain, and liver and kidney.

摘要

为了研究线粒体氧化磷酸化调控中的生理多样性,我们测定了肌肉、心脏、肝脏、肾脏和大脑中呼吸链的组成和功能特征。首先,通过不同组织切片的电子显微镜照片,我们观察到线粒体含量和结构的重要差异。蛋白质免疫印迹法对呼吸链酶含量的分析也显示,不同组织之间存在很大差异,这与线粒体转录因子A的表达水平和柠檬酸合酶的活性密切相关。在分离的线粒体上,我们观察到呼吸链复合物之间的摩尔比是保守的,辅酶Q和细胞色素c的化学计量是可变的,不同组织中复合物II:辅酶Q:复合物III:细胞色素c:复合物IV的典型值为[1 - 1.5]:[30 - 135]:[3]:[9 - 35]:[6.5 - 7.5]。功能分析揭示了呼吸链复合物最大速度的重要差异,心脏中的值更高。然而,催化常数的计算表明,大脑中含有活性更高的酶复合物。因此,我们的研究表明,在组织中,氧化磷酸化能力高度可变且多样,这取决于以下不同组合:1)线粒体含量,2)呼吸链复合物的数量,以及3)它们的内在活性。与状态3呼吸所需的量相比,所有组织中酶容量和中间底物浓度都有大量过剩。总之,我们将数据进行了主成分分析,结果显示出三组组织:肌肉和心脏、大脑、肝脏和肾脏。

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