首页> 外文期刊>Protoplasma: An International Journal of Cell Biology >MODES OF COENZYME Q FUNCTION IN ELECTRON TRANSFER
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MODES OF COENZYME Q FUNCTION IN ELECTRON TRANSFER

机译:电子转移中辅酶Q功能的模式

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摘要

In the mitochondrial respiratory chain, coenzyme Q acts in different ways. A diffusable coenzyme Q pool as a common substrate-like intermediate links the low-potential complexes with complex III. Its diffusion in the lipids is not rate-limiting for electron transfer, but its content is not saturating for maximal rate of NADH oxidation. Protein-bound coenzyme Q is involved in energy conservation, and may be part of enzyme supercomplexes, as in succinate cytochrome c reductase. The reason for lack of kinetic saturation of the respiratory chain by quinone concentration is in the low extent of solubility of monomeric coenzyme Q in the membrane lipids. Assays of respiratory enzymes are performed using water soluble coenzyme Q homologs and analogs; several problems exist in using oxidized quinones as accepters of coenzyme Q reductases. In particular, for complex I no acceptor appears to favorably substitute the endogenous quinone. In addition, quinone reduction sites in complex III compete with the sites in the dehydrogenases, particularly when using duroquinone. The different extent by which these sites operate when different donor substrates (NADH, succinate, glycerol-3-phosphate) are used is best explained by different exposure of the quinone acceptor sites in the dehydrogenases. [References: 82]
机译:在线粒体呼吸链中,辅酶Q以不同的方式起作用。可扩散的辅酶Q库作为常见的底物状中间体连接低电位复合物与复合物III。它在脂质中的扩散对电子转移没有速率限制,但对于最大的NADH氧化速率,其含量不会饱和。结合蛋白质的辅酶Q参与节能,并且可能是酶超复合物的一部分,如琥珀酸细胞色素C还原酶。醌浓度缺乏呼吸链的动力学饱和的原因是单体辅酶Q在膜脂中的溶解度低。使用水溶性辅酶Q同源物和类似物进行呼吸酶的测定。使用氧化醌作为辅酶Q还原酶的受体存在几个问题。特别地,对于复合物I,没有受体似乎有利地取代了内源性醌。另外,复合物III中的醌还原位点与脱氢酶中的位点竞争,特别是当使用杜罗醌时。当使用不同的供体底物(NADH,琥珀酸酯,3-磷酸甘油酯)时,这些位点的不同作用程度最好通过脱氢酶中醌受体位点的不同暴露来解释。 [参考:82]

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