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线粒体复合物I的质子泵浦:泛醌类似物的差异激活作用

Proton pumping of mitochondrial complex I: differential activation by analogs of ubiquinone.

作者信息

Helfenbaum L, Ngo A, Ghelli A, Linnane A W, Degli Esposti M

机构信息

Centre for Molecular Biology and Medicine, Monash University, Clayton, Victoria, Australia.

出版信息

J Bioenerg Biomembr. 1997 Feb;29(1):71-80. doi: 10.1023/a:1022415906999.

Abstract

As part of the ongoing studies aimed at elucidating the mechanism of the energy conserving function of mitochondrial complex I, NADH: ubiquinone (Q) reductase, we have investigated how short-chain Q analogs activate the proton pumping function of this complex. Using a pH-sensitive fluorescent dye we have monitored both the extent and initial velocity of proton pumping of complex I in submitochondrial particles. The results are consistent with two sites of interaction of Q analogs with complex I, each having different proton pumping capacity. One is the physiological site which leads to a rapid proton pumping and a stoichiometric consumption of NADH associated with the reduction of the most hydrophobic Q analogs. Of these, heptyl-Q appears to be the most efficient substrate in the assay of proton pumping. Q analogs with a short-chain of less than six carbons interact with a second site which drives a slow proton pumping activity associated with NADH oxidation that is overstoichiometric to the reduced quinone acceptor. This activity is also nonphysiological, since hydrophilic Q analogs show little or no respiratory control ratio of their NADH:Q reductase activity, contrary to hydrophobic Q analogs.

摘要

作为旨在阐明线粒体复合物I(NADH:泛醌(Q)还原酶)能量保存功能机制的正在进行的研究的一部分,我们研究了短链Q类似物如何激活该复合物的质子泵功能。使用对pH敏感的荧光染料,我们监测了亚线粒体颗粒中复合物I质子泵的程度和初始速度。结果与Q类似物与复合物I的两个相互作用位点一致,每个位点具有不同的质子泵能力。一个是生理位点,它导致快速的质子泵浦以及与最疏水的Q类似物还原相关的NADH的化学计量消耗。其中,庚基-Q似乎是质子泵浦测定中最有效的底物。碳链少于六个碳的短链Q类似物与第二个位点相互作用,该位点驱动与NADH氧化相关的缓慢质子泵浦活性,该活性相对于还原的醌受体是超化学计量的。这种活性也是非生理性的,因为与疏水Q类似物相反,亲水Q类似物的NADH:Q还原酶活性几乎没有或没有呼吸控制率。

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