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Mitochondrial F-ATP Synthase and Its Transition into an Energy-Dissipating Molecular Machine

机译:线粒体F-ATP合酶及其向耗能分子机器的转化

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摘要

The mitochondrial F-ATP synthase is the principal energy-conserving nanomotor of cells that harnesses the proton motive force generated by the respiratory chain to make ATP from ADP and phosphate in a process known as oxidative phosphorylation. In the energy-converting membranes, F-ATP synthase is a multisubunit complex organized into a membrane-extrinsic F1 sector and a membrane-intrinsic FO domain, linked by central and peripheral stalks. Due to its essential role in the cellular metabolism, malfunction of F-ATP synthase has been associated with a variety of pathological conditions, and the enzyme is now considered as a promising drug target for multiple disease conditions and for the regulation of energy metabolism. We discuss structural and functional features of mitochondrial F-ATP synthase as well as several conditions that partially or fully inhibit the coupling between the F1 catalytic activities and the FO proton translocation, thus decreasing the cellular metabolic efficiency and transforming the enzyme into an energy-dissipating structure through molecular mechanisms that still remain to be defined.
机译:线粒体F-ATP合酶是细胞的主要节能纳米马达,它利用呼吸链产生的质子原动力,以称为ADP和磷酸盐的方式制造ATP,称为氧化磷酸化。在能量转换膜中,F-ATP合酶是一个多亚基复合物,组织成膜外源性F1区段和膜内源性FO结构域,由中枢和外周茎连接。由于其在细胞代谢中的重要作用,F-ATP合酶的功能失常与多种病理状况有关,现在该酶被认为是多种疾病状况和能量代谢调节的有希望的药物靶标。我们讨论了线粒体F-ATP合酶的结构和功能特征,以及部分或完全抑制F1催化活性和FO质子转运之间耦合的几种条件,从而降低了细胞代谢效率并将酶转化为耗能通过分子机制的结构仍然有待确定。

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