Radboud Institute for Molecular Life Sciences, Department of Pediatrics, Radboud University Medical Center, Geert Grooteplein-Zuid 10, 6525, GA, Nijmegen, The Netherlands.
Cluster of Excellence Macromolecular Complexes, Goethe-University, Max von Laue Str. 9, 60438, Frankfurt am Main, Germany.
Nat Commun. 2018 Oct 29;9(1):4500. doi: 10.1038/s41467-018-06955-y.
Complex I (proton-pumping NADH:ubiquinone oxidoreductase) is the largest enzyme of the mitochondrial respiratory chain and a significant source of reactive oxygen species (ROS). We hypothesized that during energy conversion by complex I, electron transfer onto ubiquinone triggers the concerted rearrangement of three protein loops of subunits ND1, ND3, and 49-kDa thereby generating the power-stoke driving proton pumping. Here we show that fixing loop TMH1-2 to the nearby subunit PSST via a disulfide bridge introduced by site-directed mutagenesis reversibly disengages proton pumping without impairing ubiquinone reduction, inhibitor binding or the Active/Deactive transition. The X-ray structure of mutant complex I indicates that the disulfide bridge immobilizes but does not displace the tip of loop TMH1-2. We conclude that movement of loop TMH1-2 located at the ubiquinone-binding pocket is required to drive proton pumping corroborating one of the central predictions of our model for the mechanism of energy conversion by complex I proposed earlier.
复合体 I(质子泵 NADH:泛醌氧化还原酶)是线粒体呼吸链中最大的酶,也是活性氧(ROS)的重要来源。我们假设,在复合体 I 的能量转换过程中,电子转移到泛醌上会触发 ND1、ND3 和 49-kDa 亚基三个蛋白环的协同重排,从而产生驱动质子泵的动力冲程。在这里,我们通过定点突变引入二硫键将 TMH1-2 环固定到附近的 PSST 亚基上,结果表明这种固定可使质子泵的功能可逆失活,而不损害泛醌还原、抑制剂结合或活性/失活转变。突变复合体 I 的 X 射线结构表明,二硫键固定但不移动 TMH1-2 环的末端。我们得出结论,位于泛醌结合口袋的 TMH1-2 环的运动是驱动质子泵的必要条件,这证实了我们之前提出的复合体 I 能量转换机制模型的一个核心预测。
Zotero 插件
