生物
ATP合成酶γ亚单位
蛋白质亚单位
ATP合酶
化学渗透
生物物理学
Giα亚单位
三磷酸腺苷
ATP水解
生物化学
ATP酶
酶
基因
作者
Yuezheng Lai,Yuying Zhang,Shan Zhou,Jinxu Xu,Zhanqiang Du,Ziyan Feng,Long Yu,Ziqing Zhao,Weiwei Wang,Yanting Tang,Xiuna Yang,Luke W. Guddat,Fengjiang Liu,Gao Yan,Zihe Rao,Haiming Gong
出处
期刊:Molecular Cell
[Elsevier]
日期:2023-05-26
卷期号:83 (12): 2137-2147.e4
被引量:31
标识
DOI:10.1016/j.molcel.2023.04.029
摘要
Biological energy currency ATP is produced by F1Fo-ATP synthase. However, the molecular mechanism for human ATP synthase action remains unknown. Here, we present snapshot images for three main rotational states and one substate of human ATP synthase using cryoelectron microscopy. These structures reveal that the release of ADP occurs when the β subunit of F1Fo-ATP synthase is in the open conformation, showing how ADP binding is coordinated during synthesis. The accommodation of the symmetry mismatch between F1 and Fo motors is resolved by the torsional flexing of the entire complex, especially the γ subunit, and the rotational substep of the c subunit. Water molecules are identified in the inlet and outlet half-channels, suggesting that the proton transfer in these two half-channels proceed via a Grotthus mechanism. Clinically relevant mutations are mapped to the structure, showing that they are mainly located at the subunit-subunit interfaces, thus causing instability of the complex.
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