机械转化
跨膜结构域
机械敏感通道
跨膜蛋白
生物物理学
压电1
门控
螺旋(腹足类)
化学
离子通道
细胞生物学
膜
生物
生物化学
受体
蜗牛
生态学
作者
Qiancheng Zhao,Heng Zhou,Shaopeng Chi,Yanfeng Wang,Jianhua Wang,Jie Geng,Kun Wu,Wenhao Liu,Tingxin Zhang,Meng‐Qiu Dong,Jiawei Wang,Xueming Li,Bailong Xiao
出处
期刊:Nature
[Springer Nature]
日期:2018-01-22
卷期号:554 (7693): 487-492
被引量:443
摘要
The mechanosensitive Piezo channels function as key eukaryotic mechanotransducers. However, their structures and mechanogating mechanisms remain unknown. Here we determine the three-bladed, propeller-like electron cryo-microscopy structure of mouse Piezo1 and functionally reveal its mechanotransduction components. Despite the lack of sequence repetition, we identify nine repetitive units consisting of four transmembrane helices each-which we term transmembrane helical units (THUs)-which assemble into a highly curved blade-like structure. The last transmembrane helix encloses a hydrophobic pore, followed by three intracellular fenestration sites and side portals that contain pore-property-determining residues. The central region forms a 90 A-long intracellular beam-like structure, which undergoes a lever-like motion to connect THUs to the pore via the interfaces of the C-terminal domain, the anchor-resembling domain and the outer helix. Deleting extracellular loops in the distal THUs or mutating single residues in the beam impairs the mechanical activation of Piezo1. Overall, Piezo1 possesses a unique 38-transmembrane-helix topology and designated mechanotransduction components, which enable a lever-like mechanogating mechanism.
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