压电1
生物物理学
机械转化
细胞骨架
离子通道
膜曲率
膜
化学
幽灵蛋白
机械敏感通道
生物
细胞生物学
细胞
生物化学
脂质双层
受体
作者
Andra C. Dumitru,Amaury Stommen,Melanie Koehler,Anne‐Sophie Cloos,Jinsung Yang,Arnaud Leclercqz,Donatienne Tyteca,David Alsteens
出处
期刊:Nano Letters
[American Chemical Society]
日期:2021-06-14
卷期号:21 (12): 4950-4958
被引量:27
标识
DOI:10.1021/acs.nanolett.1c00599
摘要
PIEZO1 ion channels are activated by mechanical stimuli, triggering intracellular chemical signals. Recent structural studies suggest that plasma membrane tension or local curvature changes modulate PIEZO1 channel gating and activation. However, whether PIEZO1 localization is governed by tension gradients or long-range mechanical perturbations across the cells is still unclear. Here, we probe the nanoscale localization of PIEZO1 on red blood cells (RBCs) at high resolution (∼30 nm), and we report for the first time the existence of submicrometric PIEZO1 clusters in native conditions. Upon interaction with Yoda1, an allosteric modulator, PIEZO1 clusters increase in abundance in regions of higher membrane tension and lower curvature. We further show that PIEZO1 ion channels interact with the spectrin cytoskeleton in both resting and activated states. Our results point toward a strong interplay between plasma membrane tension gradients, curvature, and cytoskeleton association of PIEZO1.
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