A Piezo1 Open State Reveals a Multi-fenestrated Ion Permeation Pathway

Author:

Jiang Wenjuan,Del Rosario John SmithORCID,Botello-Smith Wesley,Zhao Siyuan,Lin Yi-chun,Zhang Han,Lacroix JérômeORCID,Rohacs TiborORCID,Luo Yun LynaORCID

Abstract

ABSTRACTForce-sensing Piezo channels are essential to many aspects of vertebrate physiology. Activation of Piezo1 is facilitated by the presence of negative membrane lipids in the inner leaflet, such as phosphatidylinositol-4,5-bisphosphate (PIP2). Here, to study how Piezo1 opens, we performed molecular dynamics simulations of Piezo1 in membranes flattened by the periodic boundary effect and with or without PIP2 lipids. The Piezo1 pore spontaneously opens in the asymmetrical bilayer but not in the symmetric membrane or when PIP2 lipids are neutralized. Electrophysiological characterization of putative PIP2-interacting Piezo1 residues suggests the contribution of multiple PIP2 binding sites. Our Piezo1 open state recapitulates ionic selectivity, unitary conductance and mutant phenotypes obtained from numerous experimental studies. Tracking ion diffusion through the open pore reveals the presence of intracellular and extracellular fenestrations, delineating a multi-fenestrated permeation pathway. This open state sheds light on the mechanisms of lipid modulation, permeation, and selectivity in a Piezo channel.

Publisher

Cold Spring Harbor Laboratory

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