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Sphingomyelinase Disables Inactivation in Endogenous PIEZO1 Channels

Jian Shi, Adam J. Hyman, Dario De Vecchis, Jiehan Chong, Laeticia Lichtenstein, T. Simon Futers, Myriam Rouahi, Anne Nègre‐Salvayre, Nathalie Augè, Antreas C. Kalli, David J. Beech

2020Cell Reports88 citationsDOIOpen Access PDF

Abstract

Endogenous PIEZO1 channels of native endothelium lack the hallmark inactivation often seen when these channels are overexpressed in cell lines. Because prior work showed that the force of shear stress activates sphingomyelinase in endothelium, we considered if sphingomyelinase is relevant to endogenous PIEZO1. Patch clamping was used to quantify PIEZO1-mediated signals in freshly isolated murine endothelium exposed to the mechanical forces caused by shear stress and membrane stretch. Neutral sphingomyelinase inhibitors and genetic disruption of sphingomyelin phosphodiesterase 3 (SMPD3) cause PIEZO1 to switch to profoundly inactivating behavior. Ceramide (a key product of SMPD3) rescues non-inactivating channel behavior. Its co-product, phosphoryl choline, has no effect. In contrast to ceramide, sphingomyelin (the SMPD3 substrate) does not affect inactivation but alters channel force sensitivity. The data suggest that sphingomyelinase activity, ceramide, and sphingomyelin are determinants of native PIEZO gating that enable sustained activity.

Topics & Concepts

SphingomyelinSphingomyelin phosphodiesteraseCeramidePIEZO1Cell biologyChemistryEndogenyGatingBiophysicsLipid signalingBiochemistryBiologyIon channelMechanosensitive channelsMembraneEnzymeApoptosisReceptorErythrocyte Function and PathophysiologyBlood properties and coagulationSphingolipid Metabolism and Signaling
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