Author:
Henze Erik,Ehrlich Jacqueline J.,Burkhardt Russell N.,Fox Bennett W.,Michalski Kevin,Kramer Lydia,Lenfest Margret,Boesch Jordyn M.,Schroeder Frank C.,Kawate Toshimitsu
Abstract
AbstractAdenosine triphosphate (ATP) serves as an extracellular messenger that mediates diverse cell-to-cell communication. Compelling evidence supports that ATP is released from cells through pannexins, a family of heptameric large pore-forming channels. However, the activation mechanisms that trigger ATP release by pannexins remain poorly understood. Here, we discover lysophospholipids as endogenous pannexin activators, using activity-guided fractionation of mouse tissue extracts combined with untargeted metabolomics and electrophysiology. We show that lysophospholipids directly and reversibly activate pannexins in the absence of other proteins. Molecular docking, mutagenesis, and single-particle cryo-EM reconstructions suggest that lysophospholipids open pannexin channels by altering the conformation of the N-terminal domain. Our results provide a connection between lipid metabolism and ATP signaling, both of which play major roles in inflammation and neurotransmission.One-Sentence SummaryUntargeted metabolomics discovers a class of messenger lipids as endogenous activators of membrane channels important for inflammation and neurotransmission.
Publisher
Cold Spring Harbor Laboratory
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