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Ferroptotic pores induce Ca2+ fluxes and ESCRT-III activation to modulate cell death kinetics

Lohans Pedrera, Rafael A. Espiritu, Uris Ros, Josephine Weber, Anja Schmitt, Jenny Stroh, Stephan Hailfinger, Silvia von Karstedt, Ana J. García‐Sáez

2020Cell Death and Differentiation298 citationsDOIOpen Access PDF

Abstract

Abstract Ferroptosis is an iron-dependent form of regulated necrosis associated with lipid peroxidation. Despite its key role in the inflammatory outcome of ferroptosis, little is known about the molecular events leading to the disruption of the plasma membrane during this type of cell death. Here we show that a sustained increase in cytosolic Ca 2+ is a hallmark of ferroptosis that precedes complete bursting of the cell. We report that plasma membrane damage leading to ferroptosis is associated with membrane nanopores of a few nanometers in radius and that ferroptosis, but not lipid peroxidation, can be delayed by osmoprotectants. Importantly, Ca 2+ fluxes during ferroptosis induce the activation of the ESCRT-III-dependent membrane repair machinery, which counterbalances the kinetics of cell death and modulates the immunological signature of ferroptosis. Our findings with ferroptosis provide a unifying concept that sustained increase of cytosolic Ca 2+ prior to plasma membrane rupture is a common feature of regulated types of necrosis and position ESCRT-III activation as a general protective mechanism in these lytic cell death pathways.

Topics & Concepts

Cell biologyProgrammed cell deathCytosolChemistryESCRTLipid peroxidationGPX4Lipid bilayerNecroptosisBystander effectPhospholipid scramblaseEndosomeIntracellularBiophysicsBiologyApoptosisMembraneOxidative stressBiochemistryPhospholipidImmunologyPhosphatidylserineCatalaseGlutathione peroxidaseEnzymeFerroptosis and cancer prognosisTrace Elements in HealthHeme Oxygenase-1 and Carbon Monoxide