Litcius/Paper detail

Both ANT and ATPase are essential for mitochondrial permeability transition but not depolarization

Maria Neginskaya, Sally E. Morris, Evgeny V. Pavlov

2022iScience34 citationsDOIOpen Access PDF

Abstract

An increase in permeability of the mitochondrial inner membrane, mitochondrial permeability transition (PT), is the central event responsible for cell death and tissue damage in conditions such as stroke and heart attack. PT is caused by the cyclosporin A (CSA)-dependent calcium-induced pore, the permeability transition pore (PTP). The molecular details of PTP are incompletely understood. We utilized holographic and fluorescent microscopy to assess the contribution of ATP synthase and adenine nucleotide translocator (ANT) toward PTP. In cells lacking either ATP synthase or ANT, we observed CSA-sensitive membrane depolarization, but not high-conductance PTP. In wild-type cells, calcium-induced CSA-sensitive depolarization preceded opening of PTP, which occurred only after nearly complete mitochondrial membrane depolarization. We propose that both ATP synthase and ANT are required for high-conductance PTP but not depolarization, which presumably occurs through activation of the low-conductance PT, which has a molecular nature that is different from both complexes.

Topics & Concepts

DepolarizationMitochondrial permeability transition poreANTATP synthaseMembrane potentialBiophysicsAdenine nucleotide translocatorMitochondrionChemistryInner mitochondrial membraneCell biologyBiologyProgrammed cell deathBiochemistryApoptosisEnzymeEcologyMitochondrial Function and PathologyATP Synthase and ATPases ResearchRNA modifications and cancer