Litcius/Paper detail

Regulation of mitochondrial proteostasis by the proton gradient

Maria Patrón, Daryna Tarasenko, Hendrik Nolte, Lara Kroczek, Mausumi Ghosh, Yohsuke Ohba, Yvonne Lasarzewski, Zeinab Alsadat Ahmadi, Alfredo Cabrera‐Orefice, Akinori Eyiama, Tim Kellermann, Elena I. Rugarli, Ulrich Brandt, Michael Meinecke, Thomas Langer

2022The EMBO Journal88 citationsDOIOpen Access PDF

Abstract

Abstract Mitochondria adapt to different energetic demands reshaping their proteome. Mitochondrial proteases are emerging as key regulators of these adaptive processes. Here, we use a multiproteomic approach to demonstrate the regulation of the m‐AAA protease AFG3L2 by the mitochondrial proton gradient, coupling mitochondrial protein turnover to the energetic status of mitochondria. We identify TMBIM5 (previously also known as GHITM or MICS1) as a Ca 2+ /H + exchanger in the mitochondrial inner membrane, which binds to and inhibits the m‐AAA protease. TMBIM5 ensures cell survival and respiration, allowing Ca 2+ efflux from mitochondria and limiting mitochondrial hyperpolarization. Persistent hyperpolarization, however, triggers degradation of TMBIM5 and activation of the m‐AAA protease. The m‐AAA protease broadly remodels the mitochondrial proteome and mediates the proteolytic breakdown of respiratory complex I to confine ROS production and oxidative damage in hyperpolarized mitochondria. TMBIM5 thus integrates mitochondrial Ca 2+ signaling and the energetic status of mitochondria with protein turnover rates to reshape the mitochondrial proteome and adjust the cellular metabolism.

Topics & Concepts

ProteostasisBiologyMitochondrionCell biologyMitochondrial membrane transport proteinATP–ADP translocaseInner mitochondrial membraneProteomeElectrochemical gradientBiochemistryDNAJA3Mitochondrial apoptosis-induced channelmitochondrial fusionMitochondrial DNAMembraneGeneMitochondrial Function and PathologyEnzyme Structure and FunctionATP Synthase and ATPases Research