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Global mitochondrial protein import proteomics reveal distinct regulation by translation and translocation machinery

Jasmin Schäfer, Süleyman Bozkurt, Jonas B. Michaelis, Kevin Klann, Christian Münch

2021Molecular Cell84 citationsDOIOpen Access PDF

Abstract

Most mitochondrial proteins are translated in the cytosol and imported into mitochondria. Mutations in the mitochondrial protein import machinery cause human pathologies. However, a lack of suitable tools to measure protein uptake across the mitochondrial proteome has prevented the identification of specific proteins affected by import perturbation. Here, we introduce mePRODmt, a pulsed-SILAC based proteomics approach that includes a booster signal to increase the sensitivity for mitochondrial proteins selectively, enabling global dynamic analysis of endogenous mitochondrial protein uptake in cells. We applied mePRODmt to determine protein uptake kinetics and examined how inhibitors of mitochondrial import machineries affect protein uptake. Monitoring changes in translation and uptake upon mitochondrial membrane depolarization revealed that protein uptake was extensively modulated by the import and translation machineries via activation of the integrated stress response. Strikingly, uptake changes were not uniform, with subsets of proteins being unaffected or decreased due to changes in translation or import capacity.

Topics & Concepts

BiologyMitochondrionCell biologyProteomicsTransport proteinStable isotope labeling by amino acids in cell cultureTranslation (biology)ProteomeMitochondrial membrane transport proteinCytosolQuantitative proteomicsInner mitochondrial membraneBiochemistryMessenger RNAEnzymeGeneMitochondrial Function and PathologyATP Synthase and ATPases ResearchRNA and protein synthesis mechanisms
Global mitochondrial protein import proteomics reveal distinct regulation by translation and translocation machinery | Litcius