Litcius/Paper detail

Arf1 coordinates fatty acid metabolism and mitochondrial homeostasis

Ludovic Enkler, Viktória Szentgyörgyi, Mirjam Pennauer, Cristina Prescianotto‐Baschong, Isabelle Riezman, Aneta Więsyk, Reut Ester Avraham, Martin Spiess, Einat Zalckvar, Róża Kucharczyk, Howard Riezman, Anne Spang

2023Nature Cell Biology72 citationsDOIOpen Access PDF

Abstract

Lipid mobilization through fatty acid β-oxidation is a central process essential for energy production during nutrient shortage. In yeast, this catabolic process starts in the peroxisome from where β-oxidation products enter mitochondria and fuel the tricarboxylic acid cycle. Little is known about the physical and metabolic cooperation between these organelles. Here we found that expression of fatty acid transporters and of the rate-limiting enzyme involved in β-oxidation is decreased in cells expressing a hyperactive mutant of the small GTPase Arf1, leading to an accumulation of fatty acids in lipid droplets. Consequently, mitochondria became fragmented and ATP synthesis decreased. Genetic and pharmacological depletion of fatty acids phenocopied the arf1 mutant mitochondrial phenotype. Although β-oxidation occurs in both mitochondria and peroxisomes in mammals, Arf1's role in fatty acid metabolism is conserved. Together, our results indicate that Arf1 integrates metabolism into energy production by regulating fatty acid storage and utilization, and presumably organelle contact sites.

Topics & Concepts

PeroxisomeMitochondrionBiochemistryFatty acidCitric acid cycleCell biologyBeta oxidationBiologyOrganelleFatty acid metabolismLipid metabolismLipid dropletMetabolismCatabolismChemistryGeneLipid metabolism and biosynthesisAdipose Tissue and MetabolismPeroxisome Proliferator-Activated Receptors