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Metabolic switch from fatty acid oxidation to glycolysis in knock‐in mouse model of Barth syndrome

Arpita Chowdhury, Angela Boshnakovska, Abhishek Aich, Aditi Methi, Ana Maria Vergel Leon, Ivan Silbern, Christian Lüchtenborg, Lukas Cyganek, Jan Procházka, Radislav Sedláček, Jiří Lindovský, Dominic Wachs, Zuzana Nichtová, Dagmar Zudová, Gizela Koubkova, André Fischer, Henning Urlaub, Britta Brügger, Dörthe M. Katschinski, Jan Dudek, Peter Rehling

2023EMBO Molecular Medicine29 citationsDOIOpen Access PDF

Abstract

Abstract Mitochondria are central for cellular metabolism and energy supply. Barth syndrome (BTHS) is a severe disorder, due to dysfunction of the mitochondrial cardiolipin acyl transferase tafazzin. Altered cardiolipin remodeling affects mitochondrial inner membrane organization and function of membrane proteins such as transporters and the oxidative phosphorylation (OXPHOS) system. Here, we describe a mouse model that carries a G197V exchange in tafazzin, corresponding to BTHS patients. TAZ G197V mice recapitulate disease‐specific pathology including cardiac dysfunction and reduced oxidative phosphorylation. We show that mutant mitochondria display defective fatty acid‐driven oxidative phosphorylation due to reduced levels of carnitine palmitoyl transferases. A metabolic switch in ATP production from OXPHOS to glycolysis is apparent in mouse heart and patient iPSC cell‐derived cardiomyocytes. An increase in glycolytic ATP production inactivates AMPK causing altered metabolic signaling in TAZ G197V . Treatment of mutant cells with AMPK activator reestablishes fatty acid‐driven OXPHOS and protects mice against cardiac dysfunction.

Topics & Concepts

CardiolipinOxidative phosphorylationGlycolysisMitochondrionAMPKBeta oxidationBiologyCell biologyPhosphorylationBiochemistryFatty acidMetabolismProtein kinase APhospholipidMembraneMitochondrial Function and PathologyAutophagy in Disease and TherapyMetabolism and Genetic Disorders