Litcius/Paper detail

Enhancing mitochondrial pyruvate metabolism ameliorates ischemic reperfusion injury in the heart

Joseph R. Visker, Ahmad A. Cluntun, Jesse N. Velasco‐Silva, David Eberhardt, Luis Cedeño-Rosario, Thirupura S. Shankar, Rana Hamouche, Ling Jing, Hyoin Kwak, J. Yanni Hillas, Ian Aist, Eleni Tseliou, Sutip Navankasattusas, Dipayan Chaudhuri, Gregory S. Ducker, Stavros Drakos, Jared Rutter

2024JCI Insight25 citationsDOIOpen Access PDF

Abstract

The clinical therapy for treating acute myocardial infarction is primary percutaneous coronary intervention (PPCI). PPCI is effective at reperfusing the heart; however, the rapid reintroduction of blood can cause ischemia-reperfusion (I/R). Reperfusion injury is responsible for up to half of the total myocardial damage, but there are no pharmacological interventions to reduce I/R. We previously demonstrated that inhibiting monocarboxylate transporter 4 (MCT4) and redirecting pyruvate toward oxidation can blunt hypertrophy. We hypothesized that this pathway might be important during I/R. Here, we establish that the pyruvate-lactate axis plays a role in determining myocardial salvage following injury. After I/R, the mitochondrial pyruvate carrier (MPC), required for pyruvate oxidation, is upregulated in the surviving myocardium. In cardiomyocytes lacking the MPC, there was increased cell death and less salvage after I/R, which was associated with an upregulation of MCT4. To determine the importance of pyruvate oxidation, we inhibited MCT4 with a small-molecule drug (VB124) at reperfusion. This strategy normalized reactive oxygen species (ROS), mitochondrial membrane potential (ΔΨ), and Ca2+, increased pyruvate entry to the TCA cycle, increased oxygen consumption, and improved myocardial salvage and functional outcomes following I/R. Our data suggest normalizing pyruvate-lactate metabolism by inhibiting MCT4 is a promising therapy to mitigate I/R injury.

Topics & Concepts

Reperfusion injuryGlycolysisDownregulation and upregulationReactive oxygen speciesPyruvate dehydrogenase kinaseMitochondrionChemistryMyocardial infarctionMedicinePyruvate dehydrogenase complexMetabolismInternal medicineIschemiaCardiologyPharmacologyBiochemistryEnzymeGeneCardiac Ischemia and ReperfusionFuel Cells and Related MaterialsCardiovascular Function and Risk Factors