Inhibition of sarcolemmal FAT/CD36 by sulfo-N-succinimidyl oleate rapidly corrects metabolism and restores function in the diabetic heart following hypoxia/reoxygenation

The type 2 diabetic heart oxidizes more fat and less glucose, which can impair metabolic flexibility and function. Increased sarcolemmal fatty acid translocase (FAT/CD36) imports more fatty acid into the diabetic myocardium, feeding increased fatty acid oxidation and elevated lipid deposition. Unlik...

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Bibliographic Details
Published in:Cardiovascular research 2017-06, Vol.113 (7), p.737-748
Main Authors: Mansor, Latt S, Sousa Fialho, Maria da Luz, Yea, Georgina, Coumans, Will A, West, James A, Kerr, Matthew, Carr, Carolyn A, Luiken, Joost J F P, Glatz, Jan F C, Evans, Rhys D, Griffin, Julian L, Tyler, Damian J, Clarke, Kieran, Heather, Lisa C
Format: Article
Language:English
Subjects:
Animals
CD36 Antigens - antagonists & inhibitors
CD36 Antigens - metabolism
Cell Hypoxia
Citric Acid Cycle - drug effects
Diabetes Mellitus, Type 2 - complications
Diabetes Mellitus, Type 2 - metabolism
Diabetes Mellitus, Type 2 - physiopathology
Diabetic Cardiomyopathies - drug therapy
Diabetic Cardiomyopathies - etiology
Diabetic Cardiomyopathies - metabolism
Diabetic Cardiomyopathies - physiopathology
Energy Metabolism - drug effects
Fatty Acids - metabolism
Isolated Heart Preparation
Lipid Metabolism - drug effects
Male
Myocardial Reperfusion Injury - drug therapy
Myocardial Reperfusion Injury - etiology
Myocardial Reperfusion Injury - metabolism
Myocardial Reperfusion Injury - physiopathology
Myocardium - metabolism
Oleic Acids - pharmacology
Original
Oxidation-Reduction
Oxidative Stress - drug effects
Rats, Wistar
Sarcolemma - drug effects
Sarcolemma - metabolism
Succinimides - pharmacology
Time Factors
Triglycerides - metabolism
Ventricular Function, Left - drug effects
Ventricular Pressure - drug effects
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Summary:The type 2 diabetic heart oxidizes more fat and less glucose, which can impair metabolic flexibility and function. Increased sarcolemmal fatty acid translocase (FAT/CD36) imports more fatty acid into the diabetic myocardium, feeding increased fatty acid oxidation and elevated lipid deposition. Unlike other metabolic modulators that target mitochondrial fatty acid oxidation, we proposed that pharmacologically inhibiting fatty acid uptake, as the primary step in the pathway, would provide an alternative mechanism to rebalance metabolism and prevent lipid accumulation following hypoxic stress. Hearts from type 2 diabetic and control male Wistar rats were perfused in normoxia, hypoxia and reoxygenation, with the FAT/CD36 inhibitor sulfo-N-succinimidyl oleate (SSO) infused 4 min before hypoxia. SSO infusion into diabetic hearts decreased the fatty acid oxidation rate by 29% and myocardial triglyceride concentration by 48% compared with untreated diabetic hearts, restoring fatty acid metabolism to control levels following hypoxia-reoxygenation. SSO infusion increased the glycolytic rate by 46% in diabetic hearts during hypoxia, increased pyruvate dehydrogenase activity by 53% and decreased lactate efflux rate by 56% compared with untreated diabetic hearts during reoxygenation. In addition, SSO treatment of diabetic hearts increased intermediates within the second span of the Krebs cycle, namely fumarate, oxaloacetate, and the FAD total pool. The cardiac dysfunction in diabetic hearts following decreased oxygen availability was prevented by SSO-infusion prior to the hypoxic stress. Infusing SSO into diabetic hearts increased rate pressure product by 60% during hypoxia and by 32% following reoxygenation, restoring function to control levels. Diabetic hearts have limited metabolic flexibility and cardiac dysfunction when stressed, which can be rapidly rectified by reducing fatty acid uptake with the FAT/CD36 inhibitor, SSO. This novel therapeutic approach not only reduces fat oxidation but also lipotoxicity, by targeting the primary step in the fatty acid metabolism pathway.
ISSN:0008-6363
1755-3245
DOI:10.1093/cvr/cvx045