Limited transfer of cytosolic NADH into mitochondria at high cardiac workload

Limited transfer of cytosolic NADH into mitochondria at high cardiac workload

Glycolysis supplements energy synthesis at high cardiac workloads, producing not only ATP but also cytosolic NADH and pyruvate for oxidative ATP synthesis. Despite adequate Po(2), speculation exists that not all cytosolic NADH is oxidized by the mitochondria, leading to lactate production. In this s...

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Bibliographic Details
Published in:American journal of physiology. Heart and circulatory physiology Vol. 286; no. 6; p. H2237
Main Authors: O'Donnell, J Michael, Kudej, Raymond K, LaNoue, Kathyrn F, Vatner, Stephen F, Lewandowski, E Douglas
Format: Journal Article
Language:English
Published: United States 01-06-2004
Subjects:
Acetates - pharmacokinetics
Animals
Carbon Isotopes
Coronary Circulation
Cytosol - metabolism
Dogs
Energy Metabolism - physiology
Female
Glutamic Acid - metabolism
Heart - physiology
Lactic Acid - metabolism
Magnetic Resonance Spectroscopy
Male
Mitochondria - metabolism
Myocardial Contraction - physiology
Myocardium - metabolism
NAD - metabolism
Oxygen - metabolism
Succinic Acid - metabolism
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Summary:Glycolysis supplements energy synthesis at high cardiac workloads, producing not only ATP but also cytosolic NADH and pyruvate for oxidative ATP synthesis. Despite adequate Po(2), speculation exists that not all cytosolic NADH is oxidized by the mitochondria, leading to lactate production. In this study, we elucidate the mechanism for limited cytosolic NADH oxidation and increased lactate production at high workload despite adequate myocardial blood flow and oxygenation. Reducing equivalents from glycolysis enter mitochondria via exchange of mitochondrial alpha-ketoglutarate (alpha-KG) for cytosolic malate. This exchange was monitored at baseline and at high workloads by comparing (13)C enrichment between the products of alpha-KG oxidation (succinate) and alpha-KG efflux from mitochondria (glutamate). Under general anesthesia, a left thoracotomy was performed on 14 dogs and [2-(13)C]acetate was infused into the left anterior descending artery for 40 min. The rate-pressure product was 9,035 +/- 1,972 and 21,659 +/- 5,266 mmHg.beats.min(-1) (n = 7) at baseline (n = 7) and with dobutamine, respectively. (13)C enrichment of succinate was 57 +/- 10% at baseline and 45 +/- 13% at elevated workload (not significant), confirming oxidation of [2-(13)C]acetate. However, cytosolic glutamate enrichment, a marker of cytosolic NADH transfer to mitochondria, was dramatically reduced at high cardiac workload (11 +/- 1%) vs. baseline (50 +/- 14%, P < 0.05). This reduced exchange of (13)C from alpha-KG to cytosolic glutamate at high work indicates reduced shuttling of cytosolic reducing equivalents into the mitochondria. Myocardial tissue lactate increased 78%, countering this reduced oxidation of cytosolic NADH. The findings elucidate a contributing mechanism to glycolysis outpacing glucose oxidation in the absence of myocardial ischemia.
ISSN:0363-6135
DOI:10.1152/ajpheart.01113.2003