Lipid oxidation during thermogenesis in high-altitude deer mice (Peromyscus maniculatus)

Author:

Lyons Sulayman A.1,Tate Kevin B.1,Welch Jr. Kenneth C.2,McClelland Grant B.1ORCID

Affiliation:

1. Department of Biology, McMaster University, Hamilton, Ontario, Canada

2. Department of Biological Sciences, University of Toronto Scarborough, Toronto, Ontario, Canada

Abstract

When at their maximum thermogenic capacity (cold-induced V̇o2max), small endotherms reach levels of aerobic metabolism as high, or even higher, than running V̇o2max. How these high rates of thermogenesis are supported by substrate oxidation is currently unclear. The appropriate utilization of metabolic fuels that could sustain thermogenesis over extended periods may be important for survival in cold environments, like high altitude. Previous studies show that high capacities for lipid use in high-altitude deer mice may have evolved in concert with greater thermogenic capacities. The purpose of this study was to determine how lipid utilization at both moderate and maximal thermogenic intensities may differ in high- and low-altitude deer mice, and strictly low-altitude white-footed mice. We also examined the phenotypic plasticity of lipid use after acclimation to cold hypoxia (CH), conditions simulating high altitude. We found that lipids were the primary fuel supporting both moderate and maximal rates of thermogenesis in both species of mice. Lipid oxidation increased threefold in mice from 30°C to 0°C, consistent with increases in oxidation of [13C]palmitic acid. CH acclimation led to an increase in [13C]palmitic acid oxidation at 30°C but did not affect total lipid oxidation. Lipid oxidation rates at cold-induced V̇o2max were two- to fourfold those at 0°C and increased further after CH acclimation, especially in high-altitude deer mice. These are the highest mass-specific lipid oxidation rates observed in any land mammal. Uncovering the mechanisms that allow for these high rates of oxidation will aid our understanding of the regulation of lipid metabolism.

Funder

Natural Sciences and Engineering Research Council of Canada (NSERC) Discovery Grant

NSERC Discovery Accelerator Grant

NSERC Canada Graduate Scholarship

Publisher

American Physiological Society

Subject

Physiology (medical),Physiology

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