Whole Body Deletion of AMP-activated Protein Kinase β2 Reduces Muscle AMPK Activity and Exercise Capacity

Gregory R. Steinberg; Hayley M. O'Neill; Nicolas L. Dzamko; Sandra Galic; Tim Naim; René Koopman; Sebastian B. Jørgensen; Jane Honeyman; Kimberly Hewitt; Zhi-Ping Chen; Jonathan D. Schertzer; John W. Scott; Frank Koentgen; Gordon S. Lynch; Matthew J. Watt; Bryce J. W. van Denderen; Duncan J. Campbell; Bruce E. Kemp

doi:10.1074/jbc.M110.102434

Whole Body Deletion of AMP-activated Protein Kinase β2 Reduces Muscle AMPK Activity and Exercise Capacity*

From the ^‡Department of Medicine, McMaster University, Hamilton, Ontario L8N 3Z5, Canada,
the ^§St. Vincent's Institute of Medical Research and Department of Medicine, University of Melbourne, 41 Victoria Parade, Fitzroy, Victoria 3065, Australia,
the ^¶Department of Physiology, University of Melbourne, Parkville 3052, Australia,
the ^‖Diabetes Research Unit, Novo Nordisk A/S, Maaloev 2760, Denmark,
^**Ozgene Pty., Ltd., Perth, Australia, and
the ^‡‡Department of Physiology, Monash University, Clayton, Victoria 3800, Australia

1 Canadian Research Chair in Metabolism, Obesity and Type 2 Diabetes and an honorary National Health and Medical Research Council of Australia Fellow. To whom correspondence should be addressed: 1200 Main St. W., Hamilton, Ontario L8N 3Z5, Canada. Tel.: 905-521-2100 (ext. 21691); Fax: 905-777-7856; E-mail: gsteinberg{at}mcmaster.ca.

Abstract

AMP-activated protein kinase (AMPK) β subunits (β1 and β2) provide scaffolds for binding α and γ subunits and contain a carbohydrate-binding module important for regulating enzyme activity. We generated C57Bl/6 mice with germline deletion of AMPK β2 (β2 KO) and examined AMPK expression and activity, exercise capacity, metabolic control during muscle contractions, aminoimidazole carboxamide ribonucleotide (AICAR) sensitivity, and susceptibility to obesity-induced insulin resistance. We find that β2 KO mice are viable and breed normally. β2 KO mice had a reduction in skeletal muscle AMPK α1 and α2 expression despite up-regulation of the β1 isoform. Heart AMPK α2 expression was also reduced but this did not affect resting AMPK α1 or α2 activities. AMPK α1 and α2 activities were not changed in liver, fat, or hypothalamus. AICAR-stimulated glucose uptake but not fatty acid oxidation was impaired in β2 KO mice. During treadmill running β2 KO mice had reduced maximal and endurance exercise capacity, which was associated with lower muscle and heart AMPK activity and reduced levels of muscle and liver glycogen. Reductions in exercise capacity of β2 KO mice were not due to lower muscle mitochondrial content or defects in contraction-stimulated glucose uptake or fatty acid oxidation. When challenged with a high-fat diet β2 KO mice gained more weight and were more susceptible to the development of hyperinsulinemia and glucose intolerance. In summary these data show that deletion of AMPK β2 reduces AMPK activity in skeletal muscle resulting in impaired exercise capacity and the worsening of diet-induced obesity and glucose intolerance.

Footnotes

↵2 Supported by a scholarship from the National Heart Foundation.
↵3 Supported by Research Fellowship 271-05-0697 from the Danish Medical Research Council.
↵4 Supported by research fellowships from the National Health and Medical Research Council of Australia.
↵* This work was supported in part by grants from the Australian Research Council (to B. E. K.), National Health and Medical Research Council (to D. J. C., B. E. K., G. R. S., and M. J. W.), Natural Science and Engineering Research Council of Canada (to G. R. S.), Diabetes Australia Research Trust (to G. R. S.), and the National Heart Foundation of Australia (to B. E. K. and D. J. C.).
↵ The on-line version of this article (available at http://www.jbc.org) contains supplemental Figs. S1 and S2.