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Sucrose nonfermenting AMPK-related kinase (SNARK) regulates exercise-stimulated and ischemia-stimulated glucose transport in the heart.

Citation
Sun, X. -L., et al. “Sucrose Nonfermenting Ampk-Related Kinase (Snark) Regulates Exercise-Stimulated And Ischemia-Stimulated Glucose Transport In The Heart.”. Journal Of Cellular Biochemistry, pp. 685-696.
Center Joslin Diabetes Center
Author Xiang-Lan Sun, Sarah J Lessard, Ding An, Ho-Jin Koh, Hiroyasu Esumi, Michael F Hirshman, Laurie J Goodyear
Keywords Akt substrate of 160 kDa, HL1 cardiomyocytes, glycogen, insulin
Abstract

The signaling mechanisms mediating myocardial glucose transport are not fully understood. Sucrose nonfermenting AMP-activated protein kinase (AMPK)-related kinase (SNARK) is an AMPK-related protein kinase that is expressed in the heart and has been implicated in contraction-stimulated glucose transport in mouse skeletal muscle. We first determined if SNARK is phosphorylated on Thr , a site critical for SNARK activity. Mice were treated with exercise, ischemia, submaximal insulin, or maximal insulin. Treadmill exercise slightly, but significantly increased SNARK Thr phosphorylation. Ischemia also increased SNARK Thr phosphorylation, but there was no effect of submaximal or maximal insulin. HL1 cardiomyocytes were used to overexpress wild-type (WT) SNARK and to knockdown endogenous SNARK. Overexpression of WT SNARK had no effect on ischemia-stimulated glucose transport; however, SNARK knockdown significantly decreased ischemia-stimulated glucose transport. SNARK overexpression or knockdown did not alter insulin-stimulated glucose transport or glycogen concentrations. To study SNARK function in vivo, SNARK heterozygous knockout mice (SNARK ) and WT littermates performed treadmill exercise. Exercise-stimulated glucose transport was decreased by ~50% in hearts from SNARK mice. In summary, exercise and ischemia increase SNARK Thr phosphorylation in the heart and SNARK regulates exercise-stimulated and ischemia-stimulated glucose transport. SNARK is a novel mediator of insulin-independent glucose transport in the heart.

Year of Publication
2019
Journal
Journal of cellular biochemistry
Volume
120
Issue
1
Number of Pages
685-696
Date Published
12/2019
ISSN Number
1097-4644
DOI
10.1002/jcb.27425
Alternate Journal
J. Cell. Biochem.
PMID
30256437
PMCID
PMC6347018
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