Overexpression of uncoupling protein 3 in skeletal muscle protects against fat-induced insulin resistance
Cheol Soo Choi, … , Takamasa Higashimori, Gerald I. Shulman
Cheol Soo Choi, … , Takamasa Higashimori, Gerald I. Shulman
Published July 2, 2007
Citation Information: J Clin Invest. 2007;117(7):1995-2003. https://doi.org/10.1172/JCI13579.
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Research Article Endocrinology

Overexpression of uncoupling protein 3 in skeletal muscle protects against fat-induced insulin resistance

Abstract

Insulin resistance is a major factor in the pathogenesis of type 2 diabetes and is strongly associated with obesity. Increased concentrations of intracellular fatty acid metabolites have been postulated to interfere with insulin signaling by activation of a serine kinase cascade involving PKCθ in skeletal muscle. Uncoupling protein 3 (UCP3) has been postulated to dissipate the mitochondrial proton gradient and cause metabolic inefficiency. We therefore hypothesized that overexpression of UCP3 in skeletal muscle might protect against fat-induced insulin resistance in muscle by conversion of intramyocellular fat into thermal energy. Wild-type mice fed a high-fat diet were markedly insulin resistant, a result of defects in insulin-stimulated glucose uptake in skeletal muscle and hepatic insulin resistance. Insulin resistance in these tissues was associated with reduced insulin-stimulated insulin receptor substrate 1– (IRS-1–) and IRS-2–associated PI3K activity in muscle and liver, respectively. In contrast, UCP3-overexpressing mice were completely protected against fat-induced defects in insulin signaling and action in these tissues. Furthermore, these changes were associated with a lower membrane-to-cytosolic ratio of diacylglycerol and reduced PKCθ activity in whole-body fat–matched UCP3 transgenic mice. These results suggest that increasing mitochondrial uncoupling in skeletal muscle may be an excellent therapeutic target for type 2 diabetes mellitus.

Authors

Cheol Soo Choi, Jonathan J. Fillmore, Jason K. Kim, Zhen-Xiang Liu, Sheene Kim, Emily F. Collier, Ameya Kulkarni, Alberto Distefano, Yu-Jin Hwang, Mario Kahn, Yan Chen, Chunli Yu, Irene K. Moore, Richard M. Reznick, Takamasa Higashimori, Gerald I. Shulman

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Figure 8

UCP3 overexpression increased glucose uptake and AKT activity and decreased PKCθ activity and membrane translocation of DAG in skeletal muscle of fat-matched wild-type and UCP3 transgenic mice fed HFD for 10 days.

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UCP3 overexpression increased glucose uptake and AKT activity and decrea...
n = 9–10 per group (A, B, and DG); 4 per group (C). (A) In vivo insulin-stimulated glucose uptake. ‡‡P < 0.001 versus wild type. (B) In vivo insulin-stimulated Akt2 activity. P = 0.002 versus wild type. (C) PKCθ activity, as determined by the ratio of PKCθ levels in the membrane fraction to those in the cytosolic fraction. ††P = 0.02 versus wild type. (D) Long-chain fatty acyl-CoA concentration. P = 0.001 versus wild type. (E) LPA concentration. (F) Membrane/cytosol ratio of DAG. ††P = 0.02 versus wild type. (G) Triglyceride concentration.