Uncoupling Protein 2 and Islet Function
- 1Department of Biomedical Sciences, University of Prince Edward Island, Charlottetown, Prince Edward, Canada
- 2Departments of Medicine and Physiology, University of Toronto, Toronto, Ontario, Canada
- Address correspondence and reprint requests to Dr. C.B. Chan, Department of Biomedical Sciences, University of Prince Edward Island, 550 University Ave., Charlottetown, PE C1A 4P3 Canada. E-mail: cchan{at}upei.ca
Abstract
Stressors such as chronic hyperglycemia or hyperlipidemia may lead to insufficient insulin secretion in susceptible individuals, contributing to type 2 diabetes. The molecules mediating this effect are just beginning to be identified. Uncoupling protein (UCP)-2 may be one such negative modulator of insulin secretion. Accumulating evidence shows that β-cell UCP2 expression is upregulated by glucolipotoxic conditions and that increased activity of UCP2 decreases insulin secretion. Mitochondrial superoxide has been identified as a posttranslational regulator of UCP2 activity in islets; thus, UCP2 may provide protection to β-cells at one level while simultaneously having detrimental effects on insulin secretion. Interestingly, the latter appears to be the dominant outcome, because UCP2 knockout mice display an increased β-cell mass and retained insulin secretion capacity in the face of glucolipotoxicity.
- CPT, carnitine palmitoyl transferase
- DIC, dicarboxylate carrier
- FFA, free fatty acid
- GSIS, glucose-stimulated insulin secretion
- KATP channel, ATP-dependent K+ channel
- PPAR, peroxisome proliferator-activated receptor
- ROS, reactive oxygen species
- SRE, sterol regulatory element
- UCP, uncoupling protein
Footnotes
-
This article is based on a presentation at a symposium. The symposium and the publication of this article were made possible by an unrestricted educational grant from Les Laboratoires Servier.
-
- Accepted April 28, 2003.
- Received March 13, 2003.
- DIABETES
