Journal
TOXICOLOGY MECHANISMS AND METHODS
Volume 20, Issue 4, Pages 167-174Publisher
TAYLOR & FRANCIS LTD
DOI: 10.3109/15376511003695181
Keywords
Pancreatic islets; glycolysis; NAD(P)H; mitochondrial shuttles; cytosolic oxidoreductases
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Funding
- American Diabetes Association [7-08-JF-18]
- Center for Advanced Studies of the US Coast Guard Academy
- Alexander Trust Fund
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Insulin secretion from pancreatic beta cells is a process dependent on metabolism. While oxidative stress is a well-known inducer of beta cell toxicity and impairs insulin secretion, recent studies suggest that low levels of metabolically-derived reactive oxygen intermediates (ROI) also play a positive role in insulin secretion. Glucose metabolism is directly correlated with ROI production, particularly in beta cells in which glucose uptake is proportional to the extracellular concentration of glucose. Low levels of exogenously added ROI or quinones, which stimulate ROI production, positively affect insulin secretion, while antioxidants block insulin secretion, suggesting that ROI activate unidentified redox-sensitive signal transduction components within these cells. The mitochondria are one source of ROI: increased metabolic flux increases mitochondrial membrane potential resulting in electron leakage and adventitious ROI production. A second source of ROI are cytosolic and plasma membrane oxidoreductases which oxidize NAD(P)H and directly produce ROI through the reduction of molecular oxygen. The mechanism of ROI-mediated potentiation of insulin secretion remains an important topic for future study.
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