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UCP2 is highly expressed in pancreatic alpha-cells and influences secretion and survival.


ABSTRACT: In pancreatic beta-cells, uncoupling protein 2 (UCP2) influences mitochondrial oxidative phosphorylation and insulin secretion. Here, we show that alpha-cells express significantly higher levels of UCP2 than do beta-cells. Greater mitochondrial UCP2-related uncoupling was observed in alpha-cells compared with beta-cells and was accompanied by a lower oxidative phosphorylation efficiency (ATP/O). Conversely, reducing UCP2 activity in alpha-cells was associated with higher mitochondrial membrane potential generated by glucose oxidation and with increased ATP synthesis, indicating more efficient metabolic coupling. In vitro, the suppression of UCP2 activity led to reduced glucagon secretion in response to low glucose; however, in vivo, fasting glucagon levels were normal in UCP2(-/-) mice. In addition to its effects on secretion, UCP2 played a cytoprotective role in islets, with UCP2(-/-) alpha-cells being more sensitive to specific death stimuli. In summary, we demonstrate a direct role for UCP2 in maintaining alpha-cell function at the level of glucose metabolism, glucagon secretion, and cytoprotection.

SUBMITTER: Diao J 

PROVIDER: S-EPMC2575296 | biostudies-literature | 2008 Aug

REPOSITORIES: biostudies-literature

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UCP2 is highly expressed in pancreatic alpha-cells and influences secretion and survival.

Diao Jingyu J   Allister Emma M EM   Koshkin Vasilij V   Lee Simon C SC   Bhattacharjee Alpana A   Tang Christine C   Giacca Adria A   Chan Catherine B CB   Wheeler Michael B MB  

Proceedings of the National Academy of Sciences of the United States of America 20080813 33


In pancreatic beta-cells, uncoupling protein 2 (UCP2) influences mitochondrial oxidative phosphorylation and insulin secretion. Here, we show that alpha-cells express significantly higher levels of UCP2 than do beta-cells. Greater mitochondrial UCP2-related uncoupling was observed in alpha-cells compared with beta-cells and was accompanied by a lower oxidative phosphorylation efficiency (ATP/O). Conversely, reducing UCP2 activity in alpha-cells was associated with higher mitochondrial membrane p  ...[more]

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