AI Article Synopsis
- L-arginine (l-Arg) prompts insulin secretion from β-cells, but the specific mechanism is unclear.
- Research indicates that G protein-coupled receptor GPCR6A is crucial for this process, as shown by abnormalities in glucose regulation in mice lacking this receptor.
- Experiments revealed that pancreatic islets from Gprc6a(-/-) mice had reduced size and insulin levels, indicating that l-Arg's effect on insulin release involves GPRC6A and the cAMP signaling pathway.
Article Abstract
L-arginine (l-Arg) is an insulin secretagogue, but the molecular mechanism whereby it stimulates insulin secretion from β-cells is not known. The possibility that l-Arg regulates insulin secretion through a G protein-coupled receptor (GPCR)-mediated mechanism is suggested by the high expression of the nutrient receptor GPCR family C group 6 member A (GPRC6A) in the pancreas and TC-6 β-cells and the finding that Gprc6a(-/]minus]) mice have abnormalities in glucose homeostasis. To test the direct role of GPRC6A in regulating insulin secretion, we evaluated the response of pancreatic islets derived from Gprc6a(-/]minus]) mice to L-Arg. We found that the islet size and insulin content were decreased in pancreatic islets from Gprac6a(-/]minus]) mice. These alterations were selective for β-cells, because there were no abnormalities in serum glucagon levels or glucagon content of islets derived from Gprac6a(-/]minus]) mice. Significant reduction was observed in both the pancreatic ERK response to L-Arg administration to Gprc6a(-/]minus]) mice in vivo and L-Arg-induced insulin secretion and production ex vivo in islets isolated from Gprc6a(-/]minus]) mice. L-Arg stimulation of cAMP accumulation in isolated islets isolated from Gprc6a(-/]minus]) mice was also diminished. These findings suggest that l-Arg stimulation of insulin secretion in β-cells is mediated, at least in part, through GPRC6A activation of cAMP pathways.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3512028 | PMC |
| http://dx.doi.org/10.1210/en.2012-1301 | DOI Listing |
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