G o 2 G protein mediates galanin inhibitory effects on insulin release from pancreatic β cells
G o 2 G protein mediates galanin inhibitory effects on insulin release from pancreatic β cells
The neuropeptide galanin regulates numerous physiological activities in the body, including feeding and metabolism, learning and memory, nociception and spinal reflexes, and anxiety and related behaviors. Modulation of blood glucose levels by suppressing insulin release was the first reported activity for galanin. This inhibition was mediated by one or more pertussis toxin-sensitive G proteins of the G i/o subfamily. However, the molecular identities of the specific G protein(s) and intracellular effectors have not been fully revealed. Recently, we demonstrated that mice lacking G o 2, but not other members of the G i/o protein family, secrete more insulin than controls upon glucose challenge, indicating that G o 2 is a major transducer for the inhibitory regulation of insulin secretion. In this study, we investigated galanin signaling mechanisms in β cells using cell biological and electrophysiological approaches. We found that islets lacking G o 2, but not other G i/o proteins, lose the inhibitory effect of galanin on insulin release. Potentiation of ATP-sensitive potassium (K ATP ) and inhibition of calcium currents by galanin were disrupted by anti-G o 2α antibodies. Galanin actions on K ATP and calcium currents were completely lost in G o 2 −/− β cells. Furthermore, the hyperglycemic effect of galanin is also blunted in G o 2 −/− mice. Our results demonstrate that G o 2 mediates the inhibition of insulin release by galanin by regulating both K ATP and Ca 2+ channels in mice. Our findings provide insight into galanin's action in glucose homeostasis. The results may also be relevant to the understanding of galanin signaling in other biological systems, especially the central nervous system.
- University of California, Los Angeles United States
- National Institute of Health Pakistan
- National Institutes of Health United States
- Research Triangle Park Foundation United States
- National Institute of Environmental Health Sciences United States
Islets of Langerhans, Mice, GTP-Binding Proteins, Insulin Secretion, Animals, Insulin, Galanin, Receptors, Galanin, Signal Transduction
Islets of Langerhans, Mice, GTP-Binding Proteins, Insulin Secretion, Animals, Insulin, Galanin, Receptors, Galanin, Signal Transduction
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