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Role of G-proteins in islet function in health and diabetes.

Citation
Kowluru, A. “Role Of G-Proteins In Islet Function In Health And Diabetes.”. Diabetes, Obesity & Metabolism, pp. 63-75.
Center University of Michigan
Author Anjaneyulu Kowluru
Keywords G-proteins, NADPH oxidase, Rac1, farnesylation, geranylgeranylation, islet β-cell
Abstract

Glucose-stimulated insulin secretion (GSIS) involves interplay between metabolic and cationic events. Seminal contributions from multiple laboratories affirm essential roles for small G-proteins (Rac1, Cdc42, Arf6, Rab27A) in GSIS. Activation of these signalling proteins promotes cytoskeletal remodeling, transport and docking of insulin granules on the plasma membrane for exocytotic secretion of insulin. Evidence in rodent and human islets suggests key roles for lipidation (farnesylation and geranylgeranylation) of these G-proteins for their targeting to appropriate cellular compartments for optimal regulation of effectors leading to GSIS. Interestingly, however, inhibition of prenylation appears to cause mislocalization of non-prenylated, but (paradoxically) activated G-proteins, in "inappropriate" compartments leading to activation of stress kinases and onset of mitochondrial defects, loss in GSIS and apoptosis of the islet β-cell. This review highlights our current understanding of roles of G-proteins and their post-translational lipidation (prenylation) signalling networks in islet function in normal health, metabolic stress (glucolipotoxicity and ER stress) and diabetes. Critical knowledge gaps that need to be addressed for the development of therapeutics to halt defects in these signalling steps in β-cells in models of impaired insulin secretion and diabetes are also highlighted and discussed.

Year of Publication
2017
Journal
Diabetes, obesity & metabolism
Volume
19 Suppl 1
Number of Pages
63-75
Date Published
12/2017
ISSN Number
1463-1326
DOI
10.1111/dom.13011
Alternate Journal
Diabetes Obes Metab
PMID
28880478
PMCID
PMC5657296
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