| Literature DB >> 29273589 |
Min Joo Kim1, Se Hee Min1, Seon Young Shin2, Mi Na Kim2, Hakmo Lee2, Jin Young Jang3, Sun-Whe Kim3, Kyong Soo Park1,2, Hye Seung Jung4,2.
Abstract
PERK is a pancreatic endoplasmic reticulum (ER) kinase. Its complete deletion in pancreatic β cells induces insulin deficiency; however, the effects of partial Perk suppression are unclear. We investigated the effect of partial PERK suppression using the specific PERK inhibitors GSK2606414 and GSK2656157. Low-dose GSK2606414 treatment for 24 h enhanced glucose-stimulated insulin secretion (GSIS), islet insulin content and calcium transit in mouse (at 40 nM) and human (at 50-100 nM) pancreatic islets. GSK2606414 also induced the expression of the ER chaperone BiP and the release of calcium from the ER. When Bip expression was inhibited using a Bip siRNA, the GSK2606414-induced augmentation of the ER calcium level, islet insulin contents, glucose-stimulated cytosolic calcium transit and GSIS were abrogated. In both wild-type and insulin-deficient Atg7-knockout mice, 8 weeks of GSK2656157 treatment enhanced GSIS and improved hyperglycemia without affecting body weight. In conclusion, partial PERK inhibition induced BiP expression in islets, increased glucose-stimulated calcium transit and islet insulin contents and enhanced GSIS, suggesting that low-dose PERK inhibitors could potentially be used to treat insulin deficiency.Entities:
Keywords: BiP; PERK kinase; calcium; endoplasmic reticulum; insulin; pancreatic islets
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Year: 2017 PMID: 29273589 DOI: 10.1530/JOE-17-0497
Source DB: PubMed Journal: J Endocrinol ISSN: 0022-0795 Impact factor: 4.286