| Literature DB >> 24824430 |
Masashi Yosida1, Katsuya Dezaki2, Kunitoshi Uchida3, Shiho Kodera1, Nien V Lam1, Kiyonori Ito1, Rauza S Rita2, Hodaka Yamada1, Kenju Shimomura2, San-e Ishikawa1, Hitoshi Sugawara1, Masanobu Kawakami4, Makoto Tominaga3, Toshihiko Yada5, Masafumi Kakei6.
Abstract
In pancreatic β-cells, closure of the ATP-sensitive K(+) (K(ATP)) channel is an initial process triggering glucose-stimulated insulin secretion. In addition, constitutive opening of background nonselective cation channels (NSCCs) is essentially required to effectively evoke depolarization as a consequence of K(ATP) channel closure. Thus, it is hypothesized that further opening of NSCC facilitates membrane excitability. We identified a class of NSCC that was activated by exendin (ex)-4, GLP-1, and its analog liraglutide at picomolar levels. This NSCC was also activated by increasing the glucose concentration. NSCC activation by glucose and GLP-1 was a consequence of the activated cAMP/EPAC-mediated pathway and was attenuated in TRPM2-deficient mice. The NSCC was not activated by protein kinase A (PKA) activators and was activated by ex-4 in the presence of PKA inhibitors. These results suggest that glucose- and incretin-activated NSCC (TRPM2) works in concert with closure of the KATP channel to effectively induce membrane depolarization to initiate insulin secretion. The current study reveals a new mechanism for regulating electrical excitability in β-cells and for mediating the action of glucose and incretin to evoke insulin secretion, thereby providing an innovative target for the treatment of type 2 diabetes.Entities:
Mesh:
Substances:
Year: 2014 PMID: 24824430 DOI: 10.2337/db13-1868
Source DB: PubMed Journal: Diabetes ISSN: 0012-1797 Impact factor: 9.461