| Literature DB >> 24995977 |
James C Lo1, Sanda Ljubicic2, Barbara Leibiger3, Matthias Kern4, Ingo B Leibiger3, Tilo Moede3, Molly E Kelly2, Diti Chatterjee Bhowmick2, Incoronata Murano5, Paul Cohen1, Alexander S Banks2, Melin J Khandekar2, Arne Dietrich6, Jeffrey S Flier7, Saverio Cinti5, Matthias Blüher4, Nika N Danial2, Per-Olof Berggren3, Bruce M Spiegelman8.
Abstract
A hallmark of type 2 diabetes mellitus (T2DM) is the development of pancreatic β cell failure, which results in insulinopenia and hyperglycemia. We show that the adipokine adipsin has a beneficial role in maintaining β cell function. Animals genetically lacking adipsin have glucose intolerance due to insulinopenia; isolated islets from these mice have reduced glucose-stimulated insulin secretion. Replenishment of adipsin to diabetic mice treated hyperglycemia by boosting insulin secretion. We identify C3a, a peptide generated by adipsin, as a potent insulin secretagogue and show that the C3a receptor is required for these beneficial effects of adipsin. C3a acts on islets by augmenting ATP levels, respiration, and cytosolic free Ca(2+). Finally, we demonstrate that T2DM patients with β cell failure are deficient in adipsin. These findings indicate that the adipsin/C3a pathway connects adipocyte function to β cell physiology, and manipulation of this molecular switch may serve as a therapy in T2DM.Entities:
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Year: 2014 PMID: 24995977 PMCID: PMC4128197 DOI: 10.1016/j.cell.2014.06.005
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582