| Literature DB >> 29444430 |
Marianne Böni-Schnetzler1, Stéphanie P Häuselmann2, Elise Dalmas2, Daniel T Meier2, Constanze Thienel2, Shuyang Traub2, Friederike Schulze2, Laura Steiger2, Erez Dror2, Praxedis Martin3, Pedro L Herrera4, Cem Gabay3, Marc Y Donath2.
Abstract
Interleukin-1 receptor antagonist (IL-1Ra) is elevated in the circulation during obesity and type 2 diabetes (T2D) but is decreased in islets from patients with T2D. The protective role of local IL-1Ra was investigated in pancreatic islet β cell (βIL-1Ra)-specific versus myeloid-cell (myeloIL-1Ra)-specific IL-1Ra knockout (KO) mice. Deletion of IL-1Ra in β cells, but not in myeloid cells, resulted in diminished islet IL-1Ra expression. Myeloid cells were not the main source of circulating IL-1Ra in obesity. βIL-1Ra KO mice had impaired insulin secretion, reduced β cell proliferation, and decreased expression of islet proliferation genes, along with impaired glucose tolerance. The key cell-cycle regulator E2F1 partly reversed IL-1β-mediated inhibition of potassium channel Kir6.2 expression and rescued impaired insulin secretion in IL-1Ra knockout islets. Our findings provide evidence for the importance of β cell-derived IL-1Ra for the local defense of β cells to maintain normal function and proliferation.Entities:
Keywords: ATP-sensitive K+ channel subunit Kir6.2; E2F1 transcription factor; IL-1 receptor antagonist; diabetes; glucose-stimulated insulin secretion; interleukin-1β; islet β cells; β cell proliferation
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Year: 2018 PMID: 29444430 DOI: 10.1016/j.celrep.2018.01.063
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423