| Literature DB >> 30327384 |
Emilie Courty1,2, Adrien Besseiche3, Thi Thu Huong Do1,2, Alexandrine Liboz1,2, Fatima Mohamed Aguid3, Evans Quilichini4, Melissa Buscato5, Pierre Gourdy5,6, Jean-François Gautier3,7, Jean-Pierre Riveline3,7, Cécile Haumaitre4, Marion Buyse1,2,8,9, Bruno Fève1,2,10, Ghislaine Guillemain1,2, Bertrand Blondeau11,2.
Abstract
Both type 1 and type 2 diabetes are characterized by deficient insulin secretion and decreased β-cell mass. Thus, regenerative strategies to increase β-cell mass need to be developed. To characterize mechanisms of β-cell plasticity, we studied a model of severe insulin resistance in the adult mouse and defined how β-cells adapt. Chronic corticosterone (CORT) treatment was given to adult mice and led to rapid insulin resistance and adaptive increased insulin secretion. Adaptive and massive increase of β-cell mass was observed during treatment up to 8 weeks. β-Cell mass increase was partially reversible upon treatment cessation and reinduced upon subsequent treatment. β-Cell neogenesis was suggested by an increased number of islets, mainly close to ducts, and increased Sox9 and Ngn3 mRNA levels in islets, but lineage-tracing experiments revealed that neoformed β-cells did not derive from Sox9- or Ngn3-expressing cells. CORT treatment after β-cell depletion partially restored β-cells. Finally, β-cell neogenesis was shown to be indirectly stimulated by CORT because serum from CORT-treated mice increased β-cell differentiation in in vitro cultures of pancreatic buds. Altogether, the results present a novel model of β-cell neogenesis in the adult mouse and identify the presence of neogenic factors in the serum of CORT-treated mice.Entities:
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Year: 2018 PMID: 30327384 DOI: 10.2337/db17-1314
Source DB: PubMed Journal: Diabetes ISSN: 0012-1797 Impact factor: 9.461