| Literature DB >> 30996131 |
Ercument Dirice1,2, Dario F De Jesus1,2,3, Sevim Kahraman1,2, Giorgio Basile1,2, Raymond Ws Ng1,2, Abdelfattah El Ouaamari1,2, Adrian Kee Keong Teo1,2, Shweta Bhatt1,2, Jiang Hu1,2, Rohit N Kulkarni1,2,4.
Abstract
The identification of new sources of β cells is an important endeavor with therapeutic implications for diabetes. Insulin resistance, in physiological states such as pregnancy or in pathological states such as type 2 diabetes (T2D), is characterized by a compensatory increase in β cell mass. To explore the existence of a dynamic β cell reserve, we superimposed pregnancy on the liver-specific insulin receptor-KO (LIRKO) model of insulin resistance that already exhibits β cell hyperplasia and used lineage tracing to track the source of new β cells. Although both control and LIRKO mice displayed increased β cell mass in response to the relative insulin resistance of pregnancy, the further increase in mass in the latter supported a dynamic source that could be traced to pancreatic ducts. Two observations support the translational significance of these findings. First, NOD/SCID-γ LIRKO mice that became pregnant following cotransplantation of human islets and human ducts under the kidney capsule showed enhanced β cell proliferation and an increase in ductal cells positive for transcription factors expressed during β cell development. Second, we identified duct cells positive for immature β cell markers in pancreas sections from pregnant humans and in individuals with T2D. Taken together, during increased insulin demand, ductal cells contribute to the compensatory β cell pool by differentiation/neogenesis.Entities:
Keywords: Cell Biology; Diabetes; Endocrinology; Islet cells; Mouse models
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Year: 2019 PMID: 30996131 PMCID: PMC6538348 DOI: 10.1172/jci.insight.99576
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708