Diabetes | 2019
363-OR: ChREBP-Beta Controls Both Proliferation and Cell Death of Pancreatic Beta Cells
Abstract
Glucose is a key physiological driver of adaptive beta cell mass expansion, promoting beta cell proliferation both in vitro and in vivo. Carbohydrate response element binding protein β (ChREBPβ) is upregulated in response to glucose and is required for glucose-stimulated beta cell proliferation. To study the role of ChREBPβ in beta cells, we knocked out (KO) or overexpressed (OE) ChREBPβ in mouse pancreatic beta cells using Cre LoxP approaches with either MIP-CreERT (induced by tamoxifen at 3 months of age), or the RIP-Cre model which leads to recombination specifically in β cells, early during embryogenesis (E9). We performed intraperitoneal glucose tolerance tests (IPGTTs) and assessed pancreata for proliferation (Ki67), cell death (TUNEL) and beta cell mass in the 4 mouse models. ChREBPβ MIP-CreERT KO mice displayed impaired glucose tolerance, with an increase of 25.3 ± 7.9% (N=3-4, P Disclosure L.S. Katz: None. G. Brill: None. M.A. Herman: None. D. Scott: None. Funding National Institutes of Health