366-OR: 14-3-3-ζ Contributes to Effect of ß-Cell GLP1 Receptor Signaling to Alter a-Cell Proglucagon Processing

Autor: MARLENA HOLTER, DARYL PHUONG, ISAAC S.H. LEE, MRIDUSMITA SAIKIA, LISA A. WEIKERT, ELIZABETH T. ANDERSON, QIN FU, SHENG ZHANG, KYLE SLOOP, BETHANY CUMMINGS
Rok vydání: 2022
Předmět:
Zdroj: Diabetes. 71
ISSN: 0012-1797
Popis: Glucagon like peptide 1 (GLP1) , a classically gut derived hormone, potentiates insulin secretion. New evidence suggests that α cells can produce GLP1 under certain conditions, which may offer a novel therapeutic modality for treating diabetes; however, the mechanisms regulating α cell GLP1 production are unknown. We previously found that enhanced β cell GLP1 receptor (GLP1R) signaling activates α cell GLP1 by activating prohormone convertase 1/3 (Pcsk1) expression. We tested the hypothesis that enhanced β cell GLP1R signaling activates α cell GLP1 production through paracrine factors. We studied the impact of conditioned media (CM) generated from β cell GLP1R WT and KO islets of saline (CTRL) and liraglutide (LIRA) treated mice on α cell gene expression and function. CM from LIRA treated islets increased α cell Pcsk1 expression and active GLP-1 secretion only if β cells expressed the GLP1R (Pcsk1 expression (AU) : CTRL WT=1.0±0.1, LIRA WT=2.0±0.3, CTRL KO=1.1±0.2, LIRA KO=1.1±0.2, P Disclosure M.Holter: None. B.Cummings: None. D.Phuong: None. I.S.H.Lee: None. M.Saikia: None. L.A.Weikert: Stock/Shareholder; Merck & Co., Inc., Oramed Pharmaceuticals. E.T.Anderson: None. Q.Fu: None. S.Zhang: None. K.Sloop: Employee; Eli Lilly and Company. Funding NIH/NIDDK (F30 DK126538) Department of Defense (W81XWH-18-1-0206) The Hartwell Foundation NIH/NIDDK (R56DK124853)
Databáze: OpenAIRE