1. DSpace-CRIS @ UCA
  2. Facultad de Ciencias Médicas
  3. Instituto de Investigaciones Biomédicas (BIOMED UCA-CONICET)
  4. Artículos
Por favor, use este identificador para citar o enlazar este ítem: https://repositorio.uca.edu.ar/handle/123456789/16494
Título : TRPC3 regulates islet beta-cell insulin secretion
Autor : Rached, Gaëlle 
Saliba, Youakim 
Maddah, Dina 
Hajal, Joelle 
Smayra, Viviane 
Bakhos, Jules Joel 
Groschner, Klaus 
Birnbaumer, Lutz 
Farès, Nassim 
Palabras clave : TRPC3INSULINAGLUCOSACANALES CATIONICOSPROTEINA RECEPTORA TRANSITORIA 3CELULAS BETA
Fecha de publicación : 2023
Editorial : Wiley
Cita : Rached, G. et al. TRPC3 regulates islet beta-cell insulin secretion [en línea]. Advanced Science. 2023, 10 (6). doi: 10.1002/advs.202204846. Disponible en: https://repositorio.uca.edu.ar/handle/123456789/16494
Resumen : Abstract: Insulin release is tightly controlled by glucose-stimulated calcium (GSCa) through hitherto equivocal pathways. This study investigates TRPC3, a non-selective cation channel, as a critical regulator of insulin secretion and glucose control. TRPC3’s involvement in glucose-stimulated insulin secretion (GSIS) is studied in human and animal islets. TRPC3-dependent in vivo insulin secretion is investigated using pharmacological tools and Trpc3−/− mice. TRPC3’s involvement in islet glucose uptake and GSCa is explored using fluorescent glucose analogue 2-[N-(7-nitrobenz-2-oxa-1,3-diazol-4-yl) amino]-2-deoxy-D-glucose and calcium imaging. TRPC3 modulation by a small-molecule activator, GSK1702934A, is evaluated in type 2 diabetic mice. TRPC3 is functionally expressed in human and mouse islet beta cells. TRPC3-controlled insulin secretion is KATP-independent and primarily mediated by diacylglycerol channel regulation of the cytosolic calcium oscillations following glucose stimulation. Conversely, glucose uptake in islets is independent of TRPC3. TRPC3 pharmacologic inhibition and knockout in mice lead to defective insulin secretion and glucose intolerance. Subsequently, TRPC3 activation through targeted small-molecule enhances insulin secretion and alleviates diabetes hallmarks in animals. This study imputes a function for TRPC3 at the onset of GSIS. These insights strengthen one’s knowledge of insulin secretion physiology and set forth the TRPC3 channel as an appealing candidate for drug development in the treatment of diabetes.
URI : https://repositorio.uca.edu.ar/handle/123456789/16494
ISSN : 2198-3844 (online)
Disciplina: MEDICINA
DOI: 10.1002/advs.202204846
Derechos: Acceso abierto
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