Artículos de revistas
Hyperosmotic stress activates p65/RelB NFκB in cultured cardiomyocytes with dichotomic actions on caspase activation and cell death
Fecha
2006Registro en:
FEBS Letters, Volumen 580, Issue 14, 2018, Pages 3469-3476
00145793
10.1016/j.febslet.2006.05.023
Autor
Eisner, Verónica
Quiroga, Clara
Criollo Céspedes, Alfredo
Eltit Ortega, José Miguel
Chiong Lay, Mario
Parra, Valentina
Hidalgo, Karla
Toro, Barbra
Díaz Araya, Guillermo
Lavandero González, Sergio
Institución
Resumen
NFκB is a participant in the process whereby cells adapt to stress. We have evaluated the activation of NFκB pathway by hyperosmotic stress in cultured cardiomyocytes and its role in the activation of caspase and cell death. Exposure of cultured rat cardiomyocytes to hyperosmotic conditions induced phosphorylation of IKKα/β as well as degradation of IκBα. All five members of the NFκB family were identified in cardiomyocytes. Analysis of the subcellular distribution of NFκB isoforms in response to hyperosmotic stress showed parallel migration of p65 and RelB from the cytosol to the nucleus. Measurement of the binding of NFκB to the consensus DNA κB-site binding by EMSA revealed an oscillatory profile with maximum binding 1, 2 and 6 h after initiation of the hyperosmotic stress. Supershift analysis revealed that p65 and RelB (but not p50, p52 or cRel) were involved in the binding of NFκB to DNA. Hyperosmotic stress also resulted in activation of the NFκB-lux reporter gene, transient acti