Artículo
CaMKII-dependent phosphorylation of cardiac ryanodine receptors regulates cell death in cardiac ischemia/reperfusion injury
Di Carlo, Mariano Nahuel
; Said, Matilde; Ling, Haiyun; Valverde, Carlos Alfredo
; de Giusti, Verónica Celeste
; Sommese, Leandro Matías
; Palomeque, Julieta
; Aiello, Ernesto Alejandro
; Skapura, Darlene G.; Rinaldi, Gustavo Juan
; Respress, Jonathan L.; Heller Brown, Joan; Wehrens, Xander H.T.; Salas, Margarita Ana; Mattiazzi, Ramona Alicia
; Said, Matilde; Ling, Haiyun; Valverde, Carlos Alfredo
; de Giusti, Verónica Celeste
; Sommese, Leandro Matías
; Palomeque, Julieta
; Aiello, Ernesto Alejandro
; Skapura, Darlene G.; Rinaldi, Gustavo Juan
; Respress, Jonathan L.; Heller Brown, Joan; Wehrens, Xander H.T.; Salas, Margarita Ana; Mattiazzi, Ramona Alicia
Fecha de publicación:
09/2014
Editorial:
Academic Press Ltd-elsevier Science Ltd
Revista:
Journal Of Molecular And Cellular Cardiology
ISSN:
0022-2828
Idioma:
Inglés
Tipo de recurso:
Artículo publicado
Clasificación temática:
Resumen
Ca2+-calmodulin kinase II (CaMKII) activation is deleterious in cardiac ischemia/reperfusion (I/R). Moreover, inhibition of CaMKII-dependent phosphorylations at the sarcoplasmic reticulum (SR) prevents CaMKII-induced I/R damage. However, the downstream targets of CaMKII at the SR level, responsible for this detrimental effect, remain unclear. In the present study we aimed to dissect the role of the two main substrates of CaMKII at the SR level, phospholamban (PLN) and ryanodine receptors (RyR2), in CaMKII-dependent I/R injury. In mouse hearts subjected to global I/R (45/120 min), phosphorylation of the primary CaMKII sites, S2814 on cardiac RyR2 and of T17 on PLN, significantly increased at the onset of reperfusion whereas PKA-dependent phosphorylation of RyR2 and PLN did not change. Similar results were obtained in vivo, in mice subjected to regional myocardial I/R (1/24 h). Knock-in mice with an inactivated serine 2814 phosphorylation site on RyR2 (S2814A) significantly improved post-ischemic mechanical recovery, reduced infarct size and decreased apoptosis. Conversely, knockin mice, in which CaMKII site of RyR2 is constitutively activated (S2814D), significantly increased infarct size and exacerbated apoptosis. In S2814A and S2814D mice subjected to regional myocardial ischemia, infarct size was also decreased and increased respectively. Transgenic mice with double-mutant non-phosphorylatable PLN (S16A/T17A) in the PLN knockout background (PLNDM) also showed significantly increased post-ischemic cardiac damage. This effect cannot be attributed to PKA-dependent PLN phosphorylation and was not due to the enhanced L-type Ca2+ current, present in these mice. Our results reveal a major role for the phosphorylation of S2814 site on RyR2 in CaMKII-dependent I/R cardiac damage. In contrast, they showed that CaMKII-dependent increase in PLN phosphorylation during reperfusion opposes rather than contributes to I/R damage
Palabras clave:
Ryr2 Pln
,
Camkii
,
Ischemia/Reperfusion Injury
,
Apoptosis
,
Necrosis
,
Myocardium
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Licencia
Excepto donde se diga explícitamente, este item se publica bajo la siguiente descripción:
Creative Commons Attribution-NonCommercial-ShareAlike 2.5 Unported (CC BY-NC-SA 2.5)
Identificadores
Colecciones
Articulos(CIC)
Articulos de CENTRO DE INVEST.CARDIOVASCULARES (I)
Articulos de CENTRO DE INVEST.CARDIOVASCULARES (I)
Citación
Di Carlo, Mariano Nahuel; Said, Matilde; Ling, Haiyun; Valverde, Carlos Alfredo; de Giusti, Verónica Celeste; et al.; CaMKII-dependent phosphorylation of cardiac ryanodine receptors regulates cell death in cardiac ischemia/reperfusion injury; Academic Press Ltd-elsevier Science Ltd; Journal Of Molecular And Cellular Cardiology; 74; 9-2014; 274-283
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