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Artículo

Determinants of Ca2+ release restitution: Insights from genetically altered animals and mathematical modeling

Cely Ortiz, Diana Cataloina AlejandraIcon ; Felice, Juan IgnacioIcon ; Diaz Zegarra, Leandro AgustinIcon ; Valverde, Carlos AlfredoIcon ; Federico, MarilénIcon ; Palomeque, JulietaIcon ; Wehrens, Xander H.T.; Kranias, Evangelina G.; Aiello, Ernesto AlejandroIcon ; Lascano, Elena Catalina; Negroni, Jorge Antonio; Mattiazzi, Ramona AliciaIcon
Fecha de publicación: 28/09/2020
Editorial: Rockefeller University Press
Revista: Journal Of General Physiology
ISSN: 0022-1295
e-ISSN: 1540-7748
Idioma: Inglés
Tipo de recurso: Artículo publicado
Clasificación temática:
Biofísica; Otras Ciencias Médicas; Otras Matemáticas

Resumen

Each heartbeat is followed by a refractory period. Recovery from refractoriness is known as Ca2+ release restitution (CRR), and its alterations are potential triggers of Ca2+ arrhythmias. Although the control of CRR has been associated with SR Ca2+ load and RYR2 Ca2+ sensitivity, the relative role of some of the determinants of CRR remains largely undefined. An intriguing point, difficult to dissect and previously neglected, is the possible independent effect of SR Ca2+ content versus the velocity of SR Ca2+ refilling on CRR. To assess these interrogations, we used isolated myocytes with phospholamban (PLN) ablation (PLNKO), knock-in mice with pseudoconstitutive CaMKII phosphorylation of RYR2 S2814 (S2814D), S2814D crossed with PLNKO mice (SDKO), and a previously validated human cardiac myocyte model. Restitution of cytosolic Ca2+ (Fura-2 AM) and L-type calcium current (ICaL; patch-clamp) was evaluated with a two-pulse (S1/S2) protocol. CRR and ICaL restitution increased as a function of the (S2-S1) coupling interval, following an exponential curve. When SR Ca2+ load was increased by increasing extracellular [Ca2+] from 2.0 to 4.0 mM, CRR and ICaL restitution were enhanced, suggesting that ICaL restitution may contribute to the faster CRR observed at 4.0 mM [Ca2+]. In contrast, ICaL restitution did not differ among the different mouse models. For a given SR Ca2+ load, CRR was accelerated in S2814D myocytes versus WT, but not in PLNKO and SDKO myocytes versus WT and S2814D, respectively. The model mimics all experimental data. Moreover, when the PLN ablation-induced decrease in RYR2 expression was corrected, the model revealed that CRR was accelerated in PLNKO and SDKO versus WT and S2814D myocytes, consistent with the enhanced velocity of refilling, SR [Ca2+] recovery, and CRR. We speculate that refilling rate might enhance CRR independently of SR Ca2+ load.
Palabras clave: CELLULAR PHYSIOLOGY , COMPUTATIONAL BIOLOGY , INTERCELLULAR SIGNALING , MOLECULAR PHYSIOLOGY
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info:eu-repo/semantics/openAccess 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
URI: http://hdl.handle.net/11336/143801
DOI: http://dx.doi.org/10.1085/jgp.201912512
URL: https://rupress.org/jgp/article/152/11/e201912512/152125/Determinants-of-Ca2-rel
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Articulos de CENTRO DE INVEST.CARDIOVASCULARES (I)
Citación
Cely Ortiz, Diana Cataloina Alejandra; Felice, Juan Ignacio; Diaz Zegarra, Leandro Agustin; Valverde, Carlos Alfredo; Federico, Marilén; et al.; Determinants of Ca2+ release restitution: Insights from genetically altered animals and mathematical modeling; Rockefeller University Press; Journal Of General Physiology; 152; 11; 28-9-2020; 1-13
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