Cardiomyocyte ATP Production, Metabolic Flexibility, and Survival Require Calcium Flux through Cardiac Ryanodine Receptors in Vivo

Ca2+ fluxes between adjacent organelles are thought to control many cellular processes, including metabolism and cell survival. In vitro evidence has been presented that constitutive Ca2+ flux from intracellular stores into mitochondria is required for basal cellular metabolism, but these observatio...

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Veröffentlicht in:The Journal of biological chemistry 2013-06, Vol.288 (26), p.18975-18986
Hauptverfasser: Bround, Michael J., Wambolt, Rich, Luciani, Dan S., Kulpa, Jerzy E., Rodrigues, Brian, Brownsey, Roger W., Allard, Michael F., Johnson, James D.
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Sprache:eng
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Zusammenfassung:Ca2+ fluxes between adjacent organelles are thought to control many cellular processes, including metabolism and cell survival. In vitro evidence has been presented that constitutive Ca2+ flux from intracellular stores into mitochondria is required for basal cellular metabolism, but these observations have not been made in vivo. We report that controlled in vivo depletion of cardiac RYR2, using a conditional gene knock-out strategy (cRyr2KO mice), is sufficient to reduce mitochondrial Ca2+ and oxidative metabolism, and to establish a pseudohypoxic state with increased autophagy. Dramatic metabolic reprogramming was evident at the transcriptional level via Sirt1/Foxo1/Pgc1α, Atf3, and Klf15 gene networks. Ryr2 loss also induced a non-apoptotic form of programmed cell death associated with increased calpain-10 but not caspase-3 activation or endoplasmic reticulum stress. Remarkably, cRyr2KO mice rapidly exhibited many of the structural, metabolic, and molecular characteristics of heart failure at a time when RYR2 protein was reduced 50%, a similar degree to that which has been reported in heart failure. RYR2-mediated Ca2+ fluxes are therefore proximal controllers of mitochondrial Ca2+, ATP levels, and a cascade of transcription factors controlling metabolism and survival. Background: Intracellular Ca2+ release has been implicated in ATP production in vitro. Results: In vivo deletion of Ryr2 reduces Ca2+, ATP, and oxidative metabolism, leading to metabolic reprogramming and cell death. Conclusion: RYR2 maintains cardiomyocyte ATP production and survival in vivo. Significance: This work links heart metabolism to function via Ca2+ release from intracellular stores.
ISSN:0021-9258
1083-351X
DOI:10.1074/jbc.M112.427062