Publication | Open Access
SIRT2 is a negative regulator of anoxia–reoxygenation tolerance via regulation of 14‐3‐3 ζ and BAD in H9c2 cells
86
Citations
14
References
2008
Year
14-3-3 ZetaH9c2 CellsNegative RegulatorGeneticsRedox BiologyOxidative StressTranscriptional RegulationRedox RegulatorMitochondrial Bad LocalizationCell SignalingConcurrent SirnaRedox SignalingHypoxia (Medicine)Anoxia–reoxygenation ToleranceReactive Oxygen SpecieGene ExpressionCell BiologyMitochondrial FunctionSystems BiologyMedicine
Knockdown or inhibition of SIRT2 enhances biological stress-tolerance. We extend this phenotype showing that SIRT2 knockdown reduces anoxia-reoxygenation injury in H9c2 cells. Gene array analysis following SIRT2 siRNA knockdown identifies 14-3-3 zeta as the most robustly induced gene. SIRT2 knockdown evokes induction of this chaperone, facilitating cytosolic sequestration of BAD with a corresponding reduction in mitochondrial BAD localization. Concurrent siRNA against SIRT2 and 14-3-3 zeta abolishes the SIRT2-depleted cytoprotective phenotype. SIRT2 functions to moderate cellular stress-tolerance, in part, by modulating the levels of 14-3-3 zeta with the concordant control of BAD subcellular localization.
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