AUTHOR=SanMartín Carol D., Paula-Lima Andrea C., García Alejandra , Barattini Pablo , Hartel Steffen , Núñez Marco T., Hidalgo Cecilia 

TITLE=Ryanodine receptor-mediated Ca2+ release underlies iron-induced mitochondrial fission and stimulates mitochondrial Ca2+ uptake in primary hippocampal neurons

JOURNAL=Frontiers in Molecular Neuroscience

VOLUME=7

YEAR=2014

URL=https://www.frontiersin.org/journals/molecular-neuroscience/articles/10.3389/fnmol.2014.00013

DOI=10.3389/fnmol.2014.00013

ISSN=1662-5099

ABSTRACT=<p>Mounting evidence indicates that iron accumulation impairs brain function. We have reported previously that addition of sub-lethal concentrations of iron to primary hippocampal neurons produces Ca<sup>2</sup><sup>+</sup> signals and promotes cytoplasmic generation of reactive oxygen species. These Ca<sup>2</sup><sup>+</sup> signals, which emerge within seconds after iron addition, arise mostly from Ca<sup>2</sup><sup>+</sup> release through the redox-sensitive ryanodine receptor (RyR) channels present in the endoplasmic reticulum. We have reported also that addition of synaptotoxic amyloid-β oligomers to primary hippocampal neurons stimulates RyR-mediated Ca<sup>2</sup><sup>+</sup> release, generating long-lasting Ca<sup>2</sup><sup>+</sup> signals that activate Ca<sup>2</sup><sup>+</sup>-sensitive cellular effectors and promote the disruption of the mitochondrial network. Here, we describe that 24 h incubation of primary hippocampal neurons with iron enhanced agonist-induced RyR-mediated Ca<sup>2</sup><sup>+</sup> release and promoted mitochondrial network fragmentation in 43% of neurons, a response significantly prevented by RyR inhibition and by the antioxidant agent <italic>N</italic>-acetyl-<sc>L</sc>-cysteine. Stimulation of RyR-mediated Ca<sup>2</sup><sup>+</sup> release by a RyR agonist promoted mitochondrial Ca<sup>2</sup><sup>+</sup> uptake in control neurons and in iron-treated neurons that displayed non-fragmented mitochondria, but not in neurons with fragmented mitochondria. Yet, the global cytoplasmic Ca<sup>2</sup><sup>+</sup> increase induced by the Ca<sup>2</sup><sup>+</sup> ionophore ionomycin prompted significant mitochondrial Ca<sup>2</sup><sup>+</sup> uptake in neurons with fragmented mitochondria, indicating that fragmentation did not prevent mitochondrial Ca<sup>2</sup><sup>+</sup> uptake but presumably decreased the functional coupling between RyR-mediated Ca<sup>2</sup><sup>+</sup> release and the mitochondrial Ca<sup>2</sup><sup>+</sup> uniporter. Taken together, our results indicate that stimulation of redox-sensitive RyR-mediated Ca<sup>2</sup><sup>+</sup> release by iron causes significant neuronal mitochondrial fragmentation, which presumably contributes to the impairment of neuronal function produced by iron accumulation.</p>