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Subcellular localization of hippocampal ryanodine receptor 2 and its role in neuronal excitability and memory.

Florian HiessJinjing YaoZhenpeng SongBo SunZizhen ZhangJunting HuangLina ChenAdam InstitorisJohn Paul EstilloreRuiwu WangHenk E D J Ter KeursPeter K StysGrant R GordonGerald W ZamponiAnutosh GangulyS R Wayne Chen
Published in: Communications biology (2022)
Ryanodine receptor 2 (RyR2) is abundantly expressed in the heart and brain. Mutations in RyR2 are associated with both cardiac arrhythmias and intellectual disability. While the mechanisms of RyR2-linked arrhythmias are well characterized, little is known about the mechanism underlying RyR2-associated intellectual disability. Here, we employed a mouse model expressing a green fluorescent protein (GFP)-tagged RyR2 and a specific GFP probe to determine the subcellular localization of RyR2 in hippocampus. GFP-RyR2 was predominantly detected in the soma and dendrites, but not the dendritic spines of CA1 pyramidal neurons or dentate gyrus granular neurons. GFP-RyR2 was also detected within the mossy fibers in the stratum lucidum of CA3, but not in the presynaptic terminals of CA1 neurons. An arrhythmogenic RyR2-R4496C +/- mutation downregulated the A-type K + current and increased membrane excitability, but had little effect on the afterhyperpolarization current or presynaptic facilitation of CA1 neurons. The RyR2-R4496C +/- mutation also impaired hippocampal long-term potentiation, learning, and memory. These data reveal the precise subcellular distribution of hippocampal RyR2 and its important role in neuronal excitability, learning, and memory.
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