| Literature DB >> 33264616 |
Mohammad Mehdi Maneshi1, Anna B Toth1, Toshiyuki Ishii1, Kotaro Hori1, Shogo Tsujikawa1, Andrew K Shum1, Nisha Shrestha1, Megumi Yamashita1, Richard J Miller1, Jelena Radulovic2, Geoffrey T Swanson1, Murali Prakriya3.
Abstract
Store-operated Orai1 calcium channels function as highly Ca2+-selective ion channels and are broadly expressed in many tissues including the central nervous system, but their contributions to cognitive processing are largely unknown. Here, we report that many measures of synaptic, cellular, and behavioral models of learning are markedly attenuated in mice lacking Orai1 in forebrain excitatory neurons. Results with focal glutamate uncaging in hippocampal neurons support an essential role of Orai1 channels in amplifying NMDA-receptor-induced dendritic Ca2+ transients that drive activity-dependent spine morphogenesis and long-term potentiation at Schaffer collateral-CA1 synapses. Consistent with these signaling roles, mice lacking Orai1 in pyramidal neurons (but not interneurons) exhibit striking deficits in working and associative memory tasks. These findings identify Orai1 channels as essential regulators of dendritic spine Ca2+ signaling, synaptic plasticity, and cognition.Entities:
Keywords: CRAC channels; Orai1; STIM1; calcium; dendritic calcium signaling; dendritic spines; learning and memory; long-term potentiation; synaptic plasticity
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Year: 2020 PMID: 33264616 PMCID: PMC7832685 DOI: 10.1016/j.celrep.2020.108464
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423