| Literature DB >> 33548174 |
Xingzhi He1, Jiarui Li1, Guangjun Zhou1, Jing Yang1, Sam McKenzie2, Yanjun Li1, Wenwen Li1, Jun Yu1, Yang Wang1, Jing Qu1, Zhiying Wu1, Hailan Hu3, Shumin Duan3, Huan Ma4.
Abstract
Mental experiences can become long-term memories if the hippocampal activity patterns that encode them are broadcast during network oscillations. The activity of inhibitory neurons is essential for generating these neural oscillations, but molecular control of this dynamic process during learning remains unknown. Here, we show that hippocampal oscillatory strength positively correlates with excitatory monosynaptic drive onto inhibitory neurons (E→I) in freely behaving mice. To establish a causal relationship between them, we identified γCaMKII as the long-sought mediator of long-term potentiation for E→I synapses (LTPE→I), which enabled the genetic manipulation of experience-dependent E→I synaptic input/plasticity. Deleting γCaMKII in parvalbumin interneurons selectively eliminated LTPE→I and disrupted experience-driven strengthening in theta and gamma rhythmicity. Behaviorally, this manipulation impaired long-term memory, for which the kinase activity of γCaMKII was required. Taken together, our data suggest that E→I synaptic plasticity, exemplified by LTPE→I, plays a gatekeeping role in tuning experience-dependent brain rhythms and mnemonic function.Entities:
Keywords: CaMKII; LTP; inhibitory interneurons; learning and memory; network oscillations; network plasticity; synaptic plasticity
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Year: 2021 PMID: 33548174 PMCID: PMC9239733 DOI: 10.1016/j.neuron.2021.01.014
Source DB: PubMed Journal: Neuron ISSN: 0896-6273 Impact factor: 18.688