Offline hippocampal reactivation during dentate spikes supports flexible memory.

McHugh SB
Lopes-Dos-Santos V
Castelli M
Gava GP
Thompson SE
Tam SKE
Hartwich K
Perry B
Toth R
Denison T
Sharott A
Dupret D

When we sleep, our brain stabilises new memories by having nerve cells work together. We know one type of neural activity, called sharp-wave ripples, helps with this offline process in a part of the brain called the hippocampus. This study found that a second type of activity, called dentate spikes, also helps nerve cells work together during sleep and is important for making new, adaptable memories.

Scientific Abstract

Stabilizing new memories requires coordinated neuronal spiking activity during sleep. Hippocampal sharp-wave ripples (SWRs) in the cornu ammonis (CA) region and dentate spikes (DSs) in the dentate gyrus (DG) are prime candidate network events for supporting this offline process. SWRs have been studied extensively, but the contribution of DSs remains unclear. By combining triple-ensemble (DG-CA3-CA1) recordings and closed-loop optogenetics in mice, we show that, like SWRs, DSs synchronize spiking across DG and CA principal cells to reactivate population-level patterns of neuronal coactivity expressed during prior waking experience. Notably, the population coactivity structure in DSs is more diverse and higher dimensional than that seen during SWRs. Importantly, suppressing DG granule cell spiking selectively during DSs impairs subsequent flexible memory performance during multi-object recognition tasks and associated hippocampal patterns of neuronal coactivity. We conclude that DSs constitute a second offline network event central to hippocampal population dynamics serving memory-guided behavior.

plot of LFP showing dentate spikes, and a plot of multiple neurons spiking underneath
Top: the local field potential recorded from the dentate gyrus, with dentate spike events indicated in red. Below: spikes (black ticks) fired by hippocampal principal cells are synchronised by dentate spikes.
Citation

2024. Neuron (e-Pub ahead of print).

DOI
10.1016/j.neuron.2024.08.022
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