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Hippocampal CA3 Output Is Crucial for Ripple-Associated Reactivation and Consolidation of Memory

Author(s)
Tonegawa, Susumu; Nakashiba, Toshiaki; Buhl, Derek L.; McHugh, Thomas J.
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Abstract
A widely held memory consolidation theory posits that memory of events and space is initially stored in the hippocampus (HPC) in a time-limited manner and is consolidated in the neocortex for permanent storage. Although posttraining HPC lesions result in temporally graded amnesia, the precise HPC circuits and mechanisms involved in remote memory storage remain poorly understood. To investigate the role of the trisynaptic pathway in the consolidation process we employed the CA3-TeTX transgenic mouse, in which CA3 output can be specifically and inducibly controlled. We found that posttraining blockade of CA3 output for up to 4 weeks impairs the consolidation of contextual fear memory. Moreover, in vivo hippocampal recordings revealed a reduced intrinsic frequency of CA1 ripples and a significant decrease in the experience-dependent, ripple-associated coordinated reactivation of CA1 cell pairs. Collectively, these results suggest that the posttraining integrity of the trisynaptic pathway and the ripple-associated reactivation of hippocampal memory engram are crucial for memory consolidation.
Date issued
2009-06
URI
http://hdl.handle.net/1721.1/57437
Department
Massachusetts Institute of Technology. Department of Biology; Massachusetts Institute of Technology. Department of Brain and Cognitive Sciences; Picower Institute for Learning and Memory
Journal
Neuron
Publisher
Cell Press
Citation
Nakashiba, Toshiaki et al. “Hippocampal CA3 Output Is Crucial for Ripple-Associated Reactivation and Consolidation of Memory.” Neuron 62.6 (2009): 781-787.
Version: Author's final manuscript
ISSN
0896-6273
Keywords
sysneuro, molneuro, signaling

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