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单突触海马体-前额叶投射有助于小鼠的空间记忆巩固。

Monosynaptic Hippocampal-Prefrontal Projections Contribute to Spatial Memory Consolidation in Mice.

机构信息

Institute of Experimental and Clinical Pharmacology and Toxicology,

Center for Brain, Behavior and Metabolism.

出版信息

J Neurosci. 2019 Aug 28;39(35):6978-6991. doi: 10.1523/JNEUROSCI.2158-18.2019. Epub 2019 Jul 8.

Abstract

Time locking between neocortical sleep slow oscillations, thalamo-cortical spindles, and hippocampal sharp-wave ripples has convincingly been shown to be a key element of systems consolidation. Here we investigate the role of monosynaptic projections from ventral/intermediate hippocampus to medial prefrontal cortex (mPFC) in sleep-dependent memory consolidation in male mice. Following acquisition learning in the Barnes maze, we optogenetically silenced the axonal terminals of hippocampal projections within mPFC during slow-wave sleep. This silencing during SWS selectively impaired recent but not remote memory in the absence of effects on error rate and escape latencies. Furthermore, it prevented the development of the most efficient search strategy and sleep spindle time-locking to slow oscillation. An increase in post-learning sleep sharp-wave ripple (SPWR) density and reduced time locking of learning-associated SPWR activity to sleep spindles may be a less specific response. Our results demonstrate that monosynaptic projections from hippocampus to mPFC contribute to sleep-dependent memory consolidation, potentially by affecting the temporal coupling of sleep-associated electrophysiological events. Convincing evidence supports the role of slow-wave sleep (SWS), and the relevance of close temporal coupling of neuronal activity between brain regions for systems consolidation. Less attention has been paid so far to the specific neuronal pathways underlying these processes. Here, we optogenetically silenced the direct monosynaptic projection from ventral/intermediate hippocampus (HC) to medial prefrontal cortex (mPFC) during SWS in male mice following repeated learning trials in a weakly aversive spatial task. Our results confirm the concept that the monosynaptic projection between HC and mPFC contributes to memory consolidation and support an important functional role of this pathway in shaping the temporal precision among sleep-associated electrophysiological events.

摘要

时间锁定在新皮层慢波振荡、丘脑皮质纺锤波和海马体锐波涟漪之间,已被令人信服地证明是系统巩固的关键要素。在这里,我们研究了腹侧/中间海马体到内侧前额叶皮层(mPFC)的单突触投射在雄性小鼠睡眠依赖记忆巩固中的作用。在巴恩斯迷宫中获得学习后,我们在慢波睡眠期间用光遗传学沉默 mPFC 内海马体投射的轴突末梢。这种 SWS 期间的沉默选择性地损害了最近的记忆,但不影响错误率和逃逸潜伏期。此外,它阻止了最有效的搜索策略的发展以及睡眠纺锤波与慢波的时间锁定。学习相关的 SPWR 活动与睡眠纺锤波的时间锁定减少,可能是一种不太特异的反应。我们的结果表明,海马体到 mPFC 的单突触投射有助于睡眠依赖的记忆巩固,可能通过影响睡眠相关电生理事件的时间耦合来实现。令人信服的证据支持慢波睡眠(SWS)的作用,以及脑区之间神经元活动的紧密时间耦合对于系统巩固的相关性。到目前为止,这些过程的具体神经元通路还没有得到太多关注。在这里,我们在雄性小鼠中,在重复学习试验后的弱厌恶空间任务中,用光遗传学沉默了 SWS 期间腹侧/中间海马体(HC)到内侧前额叶皮层(mPFC)的直接单突触投射。我们的结果证实了 HC 和 mPFC 之间的单突触投射有助于记忆巩固的概念,并支持该通路在塑造与睡眠相关的电生理事件之间的时间精度方面的重要功能作用。

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