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通过毒蕈碱型乙酰胆碱途径进行神经调节,可以在睡眠依赖性记忆巩固过程中促进非快速眼动(NREM)和快速眼动(REM)睡眠状态发挥不同、互补且有序的作用。

Neuromodulation via muscarinic acetylcholine pathway can facilitate distinct, complementary, and sequential roles for NREM and REM states during sleep-dependent memory consolidation.

作者信息

Satchell Michael, Fry Blaine, Noureddine Zahraa, Simmons Alexis, Ognjanovski Nicolette N, Aton Sara J, Zochowski Michal R

出版信息

bioRxiv. 2024 Jan 16:2023.05.19.541465. doi: 10.1101/2023.05.19.541465.

Abstract

UNLABELLED

Across vertebrate species, sleep consists of repeating cycles of NREM followed by REM. However, the respective functions of NREM, REM, and their stereotypic cycling pattern are not well understood. Using a simplified biophysical network model, we show that NREM and REM sleep can play differential and critical roles in memory consolidation primarily regulated, based on state-specific changes in cholinergic signaling. Within this network, decreasing and increasing muscarinic acetylcholine (ACh) signaling during bouts of NREM and REM, respectively, differentially alters neuronal excitability and excitatory/inhibitory balance. During NREM, deactivation of inhibitory neurons leads to network-wide disinhibition and bursts of synchronized activity led by firing in engram neurons. These features strengthen connections from the original engram neurons to less-active network neurons. In contrast, during REM, an increase in network inhibition suppresses firing in all but the most-active excitatory neurons, leading to competitive strengthening/pruning of the memory trace. We tested the predictions of the model against recordings from mouse hippocampus during active sleep-dependent memory storage. Consistent with modeling results, we find that functional connectivity between CA1 neurons changes differentially at transition from NREM to REM sleep during learning. Returning to the model, we find that an iterative sequence of state-specific activations during NREM/REM cycling is essential for memory storage in the network, serving a critical role during simultaneous consolidation of multiple memories. Together these results provide a testable mechanistic hypothesis for the respective roles of NREM and REM sleep, and their universal relative timing, in memory consolidation.

SIGNIFICANCE STATEMENT

Using a simplified computational model and recordings from mouse hippocampus, we show that NREM and REM sleep can play differential roles in memory consolidation. The specific neurophysiological features of the two sleep states allow for expansion of memory traces (during NREM) and prevention of overlap between different memory traces (during REM). These features are likely essential in the context of storing more than one new memory simultaneously within a brain network.

摘要

未标注

在脊椎动物物种中,睡眠由非快速眼动(NREM)和快速眼动(REM)交替出现的重复周期组成。然而,NREM、REM各自的功能以及它们刻板的循环模式尚未得到充分理解。我们使用一个简化的生物物理网络模型表明,基于胆碱能信号在特定状态下的变化,NREM睡眠和REM睡眠在记忆巩固中可发挥不同且关键的作用。在这个网络中,分别在NREM和REM期间降低和增加毒蕈碱型乙酰胆碱(ACh)信号,会以不同方式改变神经元兴奋性以及兴奋/抑制平衡。在NREM期间,抑制性神经元失活导致全网络去抑制,并引发由记忆痕迹神经元放电所主导的同步活动爆发。这些特征加强了从原始记忆痕迹神经元到活性较低的网络神经元之间的连接。相反,在REM期间,网络抑制的增加抑制了除最活跃的兴奋性神经元之外的所有神经元的放电,导致记忆痕迹的竞争性强化/修剪。我们根据在依赖睡眠的主动记忆存储过程中小鼠海马体的记录对该模型的预测进行了测试。与建模结果一致,我们发现学习过程中从NREM睡眠过渡到REM睡眠时,CA1神经元之间的功能连接性会以不同方式发生变化。回到模型,我们发现NREM/REM循环期间特定状态激活的迭代序列对于网络中的记忆存储至关重要,在多个记忆同时巩固过程中发挥关键作用。这些结果共同为NREM睡眠和REM睡眠在记忆巩固中的各自作用及其普遍的相对时间提供了一个可检验的机制假说。

意义声明

通过使用简化的计算模型和小鼠海马体的记录,我们表明NREM睡眠和REM睡眠在记忆巩固中可发挥不同作用。这两种睡眠状态的特定神经生理特征允许记忆痕迹扩展(在NREM期间)并防止不同记忆痕迹之间的重叠(在REM期间)。在大脑网络中同时存储多个新记忆的情况下,这些特征可能至关重要。

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