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NMDAR 激活调节睡眠和情绪的昼夜节律。

NMDAR activation regulates the daily rhythms of sleep and mood.

机构信息

Aptinyx Inc., Evanston, IL.

Falk Center for Molecular Therapeutics, Department of Biomedical Engineering, Northwestern University, Evanston, IL.

出版信息

Sleep. 2019 Oct 9;42(10). doi: 10.1093/sleep/zsz135.

Abstract

STUDY OBJECTIVES

The present studies examine the effects of NMDAR activation by NYX-2925 diurnal rhythmicity of both sleep and wake as well as emotion.

METHODS

Twenty-four-hour sleep EEG recordings were obtained in sleep-deprived and non-sleep-deprived rats. In addition, the day-night cycle of both activity and mood was measured using home cage ultrasonic-vocalization recordings.

RESULTS

NYX-2925 significantly facilitated non-REM (NREM) sleep during the lights-on (sleep) period, and this effect persisted for 3 days following a single dose in sleep-deprived rats. Sleep-bout duration and REM latencies were increased without affecting total REM sleep, suggesting better sleep quality. In addition, delta power during wake was decreased, suggesting less drowsiness. NYX-2925 also rescued learning and memory deficits induced by sleep deprivation, measured using an NMDAR-dependent learning task. Additionally, NYX-2925 increased positive affect and decreased negative affect, primarily by facilitating the transitions from sleep to rough-and-tumble play and back to sleep. In contrast to NYX-2925, the NMDAR antagonist ketamine acutely (1-4 hours post-dosing) suppressed REM and non-REM sleep, increased delta power during wake, and blunted the amplitude of the sleep-wake activity rhythm.

DISCUSSION

These data suggest that NYX-2925 could enhance behavioral plasticity via improved sleep quality as well as vigilance during wake. As such, the facilitation of sleep by NYX-2925 has the potential to both reduce symptom burden on neurological and psychiatric disorders as well as serve as a biomarker for drug effects through restoration of sleep architecture.

摘要

研究目的

本研究旨在考察 NYX-2925 对 NMDA 受体的激活作用对睡眠和觉醒昼夜节律以及情绪的影响。

方法

在睡眠剥夺和非睡眠剥夺大鼠中进行 24 小时睡眠脑电图记录。此外,使用家庭笼超声发声记录测量活动和情绪的昼夜节律。

结果

NYX-2925 显著促进了光照(睡眠)期间的非快速眼动(NREM)睡眠,并且这种作用在睡眠剥夺大鼠单次给药后持续了 3 天。睡眠潜伏期和 REM 潜伏期增加,而总 REM 睡眠时间不受影响,提示睡眠质量提高。此外,清醒时的δ功率降低,提示嗜睡减少。NYX-2925 还挽救了睡眠剥夺引起的学习和记忆缺陷,这是通过一种 NMDA 受体依赖性学习任务来测量的。此外,NYX-2925 增加了积极情绪,减少了消极情绪,主要是通过促进从睡眠到打闹再到睡眠的过渡。与 NYX-2925 相反,NMDA 拮抗剂氯胺酮急性(给药后 1-4 小时)抑制 REM 和 NREM 睡眠,增加清醒时的δ功率,并使睡眠-觉醒活动节律的振幅变平。

讨论

这些数据表明,NYX-2925 可以通过改善睡眠质量和提高觉醒时的警觉性来增强行为可塑性。因此,NYX-2925 促进睡眠有可能减轻神经和精神障碍的症状负担,并通过恢复睡眠结构作为药物作用的生物标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e95e/6783887/93fe2250fe89/zsz135f0001.jpg

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