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雄性小鼠自发大麻素戒断期间睡眠改变。

Altered sleep during spontaneous cannabinoid withdrawal in male mice.

机构信息

Department of Psychiatry, Harvard Medical School, McLean Hospital, Belmont, Massachusetts.

Neurolux Inc, Northfield.

出版信息

Behav Pharmacol. 2022 Apr 1;33(2&3):195-205. doi: 10.1097/FBP.0000000000000674.

Abstract

Cessation of cannabinoid use in humans often leads to a withdrawal state that includes sleep disruption. Despite important health implications, little is known about how cannabinoid abstention affects sleep architecture, in part because spontaneous cannabinoid withdrawal is difficult to model in animals. In concurrent work we report that repeated administration of the high-efficacy cannabinoid 1 (CB1) receptor agonist AM2389 to mice for 5 days led to heightened locomotor activity and paw tremor following treatment discontinuation, potentially indicative of spontaneous cannabinoid withdrawal. Here, we performed parallel studies to examine effects on sleep. Using implantable electroencephalography (EEG) and electromyography (EMG) telemetry we examined sleep and neurophysiological measures before, during, and after 5 days of twice-daily AM2389 injections. We report that AM2389 produces decreases in locomotor activity that wane with repeated treatment, whereas discontinuation produces rebound increases in activity that persist for several days. Likewise, AM2389 initially produces profound increases in slow-wave sleep (SWS) and decreases in rapid eye movement (REM) sleep, as well as consolidation of sleep. By the third AM2389 treatment, this pattern transitions to decreases in SWS and total time sleeping. This pattern persists following AM2389 discontinuation and is accompanied by emergence of sleep fragmentation. Double-labeling immunohistochemistry for hypocretin/orexin (a sleep-regulating peptide) and c-Fos (a neuronal activity marker) in lateral hypothalamus revealed decreases in c-Fos/orexin+ cells following acute AM2389 and increases following discontinuation, aligning with the sleep changes. These findings indicate that AM2389 profoundly alters sleep in mice and suggest that sleep disruption following treatment cessation reflects spontaneous cannabinoid withdrawal.

摘要

大麻素使用的停止常常导致包括睡眠中断在内的戒断状态。尽管对健康有重要影响,但对于大麻素戒断如何影响睡眠结构知之甚少,部分原因是自发的大麻素戒断在动物中难以建模。在同期的工作中,我们报告重复给予高效力大麻素 1(CB1)受体激动剂 AM2389 5 天会导致治疗停止后运动活动和爪震颤增加,这可能表明自发的大麻素戒断。在这里,我们进行了平行研究以检查对睡眠的影响。使用植入式脑电图(EEG)和肌电图(EMG)遥测技术,我们在 AM2389 每日两次注射的 5 天之前、期间和之后检查了睡眠和神经生理测量值。我们报告 AM2389 会导致运动活动减少,随着重复治疗而减弱,而停止治疗则会导致活动反弹增加,持续数天。同样,AM2389 最初会导致慢波睡眠(SWS)深度增加和快速眼动(REM)睡眠减少,以及睡眠巩固。到第三次 AM2389 治疗时,这种模式转变为 SWS 和总睡眠时间减少。这种模式在 AM2389 停止后持续存在,并伴有睡眠碎片化的出现。外侧下丘脑的下丘脑泌素/食欲素(一种睡眠调节肽)和 c-Fos(一种神经元活性标志物)的双标记免疫组织化学显示,急性 AM2389 后 c-Fos/orexin+细胞减少,停止治疗后增加,与睡眠变化一致。这些发现表明 AM2389 会极大地改变小鼠的睡眠,并表明治疗停止后睡眠中断反映了自发的大麻素戒断。

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