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基于慢性给予皮质酮的焦虑/抑郁神经内分泌小鼠模型中的非快速眼动睡眠过多及睡眠/觉醒连续性降低

NREM sleep hypersomnia and reduced sleep/wake continuity in a neuroendocrine mouse model of anxiety/depression based on chronic corticosterone administration.

作者信息

Le Dantec Y, Hache G, Guilloux J P, Guiard B P, David D J, Adrien J, Escourrou P

机构信息

Univ Paris-Sud, EA3544, Faculté de Pharmacie, 92296 Châtenay-Malabry cedex, France.

Univ Paris-Sud, EA3544, Faculté de Pharmacie, 92296 Châtenay-Malabry cedex, France.

出版信息

Neuroscience. 2014 Aug 22;274:357-68. doi: 10.1016/j.neuroscience.2014.05.050. Epub 2014 Jun 6.

Abstract

Sleep/wake disorders are frequently associated with anxiety and depression and to elevated levels of cortisol. Even though these alterations are increasingly sought in animal models, no study has investigated the specific effects of chronic corticosterone (CORT) administration on sleep. We characterized sleep/wake disorders in a neuroendocrine mouse model of anxiety/depression, based on chronic CORT administration in the drinking water (35 μg/ml for 4 weeks, "CORT model"). The CORT model was markedly affected during the dark phase by non-rapid eye movement sleep (NREM) increase without consistent alteration of rapid eye movement (REM) sleep. Total sleep duration (SD) and sleep efficiency (SE) increased concomitantly during both the 24h and the dark phase, due to the increase in the number of NREM sleep episodes without a change in their mean duration. Conversely, the total duration of wake decreased due to a decrease in the mean duration of wake episodes despite an increase in their number. These results reflect hypersomnia by intrusion of NREM sleep during the active period as well as a decrease in sleep/wake continuity. In addition, NREM sleep was lighter, with an increased electroencephalogram (EEG) theta activity. With regard to REM sleep, the number and the duration of episodes decreased, specifically during the first part of the light period. REM and NREM sleep changes correlated respectively with the anxiety and the anxiety/depressive-like phenotypes, supporting the notion that studying sleep could be of predictive value for altered emotional behavior. The chronic CORT model in mice that displays hallmark characteristics of anxiety and depression provides an insight into understanding the changes in overall sleep architecture that occur under pathological conditions.

摘要

睡眠/觉醒障碍常与焦虑、抑郁以及皮质醇水平升高有关。尽管在动物模型中越来越多地探寻这些改变,但尚无研究调查长期给予皮质酮(CORT)对睡眠的具体影响。我们基于在饮用水中长期给予CORT(35μg/ml,持续4周,“CORT模型”),对一种焦虑/抑郁神经内分泌小鼠模型中的睡眠/觉醒障碍进行了特征描述。CORT模型在黑暗期受到显著影响,非快速眼动睡眠(NREM)增加,而快速眼动(REM)睡眠无一致改变。由于NREM睡眠发作次数增加而平均时长不变,24小时和黑暗期的总睡眠时间(SD)和睡眠效率(SE)均随之增加。相反,尽管清醒发作次数增加,但由于其平均时长减少,清醒总时长下降。这些结果反映了在活跃期NREM睡眠侵入导致的嗜睡以及睡眠/觉醒连续性的降低。此外,NREM睡眠较浅,脑电图(EEG)θ活动增加。关于REM睡眠,发作次数和时长减少,特别是在光照期的第一部分。REM和NREM睡眠变化分别与焦虑和焦虑/抑郁样表型相关,支持了研究睡眠对改变情绪行为可能具有预测价值的观点。表现出焦虑和抑郁标志性特征的小鼠慢性CORT模型为理解病理条件下整体睡眠结构的变化提供了见解。

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