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睡眠片段化持续时间对青春期小鼠空间学习和突触可塑性的不同影响。

Differential effects of duration of sleep fragmentation on spatial learning and synaptic plasticity in pubertal mice.

作者信息

Wallace Eli, Kim Do Young, Kim Kye-Min, Chen Stephanie, Blair Braden B, Williams Jeremy, Jasso Kalene, Garcia Alex, Rho Jong M, Bimonte-Nelson Heather, Maganti Rama

机构信息

University of Wisconsin School of Medicine and Public Health, Madison, WI, USA.

Barrow Neurological Institute/St Joseph's Hospital and Medical Center, Phoenix, AZ, USA.

出版信息

Brain Res. 2015 Jul 30;1615:116-128. doi: 10.1016/j.brainres.2015.04.037. Epub 2015 May 7.

Abstract

STUDY OBJECTIVE

To examine the differential effects of acute and chronic sleep fragmentation (SF) on spatial learning and memory, and hippocampal long-term potentiation (LTP) in pubertal mice.

METHODS

Two studies were performed during which adolescent C57/Bl6 mice were subjected to acute-SF 24h a day × 3 days or chronic-SF for 12h a day × 2 weeks using a programmable rotating lever that provides tactile stimulus with controls housed in similar cages. Spatial learning and memory was examined using the Morris water maze, and long-term potentiation (LTP) was evaluated after stimulation of Schaffer collaterals in CA1 hippocampus post SF. Actigraphy was used during the period of SF to monitor rest-activity patterns. Electroencephalographic (EEG) recordings were acquired for analysis of vigilance state patterns and delta-power. Serum corticosterone was measured to assess stress levels.

RESULTS

Acute-SF via tactile stimulation negatively impacted spatial learning, as well as LTP maintenance, compared to controls with no tactile stimulation. While actigraphy showed significantly increased motor activity during SF in both groups, EEG data indicated that overall sleep efficiency did not differ between baseline and SF days, but significant increases in number of wakeful bouts and decreases in average NREM and REM bout lengths were seen during lights-on. Acute sleep fragmentation did not impact corticosterone levels.

CONCLUSIONS

The current results indicate that, during development in pubertal mice, acute-SF for 24h a day × 3 days negatively impacted spatial learning and synaptic plasticity. Further studies are needed to determine if any inherent long-term homeostatic mechanisms in the adolescent brain afford greater resistance to the deleterious effects of chronic-SF.

摘要

研究目的

探讨急性和慢性睡眠片段化(SF)对青春期小鼠空间学习记忆及海马长时程增强(LTP)的不同影响。

方法

进行了两项研究,在此期间,使用可编程旋转杆对青春期C57/Bl6小鼠进行每天24小时×3天的急性睡眠片段化或每天12小时×2周的慢性睡眠片段化处理,该旋转杆提供触觉刺激,对照组小鼠饲养在类似笼子中。使用莫里斯水迷宫检测空间学习记忆,在睡眠片段化处理后刺激海马CA1区的谢弗侧支评估长时程增强(LTP)。在睡眠片段化期间使用活动记录仪监测休息-活动模式。采集脑电图(EEG)记录以分析警觉状态模式和δ波功率。测量血清皮质酮以评估应激水平。

结果

与无触觉刺激的对照组相比,通过触觉刺激进行的急性睡眠片段化对空间学习以及LTP维持产生负面影响。虽然活动记录仪显示两组在睡眠片段化期间运动活动均显著增加,但脑电图数据表明,基线期和睡眠片段化期之间总体睡眠效率没有差异,但在光照期清醒发作次数显著增加,平均非快速眼动(NREM)和快速眼动(REM)发作时长减少。急性睡眠片段化不影响皮质酮水平。

结论

当前结果表明,在青春期小鼠发育过程中,每天24小时×3天的急性睡眠片段化对空间学习和突触可塑性产生负面影响。需要进一步研究以确定青春期大脑中是否存在任何内在的长期稳态机制,使其对慢性睡眠片段化的有害影响具有更大的抵抗力。

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