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Effects of Sleep Fragmentation on Sleep and Markers of Inflammation in Mice

机译:睡眠破碎对小鼠睡眠和炎症标记的影响

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摘要

Many people in our society experience curtailment and disruption of sleep due to work responsibilities, care-giving, or life style choice. Delineating the health effect of acute and chronic disruptions in sleep is essential to raising awareness of and creating interventions to manage these prevalent concerns. To provide a platform for studying the health impact and underlying pathophysiologic mechanisms associated with inadequate sleep, we developed and characterized an approach to creating chronic disruption of sleep in laboratory mice. We used this method to evaluate how 3 durations of sleep fragmentation (SF) affect sleep recuperation and blood and lung analyte concentrations in male C57BL/6J mice. Mice housed in environmentally controlled chambers were exposed to automated SF for periods of 6, 12, or 24 h or for 12 h daily during the light (somnolent) phase for 4 sequential days. Sleep time, slow-wave amplitude, or bout lengths were significantly higher when uninterrupted sleep was permitted after each of the 3 SF durations. However, mice did not recover all of the lost slow-wave sleep during the subsequent 12- to 24-h period and maintained a net loss of sleep. Light-phase SF was associated with significant changes in serum and lung levels of some inflammatory substances, but these changes were not consistent or sustained. The data indicate that acute light-phase SF can result in a sustained sleep debt in mice and may disrupt the inflammatory steady-state in serum and lung.
机译:由于工作职责,提供照料或生活方式的选择,我们社会中的许多人会受到限制和睡眠中断。描绘急性和慢性睡眠中断对健康的影响对于提高对这些普遍关注的认识并制定干预措施至关重要。为了提供一个研究与睡眠不足有关的健康影响和潜在病理生理机制的平台,我们开发并描述了一种在实验室小鼠中造成慢性睡眠中断的方法。我们使用这种方法评估雄性C57BL / 6J小鼠的3个睡眠碎片(SF)持续时间如何影响睡眠恢复以及血液和肺中分析物的浓度。在轻度(清醒)阶段,将饲养在环境控制室中的小鼠暴露于自动SF中6、12或24小时或每天12小时,连续4天。如果在3个SF持续时间中的每一个之后都允许不间断的睡眠,则睡眠时间,慢波振幅或回合长度会明显增加。但是,小鼠在随后的12至24小时内并未恢复所有丢失的慢波睡眠,而是保持了净睡眠。轻期SF与某些炎症物质的血清和肺水平的显着变化有关,但这些变化并不一致或持续存在。数据表明,急性轻期SF可能导致小鼠持续的睡眠不足,并可能破坏血清和肺部的炎症稳态。

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