首页> 美国卫生研究院文献>American Journal of Physiology - Regulatory Integrative and Comparative Physiology >The sleep-wake cycle and motor activity but not temperature are disrupted over the light-dark cycle in mice genetically depleted of serotonin
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The sleep-wake cycle and motor activity but not temperature are disrupted over the light-dark cycle in mice genetically depleted of serotonin

机译:在基因缺失了5-羟色胺的小鼠中睡眠-觉醒周期和运动活动(而不是温度)在明暗周期中被破坏

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摘要

We examined the role that serotonin has in the modulation of sleep and wakefulness across a 12-h:12-h light-dark cycle and determined whether temperature and motor activity are directly responsible for potential disruptions to arousal state. Telemetry transmitters were implanted in 24 wild-type mice (Tph2+/+) and 24 mice with a null mutation for tryptophan hydroxylase 2 (Tph2−/−). After surgery, electroencephalography, core body temperature, and motor activity were recorded for 24 h. Temperature for a given arousal state (quiet and active wake, non-rapid eye movement, and paradoxical sleep) was similar in the Tph2+/+ and Tph2−/− mice across the light-dark cycle. The percentage of time spent in active wakefulness, along with motor activity, was decreased in the Tph2+/+ compared with the Tph2−/− mice at the start and end of the dark cycle. This difference persisted into the light cycle. In contrast, the time spent in a given arousal state was similar at the remaining time points. Despite this similarity, periods of non-rapid-eye-movement sleep and wakefulness were less consolidated in the Tph2+/+ compared with the Tph2−/− mice throughout the light-dark cycle. We conclude that the depletion of serotonin does not disrupt the diurnal variation in the sleep-wake cycle, motor activity, and temperature. However, serotonin may suppress photic and nonphotic inputs that manifest at light-dark transitions and serve to shorten the ultraradian duration of wakefulness and non-rapid-eye-movement sleep. Finally, alterations in the sleep-wake cycle following depletion of serotonin are unrelated to disruptions in the modulation of temperature.
机译:我们检查了5-羟色胺在整个12小时:12小时的明暗循环中在睡眠和清醒调节中的作用,并确定温度和运动活动是否直接导致唤醒状态的潜在破坏。遥测发射器被植入24只野生型小鼠(Tph2 + / + )和24个色氨酸羟化酶2无效突变(Tph2 -/-)的小鼠中。手术后,记录24小时的脑电图,核心体温和运动活动。在Tph2 + / + 和Tph2 -/-小鼠中,给定的唤醒状态(安静和主动的觉醒,眼动不速和矛盾的睡眠)的温度相似穿越明暗循环。与Tph2 -/-小鼠相比,在Tph2 + / + 中,主动觉醒和运动活动所花费的时间百分比在开始和结束时都降低了。黑暗周期。这种差异一直持续到光周期。相反,在给定的唤醒状态下花费的时间在其余时间点是相似的。尽管有这种相似性,但与Tph2 -/-小鼠相比,在整个光线下,Tph2 + / + 期间非快速眼动睡眠和清醒的时期较少-黑暗的周期。我们得出结论,5-羟色胺的消耗不会破坏睡眠觉醒周期,运动活动和温度的昼夜变化。然而,5-羟色胺可能会抑制在明暗过渡时出现的光和非光输入,并能缩短清醒和快速眼动睡眠的超弧度持续时间。最后,血清素耗尽后睡眠觉醒周期的改变与温度调节的中断无关。

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