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The circadian clock stops ticking during deep hibernation in the European hamster

机译:在欧洲仓鼠的深度冬眠期间昼夜节律时钟停止计时

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摘要

Hibernation is a fascinating, yet enigmatic, physiological phenomenon during which body temperature and metabolism are reduced to save energy. During the harsh season, this strategy allows substantial energy saving by reducing body temperature and metabolism. Accordingly, biological processes are considerably slowed down and reduced to a minimum. However, the persistence of a temperature-compensated, functional biological clock in hibernating mammals has long been debated. Here, we show that the master circadian clock no longer displays 24-h molecular oscillations in hibernating European hamsters. The clock genes Per1, Per2, and Bmal1 and the clock-controlled gene arginine vasopressin were constantly expressed in the suprachiasmatic nucleus during deep torpor, as assessed by radioactive in situ hybridization. Finally, the melatonin rhythm-generating enzyme, arylalkylamine N-acetyltransferase, whose rhythmic expression in the pineal gland is controlled by the master circadian clock, no longer exhibits dayight changes of expression but constantly elevated mRNA levels over 24 h. Overall, these data provide strong evidence that in the European hamster the molecular circadian clock is arrested during hibernation and stops delivering rhythmic output signals.
机译:冬眠是一种令人着迷但神秘的生理现象,在这种现象下,人体温度和新陈代谢降低以节省能量。在严峻的季节,这种策略可以通过降低体温和减少新陈代谢来节省大量能源。因此,生物过程大大减慢并且减少到最小。然而,长期以来人们一直在争论温度补偿的功能性生物钟在冬眠哺乳动物中的持久性。在这里,我们证明了在昼夜节律的欧洲仓鼠中,昼夜节律生物钟不再显示24小时分子振荡。通过放射性原位杂交评估,时钟基因Per1,Per2和Bmal1以及时钟控制基因精氨酸加压素在深to部上持续在视交叉上核中表达。最后,褪黑激素节律产生酶,芳基烷基胺N-乙酰基转移酶,其在松果体中的节律性表达受主生物钟控制,不再表现昼夜变化,而是在24小时内不断升高的mRNA水平。总体而言,这些数据提供了有力的证据,表明在欧洲仓鼠中,分子昼夜节律时钟在冬眠期间被捕,并停止传递有节奏的输出信号。

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