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Characterization of Sleep in Zebrafish and Insomnia in Hypocretin Receptor Mutants

机译:降钙素受体突变体的斑马鱼睡眠和失眠特征

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Sleep is a fundamental biological process conserved across the animal kingdom. The study of how sleep regulatory networks are conserved is needed to better understand sleep across evolution. We present a detailed description of a sleep state in adult zebrafish characterized by reversible periods of immobility, increased arousal threshold, and place preference. Rest deprivation using gentle electrical stimulation is followed by a sleep rebound, indicating homeostatic regulation. In contrast to mammals and similarly to birds, light suppresses sleep in zebrafish, with no evidence for a sleep rebound. We also identify a null mutation in the sole receptor for the wake-promoting neuropeptide hypocretin (orexin) in zebrafish. Fish lacking this receptor demonstrate short and fragmented sleep in the dark, in striking contrast to the excessive sleepiness and cataplexy of narcolepsy in mammals. Consistent with this observation, we find that the hypocretin receptor does not colocalize with known major wake-promoting monoaminergic and cholinergic cell groups in the zebrafish. Instead, it colocalizes with large populations of GABAergic neurons, including a subpopulation of Adra2a-positive GABAergic cells in the anterior hypothalamic area, neurons that could assume a sleep modulatory role. Our study validates the use of zebrafish for the study of sleep and indicates molecular diversity in sleep regulatory networks across vertebrates.
机译:睡眠是整个动物界保守的基本生物学过程。为了更好地了解整个进化过程中的睡眠,需要研究如何保持睡眠调节网络。我们提出了成年斑马鱼的睡眠状态的详细描述,其特征为可逆的不动时期,提高的唤醒阈值和位置偏好。使用轻度的电刺激剥夺休息,随后出现睡眠反弹,表明体内调节稳定。与哺乳动物相反,与鸟类相似,光线会抑制斑马鱼的睡眠,没有睡眠反弹的迹象。我们还在斑马鱼中促进唤醒的神经肽hypocretin(orexin)的唯一受体中发现一个无效突变。缺乏这种受体的鱼在黑暗中表现出短暂而零散的睡眠,这与哺乳动物嗜睡症的过度嗜睡和瘫痪形成鲜明对比。与此观察结果一致,我们发现降钙素受体与斑马鱼中已知的主要促进尾气的单胺能和胆碱能细胞群不共定位。相反,它与大量的GABA能神经元共定位,包括下丘脑前区Adra2a阳性GABA能细胞的亚群,这些神经元可能承担睡眠调节作用。我们的研究验证了斑马鱼用于睡眠研究的有效性,并表明了整个脊椎动物的睡眠调节网络中的分子多样性。

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