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斑马鱼的睡眠-觉醒调节与食欲素-褪黑素相互作用。

Sleep-wake regulation and hypocretin-melatonin interaction in zebrafish.

机构信息

Center for Narcolepsy, Department of Psychiatry and Behavioral Sciences, Howard Hughes Medical Institute, Stanford University, Palo Alto, CA 94305, USA.

出版信息

Proc Natl Acad Sci U S A. 2009 Dec 22;106(51):21942-7. doi: 10.1073/pnas.906637106. Epub 2009 Dec 4.

Abstract

In mammals, hypocretin/orexin (HCRT) neuropeptides are important sleep-wake regulators and HCRT deficiency causes narcolepsy. In addition to fragmented wakefulness, narcoleptic mammals also display sleep fragmentation, a less understood phenotype recapitulated in the zebrafish HCRT receptor mutant (hcrtr-/-). We therefore used zebrafish to study the potential mediators of HCRT-mediated sleep consolidation. Similar to mammals, zebrafish HCRT neurons express vesicular glutamate transporters indicating conservation of the excitatory phenotype. Visualization of the entire HCRT circuit in zebrafish stably expressing hcrt:EGFP revealed parallels with established mammalian HCRT neuroanatomy, including projections to the pineal gland, where hcrtr mRNA is expressed. As pineal-produced melatonin is a major sleep-inducing hormone in zebrafish, we further studied how the HCRT and melatonin systems interact functionally. mRNA level of arylalkylamine-N-acetyltransferase (AANAT2), a key enzyme of melatonin synthesis, is reduced in hcrtr-/- pineal gland during the night. Moreover, HCRT perfusion of cultured zebrafish pineal glands induces melatonin release. Together these data indicate that HCRT can modulate melatonin production at night. Furthermore, hcrtr-/- fish are hypersensitive to melatonin, but not other hypnotic compounds. Subthreshold doses of melatonin increased the amount of sleep and consolidated sleep in hcrtr-/- fish, but not in the wild-type siblings. These results demonstrate the existence of a functional HCRT neurons-pineal gland circuit able to modulate melatonin production and sleep consolidation.

摘要

在哺乳动物中,食欲素/下丘脑分泌素(HCRT)神经肽是重要的睡眠-觉醒调节剂,而 HCRT 缺乏会导致嗜睡症。除了碎片化的觉醒外,嗜睡症哺乳动物还表现出睡眠碎片化,这是一种在斑马鱼 HCRT 受体突变体(hcrtr-/-)中重现的较少被理解的表型。因此,我们使用斑马鱼来研究 HCRT 介导的睡眠巩固的潜在介质。与哺乳动物相似,斑马鱼 HCRT 神经元表达囊泡谷氨酸转运体,表明其兴奋性表型得到了保留。在稳定表达 hcrt:EGFP 的斑马鱼中可视化整个 HCRT 回路揭示了与已建立的哺乳动物 HCRT 神经解剖学的平行性,包括向松果体的投射,其中 hcrtr mRNA 表达。由于松果体产生的褪黑素是斑马鱼中主要的诱导睡眠激素,因此我们进一步研究了 HCRT 和褪黑素系统如何在功能上相互作用。在夜间,hcrtr-/-松果体中的芳香族烷基胺-N-乙酰转移酶(AANAT2)的 mRNA 水平降低,AANAT2 是褪黑素合成的关键酶。此外,HCRT 灌注培养的斑马鱼松果体可诱导褪黑素释放。这些数据表明 HCRT 可以在夜间调节褪黑素的产生。此外,hcrtr-/-鱼对褪黑素敏感,但对其他催眠化合物不敏感。褪黑素的亚阈值剂量增加了 hcrtr-/-鱼的睡眠时间和睡眠巩固,但对野生型兄弟姐妹没有影响。这些结果表明存在一个功能齐全的 HCRT 神经元-松果体回路,能够调节褪黑素的产生和睡眠的巩固。

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