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食欲素-1通过激活蓝斑核神经元来调节快速眼动睡眠。

Hypocretin-1 modulates rapid eye movement sleep through activation of locus coeruleus neurons.

作者信息

Bourgin P, Huitrón-Résendiz S, Spier A D, Fabre V, Morte B, Criado J R, Sutcliffe J G, Henriksen S J, de Lecea L

机构信息

Departments of Molecular Biology and Neuropharmacology, The Scripps Research Institute, La Jolla, California 92037, USA.

出版信息

J Neurosci. 2000 Oct 15;20(20):7760-5. doi: 10.1523/JNEUROSCI.20-20-07760.2000.

Abstract

The hypocretins (hcrts), also known as orexins, are two recently identified excitatory neuropeptides that in rat are produced by approximately 1200 neurons whose cell bodies are located in the lateral hypothalamus. The hypocretins/orexins have been implicated in the regulation of rapid eye movement (REM) sleep and the pathophysiology of narcolepsy. In the present study, we investigated whether the locus coeruleus (LC), a structure receiving dense hcrtergic innervation, which is quiescent during REM sleep, might be a target for hcrt to regulate REM sleep. Local administration of hcrt1 but not hcrt2 in the LC suppressed REM sleep in a dose-dependent manner and increased wakefulness at the expense of deep, slow-wave sleep. These effects were blocked with an antibody that neutralizes hcrt binding to hcrt receptor 1. In situ hybridization and immunocytochemistry showed the presence of hcrt receptor 1 but not the presence of hcrt receptor 2 in the LC. Iontophoretic application of hcrt1 enhanced the firing rate of LC neurons in vivo, and local injection of hcrt1 into the LC induced the expression of c-fos in the LC area. We propose that hcrt receptor 1 in the LC is a key target for REM sleep regulation and might be involved in the pathophysiological mechanisms of narcolepsy.

摘要

下丘脑分泌素(hcrts),也被称为食欲素,是最近发现的两种兴奋性神经肽,在大鼠中由大约1200个神经元产生,其细胞体位于下丘脑外侧。下丘脑分泌素/食欲素与快速眼动(REM)睡眠的调节以及发作性睡病的病理生理学有关。在本研究中,我们调查了蓝斑(LC)这个接受密集的下丘脑分泌素能神经支配且在REM睡眠期间静止的结构,是否可能是下丘脑分泌素调节REM睡眠的靶点。在蓝斑局部注射下丘脑分泌素1(hcrt1)而非下丘脑分泌素2(hcrt2)会以剂量依赖的方式抑制REM睡眠,并以深度慢波睡眠为代价增加觉醒。这些效应被一种中和下丘脑分泌素与下丘脑分泌素受体1结合的抗体所阻断。原位杂交和免疫细胞化学显示蓝斑中存在下丘脑分泌素受体1,但不存在下丘脑分泌素受体2。在体离子导入下丘脑分泌素1可提高蓝斑神经元的放电频率,并且向蓝斑局部注射下丘脑分泌素1可诱导蓝斑区域c-fos的表达。我们提出,蓝斑中的下丘脑分泌素受体1是REM睡眠调节的关键靶点,并且可能参与发作性睡病的病理生理机制。

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