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负责异相睡眠起始和维持的大鼠脑桥-延髓网络:一项联合微量注射和功能性神经解剖学研究

The rat ponto-medullary network responsible for paradoxical sleep onset and maintenance: a combined microinjection and functional neuroanatomical study.

作者信息

Boissard Romuald, Gervasoni Damien, Schmidt Markus H, Barbagli Bruno, Fort Patrice, Luppi Pierre-Hervé

机构信息

CNRS FRE 2469, Institut Fédératif des Neurosciences de Lyon (IFR 19), Université Claude Bernard Lyon I, 8 Avenue Rockefeller, 69373 LYON Cedex 08, France.

出版信息

Eur J Neurosci. 2002 Nov;16(10):1959-73. doi: 10.1046/j.1460-9568.2002.02257.x.

DOI:10.1046/j.1460-9568.2002.02257.x
PMID:12453060
Abstract

The neuronal network responsible for paradoxical sleep (PS) onset and maintenance has not previously been identified in the rat, unlike the cat. To fill this gap, this study has developed a new technique involving the recording of sleep-wake states in unanaesthetized head-restrained rats whilst locally administering pharmacological agents by microiontophoresis from glass multibarrel micropipettes, into the dorsal pontine tegmentum and combining this with functional neuroanatomy. Pharmacological agents used for iontophoretic administration included carbachol, kainic acid, bicuculline and gabazine. The injection sites and their efferents were then identified by injections of anterograde (phaseolus vulgaris leucoagglutinin) or retrograde (cholera toxin B subunit) tracers through an adjacent barrel of the micropipette assembly and by C-Fos immunostaining. Bicuculline, gabazine and kainic acid ejections specifically into the pontine sublaterodorsal nucleus (SLD) induced within a few minutes a PS-like state characterized by a continuous muscle atonia, low voltage EEG and a lack of reaction to stimuli. In contrast, carbachol ejections into the SLD induced wakefulness. In PHA-L, glycine and C-Fos multiple double-labelling experiments, anterogradely labelled fibres originating from the SLD were seen apposed on glycine and C-Fos positive neurons (labelled after 90 min of pharmacologically induced PS-like state) from the ventral gigantocellular and parvicellular reticular nuclei. Altogether, these data indicate that the SLD nuclei contain a population of neurons playing a crucial role in PS onset and maintenance. Furthermore, they suggest that GABAergic disinhibition and glutamate excitation of these neurons might also play a crucial role in the onset of PS.

摘要

与猫不同,负责异相睡眠(PS)起始和维持的神经网络此前在大鼠中尚未被确定。为填补这一空白,本研究开发了一种新技术,该技术涉及在未麻醉的头部固定大鼠中记录睡眠-觉醒状态,同时通过玻璃多管微吸管进行微量离子电泳将药理剂局部施用于脑桥背侧被盖区,并将其与功能神经解剖学相结合。用于离子电泳给药的药理剂包括卡巴胆碱、 kainic 酸、荷包牡丹碱和加巴嗪。然后通过微量移液器组件的相邻管注射顺行(菜豆凝集素)或逆行(霍乱毒素 B 亚基)示踪剂以及 C-Fos 免疫染色来确定注射部位及其传出纤维。将荷包牡丹碱、加巴嗪和 kainic 酸特异性注射到脑桥外侧背核(SLD)中,几分钟内就会诱导出一种类似 PS 的状态,其特征为持续的肌肉弛缓、低电压脑电图以及对刺激无反应。相比之下,将卡巴胆碱注射到 SLD 中会诱导觉醒。在PHA-L、甘氨酸和 C-Fos 多重双标记实验中,从 SLD 发出的顺行标记纤维可见于来自腹侧巨细胞和小细胞网状核的甘氨酸和 C-Fos 阳性神经元(在药理学诱导的类似 PS 状态 90 分钟后标记)上。总之,这些数据表明 SLD 核包含一群在 PS 起始和维持中起关键作用的神经元。此外,它们表明这些神经元的 GABA 能去抑制和谷氨酸能兴奋在 PS 起始中可能也起关键作用。

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