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本文引用的文献

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Pharmacogenetic modulation of orexin neurons alters sleep/wakefulness states in mice.阿立新神经元的药物遗传学调节改变了小鼠的睡眠/觉醒状态。
PLoS One. 2011;6(5):e20360. doi: 10.1371/journal.pone.0020360. Epub 2011 May 27.
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Optical control of zebrafish behavior with halorhodopsin.利用嗜盐菌视紫红质对斑马鱼行为进行光学控制。
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Sleep homeostasis modulates hypocretin-mediated sleep-to-wake transitions.睡眠稳态调节下丘脑分泌素介导的睡眠至觉醒转换。
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Monoaminergic neuronal changes in orexin deficient mice.食欲素缺乏小鼠中单胺能神经元的变化。
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Neuronal activity of orexin and non-orexin waking-active neurons during wake-sleep states in the mouse.小鼠清醒-睡眠状态下食欲素及非食欲素觉醒激活神经元的神经活动
Neuroscience. 2008 May 15;153(3):860-70. doi: 10.1016/j.neuroscience.2008.02.058. Epub 2008 Mar 6.
7
Neural substrates of awakening probed with optogenetic control of hypocretin neurons.通过对下丘脑泌素神经元的光遗传学控制来探究觉醒的神经基质。
Nature. 2007 Nov 15;450(7168):420-4. doi: 10.1038/nature06310. Epub 2007 Oct 17.
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Multimodal fast optical interrogation of neural circuitry.神经回路的多模态快速光学检测
Nature. 2007 Apr 5;446(7136):633-9. doi: 10.1038/nature05744.
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Multiple-color optical activation, silencing, and desynchronization of neural activity, with single-spike temporal resolution.多色光激活、沉默和神经活动去同步化,具有单尖峰时间分辨率。
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The neural circuit of orexin (hypocretin): maintaining sleep and wakefulness.食欲素(下丘脑泌素)的神经回路:维持睡眠与觉醒
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急性光遗传沉默食欲素/下丘脑分泌素神经元可诱导小鼠慢波睡眠。

Acute optogenetic silencing of orexin/hypocretin neurons induces slow-wave sleep in mice.

机构信息

Division of Cell Signaling, National Institute for Physiological Sciences, Okazaki 444-8787, Japan.

出版信息

J Neurosci. 2011 Jul 20;31(29):10529-39. doi: 10.1523/JNEUROSCI.0784-11.2011.

DOI:10.1523/JNEUROSCI.0784-11.2011
PMID:21775598
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3864636/
Abstract

Orexin/hypocretin neurons have a crucial role in the regulation of sleep and wakefulness. To help determine how these neurons promote wakefulness, we generated transgenic mice in which orexin neurons expressed halorhodopsin (orexin/Halo mice), an orange light-activated neuronal silencer. Slice patch-clamp recordings of orexin neurons that expressed halorhodopsin demonstrated that orange light photic illumination immediately hyperpolarized membrane potential and inhibited orexin neuron discharge in proportion to illumination intensity. Acute silencing of orexin neurons in vivo during the day (the inactive period) induced synchronization of the electroencephalogram and a reduction in amplitude of the electromyogram that is characteristic of slow-wave sleep (SWS). In contrast, orexin neuron photoinhibition was ineffective during the night (active period). Acute photoinhibition of orexin neurons during the day in orexin/Halo mice also reduced discharge of neurons in an orexin terminal field, the dorsal raphe (DR) nucleus. However, serotonergic DR neurons exhibited normal discharge rates in mice lacking orexin neurons. Thus, although usually highly dependent on orexin neuronal activity, serotonergic DR neuronal activity can be regulated appropriately in the chronic absence of orexin input. Together, these results demonstrate that acute inhibition of orexin neurons results in time-of-day-dependent induction of SWS and in reduced firing rate of neurons in an efferent projection site thought to be involved in arousal state regulation. The results presented here advance our understanding of the role of orexin neurons in the regulation of sleep/wakefulness and may be relevant to the mechanisms that underlie symptom progression in narcolepsy.

摘要

食欲素/下丘脑分泌素神经元在调节睡眠和觉醒中起着至关重要的作用。为了帮助确定这些神经元如何促进觉醒,我们生成了在食欲素神经元中表达盐藻菌视紫红质(orexin/Halo 小鼠)的转基因小鼠,这是一种橙光激活的神经元沉默剂。表达盐藻菌视紫红质的食欲素神经元的切片膜片钳记录表明,橙光光照立即超极化膜电位,并根据光照强度抑制食欲素神经元的放电。在白天(非活跃期)对体内食欲素神经元进行急性沉默会诱导脑电图同步,并减少肌电图振幅,这是慢波睡眠(SWS)的特征。相比之下,夜间(活跃期)食欲素神经元的光抑制无效。在 orexin/Halo 小鼠中,白天急性光抑制食欲素神经元也会降低位于食欲素终末场的中缝背核(DR)核神经元的放电。然而,在缺乏食欲素神经元的小鼠中,5-羟色胺能 DR 神经元的放电率仍保持正常。因此,尽管通常高度依赖于食欲素神经元的活动,但在慢性缺乏食欲素输入的情况下,5-羟色胺能 DR 神经元的活动可以得到适当的调节。总之,这些结果表明,急性抑制食欲素神经元会导致 SWS 的时间依赖性诱导,并降低被认为参与觉醒状态调节的传出投射部位的神经元放电率。这里呈现的结果增进了我们对食欲素神经元在睡眠/觉醒调节中的作用的理解,可能与嗜睡症症状进展的机制有关。