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本文引用的文献

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Optogenetics and thermogenetics: technologies for controlling the activity of targeted cells within intact neural circuits.光遗传学和热敏遗传学:控制完整神经回路中靶向细胞活性的技术。
Curr Opin Neurobiol. 2012 Feb;22(1):61-71. doi: 10.1016/j.conb.2011.10.023. Epub 2011 Nov 24.
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Activation of central orexin/hypocretin neurons by dietary amino acids.膳食氨基酸对中枢食欲素/下丘脑分泌素神经元的激活作用。
Neuron. 2011 Nov 17;72(4):616-29. doi: 10.1016/j.neuron.2011.08.027.
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Acute optogenetic silencing of orexin/hypocretin neurons induces slow-wave sleep in mice.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。
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Optogenetics in neural systems.光遗传学在神经科学系统中的应用。
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5
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。
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Dichotomous cellular properties of mouse orexin/hypocretin neurons.鼠食欲素/下丘脑分泌素神经元的二分细胞特性。
J Physiol. 2011 Jun 1;589(Pt 11):2767-79. doi: 10.1113/jphysiol.2011.208637. Epub 2011 Apr 11.
7
Paradoxical function of orexin/hypocretin circuits in a mouse model of Huntington's disease.亨廷顿病小鼠模型中食欲素/下丘脑分泌素回路的矛盾功能。
Neurobiol Dis. 2011 Jun;42(3):438-45. doi: 10.1016/j.nbd.2011.02.006. Epub 2011 Feb 13.
8
Immunohistochemical evidence for synaptic release of glutamate from orexin terminals in the locus coeruleus.免疫组织化学证据表明,在蓝斑核中,食欲素末梢从突触中释放谷氨酸。
Neuroscience. 2010 Sep 1;169(3):1150-7. doi: 10.1016/j.neuroscience.2010.06.003. Epub 2010 Jun 9.
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Glutamatergic signaling by mesolimbic dopamine neurons in the nucleus accumbens.中脑边缘多巴胺神经元在伏隔核中的谷氨酸能信号传递。
J Neurosci. 2010 May 19;30(20):7105-10. doi: 10.1523/JNEUROSCI.0265-10.2010.
10
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。
J Neurosci. 2009 Sep 2;29(35):10939-49. doi: 10.1523/JNEUROSCI.1205-09.2009.

光遗传探测原位下丘脑泌素/食欲素神经元到组胺神经元的快速谷氨酸能传递。

Optogenetic probing of fast glutamatergic transmission from hypocretin/orexin to histamine neurons in situ.

机构信息

Department of Pharmacology, University of Cambridge, Cambridge CB2 1PD, United Kingdom.

出版信息

J Neurosci. 2012 Sep 5;32(36):12437-43. doi: 10.1523/JNEUROSCI.0706-12.2012.

DOI:10.1523/JNEUROSCI.0706-12.2012
PMID:22956835
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6621251/
Abstract

Hypothalamic hypocretin/orexin (hcrt/orx) neurons coordinate sleep-wake cycles, reward seeking, and body energy balance. Neurochemical data suggest that hcrt/orx cells contain several transmitters, but what hcrt/orx cells release onto their projection targets is unknown. A major pathway by which hcrt/orx neurons are thought to promote arousal is through projections to tuberomammillary histamine (HA) neurons. To study the impact of the electrical activity in hcrt/orx cells on HA neurons, we genetically targeted the light-activated excitatory ion channel channelrhodopsin-2 (ChR2) to the plasma membrane of hcrt/orx cells, and performed patch-clamp recordings from HA cells in acute mouse brain slices. Stimulation of ChR2-containing fibers with millisecond flashes of blue light produced fast postsynaptic currents in HA neurons, with a high connection probability (≈60% of HA cells were connected to ≈40% of hcrt/orx cells expressing ChR2). These inputs depended on tetrodotoxin-sensitive action potentials, had kinetics typical of glutamatergic responses mediated by AMPA receptors, were blocked by the AMPA receptor blocker CNQX, and displayed multiple forms of short-term plasticity (depression in ≈70% trials, facilitation in ≈30% trials, both often in the same cell). Furthermore, stimulation of hcrt/orx axons at physiological frequencies rapidly and reversibly increased action potential firing in HA cells, an effect that was abolished by blockade of AMPA receptors. These results provide the first functional evidence that hcrt/orx neurons are capable of fast glutamatergic control of their projection targets, and suggest that variations in electrical activity of hcrt/orx axons can induce rapid changes in long-range signals generated by HA neurons.

摘要

下丘脑食欲素/orexin (hcrt/orx) 神经元协调睡眠-觉醒周期、奖励寻求和身体能量平衡。神经化学数据表明,hcrt/orx 细胞包含几种递质,但 hcrt/orx 细胞释放到其投射靶标上的物质尚不清楚。人们认为,hcrt/orx 神经元促进觉醒的主要途径是通过投射到结节乳头体组胺 (HA) 神经元。为了研究 hcrt/orx 细胞电活动对 HA 神经元的影响,我们将光激活的兴奋性离子通道通道视紫红质-2 (ChR2) 基因靶向到 hcrt/orx 细胞的质膜,并在急性小鼠脑切片中从 HA 细胞进行膜片钳记录。用毫秒级蓝色光闪烁刺激含有 ChR2 的纤维在 HA 神经元中产生快速的突触后电流,具有高连接概率(≈60%的 HA 细胞与表达 ChR2 的 ≈40%的 hcrt/orx 细胞相连)。这些输入依赖于河豚毒素敏感的动作电位,具有由 AMPA 受体介导的谷氨酸能反应的典型动力学,被 AMPA 受体阻断剂 CNQX 阻断,并显示出多种形式的短期可塑性(约 70%的试验中出现抑制,约 30%的试验中出现易化,两者通常在同一细胞中)。此外,以生理频率刺激 hcrt/orx 轴突可快速且可逆地增加 HA 细胞中的动作电位放电,该效应被 AMPA 受体阻断所消除。这些结果提供了第一个功能证据,表明 hcrt/orx 神经元能够快速进行谷氨酸能控制其投射靶标,并表明 hcrt/orx 轴突电活动的变化可以诱导由 HA 神经元产生的长程信号的快速变化。