首页> 美国卫生研究院文献>The Journal of Neuroscience >Regulation of Synaptic Efficacy in Hypocretin/Orexin-Containing Neurons by Melanin Concentrating Hormone in the Lateral Hypothalamus
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Regulation of Synaptic Efficacy in Hypocretin/Orexin-Containing Neurons by Melanin Concentrating Hormone in the Lateral Hypothalamus

机译:黑色素浓缩激素在下丘脑外侧对降钙素/含有毒素的神经元的突触功效的调节

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摘要

The lateral hypothalamus (LH) is a central hub that integrates inputs from, and sends outputs to, many other brain areas. Two groups of neurons in the LH, expressing hypocretin/orexin or melanin concentrating hormone (MCH), have been shown to participate in sleep regulation, energy homeostasis, drug addiction, motor regulation, stress response, and social behaviors. The elucidation of crosstalk between these two systems is essential to understand these behaviors and functions because there is evidence that there are reciprocal innervations between hypocretin/orexin and MCH neurons. In this study, we used MCH receptor-1 knock-out (MCHR1 KO) and wild-type (WT) mice expressing green fluorescent protein in hypocretin/orexin-containing neurons to examine the hypothesis that MCH modulates hypocretin/orexin-mediated effects on behavioral state and synaptic transmission in the LH. In MCHR1 KO mice, the efficacy of glutamatergic synapses on hypocretin/orexin neurons is potentiated and hypocretin-1-induced action potential firing is facilitated, potentially explaining an increased effect of modafinil observed in MCHR1 KO mice. In wild-type mice with intact MCHR1 signaling, MCH significantly attenuated the hypocretin-1-induced enhancement of spike frequency in hypocretin/orexin neurons. The MCH effect was dose dependent, pertussis toxin sensitive, and was abolished in MCHR1 KO mice. Consistent with this effect, MCH attenuated hypocretin-1-induced enhancement of the frequency of miniature EPSCs in hypocretin/orexin neurons. These data from MCHR1 KO and WT mice demonstrate a novel interaction between these two systems, implying that MCH may exert a unique inhibitory influence on hypocretin/orexin signaling as a way to fine-tune the output of the LH.
机译:下丘脑外侧(LH)是一个中央枢纽,可整合来自其他许多大脑区域的输入并将输出发送到许多其他大脑区域。 LH中的两组神经元表达降钙素/ orexin或黑色素浓缩激素(MCH),已被证明参与睡眠调节,能量稳态,药物成瘾,运动调节,压力反应和社交行为。阐明这两个系统之间的串扰对于理解这些行为和功能至关重要,因为有证据表明,降钙素/尿素与MCH神经元之间存在相互的神经支配。在这项研究中,我们使用了MCH受体1敲除(MCHR1 KO)和野生型(WT)小鼠在含有降钙素/尿毒蛋白的神经元中表达绿色荧光蛋白的方法,以检验MCH调节降钙素/尿素介导的对HCH的影响的假设。 LH中的行为状态和突触传递。在MCHR1 KO小鼠中,增强了谷氨酸能突触对降钙素/ orexin神经元的功效,并促进了hypocretin-1诱导的动作电位放电,这可能解释了莫达非尼在MCHR1 KO小鼠中观察到的作用增加。在具有完整MCHR1信号传导的野生型小鼠中,MCH显着减弱了hypocretin-1诱导的hypocretin / orexin神经元的突波频率增强。 MCH作用是剂量依赖性的,对百日咳毒素敏感,并且在MCHR1 KO小鼠中被取消。与此效果一致,MCH减弱了降钙素1 /诱导的神经元中微型EPSC诱导的微型EPSC频率的增加。来自MCHR1 KO和WT小鼠的这些数据证明了这两个系统之间的新型相互作用,这暗示MCH可能会对降钙素/尿素信号传导产生独特的抑制作用,从而微调LH的输出。

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