首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Selective enhancement of synaptic inhibition by hypocretin (orexin) in rat vagal motor neurons: implications for autonomic regulation.
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Selective enhancement of synaptic inhibition by hypocretin (orexin) in rat vagal motor neurons: implications for autonomic regulation.

机译:在大鼠迷走神经运动神经元中由降钙素(orexin)选择性增强突触抑制:对自主调节的影响。

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摘要

The hypocretins (orexins) are hypothalamic neuropeptides implicated in feeding, arousal, and autonomic regulation. These studies were designed to determine the actions of hypocretin peptides on synaptic transmission in the dorsal motor nucleus of the vagus nerve (DMV). Whole-cell patch-clamp recordings were made from DMV neurons in transverse slices of rat brainstem. Some of the neurons were identified as gastric-related by retrograde labeling after inoculation of the stomach wall with pseudorabies virus 152, a viral label that reports enhanced green fluorescent protein. Consistent with previous findings, hypocretins caused an inward current (6-68 pA) in most neurons at holding potentials near rest. In addition, the frequency of spontaneous IPSCs was increased in a concentration-related manner (up to 477%), with little change in EPSCs. This effect was preserved in the presence of tetrodotoxin, suggesting a presynaptic site of action. Hypocretins increased the amplitude of IPSCs evoked by electrical stimulation of the nucleus tractus solitarius (NTS) but not evoked EPSCs. Hypocretin-induced increases in the frequency of IPSCs evoked by photoactivation of caged glutamate within the NTS were also observed. Identical effects of the peptides were observed in identified gastric-related and unlabeled DMV neurons. In contrast to some previous studies, which have reported primarily excitatory actions of the hypocretins in many regions of the CNS, these data support a role for hypocretin in preferentially enhancing synaptic inhibition, including inhibitory inputs arising from neurons in the NTS. These findings indicate that the hypocretins can modulate and coordinate visceral autonomic output by acting directly on central vagal circuits.
机译:降钙素(orexin)是下丘脑神经肽,与进食,唤醒和自主调节有关。这些研究旨在确定降钙素肽对迷走神经背运动核(DMV)突触传递的作用。全细胞膜片钳记录是从大鼠脑干横切面上的DMV神经元中获得的。伪狂犬病病毒152接种胃壁后,通过逆行标记将某些神经元识别为与胃相关的神经元,而伪狂犬病病毒152是一种病毒标记,报告绿色荧光蛋白增强。与以前的发现一致,降钙素在大多数神经元处于静息状态时会引起内向电流(6-68 pA)。此外,自发IPSC的频率以浓度相关的方式增加(最高477%),而EPSC几乎没有变化。在河豚毒素的存在下,这种作用得以保留,表明突触前的作用部位。降钙素增加电刺激孤束核(NTS)引起的IPSC的幅度,但不引起EPSC的幅度。还观察到由hypocretin诱导的NTS内笼状谷氨酸的光活化引起的IPSC频率增加。在已鉴定的胃相关和未标记的DMV神经元中观察到了肽的相同作用。与以前的一些研究相反,这些研究主要报道了降钙素在中枢神经系统许多区域的兴奋作用,这些数据支持降钙素在优先增强突触抑制中的作用,包括由NTS中神经元引起的抑制性输入。这些发现表明,降钙素可能通过直接作用于中央迷走神经回路来调节和协调内脏的自主神经输出。

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