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食欲素A通过对非选择性阳离子和钾离子电导的作用使孤束核神经元去极化。

Orexin-A depolarizes nucleus tractus solitarius neurons through effects on nonselective cationic and K+ conductances.

作者信息

Yang Bo, Ferguson Alastair V

机构信息

Department of Physiology, Queen's University, Kingston, Ontario K7L 3N6, Canada.

出版信息

J Neurophysiol. 2003 Apr;89(4):2167-75. doi: 10.1152/jn.01088.2002. Epub 2002 Dec 27.

Abstract

The nucleus tractus solitarius (NTS) plays central roles in a number of autonomic functions including cardiovascular control. Orexin (ORX)-A is a 33-amino-acid peptide implicated in the central regulation of energy metabolism, sleep, and the cardiovascular system. Studies demonstrate the presence of ORX-immunoreactive axons and both OX(1)R (orexin receptor) and OX(2)R mRNA within NTS. In this study, whole cell patch-clamp recordings were obtained from NTS neurons in rat medullary slices. Current-clamp studies showed that bath application of various concentrations of ORX-A depolarized 90.7% (78 of 86) of neurons tested while the remaining cells were either unaffected or showed small hyperpolarizations in response to peptide administration. Depolarizing effects were maintained in the presence of 5 microM TTX, and were concentration dependent. Using voltage-clamp techniques, we also identified modulatory actions of ORX-A on specific ion channels. Our results demonstrate that not only does ORX-A inhibit a specific potassium conductance (the sustained K(+) current) in NTS neurons, but it also activates a nonselective cationic conductance (NSCC). These data suggest that ORX-A effects on central cardiovascular control may result from direct actions on NTS neurons and also highlight the ability of this peptide to influence neuronal excitability as a consequence of concurrent modulation of multiple ion channels.

摘要

孤束核(NTS)在包括心血管控制在内的多种自主功能中发挥着核心作用。食欲素(ORX)-A是一种由33个氨基酸组成的肽,参与能量代谢、睡眠和心血管系统的中枢调节。研究表明,在孤束核内存在ORX免疫反应性轴突以及OX(1)R(食欲素受体)和OX(2)R mRNA。在本研究中,从大鼠延髓切片中的孤束核神经元获得了全细胞膜片钳记录。电流钳研究表明,浴槽中应用不同浓度的ORX-A使90.7%(86个中的78个)受试神经元去极化,而其余细胞对肽给药无反应或表现出小的超极化。在存在5 microM河豚毒素(TTX)的情况下,去极化作用得以维持,且呈浓度依赖性。使用电压钳技术,我们还确定了ORX-A对特定离子通道的调节作用。我们的结果表明,ORX-A不仅抑制孤束核神经元中的一种特定钾电导(持续钾电流),还激活一种非选择性阳离子电导(NSCC)。这些数据表明,ORX-A对中枢心血管控制的影响可能源于对孤束核神经元的直接作用,也突出了这种肽由于同时调节多个离子通道而影响神经元兴奋性的能力。

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