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大鼠脑桥内侧网状核神经元体外兴奋性氨基酸介导的反应和突触电位

Excitatory amino acid-mediated responses and synaptic potentials in medial pontine reticular formation neurons of the rat in vitro.

作者信息

Stevens D R, McCarley R W, Greene R W

机构信息

Harvard Medical School, Massachusetts.

出版信息

J Neurosci. 1992 Nov;12(11):4188-94. doi: 10.1523/JNEUROSCI.12-11-04188.1992.

DOI:10.1523/JNEUROSCI.12-11-04188.1992
PMID:1279137
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6575987/
Abstract

Neurons of the medial pontine reticular formation (mPRF) are involved in the execution of numerous behaviors including initiation of locomotion, eye movements, startle responses, and rapid eye movement sleep phenomena. Approximately half of the afferent projections to mPRF neurons come from within the reticular formation (Shammah-Lagnado et al., 1987). In spite of the importance of reticulo-reticular connections, virtually nothing is known about transmitters mediating these synapses. In order to identify a candidate excitatory neurotransmitter, the actions of excitatory amino acids (EAAs) on the membrane properties of mPRF neurons recorded in rat brainstem slices in vitro were studied. Standard intracellular recording methods, including single-electrode voltage clamp, were used to examine the postsynaptic actions of EAAs. We also tested whether EAA antagonists block EPSPs evoked by stimulation of the contralateral reticular formation in the slices. mPRF neurons responded to both non-NMDA and NMDA agonists. NMDA-induced conductances were voltage dependent and depressed by physiological concentrations of magnesium. Stimulation of the contralateral reticular formation elicited EPSPs that were depressed by the general EAA antagonist kynurenate. Evoked EPSPs were partially depressed by 6,7-dinitroquinoxaline-2,3-dione. The evoked EPSP was further reduced by the NMDA antagonist (+/-)-2-amino-5-phosphonopentanoic acid in some cases. These results suggest that excitatory reticulo-reticular neurotransmission is mediated by an EAA. Both non-NMDA and NMDA receptors contribute to EAA neurotransmission in the mPRF formation and play an integral role in reticular formation function.

摘要

脑桥内侧网状结构(mPRF)的神经元参与多种行为的执行,包括运动的启动、眼球运动、惊吓反应和快速眼动睡眠现象。投射到mPRF神经元的传入纤维约有一半来自网状结构内部(Shammah-Lagnado等人,1987年)。尽管网状-网状连接很重要,但对于介导这些突触的神经递质却几乎一无所知。为了确定一种候选兴奋性神经递质,研究了兴奋性氨基酸(EAA)对体外大鼠脑干切片中记录的mPRF神经元膜特性的作用。使用包括单电极电压钳在内的标准细胞内记录方法来检测EAA的突触后作用。我们还测试了EAA拮抗剂是否能阻断切片中对侧网状结构刺激所诱发的兴奋性突触后电位(EPSP)。mPRF神经元对非NMDA和NMDA激动剂均有反应。NMDA诱导的电导具有电压依赖性,并被生理浓度的镁所抑制。刺激对侧网状结构可诱发EPSP,该EPSP被EAA通用拮抗剂犬尿烯酸所抑制。诱发的EPSP被6,7-二硝基喹喔啉-2,3-二酮部分抑制。在某些情况下,NMDA拮抗剂(±)-2-氨基-5-磷酸戊酸可进一步降低诱发的EPSP。这些结果表明,兴奋性网状-网状神经传递是由EAA介导的。非NMDA和NMDA受体均参与mPRF结构中的EAA神经传递,并在网状结构功能中发挥不可或缺的作用。

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