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孤束核中突触传递所固有的兴奋性氨基酸受体。

Excitatory amino acid receptors intrinsic to synaptic transmission in nucleus tractus solitarii.

作者信息

Miller B D, Felder R B

机构信息

Department of Internal Medicine, College of Medicine, University of Iowa, Iowa City 52242.

出版信息

Brain Res. 1988 Jul 26;456(2):333-43. doi: 10.1016/0006-8993(88)90236-3.

Abstract

Excitatory amino acid (EAA) receptors are present in the nucleus tractus solitarii (NTS), and there is growing evidence that L-glutamate (L-Glu) may activate neurons in this region to precipitate changes in autonomic discharge. To evaluate the potential role of EAA agonists in synaptic transmission in NTS, we studied the responses of single units in an in vitro brain slice preparation of NTS to electrical stimulation of one or both solitary tracts (TS) before, during and after superfusion with selected EAA antagonists. Dose-response studies demonstrated that the synaptic input to NTS units was substantially blocked by 2-amino-5-phosphonovaleric acid (APV) at perfusion concentrations of 1 mM, by kynurenic acid (KYN) at 10 mM, and glutamate diethylester (GDEE) at 10 mM. Using these concentrations, we examined the responses of single NTS neurons to afferent input from ipsilateral and contralateral TS stimulation before, during and after perfusion with each antagonist. KYN inhibited afferent input from one TS but not the other in 7 of 13 cells tested, inhibited both inputs in 4, and caused differential augmentation of input in two. APV caused differential inhibition of the two inputs in 4 of 9 cells tested, differential excitation in 1 and inhibition of both inputs in one. GDEE caused differential inhibition in 4 of 9 cells tested, differential excitation in 3 and inhibition of both inputs in one. When inputs from a single TS were examined, those blocked by APV were always blocked by KYN (5 of 16 inputs tested); there was overlap between the blocking effects of KYN and GDEE (4 of 12 inputs tested) and occasionally of APV and GDEE (one of 12 inputs tested). We also observed differential blocking effects of these agents on single inputs to the same neuron. Evoked responses were reduced or enhanced by only one of the two agents for 5 of 16 inputs tested with KYN and APV, 4 of 12 tested with KYN and GDEE, and 7 of 12 tested with APV and GDEE. The average reduction in synaptically evoked responses caused by blocking doses of antagonist was 85 +/- 6% for KYN, 63 +/- 28% for APV and 68 +/- 10% for GDEE. These data indicate that all 3 major EAA antagonists can selectively inhibit electrically evoked afferent input to NTS neurons and suggest a role for specific EAA receptors in mediating input to these neurons over different afferent pathways.

摘要

兴奋性氨基酸(EAA)受体存在于孤束核(NTS)中,越来越多的证据表明L-谷氨酸(L-Glu)可能激活该区域的神经元,从而引起自主神经放电的变化。为了评估EAA激动剂在NTS突触传递中的潜在作用,我们在体外NTS脑片制备中,研究了单个神经元在灌注选定的EAA拮抗剂之前、期间和之后对单侧或双侧孤束(TS)电刺激的反应。剂量反应研究表明,在灌注浓度为1 mM时,2-氨基-5-磷酸戊酸(APV)、10 mM时的犬尿氨酸(KYN)和10 mM时的谷氨酸二乙酯(GDEE)可显著阻断NTS神经元的突触输入。使用这些浓度,我们在灌注每种拮抗剂之前、期间和之后,检查了单个NTS神经元对同侧和对侧TS刺激传入输入的反应。在13个测试细胞中,KYN抑制了来自一侧TS的传入输入,但未抑制另一侧,在4个细胞中抑制了两侧的输入,在2个细胞中引起了输入的差异增强。在9个测试细胞中,APV对两个输入产生差异抑制的有4个,差异兴奋的有1个,抑制两侧输入的有1个。在9个测试细胞中,GDEE引起差异抑制的有4个,差异兴奋的有3个,抑制两侧输入的有1个。当检查来自单个TS的输入时,被APV阻断的输入总是被KYN阻断(16个测试输入中有5个);KYN和GDEE的阻断作用存在重叠(12个测试输入中有4个),APV和GDEE偶尔也有重叠(12个测试输入中有1个)。我们还观察到这些药物对同一神经元的单个输入有不同的阻断作用。在用KYN和APV测试的16个输入中,有5个、用KYN和GDEE测试的12个输入中有4个、用APV和GDEE测试的12个输入中有7个,仅两种药物中的一种使诱发反应降低或增强。阻断剂量的拮抗剂引起的突触诱发反应平均降低幅度,KYN为85±6%,APV为63±28%,GDEE为68±10%。这些数据表明,所有3种主要的EAA拮抗剂均可选择性抑制电诱发的NTS神经元传入输入,并提示特定的EAA受体在介导不同传入通路对这些神经元的输入中发挥作用。

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