多巴胺-去神经纹状体的体内电生理:聚焦于一氧化氮/cGMP信号通路。

Salvatore Galati, Vincenza D'angelo, Eugenio Scarnati, Paolo Stanzione, Alessandro Martorana, Teresa Procopio, Giuseppe Sancesario, Alessandro Stefani
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引用次数: 31

摘要

在纹状体内,气态神经递质一氧化氮(NO)是由一类含有神经元NO合成酶(nNOS)的中间神经元产生的。NO通过激活可溶性鸟苷环化酶(sGC)促进第二信使cGMP,并在谷氨酸(GLU)和DA传递的整合中发挥关键作用。本研究旨在探讨大鼠黑质纹状体通路6-羟基da (6-OHDA)损伤对NO/cGMP系统的影响。体内细胞外单单位记录是在氨基甲酸乙酯麻醉下进行的,以避免任何潜在的误导性贡献,即皮质驱动的内源性NO变化。因此,我们没有进行纹状体外电刺激,并非常关注离子电泳给药3- morpholinosydnon亚胺(sin1, no供体)、N(G)-硝基- l -精氨酸甲酯(L-NAME,非选择性NOS抑制剂)和Zaprinast (PDE抑制剂)对纹状体主要表型的影响。后者在操作上区分为沉默的中棘样神经元(MSN),其自发活动可忽略不计,但在休息时显示谷氨酸诱导的放电,以及自发活动的神经元(SAN),在很大程度上代表非突出的中间神经元。san被SIN-1和Zaprinast激发,而msn在局部离子吸附应用中表现出明显的抑制作用。在6-OHDA动物中,sin -1诱导的SANs兴奋明显增加(相反,L-NAME的抑制作用较弱)。有趣的是,在da失神经的动物中,msn的一个亚类(40%)对SIN-1表现出特殊的兴奋性反应。这些发现支持内源性NO对控制纹状体投射细胞的抑制调节作用的概念。此外,这些发现表明NO、自发活动的中间神经元和投射神经元之间的功能串扰在帕金森状态下变得至关重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
In vivo electrophysiology of dopamine-denervated striatum: focus on the nitric oxide/cGMP signaling pathway.

Within the striatum, the gaseous neurotransmitter nitric oxide (NO) is produced by a subclass of interneurons containing the neuronal NO synthase (nNOS). NO promotes the second messenger cGMP through the activation of the soluble guanyl cyclase (sGC) and plays a crucial role in the integration of glutamate (GLU) and DA transmission. The aim of this study was to characterize the impact of 6-hydroxyDA (6-OHDA) lesion of the rat nigrostriatal pathway on NO/cGMP system. In vivo extracellular single units recordings were performed under urethane anesthesia to avoid any potentially misleading contributions of cortically-driven changes on endogenous NO. Hence, no electrical extrastriatal stimulation was performed and great attention was paid to the effects of 3-morpholinosydnonimine (SIN-1, a NO donor), N(G)-nitro-L-arginine methyl ester (L-NAME, a nonselective NOS inhibitor) and Zaprinast (a PDE inhibitor) delivered by iontophoresis upon the main striatal phenotypes. The latter were operationally distinguished in silent medium spiny-like neurons (MSN), with negligible spontaneous activity but displaying glutamate-induced firing discharge at rest and spontaneously active neurons (SAN), representing to a large extent nonprojecting interneurons. SANs were excited by SIN-1 and Zaprinast while MSNs showed a clear inhibition during local iontophoretic application of SIN-1 and Zaprinast. In 6-OHDA animals, SIN-1-induced excitation in SANs was significantly increased (on the contrary, the inhibitory effect of L-NAME was less effective). Interestingly, in DA-denervated animals, a subclass of MSNs (40%) displayed a peculiar excitatory response to SIN-1. These findings support the notion of an inhibitory modulatory role exerted by endogenous NO on control striatal projection cells. In addition, these findings suggest a functional cross-talk between NO, spontaneously active interneurons, and projection neurons that becomes critical in the parkinsonian state.

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