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首页> 外文期刊>Neuroscience Research: The Official Journal of the Japan Neuroscience Society >The NR2B antagonist, ifenprodil, corrects the L-DOPA-induced deficit of bilateral movement and reduces c-Fos expression in the subthalamic nucleus of hemiparkinsonian rats
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The NR2B antagonist, ifenprodil, corrects the L-DOPA-induced deficit of bilateral movement and reduces c-Fos expression in the subthalamic nucleus of hemiparkinsonian rats

机译:NR2B拮抗剂ifenprodil可纠正L-DOPA引起的半运动性帕金森病大鼠的丘脑下核中的双侧运动缺陷并降低c-Fos表达

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The use of NR2B antagonists in Parkinsonism is still controversial. To examine their anti-parkinsonian effects, the NR2B antagonist, ifenprodil, and L-DOPA were administered together and separately in hemi-parkinsonian rats (hemi-PD) that were subjected to a cylinder test. Recovery from hypoactivity was achieved by single administration of 3-7 mg/kg of L-DOPA; however, improvement in the deficit of bilateral forelimb use was not observed. When administered alone, ifenprodil had no anti-parkinsonian effects; however, combined administration of ifenprodil and 7 mg/kg of L-DOPA significantly reversed the deficit of bilateral forelimb use without adversely affecting the L-DOPA-induced improvement in motor activity. Next, in order to identify the brain area influenced by L-DOPA and ifenprodil, quantitative analysis of L-DOPA-induced c-Fos immunoreactivity was performed in various brain areas of hemi-PD following administration of L-DOPA with and without ifenprodil. Among brain areas with robust c-Fos expression within the motor loop circuit in dopamine-depleted hemispheres, co-administered ifenprodil markedly attenuated L-DOPA-induced c-Fos expression in only the subthalamic nucleus (STN), suggesting that the STN is the primary target for the anti-parkinsonian action of NR2B antagonists. (C) 2015 Elsevier Ireland Ltd and the Japan Neuroscience Society. All rights reserved.
机译:NR2B拮抗剂在帕金森病中的使用仍存在争议。为了检查它们的抗帕金森病作用,将NR2B拮抗剂,艾芬地尔和L-DOPA分别和半定量的半帕金森病大鼠(hemi-PD)进行了气缸测试。通过单次给药3-7 mg / kg的L-DOPA可以从机能减退中恢复过来;然而,没有观察到双侧前肢使用不足的改善。单独给药时,艾芬洛地尔无抗帕金森病作用;然而,将艾芬洛地尔和7 mg / kg的L-DOPA联合使用可显着逆转双侧前肢使用的不足,而不会不利地影响L-DOPA引起的运动活动改善。接下来,为了鉴定受L-DOPA和艾芬地尔影响的脑区域,在给予和不给予艾芬地尔的情况下,在给予L-DOPA后,在半PD的各个脑区域中进行L-DOPA诱导的c-Fos免疫反应性的定量分析。在多巴胺贫乏的半球的运动回路中具有强健c-Fos表达的大脑区域中,共同使用ifenprodil仅在丘脑下丘脑核(STN)中显着减弱L-DOPA诱导的c-Fos表达,这表明STN是NR2B拮抗剂的抗帕金森病作用的主要靶标。 (C)2015 Elsevier Ireland Ltd和日本神经科学学会。版权所有。

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