mptp诱导的行为和生化缺陷:参数分析。

A Fredriksson, T Archer
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引用次数: 82

摘要

两项实验研究了长期给药神经毒素1-甲基-4-苯基-1,2,3,6-四氢吡啶(MPTP)作为小鼠帕金森病功能模型的参数效应。不同剂量的MPTP(5、10、20、30或40 mg/kg, s.c,每次注射两次)在3周或3个月的治疗-测试间隔中引起的行为缺陷,可以通过自发运动活动的显著减少来证明,从10 mg/kg剂量在3周间隔中增加,从30-40 mg/kg在3个月间隔中增加。在这些剂量水平和间隔下,小鼠纹状体中多巴胺(DA)显著减少。40 mg/kg剂量(注射两次)的行为缺陷,并在3周、6周、12周、24周和40周的间隔(单独和重复试验组)进行测试,表明运动活动、运动、饲养和总活动的所有三个参数都有明显的相对可比较的减少。在所有五个测试间隔中,DA消耗都很严重。这些结果为MPTP治疗对小鼠黑质纹状体运动系统产生永久性损伤提供了功能和神经化学证据。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
MPTP-induced behavioural and biochemical deficits: a parametric analysis.

Two experiments were performed to study the parametric effects of long-term administration of the neurotoxin, 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP), as a functional model of parkinsonism in mice. The behavioural deficits induced by different doses of MPTP (5, 10, 20, 30 or 40 mg/kg, s.c., each injected on two occasions) at a 3-week or a 3-month treatment-testing interval were evidenced by significant reductions of spontaneous motor activity, from the 10 mg/kg dosages upwards at the 3-week interval and from 30-40 mg/kg at the 3-month interval. Significant dopamine (DA) reductions in the mouse striatum were obtained at these dose levels and intervals. The behavioural deficit of the 40 mg/kg dose (injected on two occasions) and tested at the 3-, 6-, 12-, 24- and 40-week intervals (separate as well as repeated testing groups) indicated marked and relatively comparable reductions of all three parameters of motor activity, locomotion, rearing and total activity. DA depletions were severe at all five test intervals. These results offer functional and neurochemical evidence that MPTP treatment produces permanent damage to the nigrostriatal motor system in mice.

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