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首页> 外文期刊>Life sciences >Significance of glutamate and dopamine neurons in the ventral pallidum in the expression of behavioral sensitization to amphetamine.
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Significance of glutamate and dopamine neurons in the ventral pallidum in the expression of behavioral sensitization to amphetamine.

机译:腹侧苍白质中谷氨酸和多巴胺神经元在苯丙胺行为敏化的表达中的意义。

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To explore the significance of ventral pallidum (VP) during the amphetamine sensitization, we first investigated if there are neurochemical alterations in the VP during amphetamine withdrawal period. Chronic amphetamine-treated (5 mg/kg x 14 days) rats displayed an apparent locomotion sensitization as compared with saline controls when challenged with 2 mg/kg amphetamine at withdrawal days 10-14. A microdialysis analysis revealed that output of the dopamine metabolites, 3,4-dihydroxyphenylacetic acid and homovanillic acid, in the VP of amphetamine-sensitized rats increased approximately two-fold as compared to controls at both pre- and post-amphetamine challenge period. On the other hand, the in vivo glutamate output in the VP increased upon amphetamine challenge in the behaviorally sensitized rats, but not in the controls. To evaluate if drug manipulation in the VP would affect the behavioral sensitization, we treated both groups of rats with NMDA receptor antagonist, MK-801 (5 microg/microl for 5 days; bilateral) in the VP during withdrawal days 6-10. Animals were challenged with 2 mg/kg amphetamine at withdrawal day 11. The behavioral profile exhibited that MK-801 pre-treatment significantly blocked the locomotion hyperactivity in amphetamine-sensitized rats. Taken together, the current results suggest that the excitatory amino acid in the VP plays a significant role during the expression of behavioral sensitization to amphetamine.
机译:为了探讨苯丙胺致敏过程中腹侧苍白球(VP)的重要性,我们首先调查了苯丙胺戒断期间VP中是否存在神经化学改变。当在停药第10-14天用2 mg / kg苯丙胺攻击时,与盐对照相比,慢性苯丙胺治疗(5 mg / kg x 14天)的大鼠表现出明显的运动致敏性。微量透析分析显示,在苯丙胺激发前和后苯丙胺激发阶段,安非他明致敏大鼠的VP中多巴胺代谢产物3,4-二羟基苯基乙酸和高香草酸的输出量比对照组增加了约两倍。另一方面,在苯丙胺激发后,行为敏化大鼠的VP中体内谷氨酸输出增加,而对照中则没有。为了评估VP中的药物操作是否会影响行为敏感性,我们在停药期6-10天用NMDA的NMDA受体拮抗剂MK-801(5微克/微升,持续5天;双侧)对两组大鼠进行了治疗。在停药第11天,用2 mg / kg的苯丙胺对动物进行攻击。行为特征表明,MK-801预处理可显着阻断苯丙胺致敏大鼠的运动过度活跃。综上所述,目前的结果表明,VP中的兴奋性氨基酸在对苯丙胺的行为敏化的表达中起重要作用。

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