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首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >In vivo dopamine release and uptake impairments in rats treated with 3-nitropropionic acid.
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In vivo dopamine release and uptake impairments in rats treated with 3-nitropropionic acid.

机译:用3-硝基丙酸治疗的大鼠体内多巴胺释放和摄取障碍。

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Recent evidence has suggested that mitochondrial dysfunction may lead to impaired neurotransmitter exocytosis in transgenic Huntington's disease (HD) model mice. To gain insight into the impact of mitochondrial impairment on striatal dopamine release in vivo, we used fast-scan cyclic voltammetry (FSCV) at carbon fiber microelectrodes to measure dopamine release and uptake kinetics in anesthetized Lewis rats continuously treated for 5 days with 3-nitropropionic acid (3NP). Our results indicate that, even though striatal dopamine content was unchanged, remotely stimulated dopamine release evoked per electrical stimulus pulse ([DA](p)) is decreased in 3NP-treated rats (33% of that observed in sham control rats) and that this decrease is uniform throughout all stereotaxic depths tested. Nevertheless, unlike data collected previously from transgenic HD model rodents, the maximum rate of dopamine uptake (V(max)) in 3NP-treated rats is diminished (30% of controls) while K(m) is unchanged. Treatment with 3NP also resulted in a corresponding decrease in locomotor activity, presumably due in part to the impaired dopamine release. These results indicate that dopamine release is degraded in this HD model, as is observed in transgenic HD model rodents; however, the results also imply that there are fundamental differences in dopamine uptake between 3NP-treated animals and transgenic animals.
机译:最近的证据表明,线粒体功能障碍可能导致转基因亨廷顿舞蹈病(HD)模型小鼠的神经递质胞吐功能受损。为了深入了解线粒体损伤对体内纹状体多巴胺释放的影响,我们在碳纤维微电极上使用了快速扫描循环伏安法(FSCV)来测量麻醉的Lewis大鼠连续3天经3-硝基丙酸处理后的多巴胺释放和摄取动力学酸(3NP)。我们的结果表明,即使纹状体多巴胺含量不变,在3NP处理的大鼠中,每电刺激脉冲引起的远程刺激的多巴胺释放([DA](p))也会减少(占假对照大鼠的33%),并且在所有测试的立体定位深度中,这种减小是均匀的。然而,与先前从转基因HD模型啮齿动物中收集的数据不同,在3NP处理的大鼠中,多巴胺摄取的最大速率(V(max))有所降低(对照组的30%),而K(m)不变。用3NP进行治疗还导致运动活性相应降低,可能部分是由于多巴胺释放受损。这些结果表明,如在转基因HD模型啮齿动物中所观察到的,在该HD模型中多巴胺释放被降解。然而,该结果还暗示,经3NP处理的动物与转基因动物之间的多巴胺摄取存在根本差异。

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