首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Evidence on extracellular dopamine level in rat striatum: implications for the validity of quantitative microdialysis.
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Evidence on extracellular dopamine level in rat striatum: implications for the validity of quantitative microdialysis.

机译:大鼠纹状体细胞外多巴胺水平的证据:对定量微量透析有效性的影响。

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摘要

Abstract Microdialysis zero-net-flux (ZNF) method is commonly used to monitor drug-induced changes in neurotransmitter baseline and release/uptake processes. Recent studies in this field suggest that microdialysis ZNF method seriously underestimates the resting concentration of extracellular dopamine in the rat neostriatum because probe implantation preferentially damages nearby dopamine release sites and that dopamine uptake inhibition increases the relative recovery of dopamine by microdialysis. This study assessed the validity of these claims by examining current data on extracellular dopamine levels at rest and after drug application obtained by voltammetry, a technique thought to induce less tissue disruption than microdialysis. To obtain the extracellular baseline value for dopamine from the evoked overflow data, we modified the existing dopamine kinetic model to suit both the resting and stimulated circumstances. It was found that dopamine uptake inhibition did in fact decrease the microdialysisrelative recovery of dopamine, implying that the average basal extracellular dopamine level is within the range of 7-20 nm in rat striatum. This study concludes that the microdialysis ZNF method indeed underestimates the extracellular dopamine concentration, although not by as much as had been thought. Chronic microdialysis damages both neurotransmitter release and uptake, but it does so in a somewhat relative and proportional way for both processes. Thus the validity of the microdialysis ZNF method is not seriously undermined.
机译:摘要微透析零净通量(ZNF)方法通常用于监测药物引起的神经递质基线和释放/摄取过程的变化。该领域的最新研究表明,微透析ZNF方法严重低估了大鼠新纹状体中细胞外多巴胺的静息浓度,因为探针植入会优先损害附近的多巴胺释放部位,并且多巴胺摄取抑制作用会通过微透析增加多巴胺的相对恢复。这项研究通过检查有关静息时和伏安法应用药物后细胞外多巴胺水平的最新数据,评估了这些主张的有效性,该技术被认为比微透析引起的组织破坏更少。为了从诱发的溢出数据中获得多巴胺的细胞外基线值,我们修改了现有的多巴胺动力学模型,以适应静止和刺激的情况。发现多巴胺的摄取抑制实际上确实降低了微透析相对于多巴胺的恢复,这暗示大鼠纹状体中平均基础细胞外多巴胺水平在7-20nm的范围内。这项研究得出的结论是,微透析ZNF方法确实低估了细胞外多巴胺的浓度,尽管没有想象的那么高。慢性微透析会损害神经递质的释放和摄取,但在这两个过程中都以相对和成比例的方式发生。因此,不会严重损害微透析ZNF方法的有效性。

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