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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Coupled effects of mass transfer and uptake kinetics on in vivo microdialysis of dopamine.
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Coupled effects of mass transfer and uptake kinetics on in vivo microdialysis of dopamine.

机译:传质和吸收动力学对多巴胺体内微透析的耦合作用。

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摘要

Voltammetric microelectrodes and microdialysis probes were used simultaneously to monitor extracellular dopamine in rat striatum during electrical stimulation of the medial forebrain bundle. Microelectrodes were placed far away (1 mm) from, immediately adjacent to, and at the outlet of microdialysis probes. In drug-naive rats, electrical stimulation (45 Hz, 25 s) evoked a robust response at microelectrodes far away from the probes, but there was no response at microelectrodes adjacent to and at the outlet of the probes. After nomifensine administration (20 mg/kg i.p.), stimulation evoked robust responses at all three microelectrode placements. These results demonstrate first that evoked release in tissue adjacent to microdialysis probes is suppressed in comparison with evoked release in tissue far away from the probes and second that equilibration of the dopamine concentration in the extracellular fluid adjacent to and far away from the probes is prevented by the high-affinity dopamine transporter. Hence, models of microdialysis, which assume the properties of tissue to be spatially uniform, require modification to account for the distance that separates viable sites of evoked dopamine release from the probe. We introduce new mass transfer resistance parameters that qualitatively explain the observed effects of uptake inhibition on stimulation responses recorded with microdialysis and voltammetry.
机译:伏安法微电极和微透析探针同时用于监测前脑内侧束电刺激过程中大鼠纹状体中的细胞外多巴胺。将微电极放置在距微透析探针较远的位置(1毫米),紧邻微透析探针的位置以及在微透析探针的出口处。在未经药物治疗的大鼠中,电刺激(45 Hz,25 s)在远离探针的微电极处引起强烈的反应,但在邻近探针出口处的微电极处没有反应。诺米非辛给药(腹膜内注射20 mg / kg)后,刺激在所有三个微电极位置均引起强烈反应。这些结果表明,与在远离探针的组织​​中诱发的释放相比,首先抑制了在微透析探针附近的组织中诱发的释放,其次,通过防止了在与探针相邻和远离的细胞外液中多巴胺浓度的平衡,可以防止这种情况的发生。高亲和力的多巴胺转运蛋白。因此,假设组织的特性在空间上是均匀的微透析模型,则需要进行修改以考虑将诱发的多巴胺释放的活位点与探针分开的距离。我们引入了新的传质阻力参数,定性地解释了摄取抑制对微量透析和伏安法记录的刺激反应的影响。

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