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Evaluation of Drug Concentrations Delivered by Microiontophoresis

机译:通过微离子电渗疗法评估药物浓度

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Microiontophoresis uses an electric current to eject a drug solution from a glass capillary and is often utilized for targeted delivery in neurochemical investigations. The amount of drug ejected, and its effective concentration at the tip, has historically been difficult to determine, which has precluded its use in quantitative studies. To address this, a method called controlled iontophoresis was developed which employs a carbon-fiber microelectrode incorporated into a multibarreled iontophoretic probe to detect the ejection of electroactive species. Here, we evaluate the accuracy of this method. To do this, we eject different concentrations of quinpirole, a D2 receptor agonist, into a brain slice containing the dorsal striatum, a brain region with a high density of dopamine terminals. Local electrical stimulation was used to evoke dopamine release, and inhibitory actions of quinpirole on this release were examined. The amount of drug ejected was estimated by detection of a coejected electrochemical marker. Dose response curves generated in this manner were compared to curves generated by conventional perfusion of quinpirole through the slice. We find several experimental conditions must be optimized for accurate results. First, selection of a marker with an identical charge was necessary to mimic the ejection of the cationic agonist. Next, evoked responses were more precise following longer periods between the end of the ejection and stimulation. Lastly, the accuracy of concentration evaluations was improved by longer ejections. Incorporation of these factors into existing protocols allows for greater certainty of concentrations delivered by controlled iontophoresis.
机译:微离子电渗疗法使用电流从玻璃毛细管中喷出药物溶液,并经常用于神经化学研究中的靶向递送。历史上很难确定药物的喷射量及其尖端的有效浓度,这使其无法用于定量研究。为了解决这个问题,开发了一种称为受控离子电渗疗法的方法,该方法采用了将碳纤维微电极结合到多管离子电渗疗法探头中以检测电活性物质喷射的方法。在这里,我们评估这种方法的准确性。为此,我们将不同浓度的喹吡罗(一种D2受体激动剂)喷射到含有背侧纹状体的大脑切片中,该纹状体是具有高密度多巴胺末端的大脑区域。使用局部电刺激引起多巴胺释放,并研究了喹吡罗对这种释放的抑制作用。通过检测共同喷射的电化学标记物来估计喷射的药物量。将以这种方式产生的剂量反应曲线与通过切片常规灌注喹吡罗产生的曲线进行比较。我们发现必须优化几个实验条件才能获得准确的结果。首先,必须选择具有相同电荷的标记来模拟阳离子激动剂的喷射。接下来,在射血和刺激结束之间的较长时间后,诱发的反应更加精确。最后,更长的喷射时间提高了浓度评估的准确性。将这些因素整合到现有方案中,可以更确定地控制离子电渗疗法传递的浓度。

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