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首页> 外文期刊>Neuroscience Letters: An International Multidisciplinary Journal Devoted to the Rapid Publication of Basic Research in the Brain Sciences >Interactions between antiparkinsonian drugs and ABCB1/P-glycoprotein at the blood-brain barrier in a rat brain endothelial cell model.
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Interactions between antiparkinsonian drugs and ABCB1/P-glycoprotein at the blood-brain barrier in a rat brain endothelial cell model.

机译:在大鼠脑内皮细胞模型中,抗帕金森病药物与ABCB1 / P-糖蛋白在血脑屏障处的相互作用。

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摘要

Parkinson's disease is a neurodegenerative disorder that requires treatment by dopaminergic agonists, which may be responsible for central side effects. We hypothesized that the efflux transporter ABCB1/P-glycoprotein played a role in brain disposition of antiparkinsonian drugs and could control central toxicity. We aimed to evaluate antiparkinsonian drugs as ABCB1 substrates and/or inhibitors in rat brain endothelial cells GPNT, in order to predict potential clinical drug-drug interactions. Among the antiparkinsonian drugs tested, levodopa, bromocriptine, pergolide and pramipexole were ABCB1 substrates. However, only bromocriptine could inhibit ABCB1 functionality with an IC(50) of 6.71 microM on Rhodamine 123 uptake and an IC(50) of 1.71 microM on digoxine uptake. Thus, bromocriptine at 100 microM is responsible for an increase of levodopa intracellular transport of about 2.05-fold versus control. Therefore, we can conclude that bromocriptine is a potent drug for medicinal interactions in vitro. Hence, in patients with Parkinson's disease, these results may be considered to optimise treatments individually.
机译:帕金森氏病是一种神经退行性疾病,需要多巴胺能激动剂治疗,这可能是造成中枢副作用的原因。我们假设外排转运蛋白ABCB1 / P-糖蛋白在抗帕金森病药物的脑处置中起作用,并且可以控制中枢毒性。我们旨在评估抗帕金森病药物作为大鼠脑内皮细胞GPNT中的ABCB1底物和/或抑制剂,以预测潜在的临床药物相互作用。在测试的抗帕金森病药物中,左旋多巴,溴隐亭,培高利特和普拉克索是ABCB1底物。但是,只有溴隐亭可以抑制ABCB1功能,若丹明123摄取的IC(50)为6.71 microM,对地高辛的摄取的IC(50)为1.71 microM。因此,与对照相比,100 microM的溴隐亭负责左旋多巴的细胞内转运增加约2.05倍。因此,我们可以得出结论,溴隐亭是体外药物相互作用的有效药物。因此,在患有帕金森氏病的患者中,可以考虑这些结果以优化治疗方案。

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