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P-glycoprotein interactions of novel psychoactive substances - Stimulation of ATP consumption and transport across Caco-2 monolayers

机译:新型精神活性物质的P-糖蛋白相互作用-刺激ATP消耗和跨Caco-2单层运输

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摘要

In contrast to drugs for therapeutic use, there are only few data available concerning interactions between P-glycoprotein (P-gp) and drugs of abuse (DOA). In this work, interactions between structurally diverse DOA and P-gp were investigated using different strategies. First, the effect on the P-gp ATPase activity was studied by monitoring of ATP consumption after addition to recombinant, human P-gp. Second, DOA showing an increased ATP consumption were further characterized regarding their transport across filter grown Caco-2- monolayers. Analyses were performed by luminescence and liquid chromatography-mass spectrometry, respectively. Among the nine DOA initially screened, benzedrone, diclofensine, glaucine, JWH-200, MDBC, WIN-55,212-2 showed an increase of ATP consumption in the ATPase stimulation assay. In Caco-2 transport studies, Glaucine, JWH-200, mitragynine, WIN-55,212-2 could moreover be identified as non-transported substrates, but inhibitors of P-gp activity. Thus, drug-drug or drug-food interactions should be very likely for these compounds. (C) 2015 Elsevier Inc. All rights reserved.
机译:与用于治疗的药物相比,仅有很少的关于P-糖蛋白(P-gp)与滥用药物(DOA)之间相互作用的数据。在这项工作中,使用不同的策略研究了结构多样的DOA和P-gp之间的相互作用。首先,通过监测重组人P-gp加入后的ATP消耗来研究对P-gp ATPase活性的影响。第二,DOA表现出增加的ATP消耗,通过其在过滤器中生长的Caco-2-单层的转运得以进一步表征。分别通过发光和液相色谱-质谱法进行分析。在最初筛选的九种DOA中,苯甲酮,双氯芬新,青光油,JWH-200,MDBC,WIN-55,212-2在ATPase刺激试验中显示ATP消耗增加。在Caco-2转运研究中,还可将Glaucine,JWH-200,mitragynine,WIN-55,212-2鉴定为非转运底物,但可抑制P-gp活性。因此,对于这些化合物,药物-药物或药物-食物的相互作用应该是非常可能的。 (C)2015 Elsevier Inc.保留所有权利。

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