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Monoamine transporters and psychostimulant drugs.

机译:单胺转运蛋白和精神刺激药。

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摘要

Most psychostimulants interact with monoamine transport proteins. This paper reviews work our laboratory has conducted to investigate the interaction of psychostimulants with monoamine transporters in order to advance our understanding of how these drugs affect the brain. We review two topics: (1) characterization of multiple binding sites for cocaine-like drugs and (2) an examination of the mechanisms of action of amphetamine-type anorectic agents. We conclude that the brain contains high abundance nonclassical binding sites for cocaine-like drugs that have micromolar affinity for cocaine and that none of the clinically available amphetamine-type appetite suppressants are equipotent substrates for dopamine transporter (DAT) and serotonin transporter (SERT) proteins. Future medications discovery efforts should focus on identifying new compounds which possess the equipotent substrate activity at DAT and SERT, but which lack the adverse effects of stimulants developed decades ago.
机译:大多数精神兴奋剂与单胺转运蛋白相互作用。本文回顾了我们实验室为研究精神刺激剂与单胺转运蛋白之间的相互作用所做的工作,以增进我们对这些药物如何影响大脑的理解。我们审查了两个主题:(1)可卡因样药物的多个结合位点的表征,以及(2)苯丙胺类厌食药作用机制的检查。我们得出的结论是,大脑对可卡因样药物具有很高的非经典结合位点,这些药物对可卡因具有微摩尔的亲和力,而且临床上可用的苯丙胺类食欲抑制剂均不是多巴胺转运蛋白(DAT)和5-羟色胺转运蛋白(SERT)蛋白的等价底物。未来的药物发现工作应着重于鉴定在DAT和SERT上具有相同底物活性但缺乏数十年前开发的兴奋剂的不利影响的新化合物。

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