Negus S Stevens, Banks Matthew L
Department of Pharmacology and Toxicology, Virginia Commonwealth University, Richmond, VA, USA.
Curr Top Behav Neurosci. 2017;32:119-131. doi: 10.1007/7854_2016_18.
Many cathinone analogs act as substrates or inhibitors at dopamine, norepinephrine, and serotonin transporters (DAT, NET, SERT, respectively). Drug selectivity at DAT vs. SERT is a key determinant of abuse potential for monoamine transporter substrates and inhibitors, such that potency at DAT > SERT is associated with high abuse potential, whereas potency at DAT < SERT is associated with low abuse potential. Quantitative structure-activity relationship (QSAR) studies with a series of 4-substituted methcathinone analogs identified volume of the 4-position substituent on the methcathinone phenyl ring as one structural determinant of both DAT vs. SERT selectivity and abuse-related behavioral effects in an intracranial self-stimulation procedure in rats. Subsequent modeling studies implicated specific amino acids in DAT and SERT that might interact with 4-substituent volume to determine effects produced by this series of cathinone analogs. These studies illustrate use of QSAR analysis to investigate pharmacology of cathinones and function of monoamine transporters.
许多卡西酮类似物分别作为多巴胺、去甲肾上腺素和5-羟色胺转运体(分别为DAT、NET、SERT)的底物或抑制剂。DAT与SERT的药物选择性是单胺转运体底物和抑制剂滥用潜力的关键决定因素,因此,DAT的效力>SERT与高滥用潜力相关,而DAT的效力<SERT与低滥用潜力相关。对一系列4-取代甲卡西酮类似物进行的定量构效关系(QSAR)研究确定,甲卡西酮苯环上4-位取代基的体积是DAT与SERT选择性以及大鼠颅内自我刺激实验中与滥用相关行为效应的一个结构决定因素。随后的模型研究表明,DAT和SERT中的特定氨基酸可能与4-取代基体积相互作用,以确定这一系列卡西酮类似物产生的效应。这些研究说明了QSAR分析在研究卡西酮药理学和单胺转运体功能方面的应用。