Center for Physiology and Pharmacology, Institute of Pharmacology, Medical University of Vienna, Waehringerstrasse 13A, 1090, Vienna, Austria.
Institut Cochin, INSERM U1016, CNRS UMR8104, Université Paris Descartes, Sorbonne Paris Cité, 27 rue du Faubourg St-Jacques, 75014, Paris, France.
Psychopharmacology (Berl). 2019 Mar;236(3):953-962. doi: 10.1007/s00213-018-5075-5. Epub 2018 Oct 22.
Synthetic cathinones continue to emerge in recreational drug markets worldwide. 1-(1,3-Benzodioxol-5-yl)-2-(methylamino)butan-1-one (butylone) and 1-(1,3-benzodioxol-5-yl)-2-(methylamino)pentan-1-one (pentylone) are derivatives of the cathinone compound, 1-(1,3-benzodioxol-5-yl)-2-(methylamino)propan-1-one (methylone), that are being detected in drug products and human casework.
The purpose of the present study was to examine the neuropharmacology of butylone and pentylone using in vitro and in vivo methods.
In vitro uptake and release assays were carried out in rat brain synaptosomes and in cells expressing human dopamine transporters (DAT) and 5-HT transporters (SERT). In vivo microdialysis was performed in the nucleus accumbens of conscious rats to assess drug-induced changes in neurochemistry.
Butylone and pentylone were efficacious uptake blockers at DAT and SERT, though pentylone was more DAT-selective. Both drugs acted as transporter substrates that evoked release of [H]5-HT at SERT, while neither evoked release at DAT. Consistent with the release data, butylone and pentylone induced substrate-associated inward currents at SERT but not DAT. Administration of butylone or pentylone to rats (1 and 3 mg/kg, i.v.) increased extracellular monoamines and motor activity, but pentylone had weaker effects on 5-HT and stronger effects on motor stimulation.
Our data demonstrate that increasing the α-carbon chain length of methylone creates "hybrid" transporter compounds which act as DAT blockers but SERT substrates. Nevertheless, butylone and pentylone elevate extracellular dopamine and stimulate motor activity, suggesting both drugs possess significant risk for abuse.
合成卡西酮在全球的娱乐性毒品市场中不断涌现。1-(1,3-苯并二恶唑-5-基)-2-(甲基氨基)丁-1-酮(丁酮)和 1-(1,3-苯并二恶唑-5-基)-2-(甲基氨基)戊-1-酮(戊酮)是卡西酮化合物 1-(1,3-苯并二恶唑-5-基)-2-(甲基氨基)丙-1-酮(甲基酮)的衍生物,在药物产品和人体案例中都有检测到。
本研究旨在通过体外和体内方法研究丁酮和戊酮的神经药理学。
在大鼠脑突触体和表达人多巴胺转运体(DAT)和 5-羟色胺转运体(SERT)的细胞中进行摄取和释放测定。在清醒大鼠的伏隔核中进行体内微透析,以评估药物引起的神经化学变化。
丁酮和戊酮是 DAT 和 SERT 的有效摄取阻断剂,尽管戊酮对 DAT 的选择性更高。两种药物均为转运体底物,可引起 SERT 中 [H]5-HT 的释放,而在 DAT 中则不会。与释放数据一致,丁酮和戊酮在 SERT 上引起与底物相关的内向电流,但在 DAT 上则不会。给予大鼠丁酮或戊酮(1 和 3 mg/kg,iv)增加了细胞外单胺和运动活动,但戊酮对 5-HT 的作用较弱,对运动刺激的作用较强。
我们的数据表明,增加甲基酮的α-碳原子链长度会产生作为 DAT 阻断剂但 SERT 底物的“杂交”转运体化合物。然而,丁酮和戊酮可增加细胞外多巴胺并刺激运动活动,这表明这两种药物都具有明显的滥用风险。
