Department of Psychiatry & McKnight Brain Institute, University of Florida College of Medicine, Gainesville, FL 32610-0256, USA.
Med Hypotheses. 2013 Sep;81(3):450-5. doi: 10.1016/j.mehy.2013.06.007. Epub 2013 Jul 8.
Consensus in the most recent literature indicates that psychoactive "bath salts" is a relatively new drug-combination that was added to Schedule I classification in October 2011. Common ingredients include the cathinone analogs: mephedrone and methylenedioxypyrovalerone (MDPV). The mechanism of action of these synthetic cathinone analogs has not yet been well studied. We propose an intensive systematic investigation to determine the potential for cathinones to produce neurotoxic effects in various brain regions. In spite of a lack of evidence, for neurotoxicity there are number of horrific cases now on record that suggest intensification of research is needed. For example, a suicide by hanging had high 3,4-MDPV concentration while a driver under the influence had the highest reported methylone (MEPH) concentration. More interestingly, there have been consistent case reports indicating delayed responses, including: severe agitation with possible psychosis, suicidal ideation, rhabdomyolysis, hypertension, tachycardia, and death. In animal studies, amphetamine (AMPH), methamphetamine (METH) and cocaine release dopamine (DA), similarly to the action of cathinone and particular cathinone analogues. Two components of bath salts, MEPH and MDPV produce opposite effects at human dopamine transporter (hDAT) comparable to METH and cocaine, respectively. Moreover, it has already been found by others that MEPH is almost as potent as METH; and MDPV is much more potent than cocaine with longer lasting effects. It has been conjectured correctly that bath salts containing MDPV and MEPH (or a similar drug) might be expected both, to initially release DA and subsequently prevent its reuptake via hDAT. The null hypothesis, that cathinones do not cause neurotoxicity to dopamine nerve endings of the striatum, seems parsimonious and requires intensive investigation. Our hypothesis is that when consumed by humans, cathinones may induce neurotoxic pathways involving the neuro-glial-microglia and/or specific inflammation, that may help explain the clinically observed delayed response. We intend to explore this hypothesis utilizing a novel proteomic and biomarker technique developed by scientists at the McKnight Brain Institute, University of Florida as well as magnetic-resonance imaging across pre-frontal orbital cortex-cingulate gyrus and mesolimbic pathways of the brain of rodents.
最新文献中的共识表明,精神活性“浴盐”是一种相对较新的药物组合,于 2011 年 10 月被列入附表 I 分类。常见成分包括卡他酮类似物:甲卡西酮和 3,4-亚甲二氧基吡咯戊酮(MDPV)。这些合成卡他酮类似物的作用机制尚未得到很好的研究。我们提出了一项深入的系统研究,以确定卡他酮是否有可能在各种大脑区域产生神经毒性作用。尽管缺乏证据,但有许多可怕的病例表明,需要加强研究。例如,一起自杀案件中发现死者的 3,4-MDPV 浓度很高,而一名受影响的司机则报告了最高的甲基酮(MEPH)浓度。更有趣的是,有一致的病例报告表明存在延迟反应,包括:严重的躁动伴可能的精神病、自杀意念、横纹肌溶解症、高血压、心动过速和死亡。在动物研究中,安非他命(AMPH)、甲基苯丙胺(METH)和可卡因释放多巴胺(DA),类似于卡他酮和特定卡他酮类似物的作用。浴盐的两种成分,MEPH 和 MDPV,在人类多巴胺转运体(hDAT)上产生相反的作用,分别类似于 METH 和可卡因。此外,其他人已经发现 MEPH 几乎与 METH 一样有效;而 MDPV 的效力比可卡因强得多,作用持续时间也更长。浴盐中含有 MDPV 和 MEPH(或类似药物)的假设是合理的,它们可能会同时释放 DA,随后通过 hDAT 阻止其再摄取。卡他酮不会对纹状体多巴胺神经末梢造成神经毒性的零假设似乎很合理,需要进行深入研究。我们的假设是,当人类摄入卡他酮时,可能会引起涉及神经胶质-小胶质细胞和/或特定炎症的神经毒性途径,这可能有助于解释临床上观察到的延迟反应。我们打算利用佛罗里达大学麦克奈特脑研究所的科学家开发的一种新的蛋白质组学和生物标志物技术,以及对啮齿动物大脑前额眶皮质-扣带回和中脑边缘通路的磁共振成像来探索这一假设。
