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N,N-二甲基戊酮及其相关类似物的毒理学评估、尸检病例描述和药理活性

Toxicological evaluation, postmortem case descriptions, and pharmacological activity of N,N-dimethylpentylone and related analogs.

作者信息

Fogarty Melissa F, Walton Sara E, Truver Michael T, Glatfelter Grant C, Krotulski Alex J, Papsun Donna M, Lamb Michael, Chronister Chris W, Goldberger Bruce A, Walther Donna, Barba Kristie, Baumann Michael H, Logan Barry K

机构信息

Center for Forensic Science Research and Education, Fredric Rieders Family Foundation, Horsham, PA 19044, United States.

Forensic Toxicology Laboratory, Department of Pathology, Immunology and Laboratory Medicine, University of Florida College of Medicine, Gainesville, FL 32607, United States.

出版信息

J Anal Toxicol. 2025 Mar 10;49(3):143-151. doi: 10.1093/jat/bkaf002.

Abstract

Identification of N,N-dimethylpentylone (DMP) in counterfeit "Ecstasy" and "Molly" tablets poses risk to public health due to its adverse effects. Little information is available regarding the pharmacological activity or relevant blood or tissue concentrations of DMP, and even less is known about other structurally related beta-keto methylenedioxyamphetamine analogs on recreational drug markets, such as N-propyl butylone. Here, a novel toxicological assay utilizing liquid chromatography-tandem quadrupole mass spectrometry was developed and validated for the quantitation of DMP and five related synthetic cathinones [eutylone, pentylone, N-ethyl pentylone (NEP), N-propyl butylone, and N-cyclohexyl butylone], with chromatographic resolution from isomeric variants and quantitation performed by standard addition. A forensic series of 125 cases is presented for DMP and related analogs, along with pharmacological activity assessments using monoamine transporter and mouse behavioral assays. The blood concentration range for DMP in postmortem forensic cases was 3.3-4600 ng/mL (mean: 320 ± 570 ng/mL, median: 150 ng/mL), whereas pentylone, the primary N-desmethyl metabolite of DMP, was identified in 98% of cases with a concentration range 1.3-710 ng/mL (mean ± SD: 105 ± 120 ng/mL, median: 71 ng/mL). N-Propyl butylone, a newly identified synthetic cathinone, was quantitated in seven cases (mean ± SD: 82 ± 75 ng/mL, median: 50 ng/mL, range: 1.7-200 ng/mL). DMP displayed potent uptake inhibition at the dopamine transporter [half maximal inhibitory concentration (IC50) of 49 nM], with 100-fold weaker potency at the serotonin transporter (IC50 = 4990 nM). DMP was a locomotor stimulant in mice [medium effective dose (ED50) of 3.5 mg/kg] exhibiting potency relatively similar to eutylone, NEP, and pentylone. Our results show that DMP is a psychomotor stimulant associated with adverse clinical outcomes leading to death. Forensic laboratories must continue to update testing methods to capture emerging drugs, with specific emphasis on resolution and identification of isomeric species. Following the scheduling of DMP in early 2024, there could be an anticipated market shift toward a new unregulated synthetic stimulant to replace DMP.

摘要

在假冒的“摇头丸”和“莫莉”片剂中鉴定出N,N-二甲基戊酮(DMP)因其不良影响对公众健康构成风险。关于DMP的药理活性或相关血液或组织浓度的信息很少,对于娱乐性毒品市场上其他结构相关的β-酮亚甲二氧基苯丙胺类似物,如N-丙基丁酮,了解更少。在此,开发并验证了一种利用液相色谱-串联四极杆质谱的新型毒理学分析方法,用于定量DMP和五种相关的合成卡西酮[乙酮、戊酮、N-乙基戊酮(NEP)、N-丙基丁酮和N-环己基丁酮],通过标准加入法进行定量,实现了异构体变体的色谱分离。展示了125例DMP及相关类似物的法医案例系列,以及使用单胺转运体和小鼠行为分析进行的药理活性评估。法医尸检案例中DMP的血液浓度范围为3.3 - 4600 ng/mL(平均值:320±570 ng/mL,中位数:150 ng/mL),而DMP的主要N-去甲基代谢物戊酮在98%的案例中被鉴定出,浓度范围为1.3 - 710 ng/mL(平均值±标准差:105±120 ng/mL,中位数:71 ng/mL)。新鉴定的合成卡西酮N-丙基丁酮在7例案例中被定量(平均值±标准差:82±75 ng/mL,中位数:50 ng/mL,范围:1.7 - 200 ng/mL)。DMP对多巴胺转运体表现出强效摄取抑制作用[半数最大抑制浓度(IC50)为49 nM],对5-羟色胺转运体的效力弱100倍(IC50 = 4990 nM)。DMP是小鼠的运动兴奋剂[半数有效剂量(ED50)为3.5 mg/kg],其效力与乙酮、NEP和戊酮相对相似。我们的结果表明,DMP是一种与导致死亡的不良临床后果相关的精神运动兴奋剂。法医实验室必须继续更新检测方法以捕获新出现的毒品,特别强调异构体种类的分离和鉴定。在2024年初将DMP列入管制后,预计市场可能会转向一种新的不受管制的合成兴奋剂来取代DMP。

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