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The first reported fatality associated with the synthetic opioid 3,4-dichloro-N-[2-(dimethylamino)cyclohexyl]-N-methylbenzamide (U-47700) and implications for forensic analysis

机译:首次报道的与合成阿片样物质3,4-二氯-N- [2-(二甲基氨基)环己基] -N-甲基苯甲酰胺有关的死亡(U-47700)及其法医分析意义

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摘要

The search for synthetic opioids as alternatives to opium-based derivatives has provided an important impulse to drug development around the globe. An important goal in the systematic evaluation of new drug candidates is the identification of compounds that provide a more favorable side-effect profile, which includes reduced dependence-producing properties and abuse liability. A rich source of information about these research efforts can be found in the scientific literature. However, the exploration of these important discoveries has also been increasingly mined by largescale producers of these materials, which are then offered for sale. These so-called ‘research chemicals’ or new psychoactive substances (NPS)[1] have created challenges to policy makers, clinicians, and law enforcement around the world.[2]\udRecent examples of synthetic opioids that emerged as NPS on the market, and which were associated with severe cases of adverse effects, include 3,4-dichloro-N-\ud{[1-(dimethylamino)cyclohexyl]methyl}benzamide (AH-7921), 1-cyclohexyl-4-(1,2-\uddiphenylethyl)piperazines (MT-45) and N-phenyl-N-[1-(2-phenylethyl)piperidin-4-\udyl]acetamide (acetylfentanyl), respectively (Figure 1). Following the recommendation provided by the World Health Organization’s Expert Committee on Drug Dependence\ud(ECDD),[3] AH-7921 was placed in Schedule I of the 1961 Single Convention, as amended by the 1972 Protocol in 2015.[4] Furthermore, ECDD’s recommendation to place MT-45 into Schedule I and acetylfentanyl in Schedules I and IV of the same Convention[5] have been recently confirmed by the Commission on Narcotic Drugs.[6]\ud-Dichloro-N-[2-(dimethylamino)cyclohexyl]-N-methylbenzamide (U-47700) (Figure\ud1) has recently emerged on the market and can be purchased from various Internet retailers and is a structural isomer of AH-7921 (Figure 1). The preparation of U-\ud47700 and other derivatives was disclosed by the Upjohn Company in the 1970s[7] followed by the recognition that U-47700 showed increased analgesic properties and morphine-like behavioural features in mice compared to morphine itself.[8,9] The presence of two chiral centres gives rise to a cis- and trans- racemic mixture with the trans-form being advertised for sale. Binding studies also revealed that U-47700 displayed an appreciable selectivity for the μ-opioid receptor over the −opioid receptor.[10,11] A variety of cyclohexyl trans-1,2-diamines have been found to be potent analgesics and the vicinal 1,2-diamine pattern has provided access to a large range of substances with diverse biological activities.[12-14]\udSince U-47700 did not progress to clinical trials, there is no direct clinical information pertaining to its effects. Keeping in mind the various limitations that may be associated with descriptions obtained from self-reporting users, its effects have been described with various positive and negative symptoms but appeared to be essentially comparable to other opioids. Specifically, euphoria was reported in individuals, sometimes being short-lived, as well as general lift in mood with these desired effects being experienced in waves. The negative effects were also opioid based, including nausea with some users describing respiratory depression. For some users, U-47700 had a shorter duration of action and the urge to keep re-dosing was stated as being very high.
机译:寻找合成的阿片类药物替代鸦片基衍生物为全球药物开发提供了重要动力。系统评价新候选药物的一个重要目标是鉴定具有更有利副作用的化合物,包括降低产生依赖性的特性和滥用责任。在科学文献中可以找到有关这些研究工作的丰富信息。但是,这些材料的大规模生产者也越来越多地探索这些重要发现,然后将其出售。这些所谓的“研究用化学品”或新型精神活性物质(NPS)[1]给全球的决策者,临床医生和执法人员带来了挑战。[2] \ ud市场上以NPS形式出现的合成阿片类药物的最新实例,与严重的不良反应相关,包括3,4-二氯-N- \ ud {[1-(二甲基氨基)环己基]甲基}苯甲酰胺(AH-7921),1-环己基-4-(1, 2- \ uddiphenylethyl)哌嗪(MT-45)和N-苯基-N- [1-(2-(苯基苯基)哌啶丁-4- \ udyl]乙酰胺(乙酰芬太尼)(图1)。根据世界卫生组织药物依赖性专家委员会的建议\ ud(ECDD),[3] AH-7921被列入1961年《单一公约》附表一,并于1972年的《议定书》于2015年进行了修订。[4]此外,麻醉药品委员会最近确认了欧洲经委会关于将MT-45列入同一公约的附表一和乙酰芬太尼的建议[5]。[6] \ ud-Dichloro-N- [2- (二甲基氨基)环己基] -N-甲基苯甲酰胺(U-47700)(图\ ud1)最近在市场上出现,可以从各种互联网零售商处购买,并且是AH-7921的结构异构体(图1)。 U- \ ud47700和其他衍生物的制备方法由Upjohn公司在1970年代公开[7],随后认识到,与吗啡本身相比,U-47700在小鼠中显示出更高的止痛特性和类似吗啡的行为特征。[8, 9]两个手性中心的存在产生了顺式和反式外消旋混合物,其反式形式被广告出售。结合研究还显示,U-47700对μ阿片受体的选择性优于β阿片受体。[10,11]已发现各种环己基反式1,2-二胺是有效的止痛药,邻位的1,2-二胺模式提供了广泛的具有多种生物活性的物质的途径。[12-14] \ ud由于U-47700尚未进行临床试验,因此没有关于其作用的直接临床信息。考虑到可能与自我报告使用者的描述有关的各种限制,已经以各种积极和消极的症状描述了其作用,但似乎与其他阿片类药物具有可比性。具体来说,据报道,个体中的欣快感有时会短暂存在,情绪普遍升高,而这些期望的效果会在波浪中发生。负面影响也基于阿片类药物,包括恶心,一些使用者描述呼吸抑制。对于某些用户而言,U-47700的作用时间较短,并且据称保持重新加药的冲动非常强烈。

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