Hallucinogens

致幻剂
  • 文章类型: Journal Article
    非法毒品市场在不断发展,随着新药的产生和现有药物的修改。掺假经常被添加到混合物中,主要物质可能会被新物质秘密取代。曾经已知的平板电脑现在可以与出售的平板电脑大不相同,都是由于追求利润和逃避现行药品法规。这些药物成分的改变对社会构成威胁,因为它们的影响仍然没有得到很好的理解。因此,获取非法药物的化学概况对警察情报和公共卫生发展至关重要。这项研究介绍了2012年至2021年在里约热内卢(巴西)缉获的摇头丸的化学指纹图谱。将片剂样品称重,提取,用甲醇稀释,和酸化前分析使用气相色谱高分辨率质谱和衰减全反射傅里叶变换红外光谱。发现的主要成分是MDMA和clobenzorex,随着MDA的出现减少,MDEA,2C-B结果还表明,研究地点发生的大事件影响了摇头丸的化学指纹。共27种切割剂组合,包括咖啡因,麻黄碱,和麻醉剂,已确定。在整个评估期间,在高速公路附近地区观察到了由氯苯并雷克组成的样品,这表明该产品主要由卡车司机使用。这些发现可以帮助警察情报部门在重大事件中预测非法市场的行为,确定交通路线,并支持公共卫生倡议。
    The illegal drug market is constantly evolving, with new drugs being created and existing ones being modified. Adulterants are often added to the mix, and the primary substance may be secretly replaced by a new one. Once-known tablets can now be vastly different from what they are sold as, all due to the pursuit of profit and evasion of current drug regulations. These alterations in drug composition pose a threat to society, as their effects are still not well understood. Therefore, it is crucial for police intelligence and public health development to obtain the chemical profiles of illicit drugs. This study presents the chemical fingerprinting of ecstasy tablets seized in the state of Rio de Janeiro (Brazil) between 2012 and 2021. The tablet samples were weighed, extracted, diluted with methanol, and acidified before analysis using gas chromatography high-resolution mass spectrometry and attenuated total reflection Fourier transform infrared spectroscopy. The major constituents found were MDMA and clobenzorex, with fewer occurrences of MDA, MDEA, and 2C-B. The results also indicate that the occurrence of mega-events in the study location impacted the chemical fingerprints of ecstasy. A total of 27 combinations of cutting agents, including caffeine, ephedrine, and anesthetics, were identified. Samples composed of clobenzorex were observed throughout the evaluated period in areas near highways, suggesting that this product is mainly used by truck drivers. These findings can help police intelligence units anticipate the behavior of the illicit market during major events, identify traffic routes, and support public health initiatives.
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  • 文章类型: Journal Article
    背景:美国(US)继续经历前所未有的过量死亡率,并且越来越需要确定有效的减少伤害的做法。加拿大的研究将通过减少危害机构捐赠大麻描述为减轻更有害药物的负面影响的辅助策略。本案例研究描述了运营物流,可行性,以及通过密歇根州农村地区的减少伤害计划实施的大麻捐赠计划的潜在好处。
    方法:我们采用了社区驱动的研究方法,从减少危害计划的工作人员那里收集有关密歇根州大麻捐赠工作的实施和发展的信息。我们还检查了20个月(2021年9月至2023年5月)的大麻公司行政数据,以比较大麻产品的销售和捐赠情况。十名有大麻经验的减少伤害的客户接受了大麻捐赠,临床工作人员确定客户的兴趣和适当性,并提供每周提货或送货。为了扩大产品的可用性和可持续性,我们检查了一家自愿提供捐款的商业大麻公司的行政数据。这些行政数据表明,虽然花卉产品占成人和医疗销售的大部分,可食用,油,和局部产品占主导地位的捐赠。Further,成本分析表明,捐赠仅占总销售额的1%,远远低于预期的年度捐赠金额。
    结论:研究表明,通过用大麻代替,有可能减少与酒精和药物使用相关的更危险物质的危害。这个案例研究是第一个记录大麻捐赠作为美国减少伤害的做法,并表明取决于州法律的可持续性潜力。本案例研究的结果为调查大麻捐赠作为美国减少伤害的策略提供了一个起点;未来的研究需要充分了解个人层面的结果。公共卫生影响,必要的法律法规,以及通过减少伤害组织进行大麻捐赠计划的最佳做法。
    BACKGROUND: The United States (US) continues to experience unprecedented rates of overdose mortality and there is increased need to identify effective harm reduction practices. Research from Canada describes cannabis donation through harm reduction agencies as an adjunctive strategy to mitigate the negative consequences of more harmful drugs. This case study describes the operational logistics, feasibility, and potential benefits of a cannabis donation program that was operated through a harm reduction program in rural Michigan.
    METHODS: We applied a community driven research approach to gather information from harm reduction program staff about the implementation and evolution of cannabis donation efforts in Michigan. We also examined 20-months (September 2021 through May 2023) of administrative data from a cannabis company to compare the sale and donation of cannabis products. Ten cannabis-experienced harm reduction clients received cannabis donations, with clinical staff determining client interest and appropriateness, and providing weekly pick-up or delivery. To expand product availability and sustainability, we examined administrative data from a commercialcannabis company that volunteered to provide donations. This administrative data suggests that while flower products constitute most of the adult and medical sales, edible, oil, and topical products predominated donations. Further, cost analysis suggests that donations represent only 1% of total gross sales and account for much less than the expected yearly donation amount.
    CONCLUSIONS: Research suggests there is potential to reduce alcohol and drug use related harms of more dangerous substances through substitution with cannabis. This case study is the first to document cannabis donation as a harm reduction practice in the US and suggests potential for sustainability dependent on state laws. Findings from this case study provide a starting point for inquiry into cannabis donation as a harm reduction strategy in the US; future research is needed to fully understand the individual-level outcomes, public health impacts, necessary legal regulations, and best practices for cannabis donation programs through harm reduction organizations.
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  • 文章类型: Journal Article
    背景:5-甲氧基-N-甲基-N-异丙基色胺(5-MeO-MiPT,在网上被称为“Moxy”)是一种新的迷幻色胺,于2014年在意大利国家领土上首次发现。它的致幻剂作用广为人知;然而,关于其药物毒理学作用的信息很少。
    目的:在Carabinieri臂缉获这种新的精神活性物质并发生人类中毒病例后,在当前的研究中,我们的目标是表征全身给药5-MeO-MiPT(0.01-30mg/kgi.p.)对感觉运动(视觉,声学,和整体触觉)反应,体温调节,和刺激CD-1雄性小鼠的运动活动(阻力和加速度测试)。我们还评估了感觉门控的变化(PPI,前脉冲抑制;0.01-10mg/kgi.p.)和心肺参数(MouseOx和BP-2000;30mg/kgi.p.)。最后,我们研究了计算机模拟ADMET(吸收,分布,新陈代谢,排泄,毒性)与5-甲氧基-N相比,5-MeO-MiPT的概况,N-二异丙基色胺(5-MeO-DIPT)和N,N-二甲基色胺(DMT)。
    结果:这项研究表明,5-MeO-MiPT剂量依赖性地抑制感觉运动和PPI反应,在高剂量下,诱导小鼠刺激的运动活动和心肺变化的损害。计算机预测显示,5-MeO-MiPT毒代动力学谱与5-MeO-DIPT和DMT具有相似性,并且突出了与该化合物相关的细胞色素风险。
    结论:消耗5-MeO-MiPT会影响进行活动的能力,并对人类健康状况构成风险,正如在小鼠中诱导的效应和中毒病例中发生的症状之间的对应关系所表明的那样。然而,我们的研究结果表明,5-MeO-MiPT不应被排除在精神病治疗领域的研究之外.
    BACKGROUND: The 5-methoxy-N-methyl-N-isopropyltryptamine (5-MeO-MiPT, known online as \"Moxy\") is a new psychedelic tryptamine first identified on Italian national territory in 2014. Its hallucinogen effects are broadly well-known; however, only few information is available regarding its pharmaco-toxicological effects.
    OBJECTIVE: Following the seizure of this new psychoactive substances by the Arm of Carabinieri and the occurrence of a human intoxication case, in the current study we had the aim to characterize the in vivo acute effects of systemic administration of 5-MeO-MiPT (0.01-30 mg/kg i.p.) on sensorimotor (visual, acoustic, and overall tactile) responses, thermoregulation, and stimulated motor activity (drag and accelerod test) in CD-1 male mice. We also evaluated variation on sensory gating (PPI, prepulse inhibition; 0.01-10 mg/kg i.p.) and on cardiorespiratory parameters (MouseOx and BP-2000; 30 mg/kg i.p.). Lastly, we investigated the in silico ADMET (absorption, distribution, metabolism, excretion, toxicity) profile of 5-MeO-MiPT compared to 5-methoxy-N,N-diisopropyltryptamine (5-MeO-DIPT) and N,N-dimethyltryptamine (DMT).
    RESULTS: This study demonstrates that 5-MeO-MiPT dose-dependently inhibits sensorimotor and PPI responses and, at high doses, induces impairment of the stimulated motor activity and cardiorespiratory changes in mice. In silico prediction shows that the 5-MeO-MiPT toxicokinetic profile shares similarities with 5-MeO-DIPT and DMT and highlights a cytochrome risk associated with this compound.
    CONCLUSIONS: Consumption of 5-MeO-MiPT can affect the ability to perform activities and pose a risk to human health status, as the correspondence between the effects induced in mice and the symptoms occurred in the intoxication case suggests. However, our findings suggest that 5-MeO-MiPT should not be excluded from research in the psychiatric therapy field.
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  • 文章类型: Case Reports
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  • 文章类型: Review
    N-苄基苯乙胺衍生物是具有致幻特性的5-HT2A受体激动剂,包括NBOMe(N-(2-甲氧基苄基)-2-(3,4,5-三甲氧基苯基)乙-1-胺)和NBOH(2-((2,5-二甲氧基苯乙基)氨基)甲基)苯酚。我们在此报告了一名23岁男子的病例,该男子在食用标记为25I-NBOH的粉末后出现5-羟色胺能综合征和意识丧失。使用液相色谱高分辨率质谱法对生物样品进行毒理学分析。通过认证的参考材料鉴定并确认了两种新的精神活性物质:25E-NBOH(2-(((4-乙基-2,5-二甲氧基苯乙基)氨基)甲基)苯酚和MDPHP(1-(苯并[d][1,3]二氧杂环戊醇-5-基)-2-(吡咯烷-1-基)己-1-酮)。在患者的医疗护理期间给药的药物在血浆和尿液中被发现。25E-NBOH和MDPHP在血浆中的浓度分别为2.3ng/mL和3.4ng/mL,和25.7ng/mL和30.5ng/mL的尿液。25I-NBOH(2-(((4-碘-2,5-二甲氧基苯乙基)氨基)甲基)苯酚)在两个样品中均被特异性地搜索并且未被检测到。讨论了这些结果以及有关暴露于N-苄基苯乙胺衍生物的人类病例的文献综述。使用分子网络方法,我们提出了第一个使用真实生物样本(血浆和尿液)的25E-NBOH代谢研究。我们描述了七种代谢物(M1至M7),包括两个I相(m/z330.172;m/z288.160)和五个II相代谢物(m/z464.191,m/z478.207,m/z492.223,m/z508.218;m/z396.156)。M6(m/z492.223)是在血浆和尿液中检测到的最强离子,并且可以被提出作为相关的25E-NBOH消耗标记。总的来说,我们描述了一例25E-NBOH中毒的原始病例,并确定了可能用作消费标志物的代谢物,以更高的置信水平和可能更长的检测窗口检测25E-NBOH中毒.
    N-Benzylphenethylamine derivatives are 5-HT2A receptor agonists with hallucinogenic properties, including NBOMe (N-(2-methoxybenzyl)-2-(3,4,5-trimethoxyphenyl)ethan-1-amine) and NBOH (2-(((2,5-dimethoxyphenethyl)amino)methyl)phenol). We reported here the case of a 23-year-old man who presented a serotoninergic syndrome and a loss of consciousness following the consumption of a powder labelled as 25I-NBOH. Toxicological analyses of biological samples were carried out using a liquid chromatography high-resolution mass spectrometry. Two new psychoactive substances were identified and confirmed with certified reference materials: 25E-NBOH (2-(((4-ethyl-2,5-dimethoxyphenethyl)amino)methyl)phenol) and MDPHP (1-(benzo[d][1,3]dioxol-5-yl)-2-(pyrrolidin-1-yl)hexan-1-one). Pharmaceuticals administered to the patient during his medical care were found in plasma and urine. 25E-NBOH and MDPHP concentrations were respectively at 2.3 ng/mL and 3.4 ng/mL in plasma, and 25.7 ng/mL and 30.5 ng/mL in urine. 25I-NBOH (2-(((4-iodo-2,5-dimethoxyphenethyl)amino)methyl)phenol) was specifically searched in both samples and was not detected. These results are discussed along with a literature review on human cases of exposure to N-benzylphenethylamine derivatives. Using molecular networking approach, we propose the first 25E-NBOH metabolism study using authentic biological samples (plasma and urine). We described seven metabolites (M1 to M7), including two phase I (m/z 330.172; m/z 288.160) and five phase II metabolites (m/z 464.191, m/z 478.207, m/z 492.223, m/z 508.218; m/z 396.156). The M6 (m/z 492.223) was the most intense ion detected in plasma and urine and could be proposed as a relevant 25E-NBOH consumption marker. Overall, we described an original case of 25E-NBOH poisoning and identified metabolites that could potentially be used as consumption markers to detect 25E-NBOH intoxications with a higher confidence level and probably a longer detection window.
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  • 文章类型: Case Reports
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  • 文章类型: Journal Article
    最近出现了关于对迷幻药及其治疗潜力的不加批判的积极评价和炒作的争议。批评包括研究设计和报告风格偏向正面而不是负面结果。本研究的动机是希望通过故意专注于负面结果来解决这种所谓的偏见,定义为迷幻药使用后持续至少72小时的自我感知的“消极”心理反应。这种选择性聚焦的一个强有力的理由是,它可能会提高我们捕捉否则错过的负面反应案例的能力,使我们能够验证它们的存在并更好地检查它们的性质,以及可能的原因,这可以激发风险缓解策略。通过在社交媒体上发布的广告,招募的个体报告自使用以来对迷幻药(定义为经典迷幻药加MDMA)的负面心理反应持续超过72小时.志愿者被引导到需要定量和定性输入的在线问卷。这项研究的关键第二阶段涉及审查所有提交的案件,确定最严重的-例如,在进行新的精神病诊断或先前存在的症状在迷幻药使用后变得更糟,并邀请这些人参加与我们研究小组两名成员的半结构化访谈,在此期间,对参与者的经验和背景进行了更深入的检查。根据这些采访的内容,对每个案例进行了简要总结,探索性主题分析用于确定突出和一致的主题并推断常见原因。32名个人完全完成了入职问卷(56%为男性,53%<25岁);37.5%的完成者在迷幻经历后出现了精神病诊断,87%的人出现或恶化了焦虑症状。20个看似严重的案件被邀请接受采访;其中,15接受了平均持续60分钟的深入采访。这个样本是40%的男性,平均年龄=31±7。15个中的五个(即,33%)报告在使用迷幻药后接受了新的精神病诊断,并且所有15个报告在使用后出现或恶化了精神病症状,以焦虑症状为主(93%)。对访谈内容的提炼提出了以下潜在的因果因素:经验期间或周围的不安全或复杂的环境,不愉快的急性经历(经典迷幻药),先前的心理脆弱,高或未知的药物数量和年轻的年龄。当前的探索性发现证实了通过迷幻药使用但由于设计限制和样本量的原因,不能用来推断其患病率。根据采访报道,我们可以推断一个共同的,尽管是多方面的,因果机制,即一种促可塑性药物-通常“过量”-与不利的背景条件和/或特殊的心理脆弱性-年龄小或重要的精神病史相结合。由于样本量小,选择性样本和研究重点,因此应谨慎解释结果。
    Recent controversies have arisen regarding claims of uncritical positive regard and hype surrounding psychedelic drugs and their therapeutic potential. Criticisms have included that study designs and reporting styles bias positive over negative outcomes. The present study was motivated by a desire to address this alleged bias by intentionally focusing exclusively on negative outcomes, defined as self-perceived \'negative\' psychological responses lasting for at least 72 h after psychedelic use. A strong justification for this selective focus was that it might improve our ability to capture otherwise missed cases of negative response, enabling us to validate their existence and better examine their nature, as well as possible causes, which could inspire risk-mitigation strategies. Via advertisements posted on social media, individuals were recruited who reported experiencing negative psychological responses to psychedelics (defined as classic psychedelics plus MDMA) lasting for greater than 72 h since using. Volunteers were directed to an online questionnaire requiring quantitative and qualitative input. A key second phase of this study involved reviewing all of the submitted cases, identifying the most severe-e.g., where new psychiatric diagnoses were made or pre-existing symptoms made worse post psychedelic-use-and inviting these individuals to participate in a semi-structured interview with two members of our research team, during which participant experiences and backgrounds were examined in greater depth. Based on the content of these interviews, a brief summary of each case was compiled, and an explorative thematic analysis was used to identify salient and consistent themes and infer common causes. 32 individuals fully completed an onboarding questionnaire (56% male, 53% < age 25); 37.5% of completers had a psychiatric diagnosis that emerged after their psychedelic experience, and anxiety symptoms arose or worsened in 87%. Twenty of the seemingly severer cases were invited to be interviewed; of these, 15 accepted an in-depth interview that lasted on average 60 min. This sample was 40% male, mean age = 31 ± 7. Five of the 15 (i.e., 33%) reported receiving new psychiatric diagnoses after psychedelic-use and all fifteen reported the occurrence or worsening of psychiatric symptoms post use, with a predominance of anxiety symptoms (93%). Distilling the content of the interviews suggested the following potential causal factors: unsafe or complex environments during or surrounding the experience, unpleasant acute experiences (classic psychedelics), prior psychological vulnerabilities, high- or unknown drug quantities and young age. The current exploratory findings corroborate the reality of mental health iatrogenesis via psychedelic-use but due to design limitations and sample size, cannot be used to infer on its prevalence. Based on interview reports, we can infer a common, albeit multifaceted, causal mechanism, namely the combining of a pro-plasticity drug-that was often \'over-dosed\'-with adverse contextual conditions and/or special psychological vulnerability-either by young age or significant psychiatric history. Results should be interpreted with caution due to the small sample size and selective sample and study focus.
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  • 文章类型: Historical Article
    This article describes the associations and controversies between indigenous and western uses of ayahuasca between 1850 and 1950 in relation to the \"psychedelic renaissance.\" This movement has gained scientific attention since 2000, but hearkens back to the 1960s and 1970s, when anti-drug policy halted research on the \"therapeutic potential\" of psychoactive substances. Pioneering studies on ayahuasca date back to the early twentieth century and mention reports of expeditions to Amazonia from 1850 onward. Here, these articles and reports are analyzed according to the historical aspect of actor-network theory and recent studies. We infer that history casts light on the current political debate about indigenous uses, classifications, and meanings, pharmaceutical interest in ayahuasca, and the debate on \"drugs.\"
    O artigo descreve associações e controvérsias entre usos indígenas e ocidentais da ayahuasca, de 1850 a 1950, na relação com o “renascimento psicodélico”. Destaque na ciência desde 2000, esse movimento faz referência a 1960-1970, quando políticas antidrogas suspenderam pesquisas sobre “potenciais terapêuticos” de substâncias psicoativas. Argumenta-se que estudos pioneiros com a ayahuasca datam do início do século XX e mencionam relatos de expedições à Amazônia desde 1850. Esses artigos e relatos são analisados pelo aspecto histórico da teoria do ator-rede e de estudos recentes. Infere-se que a história ilumina o debate político atual sobre os usos, classificações e significados indígenas; o interesse farmacêutico na ayahuasca; e a discussão sobre “drogas”.
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  • 文章类型: Randomized Controlled Trial
    目的:这项定性研究的主要目的是描述第一个随机对照试验中的心理变化机制,即psilocybin辅助心理治疗治疗酒精使用障碍(AUD)。有关迷幻疗法涉及的心理过程的理论仍然不发达。
    方法:参与者(N=13)主要被确定为非西班牙裔和白人,男性和女性的比例大致相同。参与者就他们在研究中的主观经历进行了半结构化访谈。问题探讨了参与者在研究前后饮酒的性质,以及应对强烈情绪的应对方式,压力,和对酒精的渴望。使用Dedoose软件对逐字记录进行编码,内容进行了解释现象学分析。
    结果:参与者报告说,psilocybin治疗帮助他们处理与痛苦的过去事件有关的情绪,并有助于促进自我同情状态,自我意识,和相互联系的感觉。psilocybin会议期间的急性状态被描述为发展更多的自我同情调节负面影响奠定了基础。参与者还描述了治疗后新发现的归属感和改善的人际关系质量。
    结论:我们的结果支持psilocybin增加自我相关加工的延展性的断言,并减少基于羞耻和自我批评的思维模式,同时改善影响调节和减少对酒精的渴望。这些发现表明,将自我同情训练与迷幻疗法相结合的社会心理疗法可能是增强AUD治疗心理结果的有用工具。(PsycInfo数据库记录(c)2023年APA,保留所有权利)。
    OBJECTIVE: The primary aim of this qualitative study was to delineate psychological mechanisms of change in the first randomized controlled trial of psilocybin-assisted psychotherapy to treat alcohol use disorder (AUD). Theories regarding psychological processes involved in psychedelic therapy remain underdeveloped.
    METHODS: Participants (N = 13) mostly identified as non-Hispanic and White, with approximately equal proportions of cisgender men and women. Participants engaged in semistructured interviews about their subjective experiences in the study. Questions probed the nature of participants\' drinking before and after the study as well as coping patterns in response to strong emotions, stress, and cravings for alcohol. Verbatim transcripts were coded using Dedoose software, and content was analyzed with interpretive phenomenological analysis.
    RESULTS: Participants reported that the psilocybin treatment helped them process emotions related to painful past events and helped promote states of self-compassion, self-awareness, and feelings of interconnectedness. The acute states during the psilocybin sessions were described as laying the foundation for developing more self-compassionate regulation of negative affect. Participants also described newfound feelings of belonging and an improved quality of relationships following the treatment.
    CONCLUSIONS: Our results support the assertion that psilocybin increases the malleability of self-related processing, and diminishes shame-based and self-critical thought patterns while improving affect regulation and reducing alcohol cravings. These findings suggest that psychosocial treatments that integrate self-compassion training with psychedelic therapy may serve as a useful tool for enhancing psychological outcomes in the treatment of AUD. (PsycInfo Database Record (c) 2024 APA, all rights reserved).
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