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N,N-二甲基色胺的人体精神药理学

Human psychopharmacology of N,N-dimethyltryptamine.

作者信息

Strassman R J

机构信息

Department of Psychiatry, University of New Mexico, Albuquerque 87131-5326, USA.

出版信息

Behav Brain Res. 1996;73(1-2):121-4. doi: 10.1016/0166-4328(96)00081-2.

Abstract

We generated dose-response data for the endogenous and ultra-short-acting hallucinogen, N,N-dimethyltryptamine (DMT), in a cohort of experienced hallucinogen users, measuring multiple biological and psychological outcome measures. Subjective responses were quantified with a new rating scale, the HRS, which provided better resolution of dose effects than did the biological variables. A tolerance study then was performed, in which volunteers received four closely spaced hallucinogenic doses of DMT. Subjective responses demonstrated no tolerance, while biological measures were inconsistently reduced over the course of the sessions. Thus, DMT remains unique among classic hallucinogens in its inability to induce tolerance to its psychological effects. To assess the role of the 5-HT1A site in mediating DMT's effects, a pindolol pre-treatment study was performed. Pindolol significantly increased psychological responses to DMT, suggesting a buffering effect of 5-HT1A agonism on 5-HT2-mediated psychedelic effects. These data are opposite to those described in lower animal models of hallucinogens' mechanisms of action.

摘要

我们在一组有使用致幻剂经验的使用者中,生成了内源性超短效致幻剂N,N-二甲基色胺(DMT)的剂量反应数据,测量了多种生物学和心理学结果指标。主观反应通过一种新的评分量表——致幻剂评分量表(HRS)进行量化,该量表比生物学变量能更好地分辨剂量效应。随后进行了一项耐受性研究,志愿者接受了四个间隔紧密的致幻剂量的DMT。主观反应未显示出耐受性,而生物学指标在整个实验过程中减少情况不一。因此,DMT在经典致幻剂中仍然独特,因为它无法诱导对其心理效应产生耐受性。为了评估5-HT1A位点在介导DMT效应中的作用,进行了一项心得安预处理研究。心得安显著增加了对DMT的心理反应,表明5-HT1A激动对5-HT2介导的迷幻效应有缓冲作用。这些数据与在较低等动物模型中描述的致幻剂作用机制的数据相反。

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