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内源性精神活性色胺再探讨:二甲基色胺的抗焦虑作用

Endogenous psychoactive tryptamines reconsidered: an anxiolytic role for dimethyltryptamine.

作者信息

Jacob Michael S, Presti David E

机构信息

Department of Molecular and Cell Biology, University of California, Berkeley, CA 94720-3200, USA.

出版信息

Med Hypotheses. 2005;64(5):930-7. doi: 10.1016/j.mehy.2004.11.005.

DOI:10.1016/j.mehy.2004.11.005
PMID:15780487
Abstract

The presence of the potent hallucinogenic psychoactive chemical N,N-dimethyltryptamine (DMT) in the human body has puzzled scientists for decades. Endogenous DMT was investigated in the 1960s and 1970s and it was proposed that DMT was involved in psychosis and schizophrenia. This hypothesis developed from comparisons of the blood and urine of schizophrenic and control subjects. However, much of this research proved inconclusive and conventional thinking has since held that trace levels of DMT, and other endogenous psychoactive tryptamines, are insignificant metabolic byproducts. The recent discovery of a G-protein-coupled, human trace amine receptor has triggered a reappraisal of the role of compounds present in limited concentrations in biological systems. Interestingly enough, DMT and other psychoactive tryptamine hallucinogens elicit a robust response at the trace amine receptor. While it is currently accepted that serotonin 5-HT(2A) receptors play a pivotal role in the activity of hallucinogenic/psychedelic compounds, we propose that the effects induced by exogenous DMT administration, especially at low doses, are due in part to activity at the trace amine receptor. Furthermore, we suggest that endogenous DMT interacts with the TA receptor to produce a calm and relaxed mental state, which may suppress, rather than promote, symptoms of psychosis. This hypothesis may help explain the inconsistency in the early analysis of endogenous DMT in humans. Finally, we propose that amphetamine action at the TA receptor may contribute to the calming effects of amphetamine and related drugs, especially at low doses.

摘要

人体中强效致幻精神活性化学物质N,N-二甲基色胺(DMT)的存在困扰了科学家数十年。20世纪60年代和70年代对内源性DMT进行了研究,有人提出DMT与精神病和精神分裂症有关。这一假设是通过比较精神分裂症患者和对照受试者的血液及尿液得出的。然而,这项研究的大部分结果都没有定论,此后传统观点认为,痕量水平的DMT以及其他内源性精神活性色胺是无足轻重的代谢副产物。最近发现的一种G蛋白偶联的人类痕量胺受体引发了对生物系统中低浓度存在的化合物作用的重新评估。有趣的是,DMT和其他精神活性色胺致幻剂在痕量胺受体上会引发强烈反应。虽然目前人们认为5-羟色胺5-HT(2A)受体在致幻/迷幻化合物的活性中起关键作用,但我们认为,外源性给予DMT所诱导的效应,尤其是低剂量时的效应,部分归因于痕量胺受体的活性。此外,我们认为内源性DMT与TA受体相互作用,产生一种平静和放松的精神状态,这可能会抑制而非促进精神病症状。这一假设可能有助于解释早期对人体内源性DMT分析结果的不一致性。最后,我们提出苯丙胺在TA受体上的作用可能有助于解释苯丙胺及相关药物的镇静作用,尤其是低剂量时的作用。

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