Major Depressive Disorder (MDD)Depressive DisordersAnxiety DisordersHealthy VolunteersSafety & Risk ManagementDMTPlacebo

Safety, tolerability and subjective effects of vaporized N,N-Dimethyltryptamine: A randomized double-blind clinical trial

This first RCT (n=25) of vaporised DMT (60mg) demonstrated that DMT significantly increased subjective experience measures while causing only transient, safe physiological changes and predominantly mild adverse events. This suggests that inhaled DMT is safe, well-tolerated, and effective at inducing profound altered states of consciousness. Significant correlations were observed between physiological responses and subjective experiences.

Authors

  • Fernanda Palhano-Fontes
  • Draulio Araújo
  • Nathalia Galvão-Coelho

Published

European Neuropsychopharmacology
individual Study

Abstract

Vaporized N,N-Dimethyltryptamine (DMT) has a short duration and simple application, prompting this technique as a new approach for psychedelics’ clinical use. Building on our initial dose-ascending studies and addressing potential confounding effects of dosing order, this study is the first to evaluate inhaled DMT in a randomized, placebo-controlled, double-blind design. Given DMT’s therapeutic potential, we aimed to assess its safety, tolerability, and subjective effects compared to an active placebo. Twenty-five healthy participants completed two treatment sessions, receiving DMT (60 mg) or active placebo (0.6 mg DMT) in a crossover design with a two-hour interval between the sessions. Subjective experiences were evaluated using measures of intensity and valence, the Five Dimensions of Altered States of Consciousness Questionnaire (5D-ASC), the Hallucinogen Rating Scale (HRS), and the Mystical Experiences Questionnaire (MEQ). Physiological parameters were monitored, including systolic and diastolic blood pressure, heart rate, respiratory rate, and peripheral oxygen saturation. Biological responses were analysed through various biochemical biomarkers. Adverse events were recorded. Compared to placebo, DMT significantly increased subjective measures of intensity, as well as most 5DASC, HRS, and MEQ factors, except for 5D-ASC Anxiety, Audio-Visual Synaesthesia and Vigilance Reduction subscales. DMT transiently increased physiological parameters within safe limits. Biochemical changes were not clinically relevant. The adverse events were predominantly mild and transient. Physiological increases were significantly correlated with subjective experiences, providing insights into the interaction between physiological responses and altered states of consciousness. Our findings suggest that inhaled DMT is safe, well-tolerated, and capable of inducing profound altered states of consciousness.

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Research Summary of 'Safety, tolerability and subjective effects of vaporized N,N-Dimethyltryptamine: A randomized double-blind clinical trial'

Editorial

βBlossom's Take

This trial is useful because it gives vaporised DMT a proper randomised, blinded safety test rather than relying on open-label dose-ascending studies. The acute state is brief but the data are clearer for it, and that makes the paper a solid reference point for later work on dosing, tolerability, and whether rapid-onset DMT can be handled safely in a clinical setting.

Introduction

Major Depressive Disorder (MDD) is a leading contributor to global disease burden and is frequently accompanied by maladaptive cognitive schemas—pessimistic beliefs about the self and future—that are thought to sustain depressive symptoms. Cognitive behavioural therapy combined with selective serotonin reuptake inhibitors (SSRIs) is a common first-line approach, and previous studies have shown that psychedelic-assisted interventions, when delivered with psychological support, can produce rapid and sustained reductions in depressive symptoms. A mechanistic hypothesis addressed in the literature is that classic psychedelics acting at the serotonin 2A receptor (5-HT2A R) may temporarily increase neural and psychological plasticity, creating a window for adaptive revision of entrenched negative cognitive biases.

Methods

Henry and colleagues conducted a two-arm, randomized controlled trial comparing psilocybin therapy with escitalopram in patients with MDD. Fifty-nine participants were randomised and matched for age, gender and education, with 30 allocated to the psilocybin arm and 29 to the escitalopram arm. Trial registration and ethics approvals were obtained and all participants provided written informed consent.

Results

The main cognitive-bias outcomes showed divergent patterns across treatments. On the self-report Life Orientation Test–Revised (LOT-R), a time × condition interaction was reported (F(1,57)=15.89, p=0.0002); post-hoc tests indicated a large and significant increase in optimism scores in the psilocybin group at six weeks (effect size reported as d=1.1), with no change following escitalopram. The Prediction of Future Life Events (POFLE) behavioural task produced a significant main effect of time (F(1,99)=20.86, p<0.0001) but no overall condition effect. Further analyses found a time × condition interaction for forecasting of desirable events (F(1,44)=7.93, p=0.007), although there was a baseline between-group difference in forecasting of desirable events (psilocybin group more pessimistic at baseline). After adjusting for baseline scores via ANCOVA, no significant between-group difference in change was observed; nevertheless, within-condition tests showed a significant increase in optimism for desirable events after psilocybin. Conversely, escitalopram produced a within-condition improvement in pessimism for undesirable events (M diff ≈0.07, SE≈0.03, p=0.018, d≈0.5).

Discussion

Henry and colleagues interpret the findings as indicating that two high-dose psilocybin sessions, delivered with psychological support, produced broader and larger reductions in negative cognitive bias than six weeks of escitalopram. Specifically, psilocybin was associated with increased self-reported optimism (LOT-R), improved forecasting for desirable future events (POFLE, within-condition), and reductions across all subscales of dysfunctional attitudes (DAS-24). Escitalopram produced improvements in depressive symptoms and in the achievement subscale of the DAS-24 and reduced pessimism for undesirable events, which the authors discuss in relation to possible SSRI-associated affective blunting. The investigators link their results to serotonergic mechanisms—particularly 5-HT2A R-mediated plasticity—and to predictive-processing frameworks that posit psychedelics reduce the precision-weighting of entrenched predictive models, thereby enabling revision of maladaptive beliefs. The discussion emphasises the role of psychological support (set and setting, therapeutic alliance, music, preparatory and integration sessions) in shaping outcomes and notes that different models of psychotherapy delivery exist in the field.

Conclusion

The authors conclude that psilocybin therapy produced more robust and comprehensive improvements in measures of negative cognitive bias in patients with MDD than a six-week course of escitalopram, supporting further investigation of safety and efficacy at larger scale.

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