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June 2026

MDMA

What June 2026's 16 new studies found, synthesized from the papers below. All MDMA research →

The synthesis

Synthesized from 16 studies in the library · AI-generated, grounded in the abstracts below

Found by searching the library for MDMA, ecstasy, molly, methylenedioxymethamphetamine, then ranked by relevance.

In June 2026, MDMA research showed that a booster dose prolongs subjective effects without increasing peak intensity, and that MDMA-assisted therapy produced large reductions in social anxiety symptoms in an open-label trial. A systematic review and meta-analysis confirmed a moderate-to-large effect of MDMA-assisted psychotherapy for PTSD, but a commentary highlighted unresolved challenges including blinding difficulties, expectancy effects, and limited mechanistic clarity. The evidence is promising but constrained by small samples, open-label designs, and unresolved methodological issues.

Confidence in the evidence

Low-Moderate
  • One small (N=25) double-blind crossover study on booster dosing provides controlled evidence for effect prolongation.
  • One small (N=20) open-label wait-list controlled trial for social anxiety shows large effect but lacks blinding and placebo control.
  • A systematic review of 11 RCTs (N=358) supports MDMA for PTSD with moderate-to-large effect and low heterogeneity, but a commentary notes major limitations in blinding and expectancy.
  • Several studies are preclinical, qualitative protocols, or psychometric validations, not directly addressing clinical efficacy.
  • The evidence base is limited by small sample sizes, open-label designs, and lack of long-term durability data.
How we rate confidence

Confidence reflects the strength of the underlying evidence, not whether the result is favorable. It weighs the number and size of studies, their design (randomized trials count for more than observational or single-case work), how consistently they point the same way, and their risk of bias.

Tiers run from Insufficient to High. High is rare in this field: small, early, or open-label studies land lower even when their direction is encouraging.

Evidence by study

Direction is each study's finding relative to your question: Supports, Opposes, No effect, Mixed, or Unclear.

A booster dose of MDMA prolonged subjective drug effects compared to a single dose (5.6 vs 4.6 hours) without increasing peak effects, but acute and subacute adverse effects were more common.

double-blind, randomized, placebo-controlled, crossover study · Sample size: 25

MDMA-assisted therapy produced a large reduction in social anxiety symptoms (mean difference -43.3 on LSAS, Hedge's g=2.8) compared to waitlist, with no serious adverse events.

randomized, open-label, wait-list controlled trial · Sample size: 20

MDMA-assisted psychotherapy demonstrated a significant moderate-to-large reduction in PTSD symptom severity with negligible heterogeneity, and participants were more likely to achieve clinical response and loss of PTSD diagnosis.

systematic review and meta-analysis · Sample size: 358

The commentary acknowledges MDMA's therapeutic promise but emphasizes unresolved challenges including blinding difficulties, expectancy effects, absence of active comparators, limited mechanistic clarity, and safety monitoring concerns.

commentary

Trait negative emotionality showed a trend-level association with greater MDMA-induced peak friendliness change and predicted oxytocin release after accounting for sex, but findings are preliminary due to small sample.

within-subject, double-blind, placebo-controlled secondary analysis · Sample size: 30

Weekend ecstasy use was associated with lower Monday mood, but this effect was largely accounted for by increased time in bed, suggesting recovery-related behaviors rather than direct drug effects.

retrospective analysis of daily diary reports · Sample size: 17

MDMA was predominantly consumed in recreational contexts (80.6% past-year prevalence), with low adherence to recommended dose intervals (27.5%) and frequent co-use with alcohol and cannabis.

mixed-methods survey and qualitative · Sample size: 1412

This protocol describes an open-label qualitative study to investigate psychological mechanisms of MDMA-assisted psychotherapy, but no results are reported.

protocol for qualitative mechanistic study · Sample size: 25

MDMA inhibited CYP2D6 in rats, with concentration-dependent effects; inhibition was observed at 1 hour but not at 1 week or 1 month at therapeutic concentrations, but persisted at saturated concentrations.

preclinical animal study · Sample size: 32

MDMA did not exacerbate heroin withdrawal-induced weight loss, and showed region-specific effects on astrocytic activation in the basolateral amygdala, suggesting interactive effects with heroin.

preclinical animal study

MDA was detected in 31.1% of seized ecstasy samples, surpassing MDMA (25.6%), with a marked rise after 2020, indicating a shift in ecstasy use patterns in Brazil.

forensic and toxicological analysis

A field-portable device using deep learning achieved 98% accuracy in classifying MDMA tablet dosage brackets and 96% accuracy for cocaine/ketamine purity estimation.

device development and validation study · Sample size: 62

The French version of the 5D-ASC questionnaire showed good internal consistency (α=0.95) and acceptable fit for the 11-subscale structure, supporting its use in francophone research.

psychometric validation study · Sample size: 777

This article discusses blinding, expectancy, and the active placebo paradox in MDMA research, but no empirical data are reported.

theoretical/commentary

This article discusses clinical and non-clinical use of MDMA, but no empirical data are reported.

theoretical/commentary

The VA has launched a clinical trial of MDMA-assisted therapy for PTSD and alcohol use disorder, but no results are reported.

news release

Points of agreement

  • MDMA-assisted therapy shows promising efficacy signals for PTSD and social anxiety in clinical trials.
  • Booster dosing prolongs subjective effects of MDMA without increasing peak intensity.
  • Recreational MDMA use is associated with low adherence to harm reduction practices and frequent polysubstance use.
  • Methodological challenges such as blinding difficulties and expectancy effects are acknowledged across multiple sources.

Conflicts

  • The systematic review reports a moderate-to-large effect for MDMA in PTSD, while the commentary emphasizes that the evidence base is constrained by major limitations including blinding and expectancy.
  • Laboratory studies find minimal residual mood effects, but naturalistic data show a Monday mood decline that may be driven by recovery behaviors rather than direct drug effects.

Gaps

  • Long-term durability of treatment gains from MDMA-assisted therapy is not established.
  • Mechanistic understanding of MDMA's therapeutic effects remains limited, especially psychological and relational processes.
  • Safety data are heterogeneous and insufficiently characterized, particularly for long-term outcomes.
  • Blinding integrity and expectancy effects are not adequately addressed in most trials.
  • Generalizability is limited by predominantly white, non-clinical samples in many studies.
  • Dose optimization and the role of booster doses in clinical settings require further investigation.
Browse these studies in the library