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March 2026

MDMA

What March 2026's 17 new studies found, synthesized from the papers below. All MDMA research →

The synthesis

Synthesized from 17 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.

Research on MDMA in March 2026 confirms that MDMA-assisted therapy reduces PTSD symptoms (moderate-to-large effect sizes) and increases response/remission rates, but the evidence is rated low certainty due to blinding challenges, expectancy effects, and high risk of bias. Preclinical studies show MDMA enhances fear extinction via prefrontal plasticity and reduces stress-induced alcohol intake in a genotype-dependent manner, while also revealing transient next-day anxiety and serotonin reductions in rats. A key caveat is that no new large-scale, well-controlled human trials were published in this period, and the FDA declined approval in 2024 citing insufficient evidence.

Confidence in the evidence

Low-Moderate
  • Two meta-analyses (27849, 25094) include 6-8 RCTs with 286-298 participants, showing consistent positive effects but low GRADE certainty due to high risk of bias and functional unblinding.
  • Preclinical studies (28514, 25183, 25152) provide mechanistic support but are animal models with small samples and mixed results (e.g., transient anxiety, no lasting recall effects).
  • No new large-scale, double-blind, active-comparator human trials were published in this period; the evidence base remains limited by small samples, lack of diversity, and expectancy confounds.
  • Reviews (25110, 27897, 24928) consistently highlight methodological limitations and caution against overinterpretation, reinforcing low-moderate confidence.
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.

MDMA-assisted therapy showed greater reduction in PTSD symptoms (Hedges' g = -0.71) and higher response (RR=1.35) and remission (RR=2.25) rates compared to control, but evidence was rated low certainty by GRADE.

systematic review and meta-analysis Sample size: 286

MDMA acutely reduced freezing during extinction but had no lasting effect on drug-free recall; it prevented shock-related increase in alcohol consumption only in iP rats, suggesting genotype-dependent effects.

preclinical (rat model)

MDMA-AT shows promising outcomes in RCTs with high response/remission rates, but key limitations include blinding challenges, lack of active comparators, inadequate safety monitoring, and limited generalizability.

review

MDMA-AT was associated with reductions in PTSD symptom severity (SMD=-1.19) and dissociative symptoms (SMD=-0.37), but most studies had high risk of bias and overall certainty was low.

systematic review and meta-analysis Sample size: 298

MDMA increased spine density and spinogenesis in prefrontal cortex, accelerated representational drift, and strengthened infralimbic cortex correlation with freezing suppression, suggesting enhanced neuroplasticity underlying extinction learning.

preclinical (mouse model)

Repeated low-dose MDMA caused transient next-day anxiety-like behavior and reduced serotonin in nucleus accumbens, but no effect on anhedonia-like behavior; effects resolved by day 15.

preclinical (rat model)

MDMA and ketamine IV have the greatest support for efficacy in PTSD, but caution is needed due to treatment expectancy effects and potential for inadequate blinding.

systematic review

Psychedelic research in pediatric populations is emerging but requires caution due to developmental vulnerabilities; MDMA is not yet studied in adolescents.

review

Integration of MDMA with psychoanalysis appeared to facilitate access to unconscious material and therapeutic progress in a single OCD case, but efficacy requires systematic investigation.

case report Sample size: 1

The paper argues that embedding MDMA in structured cognitive-behavioral protocols may blunt its transformative effects and that the patient-directed model should be preserved and refined.

theoretical/perspective

Commentary on critical considerations for clinical translation of MDMA-assisted psychotherapy in major depression.

commentary

Stereoselective analysis of MDMA and MDA in oral fluid showed faster elimination of S-(+)-MDMA (half-life 3.3h) vs R-(-)-MDMA (4.8h), enabling estimation of time since ingestion.

observational (pharmacokinetic) Sample size: 161

Amino acid prodrugs of MDMA (MDMA-Trp, MDMA-Lys, MDMA-Gly) are cleaved to MDMA in zebrafish, liver S9, and human urine, with unique biomarkers for MDMA-Trp; no cleavage in blood.

preclinical (zebrafish, human liver S9, human urine)

Corrigendum to a previous study on Withania somnifera influencing MDMA-induced effects in mice; no new findings.

corrigendum

Correction to a study on next-generation MDMA analogue SDMA; all results and conclusions remain accurate.

correction

Experts agreed that 150 mg free-base MDMA is a reasonable threshold for issuing public drug alerts, though thresholds cannot account for evolving trends.

qualitative Sample size: 15

History with eutylone attenuated eutylone-induced taste avoidance but did not affect MDMA- or cocaine-induced avoidance; eutylone history increased cocaine place preference but not MDMA's.

preclinical (rat model)

Points of agreement

  • MDMA-assisted therapy reduces PTSD symptoms with moderate-to-large effect sizes in meta-analyses of RCTs.
  • MDMA enhances fear extinction and prefrontal neuroplasticity in animal models.
  • Methodological limitations (blinding, expectancy, high risk of bias) are consistently noted across human studies.
  • MDMA's effects on alcohol consumption and anxiety are genotype- and sex-dependent in preclinical models.

Conflicts

  • One meta-analysis (27849) reports Hedges' g = -0.71 for PTSD symptoms, while another (25094) reports SMD = -1.19, possibly due to different inclusion criteria or analytic methods.
  • Preclinical studies show MDMA reduces stress-induced alcohol intake in iP rats but not Wistar rats (28514), and transient anxiety in rats (25152) contrasts with therapeutic anxiolytic effects in humans.
  • The patient-directed model (25131) argues against structured protocols, while other reviews (25110) call for integration with established trauma-focused therapies.

Gaps

  • No new large-scale, double-blind, active-comparator human trials published in this period.
  • Long-term durability of MDMA-AT effects beyond short-term follow-up is not established.
  • Safety and efficacy in adolescents and diverse populations remain unstudied.
  • Mechanisms of action (e.g., neuroplasticity, fear extinction) are primarily from animal models; human neural evidence is lacking.
  • Optimal dosing, number of sessions, and therapeutic model (structured vs. patient-directed) are not resolved.
Browse these studies in the library