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MDMA-Assisted Therapy for Treatment-Resistant Posttraumatic Stress Disorder (PTSD) – One step further toward a patient-centered treatment pathway

S. Pratas Penedos, M.j. Freire, I. Fonseca, A. Franco, N. Ribeiro, L. Moreno, M.m. Magalhães, P.a. Afonso, I.m. Alves, L. Paulino, C. Ramos, M.m. Figueiredo, L. Madruga, A. Gamito

European Psychiatry June 1, 2022 Peer reviewed DOI: 10.1192/j.eurpsy.2022.1731

Summary

MDMA-assisted psychotherapy shows promise for treating refractory PTSD, with early clinical trials indicating a full remission of symptoms in 67% of patients two months post-treatment. The therapy appears to be safe, with no increase in suicidality or other adverse events reported. Mechanisms may involve neuroplasticity and emotional engagement facilitated by MDMA's effects on brain activity and neurotransmitter release. This approach could be crucial given the ongoing mental health challenges stemming from the COVID-19 pandemic.

Study at a glance

Design systematic review
Key finding A recently completed phase 3 trial reported full remission of PTSD symptoms in 67% of patients at 2 months.

Abstract

IntroductionPTSD is a chronic, debilitating condition with limited treatment efficacy. Accessing traumatic memories often leads to overwhelming distress, impacting treatment process. Current approved pharmacological treatments have exhibited small to moderate effects when compared with placebo. Evidence suggests 3,4,-methylene-dioxymethamphetamine(MDMA)-assisted psychotherapy as a viable option for refractory PTSD.ObjectivesComprehensive review of early clinical research, proposed mechanisms, safety and emerging therapeutic models.MethodsEligible studies will be identified through strategic search of MEDLINE.ResultsPre-clinical and imaging studies suggest memory reconsolidation and fear extinction as candidate psychological and neurological mechanisms, involving MDMA’s combined effects of increasing serotonergic activity, as well the release of oxytocin and brain-derived neurotrophic factor in key memory and emotional circuits. Resulting reduction in amygdala and insula activation and increasing connectivity between the amygdala and hippocampus may create a “tolerance window” of neuroplasticity for emotional engagement and reprocessing of traumatic memories during psychotherapy. Early clinical trials report impressive and durable reduction in PTSD symptoms, with a safety profile comparable to that of SSRIs. A recently completed randomized, double-blind, placebo-controlled phase 3 trial reported full remission of PTSD symptoms in 67% of patients at 2 months, with no increase in suicidality, cardiovascular events or abuse behavior. Emerging treatment models underline the importance of unmedicated therapeutic sessions for preparation for the experience and subsequent integration as essential for full benefit and safety of the clinical context.ConclusionsThe psychological impact associated with the COVID-19 pandemic is an reminder of the emotional and economic burden associated with PTSD. MDMA-assisted therapy may be a breakthrough approach meriting further multidisciplinary investment and clinical research.DisclosureNo significant relationships.

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