Altered brain activity and functional connectivity after MDMA-assisted therapy for post-traumatic stress disorder

Singleton, Scott; Mithoefer, Michael C.; Hanlon, Colleen A.; George, Mark S.; Mithoefer, Annie; Mithoefer, Oliver; Coker, Allison; Yazar‐Klosinski, Berra; Emerson, Amy; Doblin, Rick; Kuceyeski, Amy

doi:10.3389/fpsyt.2022.947622

Cited by 12 publications

(7 citation statements)

References 112 publications

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“…In addition, the interpretation of the findings mentioned above are limited by the heterogeneous research methods used, including the types of tasks, as well as the way drugs were administered (e.g., intranasal versus oral administration). Other recent studies using ketamine 59, 60 or psychedelics 61 were not included as they did not compared patients with PTSD to groups of TEC or HCs. An important limitation is the exclusion of studies of PTSD patients showing severe comorbid disorders; although this would represent a more ecological group, it could also hinder the effects of the studied pharmacological agents on brain function solely associated with PTSD.…”

Section: Discussionmentioning

confidence: 99%

“…Other recent studies using ketamine 59,60 or psychedelics 61 were not included as they did not compared patients with PTSD to groups of TEC or HCs. An important limitation is the exclusion of studies of PTSD patients showing severe comorbid disorders; although this would represent a more ecological group, it could also hinder the effects of the studied pharmacological agents on brain function solely associated with PTSD.…”

Section: Limitationsmentioning

confidence: 99%

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Functional brain changes after pharmacological interventions in post-traumatic stress disorder: A systematic review of clinical trials

Lotfinia

Afshar

Yaseri

et al. 2023

Preprint

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BackgroundPosttraumatic stress disorder (PTSD) is a complex and heterogeneous mental health condition that can develop after exposure to a traumatic event. Clinical trials have used new pharmacological agents to treat PTSD, but their associated neural correlates remain unclear. The present systematic review aims to summarise the changes in brain function associated with the use these pharmacological agents in PTSD.MethodsClinical trials using functional magnetic resonance imaging (fMRI), either at rest or during the performance of tasks, were included if they compared the effects of pharmacological agents in patients with PTSD to either trauma-exposed controls or never exposed to trauma healthy controls.ResultsTwelve studies were included, of which eight used intranasal oxytocin, two used hydrocortisone, and one used Tolcapone. Oxytocin administration was associated with normalisation of functional connectivity between the ventromedial prefrontal cortex and amygdala, as well as enhanced the function of brain regions specifically involved in emotion processing (e.g., amygdala), working memory (e.g., dorsolateral prefrontal cortex), reward (putamen). Hydrocortisone did not influence brain function at rest or during the performance of an autobiographical memory task, while tolcapone was associated with increased function in frontal, parietal and striatal regions during the performance of an emotional working memory task.ConclusionsThis systematic review identified preliminary evidence for normalizing brain function after use of alternative pharmacological agents to first-line pharmacological treatments.

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Section: Discussionmentioning

confidence: 99%

Section: Limitationsmentioning

confidence: 99%

Functional brain changes after pharmacological interventions in post-traumatic stress disorder: A systematic review of clinical trials

Lotfinia

Afshar

Yaseri

et al. 2023

Preprint

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“…34 Meanwhile, neuroimaging studies on humans have discovered that MDMA decreases cerebral blood flow, a measure of brain activity, in the amygdala. 35 In addition, MDMA elevates functional connectivity between the amygdala and hippocampus 35,36 (note that the second study only found a trend-level effect), a region that supports the encoding and retrieval of memories. 37 Taken together, these findings from both humans and rodents seem to be consistent with the clinical observation that MDMA-assisted therapy facilitates access to traumatic memories that were previously repressed.…”

Section: Chemistry and Mechanism Of Actionmentioning

confidence: 95%

Psychedelic Therapy: A Primer for Primary Care Clinicians—3,4-Methylenedioxy-methamphetamine (MDMA)

Shinozuka,

Tabaac,

Arenas

et al. 2024

American Journal of Therapeutics

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Background: After becoming notorious for its use as a party drug in the 1980s, 3,4-methylenedioxy-methampetamine (MDMA), also known by its street names “molly” and “ecstasy,” has emerged as a powerful treatment for post-traumatic stress disorder (PTSD). Areas of Uncertainty: There are extensive data about the risk profile of MDMA. However, the literature is significantly biased. Animal models demonstrating neurotoxic or adverse effects used doses well beyond the range that would be expected in humans (up to 40 mg/kg in rats compared with roughly 1–2 mg/kg in humans). Furthermore, human samples often comprise recreational users who took other substances in addition to MDMA, in uncontrolled settings. Therapeutic Advances: Phase III clinical trials led by the Multidisciplinary Association for Psychedelic Studies (MAPS) have shown that MDMA-assisted psychotherapy has an effect size of d = 0.7–0.91, up to 2–3 times higher than the effect sizes of existing antidepressant treatments. 67%–71% of patients who undergo MDMA-assisted psychotherapy no longer meet the diagnostic criteria for PTSD within 18 weeks. We also describe other promising applications of MDMA-assisted psychotherapy for treating alcohol use disorder, social anxiety, and other psychiatric conditions. Limitations: Thus far, almost all clinical trials on MDMA have been sponsored by a single organization, MAPS. More work is needed to determine whether MDMA-assisted therapy is more effective than existing nonpharmacological treatments such as cognitive behavioral therapy. Conclusions: Phase III trials suggest that MDMA is superior to antidepressant medications for treating PTSD. Now that MAPS has officially requested the Food and Drug Administration to approve MDMA as a treatment for PTSD, legal MDMA-assisted therapy may become available as soon as 2024.

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“…Zudem wird davon ausgegangen, dass MDMA durch die Erhöhung der Konnektivität zwischen Amygdala und Hippocampus die Aufarbeitung traumatischer Erinnerungen im Rahmen des therapeutischen Prozesses begünstigen kann [7]. Eine fMRT-Studie konnte nach einer MDMA-gestützten Therapie eine Veränderung in Gehirnregionen nachweisen, welche mit Angst, PTBS und autobiografischen Gedächtnisprozessen assoziiert sind [8]. Zusätzlich sollte erwähnt werden, dass alle klinische Studien mit dem MDMA-Razemat durchgeführt worden sind.…”

Section: Neurobiologieunclassified

MDMA-gestützte Therapie

Bechtold,

Repantis

2024

Nervenheilkunde

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ZUSAMMENFASSUNGNeben den klassischen Psychedelika, z. B. Psilocybin, werden wieder vermehrt andere Substanzen wie 3,4-Methylendioxy-N-methylamphetamin (MDMA) erforscht. Das Entaktogen („innerlich berührend“) ist in den USA nur noch wenige Schritte von einer möglichen Zulassung zur Behandlung der posttraumatischen Belastungsstörung entfernt. Dieser Artikel soll einen Überblick über die Wirkung, den Einsatz im therapeutischen Setting sowie den Forschungsstand geben. Hierbei sollen insbesondere Sicherheitsaspekte der MDMA-gestützten Therapie beleuchtet werden. Zuletzt folgt ein Ausblick auf eine mögliche Zulassung und damit einhergehende offene Fragen, wie beispielsweise die Umsetzung in der klinischen Praxis. Auch die Notwendigkeit weiterer Studien wird diskutiert.

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Altered brain activity and functional connectivity after MDMA-assisted therapy for post-traumatic stress disorder

Cited by 12 publications

References 112 publications

Functional brain changes after pharmacological interventions in post-traumatic stress disorder: A systematic review of clinical trials

Functional brain changes after pharmacological interventions in post-traumatic stress disorder: A systematic review of clinical trials

Psychedelic Therapy: A Primer for Primary Care Clinicians—3,4-Methylenedioxy-methamphetamine (MDMA)

MDMA-gestützte Therapie

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