MDMA is certainly damaging after 25 years of empirical research: a reply and refutation of Doblin<i>et al</i>. (2014)

Parrott, Andrew C.

doi:10.1002/hup.2390

Cited by 26 publications

(22 citation statements)

References 87 publications

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“…While some concerns may remain about possible neurotoxicity or adverse cognitive effects associated with chronic abuse of ‘Ecstasy’ (Parrott, 2013, 2014), such effects have not been observed in individuals undergoing limited exposure to pure MDMA in controlled settings (Doblin et al, 2014). Nevertheless, ongoing clinical MDMA research should continue to address these concerns through rigorous monitoring of acute and persisting adverse effects as assessed in previous studies (Mithoefer et al, 2011).…”

Section: Discussionmentioning

confidence: 99%

Clinical applications of hallucinogens: A review.

Garcia-Romeu

Kersgaard

Addy³

2016

Experimental and Clinical Psychopharmacology

147

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Hallucinogens fall into several different classes, as broadly defined by pharmacological mechanism of action, and chemical structure. These include psychedelics, entactogens, dissociatives, and other atypical hallucinogens. Although these classes do not share a common primary mechanism of action, they do exhibit important similarities in their ability to occasion temporary but profound alterations of consciousness, involving acute changes in somatic, perceptual, cognitive, and affective processes. Such effects likely contribute to their recreational use. However, a growing body of evidence indicates that these drugs may have therapeutic applications beyond their potential for abuse. This review will present data on several classes of hallucinogens with a particular focus on psychedelics, entactogens, and dissociatives, for which clinical utility has been most extensively documented. Information on each class is presented in turn, tracing relevant historical insights, highlighting similarities and differences between the classes from the molecular to the behavioral level, and presenting the most up-to-date information on clinically oriented research with these substances, with important ramifications for their potential therapeutic value.

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Section: Discussionmentioning

confidence: 99%

Clinical applications of hallucinogens: A review.

Garcia-Romeu

Kersgaard

Addy³

2016

Experimental and Clinical Psychopharmacology

147

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“…There are other issues which need to be mentioned, although they have been debated more fully in two earlier articles (Parrott 2007;2013). For instance, one key question is the neurochemical model thought to underlie therapeutic improvement.…”

Section: Other Issues For Considerationmentioning

confidence: 98%

The Potential Dangers of Using MDMA for Psychotherapy

Parrott

2014

Journal of Psychoactive Drugs

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MDMA has properties that may make it attractive for psychotherapy, although many of its effects are potentially problematic. These contrasting effects will be critically reviewed in order to assess whether MDMA could be safe for clinical usage. Early studies from the 1980s noted that MDMA was an entactogen, engendering feelings of love and warmth. However, negative experiences can also occur with MDMA since it is not selective in the thoughts or emotions it releases. This unpredictability in the psychological material released is similar to another serotonergic drug, LSD. Acute MDMA has powerful neurohormonal effects, increasing cortisol, oxytocin, testosterone, and other hormone levels. The release of oxytocin may facilitate psychotherapy, whereas cortisol may increase stress and be counterproductive. MDMA administration is followed by a period of neurochemical recovery, when low serotonin levels are often accompanied by lethargy and depression. Regular usage can also lead to serotonergic neurotoxicity, memory problems, and other psychobiological problems. Proponents of MDMA-assisted therapy state that it should only be used for reactive disorders (such as PTSD) since it can exacerbate distress in those with a prior psychiatric history. Overall, many issues need to be considered when debating the relative benefits and dangers of using MDMA for psychotherapy.

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“…Based on two ecstasy sessions per year (one pill per session), the number of 27 MRDs in Scotland gives an estimated risk of MRD of 0.03% (one death per 3300 pills). Considering that in 2017 solely MDMA was involved in only three MRDs (NRS, 2018) (in 2014, the estimated risk of MDMA alone in 2017 (per session) is 0.003% (3/(2×45,000). Table 4 also depicts the yearly risk of fatalities per user related to chronic alcohol use in the UK (0.01-0.02%), and to heroin+morphine use (0.35%), cocaine use (0.05%) and amphetamine use (0.005%) in England and Wales.…”

Section: Ecstasy-related Fatal Incidentsmentioning

confidence: 99%

Fatal and non-fatal health incidents related to recreational ecstasy use

2020

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Background:The recreational drug ecstasy (3,4-methylenedioxymethamphetamine) is currently used world-wide. Severe (including fatal) health incidents related to ecstasy have been reported but a risk assessment of acute non-fatal and fatal ecstasy-related health incidents has never been performed. Methods: In the current risk assessment review, national data of non-fatal health incidents collected in the Netherlands were combined with the nationwide exposure to ecstasy, that is, last-year prevalence of ecstasy use. In addition, the annual number of ecstasy-related deaths in Great Britain (Scotland, Wales and England) was used to assess the risk of fatal ecstasy-related cases. Results: In the Netherlands, the estimated risk of a moderate to severe acute health incident following the use of ecstasy is one in 900 pills (0.11%), whereas for cocaine it is one in 1600 doses (0.06%) and for gamma-hydroxybutyrate one in 95 doses (1.05%). With respect to ecstasy-related deaths in Great Britain, the estimated risk of ecstasy alone per user is 0.01-0.06%, which is close to the range of the fatality risk in chronic alcohol users (0.01-0.02%), amphetamine users (0.005%) and cocaine users (0.05%), but much lower than that of opiate use (heroin and morphine: 0.35%). Conclusion:The current review shows that almost no data are available on the health risks of ecstasy use. The few data that are available show that ecstasy is not a safe substance. However, compared to opiates (heroin, morphine), the risk of acute ecstasy-related adverse health incidents per ecstasy user and per ecstasy use session is relatively low.

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MDMA is certainly damaging after 25 years of empirical research: a reply and refutation of Doblinet al. (2014)

Cited by 26 publications

References 87 publications

Clinical applications of hallucinogens: A review.

Clinical applications of hallucinogens: A review.

The Potential Dangers of Using MDMA for Psychotherapy

Fatal and non-fatal health incidents related to recreational ecstasy use

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