The Pharmacology and Clinical Pharmacology of 3,4-methylenedioxymethamphetamine (MDMA, "ecstasy")

Overview

Journal Pharmacol Rev

Specialty Pharmacology

Date 2003 Jul 19

PMID 12869661

Citations 329

Authors

A Richard Green

Annis O Mechan

J Martin Elliott

Esther OShea

M Isabel Colado

Affiliations

Soon will be listed here.

Abstract

The amphetamine derivative (+/-)-3,4-methylenedioxymethamphetamine (MDMA, ecstasy) is a popular recreational drug among young people, particularly those involved in the dance culture. MDMA produces an acute, rapid enhancement in the release of both serotonin (5-HT) and dopamine from nerve endings in the brains of experimental animals. It produces increased locomotor activity and the serotonin behavioral syndrome in rats. Crucially, it produces dose-dependent hyperthermia that is potentially fatal in rodents, primates, and humans. Some recovery of 5-HT stores can be seen within 24 h of MDMA administration. However, cerebral 5-HT concentrations then decline due to specific neurotoxic damage to 5-HT nerve endings in the forebrain. This neurodegeneration, which has been demonstrated both biochemically and histologically, lasts for months in rats and years in primates. In general, other neurotransmitters appear unaffected. In contrast, MDMA produces a selective long-term loss of dopamine nerve endings in mice. Studies on the mechanisms involved in the neurotoxicity in both rats and mice implicate the formation of tissue-damaging free radicals. Increased free radical formation may result from the further breakdown of MDMA metabolic products. Evidence for the occurrence of MDMA-induced neurotoxic damage in human users remains equivocal, although some biochemical and functional data suggest that damage may occur in the brains of heavy users. There is also some evidence for long-term physiological and psychological changes occurring in human recreational users. However, such evidence is complicated by the lack of knowledge of doses ingested and the fact that many subjects studied are or have been poly-drug users.

Citing Articles

Licit use of illicit drugs for treating depression: the pill and the process.

Torrado Pacheco A, Moghaddam B J Clin Invest. 2025; 134(12).

PMID: 40047885 PMC: 11178541. DOI: 10.1172/JCI180217.

MDMA for treatment of PTSD and neurorehabilitation in military populations.

Dunn W, Bershad A, Krantz D, Vermetten E NeuroRehabilitation. 2024; 55(3):357-368.

PMID: 39331116 PMC: 11612990. DOI: 10.3233/NRE-230270.

Design and methodology of the first open-label trial of MDMA-assisted therapy for veterans with post-traumatic stress disorder and alcohol use disorder: Considerations for a randomized controlled trial.

Eaton E, Capone C, Gully B, Brown Z, Monnig M, Worden M Contemp Clin Trials Commun. 2024; 41:101333.

PMID: 39262902 PMC: 11387902. DOI: 10.1016/j.conctc.2024.101333.

Bioisosteric analogs of MDMA: Improving the pharmacological profile?.

Alberto-Silva A, Hemmer S, Bock H, da Silva L, Scott K, Kastner N J Neurochem. 2024; 168(9):2022-2042.

PMID: 38898705 PMC: 11449655. DOI: 10.1111/jnc.16149.

Effect of MDMA-assisted therapy on mood and anxiety symptoms in advanced-stage cancer (EMMAC): study protocol for a double-blind, randomised controlled trial.

Bhagavan C, Glue P, Evans W, Reynolds L, Turner T, King C Trials. 2024; 25(1):336.

PMID: 38773523 PMC: 11110200. DOI: 10.1186/s13063-024-08174-x.