Long-term effects of ‘ecstasy’ abuse on the human brain studied by FDG PET

Buchert, Ralph; Obrocki, Jost; Thomasius, Rainer; Väterlein, O; Petersen, Kay Uwe; Jenicke, L.; Bohuslavizki, K. H.; Clausen, M.

doi:10.1097/00006231-200108000-00007

Cited by 61 publications

(62 citation statements)

References 34 publications

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“…Although this study and some other studies showed that adverse effects of a low ecstasy dose are limited (Downing, 1986;Vollenweider et al, 1998), there are various factors (eg, poor metabolism, hypertension, young age, simultaneous use of other substances, environmental conditions) that might contribute to individual or situational vulnerability for acute adverse effects and long-term neurotoxicity of ecstasy (Buchert et al, 2001;Obrocki et al, 2002;Green et al, 2004;Segura et al, 2005). Therefore, it is not possible to state that incidental use of ecstasy is completely safe.…”

Section: Discussionmentioning

confidence: 64%

A Prospective Cohort Study on Sustained Effects of Low-Dose Ecstasy Use on the Brain in New Ecstasy Users

Win

Reneman

Jager

et al. 2006

Neuropsychopharmacol

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It is debated whether ecstasy use has neurotoxic effects on the human brain and what the effects are of a low dose of ecstasy use. We prospectively studied sustained effects (42 weeks abstinence) of a low dose of ecstasy on the brain in ecstasy-naive volunteers using a combination of advanced MR techniques and self-report questionnaires on psychopathology as part of the NeXT (Netherlands XTC Toxicity) study. Outcomes of proton magnetic resonance spectroscopy ( 1 H-MRS), diffusion tensor imaging (DTI), perfusion-weighted imaging (PWI), and questionnaires on depression, impulsivity, and sensation seeking were compared in 30 subjects (12M, 21.873.1 years) in two sessions before and after first ecstasy use (1.871.3 tablets). Interval between baseline and follow-up was on average 8.176.5 months and time between last ecstasy use and follow-up was 7.774.4 weeks. Using 1 H-MRS, no significant changes were observed in metabolite concentrations of N-acetylaspartate (NAA), choline (Cho), myo-inositol (mI), and creatine (Cr), nor in ratios of NAA, Cho, and mI relative to Cr. However, ecstasy use was followed by a sustained 0.9% increase in fractional anisotropy (FA) in frontoparietal white matter, a 3.4% decrease in apparent diffusion (ADC) in the thalamus and a sustained decrease in relative regional cerebral blood volume (rrCBV) in the thalamus (À6.2%), dorsolateral frontal cortex (À4.0%), and superior parietal cortex (À3.0%) (all significant at po0.05, paired t-tests). After correction for multiple comparisons, only the rrCBV decrease in the dorsolateral frontal cortex remained significant. We also observed increased impulsivity ( + 3.7% on the Barratt Impulsiveness Scale) and decreased depression (À28.0% on the Beck Depression Inventory) in novel ecstasy users, although effect sizes were limited and clinical relevance questionable. As no indications were found for structural neuronal damage with the currently used techniques, our data do not support the concern that incidental ecstasy use leads to extensive axonal damage. However, sustained decreases in rrCBV and ADC values may indicate that even low ecstasy doses can induce prolonged vasoconstriction in some brain areas, although it is not known whether this effect is permanent. Additional studies are needed to replicate these findings.

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Section: Discussionmentioning

confidence: 64%

A Prospective Cohort Study on Sustained Effects of Low-Dose Ecstasy Use on the Brain in New Ecstasy Users

Win

Reneman

Jager

et al. 2006

Neuropsychopharmacol

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“…A single study of resting metabolism in a large cohort of MDMA users (reviewed below) revealed significantly lower metabolic rate in bilateral caudate and putamen and left amygdala (Buchert et al 2001;Obrocki et al 2002) but these regions did not show gray matter alterations in the Cowan et al (2003) VBM study. Chang et al (2000), in their previously mentioned CBF study, detected a negative correlation between duration of MDMA use and global brain volume, but overall found no differences between MDMA users and controls in global brain volume, global cerebrospinal fluid (CSF), and percent CSF.…”

Section: Brain Volumementioning

confidence: 99%

“…Because basic research findings have associated MDMA exposure with specific long-term effects on 5-HT function, neuroimaging studies in human MDMA users have directly assayed components of the 5-HT system (McCann et al 1998;Semple et al 1999;Reneman et al 2000aReneman et al ,b, 2001aReneman et al , 2002cBuchert et al 2004;de Win et al 2004;McCann et al 2005), have assessed brain structure or function potentially altered as a secondary consequence of perturbed 5-HT function, or have examined brain regions implicated in MDMA-induced cognitive alterations (Chang et al 1999(Chang et al , 2000Obrocki et al 1999Obrocki et al , 2002Buchert et al 2001;Gamma et al 2001;Obergriesser et al 2001;Reneman et al 2001dReneman et al ,e, 2002dCowan et al 2003;Daumann et al 2003aDaumann et al ,b, 2004aDaumann et al ,b, 2005Jacobsen et al 2004;Moeller et al 2004;reviewed in Morgan 2000;Parrott 2001;Montoya et al 2002). This review examines currently available findings in the context of putative 5-HT toxicity and/or functional alterations with regard to brain structure and physiology.…”

Section: Introductionmentioning

confidence: 99%

Neuroimaging research in human MDMA users: a review

Cowan

2006

Psychopharmacology

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Rationale Determining whether, under what circumstances, and to what extent 3,4-methylenedioxymethamphetamine (MDMA) exposure produces chronic changes in human brain function is a critical public health issue. MDMA is a widely used recreational drug commonly sold as "Ecstasy". Because findings from the animal literature have indicated that specific dosage regimens of MDMA can produce longlasting alterations in serotonergic function, existing studies of MDMA effects in humans have examined brain serotonin (5-HT) transporters (5-HTT) and receptors or have examined brain structures or functions potentially affected by MDMA. Objectives The objectives of this review are to provide a background for interpreting human MDMA neuroimaging research, to examine existing neuroimaging data regarding the rationale for and limitations to human MDMA research, and to provide suggestions for improving the design and interpretation of future neuroimaging approaches. Results Of the existing neuroimaging studies in human MDMA users, few experimental designs have been replicated across different research groups. Only investigations employing nuclear imaging methods to assay brain 5-HTT levels have been replicated across methods and research laboratories. These studies have found reduced levels of the 5-HTT in recently abstinent MDMA users with some evidence for normalization of 5-HTT levels with prolonged abstinence. However, the sensitivity of these methods is unknown.Conclusions The current state of neuroimaging in human MDMA users does not permit conclusions regarding the long-term effects of MDMA exposure. Future study designs might benefit from improved sample homogeneity, increased length of MDMA abstinence, longitudinal study design, test-retest measures, serotonergic specificity, and multimodal approaches.

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“…Regions of interest (ROIs) were chosen according to ROIs described in humans [26,32]. Twelve ROIs were manually drawn on coronal sections: cerebellum, brain stem, thalamus, hippocampus, caudate-putamen, frontal cortex, amygdala, somatosensory cortex, visual cortex, auditory cortex, superior colliculus and whole brain.…”

Section: Animals Drug Administration and Experimental Protocolmentioning

confidence: 99%

“…Several markers for these systems (SERT, 5-HT 1A , 5-HT 2A ) are currently being investigated [24,25]. Buchert et al have proposed that MDMA-induced functional alterations of the serotonergic system may affect the glucose metabolism of cortical and subcortical structures [26]. However, possible effects of MDMA on regional brain glucose metabolism and blood glucose levels have received relatively little attention.…”

Section: Introductionmentioning

confidence: 99%

Effects of MDMA on blood glucose levels and brain glucose metabolism

Soto-Montenegro

Vaquero

Arango

et al. 2007

Eur J Nucl Med Mol Imaging

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Purpose This study was designed to assess changes in glucose metabolism in rats administered single or repeated doses of MDMA. Methods Two different experiments were performed: (1) A single-dose study with four groups receiving 20 mg/kg, 40 mg/kg, saline or heat, and (2) a repeated-dose study with two groups receiving three doses, at intervals of 2 h, of 5 mg/kg or saline. Rats were imaged using a dedicated small-animal PET scanner 1 h after single-dose administration or 7 days after repeated doses. Glucose metabolism was measured in 12 cerebral regions of interest. Rectal temperature and blood glucose were monitored. Results Peak body temperature was reached 1 h after MDMA administration. Blood glucose levels decreased significantly after MDMA administration. In the single-dose experiment, brain glucose metabolism showed hyperactivation in cerebellum and hypo-activation in the hippocampus, amygdala and auditory cortex. In the repeated-dose experiment, brain glucose metabolism did not show any significant change at day 7.Conclusion These results are the first to indicate that MDMA has the potential to produce significant hypoglycaemia. In addition, they show that MDMA alters glucose metabolism in components of the motor, limbic and somatosensory systems acutely but not on a long-term basis.

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Long-term effects of ‘ecstasy’ abuse on the human brain studied by FDG PET

Cited by 61 publications

References 34 publications

A Prospective Cohort Study on Sustained Effects of Low-Dose Ecstasy Use on the Brain in New Ecstasy Users

A Prospective Cohort Study on Sustained Effects of Low-Dose Ecstasy Use on the Brain in New Ecstasy Users

Neuroimaging research in human MDMA users: a review

Effects of MDMA on blood glucose levels and brain glucose metabolism

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