Repeated administration of MDMA causes transient down-regulation of
serotonin 5-HT2 receptors
by
Scheffel U, Lever JR, Stathis M, Ricaurte GA
Department of Radiology,
Johns Hopkins Medical Institutions,
Baltimore, MD
21205.
Neuropharmacology 1992 Sep; 31(9):881-93
ABSTRACT
The present study examined short- and long-term effects of MDMA
(3,4-methylene-dioxymethamphetamine) on serotonin (5-HT2 and 5-HT1c) receptors
in the brain of the rat. N1-Methyl-2-[125I]lysergic acid diethylamide
([125I]MIL) was used to label these receptors in vitro and in vivo. The
usefulness of [125I]MIL for in vivo detection of changes in 5-HT2 receptors was
confirmed in preliminary experiments in which rats were treated chronically with
mianserin (5 mg/kg, once daily for 10 days). Decreases in specific in vivo
binding of [125I]MIL, after treatment with mianserin were found to be of the
same magnitude as those determined by others, using in vitro methods. The MDMA
(8 doses; 5-20 mg/kg each) was administered to rats over a period of 4 days. At
various times after administration of the last dose of MDMA, the binding of
[125I]MIL was measured. Acutely, treatment with MDMA (20 mg/kg) reduced specific
in vivo binding of [125I]MIL in all regions of brain studied. For example, in
the frontal cortex, specific binding of [125I]MIL was decreased by 80% at 6 hr
and by 62% at 24 hr, after cessation of treatment with MDMA. Twenty-one days
after administration of MDMA however, the number of binding sites for [125I]MIL
was back to control levels. Reductions in in vivo binding of [125I]MIL in
frontal cortex were dependent on the dose of MDMA injected and were associated
with decreases in the number of binding sites for [125I]MIL (Bmax values) in
tissue homogenates of the same area. Autoradiographic studies of MDMA-treated
rats confirmed the decreased density of 5-HT2 receptors and also suggested that
the 5-HT1c receptor of the choroid plexus was not affected. These results
indicate that repeated administration of MDMA caused transient down-regulation
of 5-HT2 receptors in the brain of the rat. Further, they demonstrated that
[125I]MIL is a suitable radioligand for labeling 5-HT2 receptors, both in vitro
and in vivo. Once labeled with an appropriate radionuclide for SPECT (single
photon emission computed tomography) or PET (positron emission tomography), MIL
should prove useful for monitoring changes in the density of serotonin receptors
in the living mammalian brain.
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