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- From: lamont@hyperreal.com (Lamont Granquist)
- Newsgroups: alt.drugs,alt.psychoactives,sci.med.psychobiology
- Subject: MDMA Neurophamacology
- Date: 23 Jun 1994 09:26:59 GMT
- Message-ID: <2ubkh3$kb5@news.u.washington.edu>
-
- Check this out for accuracy -- ignore spelling errors, i haven't bothered
- to run it through a spell-checker yet, which should catch them...
-
- If anyone has any suggestions of good introductions to neurpharm for the
- "public" along the lines of Synder's book, i'd appreciate it.
-
- MDMA Neuropharmacology
-
- MDMA is primarily a seritonergic (5-HTergic) drug. Serotonin
- (5-hydroxytrytamine, 5-HT) is one of the major neurotransmitters in the
- brain, and is synthesized from tryptophan through the intermediate
- 5-hydroxytryptophan. It is synthesized in 5-HT neurons, and stored in
- synaptic vesicles. These vesicles release their 5-HT into the synaptic
- cleft in response to the firing of the 5-HT neurons. In the synaptic
- cleft the 5-HT neurotransmitter excerts its action on both pre- and
- post- synaptic receptor sites (sites on the 5-HT neuron itself, and on
- the neuron which it is communicating with.) 5-HT is then taken back
- into the 5-HT neuron via the synaptic membrane 5-HT transporter (aka
- "reuptake pump"), where it is again stored in the synaptic vesicles.
- 5-HT is metabolized primarily by monoamine oxidase (MAO) into
- 5-hydroxyindileacetic acid (5-HIAA).
- Serotonin is thought to be responsible for many psychological (and
- physiological) states including mood and sleep. It has been particularly
- associated with major depression and obsessive compulsive disorder, and
- drugs to treat these disorders tend to effect 5-HT (although things are
- not quite clear-cut).
- MDMA blocks the reuptake of 5-HT, similarly to SSRI (serotonin
- specific reuptake inhibiting) anti-depressants such as fluoxetine (Prozac),
- sertraline, and paroxetine. Unlike those drugs, however, MDMA appears
- to enter the neuron, either through passive diffusion or directly
- through the reuptake transporter, and causes the release of 5-HT. This
- release is calcium-independent (i.e. independent of the firing of the
- 5-HT neuron) and appears to come from cytoplasmic stores rather than
- from synaptic vesicles. The released 5-HT then enters the synaptic cleft
- through the 5-HT transporter. MDMA thus acts on 5-HT similarly to the way
- amphetamines act on dopamine.
- It is thought that this efflux of 5-HT into the synaptic cleft, and
- the subsequent action of this 5-HT on pre- and post- synaptic binding
- sites is central to MDMA's neuropharmacology. MDMA, however, has
- micromolar potency for the serotonin 5-HT2, muscarinic M1, alpha-2 adrenergic
- and histamine H1 receptors. Agonist (stimulation rather than blocking)
- properties at the 5-HT2 receptor have been found to fairly universally be
- associated with "classical" psychedelic drugs such as LSD, psilocybin and
- mescaline. It is possible that some of MDMA's "psychedelic" effect occurs
- because of interactions with this receptor. The alpha-2 adrenergic receptor
- may be associated with some of the carciovascular effects of MDMA.
- MDMA also releases dopamine which may be central to both its
- psychological action and to its neurotoxicity in animal studies. Pre-
- treatment of an animal with a drug which blocks dopamine release will
- also block MDMA neurotoxicity. Also, serotonin specific releasing agents
- which are non-dopaminergic have been synthesized and been found to be
- devoid of MDMA's neurotoxicity in animals, they have also been found to
- be devoid of MDMA's psychological effects. MDMA tends to indirectly
- *inhibit* the firing and release of dopamine in nigrostriatal dopamine
- neurons (neurons projecting from the substantia nigra to the striatum) due
- to local 5-HT release.
- MDMA doses of 20mg/kg in animals can reduce levels of tryptophan
- hydroxylase, which is the rate-limiting enzyme in 5-HT synthesis. It is
- thought that this occurs because of oxidative stress which MDMA places
- on the neuron. This oxidative stress might occur through several
- possible channels (the metabolism of MDMA into a toxic Quinoid, 5-HT
- derived toxins, 5-HT mediated cellular events, or temporary inhibition
- of monoamine oxidase) and the exact mechanism is presently unknown. It is
- thought that this oxidative stress also leads to the neurodegenerative
- destruction of 5-HT axons which is observed to occur with large doses of
- MDMA in animals. Anti-oxidants, anti-dopaminergic agents, agents which
- block intracellular calcium increases and pre- or post- treatment (up to
- 6 hours) with fluoxetine all block MDMA's neurotoxicity. Research
- ontinues on the exact mechanism of MDMA-induced toxicity.
- In summary, MDMA effects 5-HT similarly to the way that amphetamines
- effect dopamine, by inhibiting the reuptake and causing the release of 5-HT.
- This effect is somewhat similar to the effect that SSRI anti-depressant
- drugs have. It also effects the 5-HT2 (psychedelic) and alpha-2 adrenergic
- (cardiovascular) receptor sites. Also, its effects on dopamine appear, at
- this point, to be involved both with its neurotoxicity and psychological
- effects. For more information, see:
-
- Rattray-M. "Ecstasy: towards an understanding of the biochemical
- basis of the actions of MDMA." Essays in Biochemistry. 26:77-87.
- 1991.
-
- And for general info:
-
- Synder, Solomon H. "Drugs and the Brain." Scientific American Books.
- 1986. (slightly out of date, but a good introduction).
-
- Cooper-JR, Bloom-FE, Roth-RH. "The Biochemical Basis of Neuro-
- Pharmacology." Oxford Uniersity Press. 1991 (6th ed). (the bible
- for grad students)
-
- --
- Lamont Granquist (lamont@hyperreal.com)
- "And then the alien anthropologists - Admitted they were still perplexed - But
- on eliminating every other reason - For our sad demise - They logged the only
- explanation left - This species has amused itself to death" -- Roger Waters
-
-
-
