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MDMA AND ITS STEREOISOMERS AS

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Title: MDMA AND ITS STEREOISOMERS AS


1
MDMA AND ITS STEREOISOMERS AS REINFORCERS IN
RHESUS MONKEYS Serotonergic Involvement
William Fantegrossi, Biopsychology Gail Winger
and James Woods, Pharmacology
Thomas Ullrich and Kenner Rice
2
(No Transcript)
3
  • MDMA exerts preferential effects on central 5-HT
    systems
  • blocks reuptake mechanisms
  • stimulates 5-HT release

4
  • Racemic MDMA elicits conditioned place preference
  • in rats (Marona-Lewicka et al., 1996)
  • Racemic MDMA decreases the threshold for
    rewarding
  • electrical stimulation of the brain in rats
  • (Hubner et al., 1987)
  • Racemic MDMA has twice been shown to act as a
  • reinforcer in intravenous self-administration
  • paradigms in primates (Beardsley et al., 1986
  • Lamb and Griffiths, 1987)
  • The reinforcing effects of the stereoisomers
    have
  • not been previously assessed.

5
  • Drug discrimination studies suggest that the
  • MDMA stereoisomers may have different
  • subjective effects
  • the discriminable cue of S()-MDMA may be
  • more likely to be reported as dopaminergic
  • than serotonergic
  • (generalizes to amphetamine, not mescaline)
  • the stimulus properties of R(-)-MDMA may be
  • more likely to be reported as serotonergic
  • than dopaminergic
  • (generalizes to mescaline, not amphetamine)
  • (Glennon et al., 1988 Baker et al., 1995 Baker
    and Taylor, 1997.)

6
  • Schedule was FR10 TO 1 min.
  • Total session length (including time outs) was 60
    min.
  • Two sessions run per day.
  • To aggregate data across all four experimental
    animals, data were normalized to percent of
    cocaine control responding, and infusions of 0.01
    mg/kg/inj cocaine were set to 100 of control.

7
Racemic MDMA and its stereoisomers are
self-administered by rhesus monkeys
8
Racemic MDMA has high affinity for 5-HT
transporters and 5-HT2 serotonin receptors
(Battaglia et al., 1988.) (-)-MDMA has higher
affinity for post-synaptic 5-HT
receptors ()-MDMA has higher affinity for 5-HT
transporters (Battaglia, personal
communication, 2001.)
9
Ketanserin is 10- to 30-fold more selective for
5-HT2A than for 5-HT2C
MDL 100907 is 100- to 300-fold more selective
for 5-HT2A than for 5-HT2C
10
  • 5 MDMA-naïve monkeys were used in these
    antagonism studies.
  • The schedule was a multiple-dose procedure
    allowing self-administration of 4 doses of drug
    per session.
  • FR30 TO45 sec, for 20 inj or 25min, with a 10 min
    TO between dose components. Session length is
    approximately 130 minutes.
  • Pretreatments were administered IM 15-min prior
    to start of session.

11
Ketanserin shifts the ascending limb, but not
the descending limb, of the cocaine
self-administration curve
12
A large dose of MDL 100907 is required to
suppress cocaine self-administration
13
Ketanserin down-shifts the ()-MDMA
self-administration curve
14
MDL 100907 right-shifts the ascending limb of the
()-MDMA self-administration curve
15
Ketanserin abolishes responding for (-)-MDMA at a
dose that does not affect cocaine-maintained
behavior
16
MDL 100907 abolishes responding for (-)-MDMA at a
dose that does not affect cocaine-maintained
behavior
17
  • DISCUSSION AND CONCLUSIONS
  • Drugs with serotonergic mechanisms of action
  • rarely maintain self-administration
  • Agonists like mescaline and DOM, SSRIs like
  • alaproclate, clomipramine, and fluoxetine,
  • and releasers like fenfluramine all fail to
  • engender significant behavior.

18
  • DISCUSSION AND CONCLUSIONS
  • However, racemic MDMA and both
  • stereoisomers are effective reinforcers
  • in rhesus monkeys.
  • The reinforcing effects of other methylenedioxy
  • analogues of amphetamine (MDE, MBDB, etc.)
  • therefore deserve further study

19
  • DISCUSSION AND CONCLUSIONS
  • Stimulation of 5-HT2A receptors appears to be
  • an integral component to the reinforcing
    effects
  • of MDMA, but not to those of cocaine.
  • 5-HT2A receptors may be particularly important
  • in the reinforcing effects of (-)-MDMA.

20
Acknowledgements
  • Expert technical assistance was provided by Amy
    Foster, Debbie Huntzinger, Sarah Pilkington, and
    Jolan Terner.
  • These studies were supported by USPHS Grants
    DA09161 and DA05923.
  • Thanks to ISGIDAR for the travel award!

21
Preliminary PET Scan Results
22
Antagonist effects are probably not
rate-dependent - 1
23
Antagonist effects are probably not
rate-dependent - 2
24
Antagonist effects are probably not
rate-dependent - 3
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