Abstract
As part of a project to develop treatment agents for cocaine abuse, (±)-threo-methylphenidate (TMP) and 11 analogs were characterized biochemically and behaviorally to assess their potential as anti-cocaine medications. The compounds contained aryl and/or nitrogen substitutions, and/or replacement of the ester function by an alcohol or ether. All of the analogs, except for theN-methyl-substituted compounds, showed increased inhibitory potency against3H-(−)-2-β-carbomethoxy-3-β-(4-fluorophenyl)tropane 1,5-naphthalenedisulfonate ([3H]WIN 35,428) ([3H]WIN) binding to the dopamine transporter, compared with TMP. In general, parallel results were obtained for inhibition of [3H]dopamine ([3H]DA) uptake. Although compounds with N-substitutions were proportionally less potent at blocking DA uptake than WIN binding (compared with the unsubstituted compounds), one such compound that was 6-fold more potent against [3H]WIN binding than [3H]DA uptake did not attenuate inhibition by cocaine of synaptosomal [3H]DA transport. The compounds were significantly less potent in displacing [3H]citalopram binding from the serotonin transporter. In cocaine discrimination studies in rats, all but two of the analogs (bothN-substituted) completely generalized with the cocaine stimulus. Robust positive correlations were observed between potency in the drug discrimination assay and activity at the dopamine transporter, but not the serotonin transporter. When tested for their ability to alter cocaine discrimination, four of the analogs (three of which hadN-substitutions and shallow dose-response curves as cocaine substitutes) actually enhanced cocaine discrimination, often at combined doses of cocaine and test compound that were inactive when given separately. Taken together, the results suggest that TMP analogs may have potential as substitution therapies for the treatment of cocaine abuse.
Footnotes
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↵1 Current address: Instructor, Division of Natural Sciences and Mathematics, Macon State College, Macon, GA.
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Supported by a grant from the National Institute on Drug Abuse (DA06305) to H.M.D., M.M.S., and S.G.H., and by a Senior Scientist Award (DA00008) to S.G.H.
- Abbreviations:
- DAT
- dopamine transporter
- DR
- discrimination ratio
- [3H]CIT
- [3H]citalopram
- [3H]DA
- [3H]dopamine
- [3H]WIN
- [3H]WIN 35,428,3H-(−)-2-β-carbomethoxy-3-β-(4-fluorophenyl)tropane 1,5-naphthanedisulfonate
- SERT
- serotonin transporter
- 3CTMP
- (±)-threo-3-chloromethylphenidate
- 3CTMPNMe
- (±)-threo-N-methyl-3-chloromethylphenidate
- 4ATMP
- (±)-threo-4-aminomethylphenidate
- 4FTMP
- (±)-threo-4-fluoromethylphenidate
- 4MeTMP
- (±)-threo-4-methylphenidate
- 4MeTMPNMe
- (±)-threo-N-methyl-4-methyl-methylphenidate
- 3,4CTMP
- (±)-threo-3,4-dichloromethylphenidate
- TMP
- (±)-threo-methylphenidate
- TMPNMe
- (±)-threo-N-methyl-methylphenidate
- TMPNBn
- (±)-threo-N-benzyl-methylphenidate
- TROHNBn
- (±)-threo-N-benzylritalinol
- TROMeNBn
- (±)-threo-N-benzylritalinol methyl ether
- ANOVA
- analysis of variance
- Received October 29, 2001.
- Accepted January 10, 2002.
- The American Society for Pharmacology and Experimental Therapeutics
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