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Vol. 288, Issue 2, 752-758, February 1999
Department of Molecular and Medical Pharmacology, UCLA School of
Medicine, Los Angeles, California (W.P.M., A.K.C., D.S.); and
Department of Psychiatry, UCSD School of Medicine, San Diego,
California (R.K., D.S.S.)
This study evaluated whether the caudate-putamen dopamine response that
has been observed after deprenyl administration could be attributed
exclusively to metabolically generated l-methamphetamine (l-MeAmp). Brain and plasma levels of deprenyl and
l-MeAmp were measured after deprenyl (10 mg/kg s.c.)
from 10 to 60 min in conscious rats. Peak caudate-putamen levels were
observed for deprenyl (15 nmol/g) at 10 min and for
l-MeAmp (3 nmol/g) at 30 min. In a parallel study,
l-MeAmp metabolism was evaluated. After
l-MeAmp (20 mg/kg s.c.), metabolite levels remained low
relative to those of the parent compound: l-amphetamine,
~5 to 12%; and
para-hydroxy-l-methamphetamine (OH-MeAmp), ~0.25%. Accordingly, l-MeAmp was
considered to be the primary pharmacologically active deprenyl
metabolite. A pharmacokinetic-pharmacodynamic analysis was then used to
relate these pharmacokinetic data to the results of previous
microdialysis studies in which increases in extracellular dopamine were
measured in the caudate-putamen after l-MeAmp (3-18
mg/kg) and after deprenyl (10 mg/kg). Dopamine response-area under
curve versus dose plots were generated and used to show that an
administered dose of 4 mg/kg l-MeAmp would be necessary
to effect a dopamine response-area under curve comparable to that
observed after the deprenyl dose. However, the present pharmacokinetic
results indicated that l-MeAmp brain levels after deprenyl corresponded to those that would be obtained from 0.4 mg/kg
l-MeAmp (i.e., one tenth of the required dose).
Collectively, these results suggest that the acute increases in
extracellular dopamine observed after deprenyl are not due uniquely to
metabolically generated l-MeAmp but also to other
actions of deprenyl at the dopamine terminal.
This article has been cited by other articles:
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 B. Ladenheim, I. N. Krasnova, X. Deng, J. M. Oyler, A. Polettini, T. H. Moran, M. A. Huestis, and J. L. Cadet Methamphetamine-Induced Neurotoxicity Is Attenuated in Transgenic Mice with a Null Mutation for Interleukin-6 Mol. Pharmacol., April 13, 2001; 58(6): 1247 - 1256. [Abstract] [Full Text]
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 D. A. Durden, L. E. Dyck, B. A. Davis, Y.-D. Liu, and A. A. Boulton Metabolism and Pharmacokinetics, in the Rat, of (R)-N-(2-Heptyl)Methyl-Propargylamine (R-2HMP), A New Potent Monoamine Oxidase Inhibitor and Antiapoptotic Agent Drug Metab. Dispos., February 1, 2000; 28(2): 147 - 154. [Abstract] [Full Text]
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