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- Title
- Clinical pharmacokinetics and pharmacodynamics of selegiline. An update.
- Author
- Mahmood I
- Address
- Division of Pharmaceutical Evaluation I, Food and Drug Administration, Rockville,
Maryland, USA. mahmoodi@cder.fda.gov
- Source
- Clin Pharmacokinet, 33(2):91-102 1997 Aug
- Abstract
- Selegiline is a selective inhibitor of monoamine oxidase-B (MAO-B) at a dose of 10
mg/day and is given to patients with Parkinson's disease as an adjunct to levodopa
therapy. By inhibiting MAO-B, selegiline increases the dopamine levels in the substantia
nigra. Selegiline also blocks dopamine re-uptake from the synaptic cleft, thus increasing
the dopamine concentrations in the brain. At a dose of 10 mg/day, selegiline is devoid of
'cheese effect'. The pharmacokinetics of selegiline are highly variable. Following an oral
dose of selegiline 10 mg, it is rapidly absorbed and metabolised to desmethylselegiline,
levoamphetamine and levomethamphetamine. The mean peak plasma concentration (Cmax) is
approximately 2 micrograms/L and the time to reach the peak is under an hour. The absolute
bioavailability of selegiline is approximately 10%. It has an apparent volume of
distribution of 1854 L. The oral clearance of selegiline (59 L/min) is many fold
higher than the liver blood flow (1.5 L/min), indicating that extrahepatic processes are
involved in the elimination of selegiline. The elimination half-life of selegiline is
about 1.5 hours. Following multiple administration of selegiline 10 mg/day, the
accumulation of both the parent compound and its metabolites have been reported. At least
a 4-fold increase in the half-lives of selegiline and desmethylselegiline has been
reported. There is at least a 3-fold increase in the Cmax and area under the
concentration-time curve of selegiline with food. One of the metabolites of selegiline,
desmethylselegiline, is believed to posses some MAO-B inhibitory property, though to a
lesser extent than that of selegiline. Within 2 to 4 hours of an oral dose of selegiline
10 mg, 86% of the platelet MAO-B activity was inhibited and it took almost 2 weeks for
platelet MAO-B activity to return to the baseline values. Transdermal administration of
selegiline resulted in an increase in the plasma concentrations of selegiline and a
decrease in the formation of its metabolites, indicating that the extensive first-pass
effect is avoided when selegiline is given transdermally.
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