Abstract
Dapsone is a potent anti-inflammatory and antibacterial agent that has been used extensively in the oral treatment of leprosy and dermatitis herpetiformis. This study compared the pharmacokinetic profile of dapsone in rats given a single oral or i.v. 12 mg/kg dose (n = 8/group) or a single dermal application of 12 or 60 mg/kg (n = 12/group) in an aqueous gel application medium containing 10 or 25% diethylene glycol monoethyl ether (DGME). Blood samples (200 μl) were collected via tail vein from each rat and pooled at intervals up to the 24-h period. A terminal blood sample was collected by cardiac puncture from each animal. Plasma concentrations of dapsone were determined by liquid chromatography atmospheric pressure ionization tandem mass spectroscopy. There was no treatment-related overt toxicity observed in any of the animals. Peak levels were reached 1 h after oral dosing (4890 ng/ml), and 6 to 8 h after dermal application, withCmax values of 1.62, 5.56, and 12.8 ng/ml, for 12 mg/kg at 10 or 25% DGME, and for 60 mg/kg at 25% DGME, respectively. Bioavailability was calculated at 78% after oral dosing and <1% after dermal application. Apparent elimination half-lives (t1/2)s were similar after i.v. and oral dosing. Both the calculated area under the plasma concentration versus time curve up to 24 h andCmax values were 3- to 4-fold higher in the dermal application group administered 12 mg/kg dapsone in 25 versus 10% DGME gel, whereas the calculated area under the plasma concentration versus time curve up to 24 h andCmax values for the 60 mg/kg group were only 3.3- and 2.3-fold greater than those obtained after application of 12 mg/kg in 25% DGME. These results show that both systemic exposure and peak plasma concentrations of dapsone are minimized by dermal versus oral administration of the compound.
Footnotes
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Send reprint requests to: David W. Osborne, Ph.D., Vice President, Pharmaceutical Development, Atrix Laboratories, Inc., 2579 Midpoint Drive, Fort Collins, CO 80525-5868. E-mail:dosborne{at}atrixlab.com
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↵1 Current address: Wil Research Laboratories, 1407 George Rd., Ashland, OH 44805-3650.
- Abbreviations used are::
- DGME
- diethylene glycol monoethyl ether
- G6PD
- glucose-6-phosphate dehydrogenase
- LC
- liquid chromatography
- AUC
- area under the plasma concentration versus time curve
- MIC
- minimum inhibitory concentration
- Received November 10, 1999.
- Accepted May 2, 2000.
- The American Society for Pharmacology and Experimental Therapeutics
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