Pharmacokinetic-Pharmacodynamic Modeling of the Inhibitory Effects of Naproxen on the Time-Courses of Inflammatory Pain, Fever, and the Ex Vivo Synthesis of TXB and PGE in Rats.
- Resource Type
- Article
- Authors
- Krekels, Elke; Angesjö, Marie; Sjögren, Ingemo; Ängeby Möller, Kristina; Berge, Odd-Geir; Visser, Sandra
- Source
- Pharmaceutical Research. Jul2011, Vol. 28 Issue 7, p1561-1576. 16p.
- Subject
- *NAPROXEN
*DRUG efficacy
*ANTIPYRETICS
*PHARMACOKINETICS
*PROSTAGLANDINS
*PHARMACODYNAMICS
*LABORATORY rats
*EFFECT of drugs on body temperature
- Language
- ISSN
- 0724-8741
Purpose: To quantify and compare the time-course and potency of the analgesic and antipyretic effects of naproxen in conjunction with the inhibition of PGE and TXB. Methods: Analgesia was investigated in a rat model with carrageenan-induced arthritis using a gait analysis method. Antipyretics were studied in a yeast-induced fever model using telemetrically recorded body temperature. Inhibition of TXB and PGE synthesis was determined ex vivo. Pharmacokinetic profiles were obtained in satellite animals. Population PKPD modeling was used to analyze the data. Results: The IC values (95% CI) of naproxen for analgesia (27 (0-130) μM), antipyretics (40 (30-65) μM) and inhibition of PGE (13 (6-45) μM) were in similar range, whereas inhibition of TXB (5 (4-8) μM) was observed at lower concentrations. Variability in the behavioral measurement of analgesia was larger than for the other endpoints. The inhibition of fever by naproxen was followed by an increased rebound body temperature. Conclusion: Due to better sensitivity and similar drug-induced inhibition, the biomarker PGE and the antipyretic effect would be suitable alternative endpoints to the analgesic effects for characterization and comparisons of potency and time-courses of drug candidates affecting the COX-2 pathway and to support human dose projections. [ABSTRACT FROM AUTHOR]