Concentrations of the des-F(6)-quinolone garenoxacin in plasma and joint cartilage of immature rats
| Autor: | Akintunde Bello, Ute Rahm, Michael Kastner, Ralf Stahlmann, Irmela Baumann-Wilschke |
|---|---|
| Rok vydání: | 2003 |
| Předmět: |
Cartilage
Articular Male Ofloxacin Health Toxicology and Mutagenesis Cmax Administration Oral Pharmacology Toxicology Garenoxacin chemistry.chemical_compound Pharmacokinetics Anti-Infective Agents Oral administration Ciprofloxacin Blood plasma medicine Animals Rats Wistar Antibacterial agent Dose-Response Relationship Drug Chemistry General Medicine Rats Specific Pathogen-Free Organisms Sparfloxacin Area Under Curve Female medicine.drug Fluoroquinolones |
| Zdroj: | Archives of toxicology. 78(2) |
| ISSN: | 0340-5761 |
| Popis: | Garenoxacin is a des-F(6)-quinolone with a broad antibacterial spectrum, which has previously been shown to exhibit low chondrotoxicity in juvenile dogs compared with several other quinolones. A study was performed to determine whether the low chondrotoxicity observed in immature rats following garenoxacin treatment could be explained by poor penetration into cartilage tissue. Garenoxacin was orally administered to immature (4- to 5-week-old) Wistar rats as a single dose-or as doses given on 5 consecutive days-of 0 (vehicle), 200, 400, and 600 mg/kg ( n=5 per dose level). Additional groups of rats were orally dosed with 600 mg/kg ofloxacin and ciprofloxacin. One knee joint of each animal (24 h after the last dose) was studied histologically after staining with Toluidine blue. The pharmacokinetics of garenoxacin in plasma (200, 400, and 600 mg/kg) and in knee joint cartilage (200 and 600 mg/kg) was assessed in separate groups of rats ( n=55 per dose level). Concentrations of garenoxacin in plasma and cartilage were measured using an HPLC method. No signs of chondrotoxicity were observed in the immature rats treated with garenoxacin or ciprofloxacin for 5 days at the doses investigated in this study. However, ofloxacin was found to induce cartilage lesions that were typical of those seen for this quinolone. Systemic exposure to garenoxacin increased as a function of dose. Across dose and study day, mean garenoxacin plasma maximum concentration ( C(max)) and area under the concentration-time curve (AUC(tau)) values were in the range 12-26 mg/l and 33-133 mgxh/l, respectively. Garenoxacin C(max) and AUC were similar on days 1 and 5, within each dose, indicating the absence of accumulation or reduction in the systemic exposure. Values determined for T(max) (0.25-1.0 h) and T(1/2) (3.8-6.4 h) of garenoxacin in plasma did not vary with dose or study day. Although peak garenoxacin concentrations in cartilage were between equal levels to and 2.5-fold of those found in plasma, the observed ratios were somewhat lower than those reported for other quinolones, e.g. ofloxacin or sparfloxacin. Since garenoxacin appeared to be well absorbed following oral administration and concentrations in cartilage tended to be higher than those in plasma, it is unlikely that the low chondrotoxicity in comparison with other quinolones is explained by differences in the pharmacokinetics of these compounds. |
| Databáze: | OpenAIRE |
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