Abstract

The pharmacokinetics of quinocetone and its major metabolites in healthy swine was investigated in this paper. Quinocetone was administered to 8 healthy cross-bread swine intravenously and orally at a dosage of 4 and 40 mg kg −1 body weight respectively in a randomized crossover design test with two-week washout period. A sensitive high-performance liquid chromatography-tandem mass spectrometry (HPLC-MS/MS) method was developed for the determination of quinocetone and its metabolite 1-desoxyquinocetone in plasma. Plasma concentration versus time profiles of quinocetone and its metabolite 1-desoxy quinocetone were analyzed by non-compartmental analysis using Winnonlin 5.2 software. Mean maximum concentrations (C max) for quinocetone was found to be (0.56±0.13) μg mL −1 at 2.92 h, after oral administration of quinocetone. Mean maximum concentrations (C max) for 1-desoxy quinocetone after intravenous or oral administration of quinocetone were (0.0095±0.0012) μg mL· 1 at 0.083 h and (0.0067±0.0053) μg mL −1 at 3.08 h. The apparent elimination half-lives (T 1/2) for quinocetone and its metabolite 1-desoxy quinocetone were (2.24±0.24) and (5.23±0.56) h after intravenous administration of quinocetone and (2.91±0.29) and (11.85±2.89) h after oral administration of quinocetone, respectively. Mean areas under the plasma concentration-time curve (AUC 0-x) for quinocetone and 1-desoxyquinocetone were (2.02±0.15) and (0.2±0.002) μg h mL −1 respectively after intravenous administration of quinocetone, and (3.5±0.79) and (0.053±0.03) μg h mL −1 after oral administration of quinocetone, respectively. Quinocetone was rapidly absorbed and metabolized in swine after oral and intravenous administration. The plasma concentration-time curve (AUC 0-x) of 1-desoxy quinocetone were much smaller than those of quinocetone, while the elimination half-lives (T 1/2) were much longer than those of quinocetone after intravenously (i.v.) or oral administration.

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