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Pharmacokinetics (PK), Pharmacodynamics (PD), and PK-PD Integration of Danofloxacin in Sheep Biological Fluids

机译:达氟沙星在绵羊生物体液中的药代动力学(PK),药效动力学(PD)和PK-PD整合

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摘要

The fluoroquinolone antimicrobial drug danofloxacin was administered to sheep intravenously (i.v.) and intramuscularly (i.m.) at a dose of 1.25 mg/kg of body weight in a two-period crossover study. The pharmacokinetic properties of danofloxacin in serum, inflamed tissue cage fluid (exudate), and noninflamed tissue cage fluid (transudate) were established by using a tissue cage model. The in vitro and ex vivo activities of danofloxacin in serum, exudate, and transudate against a pathogenic strain of Mannheimia haemolytica were established. Integration of in vivo pharmacokinetic data with the in vitro MIC provided mean values for the area under the curve (AUC)/MIC for serum, exudate, and transudate of 60.5, 85.6, and 45.7 h, respectively, after i.v. dosing and 55.9, 77.9, and 49.1 h, respectively, after i.m. dosing. After i.m. dosing, the maximum concentration/MIC ratios for serum, exudate, and transudate were 10.8, 3.0, and 1.6, respectively. The ex vivo growth inhibition data after i.m. dosing were fitted to the inhibitory sigmoid Emax equation to provide the values of AUC/MIC required to produce bacteriostasis, bactericidal activity, and elimination of bacteria. The respective values for serum were 17.8, 20.2, and 28.7 h, and slightly higher values were obtained for transudate and exudate. It is proposed that use of these data might provide a novel approach to the rational design of dosage schedules.
机译:在两个阶段的交叉研究中,氟喹诺酮类抗菌药物丹诺沙星以1.25 mg / kg体重的剂量静脉内(i.v.)和肌肉内(i.m.)施用给绵羊。通过使用组织笼模型,建立了达氟沙星在血清,发炎的组织笼液(渗出液)和非发炎的组织笼液(渗出液)中的药代动力学特性。建立了达氟沙星在血清,渗出液和渗出液中针对溶血曼海姆病菌的体外和体外活性。体内药代动力学数据与体外MIC的整合提供了静脉注射后血清,渗出液和渗出液的曲线下面积(AUC)/ MIC的平均值分别为60.5、85.6和45.7小时。在i.m.之后分别给药和55.9、77.9和49.1小时加药。在我之后给药时,血清,渗出液和渗出液的最大浓度/ MIC比分别为10.8、3.0和1.6。 i.m.之后的离体生长抑制数据将剂量与抑制性乙状结肠Emax方程拟合,以提供产生抑菌,杀菌活性和消除细菌所需的AUC / MIC值。血清的各自值为17.8、20.2和28.7小时,而渗出液和渗出液的值略高。建议使用这些数据可能为合理设计剂量方案提供一种新颖的方法。

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