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Pharmacokinetic-pharmacodynamic target attainment analysis of biapenem in adult patients: a dosing strategy.

机译:比阿培南在成年患者中的药代动力学-药效学目标实现分析:一种给药策略。

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BACKGROUND: A pharmacokinetic-pharmacodynamic (PK-PD) target attainment analysis to build a dosing strategy for biapenem in adult patients has not been conducted. METHODS: A total of 321 plasma concentration samples from 68 adult patients (1-6 samples per patient) were assayed biologically and chromatographically, and used for a population PK modeling and Monte Carlo simulation to assess the probability of attaining the PK-PD target (40% of the time above the minimum inhibitory concentration). RESULTS: The population PK model was based on the standard two-compartment model, and creatinine clearance (Cl(cr)) was the most significant covariate that affected the drug clearance. The Monte Carlo simulation demonstrated that the dosages up to 600 mg Q12H (0.5-h infusions) achieved a PK-PD target attainment probability of > or =90%, which varied with Cl(cr) of the patient and susceptibility of the tested bacterium; however, higher dosage with prolonged infusion time (600 mg Q8H, 3 h infusion) was required fora high probability against Pseudomonas aeruginosa and Haemophilus influenzae isolates in the case of Cl(cr) = 90 ml/min. CONCLUSION: These results provide guidance for constructing a PK-PD-based strategy for tailoring biapenem regimens in adult patients.
机译:背景:尚未进行药代动力学-药效学(PK-PD)目标获得分析来建立成年患者比阿培南的给药策略。方法:对68位成年患者的321份血浆浓度样品(每位患者1-6份样品)进行了生物学和色谱分析,并用于群体PK建模和Monte Carlo模拟,以评估达到PK-PD目标的可能性(在最低抑制浓度之上40%的时间)。结果:人口PK模型基于标准的两室模型,并且肌酐清除率(Cl(cr))是影响药物清除率的最显着的协变量。蒙特卡洛模拟表明,最高剂量为600 mg Q12H(0.5小时输注)的剂量可实现PK-PD目标达到概率>或= 90%,这随患者的Cl(cr)和被测细菌的敏感性而变化;但是,如果Cl(cr)= 90 ml / min,则对于铜绿假单胞菌和流感嗜血杆菌分离株的高可能性,需要更长剂量的延长输注时间(600 mg Q8H,3 h输注)。结论:这些结果为构建基于PK-PD的成年患者比阿培南方案定制策略提供了指导。

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