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头孢他啶在重症监护病房患者中的群体药代动力学:肾小球滤过率、机械通气及入院原因的影响

Population pharmacokinetics of ceftazidime in intensive care unit patients: influence of glomerular filtration rate, mechanical ventilation, and reason for admission.

作者信息

Georges Bernard, Conil Jean-Marie, Seguin Thierry, Ruiz Stéphanie, Minville Vincent, Cougot Pierre, Decun Jean-François, Gonzalez Hélène, Houin Georges, Fourcade Olivier, Saivin Sylvie

机构信息

Anesthésie Réanimation, CHU Rangueil, TSA 50032, 31059 Toulouse, France.

出版信息

Antimicrob Agents Chemother. 2009 Oct;53(10):4483-9. doi: 10.1128/AAC.00430-09. Epub 2009 Jul 27.

Abstract

The aim of this study was to develop a population-pharmacokinetic model of ceftazidime in intensive care unit patients to include the influence of patients' characteristics on the pharmacokinetics. Forty-nine patients for model building and 23 patients for validation were included in a randomized study. They received ceftazidime at 2 g three times a day or as 6 g per day continuously. A NONMEM pharmacokinetic model was constructed, and the influences of covariates were studied. The model was validated by a comparison of the predicted and observed concentrations. A final model was elaborated from the whole population. Total clearance (CL) was significantly correlated with the glomerular filtration rate (GFR) calculated by modification of the diet in renal disease (MDRD), the central volume of distribution (V1) with intubation, and the peripheral volume of distribution (V2) with the reason for admission. The mean pharmacokinetic parameters were as follows: CL, 5.48 liters/h, 40%; V1, 10.48 liters, 34%; V2, 32.12 liters, 59%; total volume, 42.60 liters, 45%; and intercompartmental clearance, 16.19 liters/h, 42%. In the polytrauma population (mechanically ventilated), the time above the MIC at steady state never corresponds to 100% for discontinuous administration, and the target concentration of five times the MIC was reached with a 6-g/day dose only for patients with an MDRD of <150 ml/min. We showed that the GFR-MDRD, mechanical ventilation, and the reason for admission may influence the achieved concentrations of ceftazidime. Our model allows the a priori dosing to be adjusted to the individual patient.

摘要

本研究的目的是建立重症监护病房患者头孢他啶的群体药代动力学模型,以纳入患者特征对药代动力学的影响。一项随机研究纳入了49例用于模型构建的患者和23例用于验证的患者。他们接受每日3次2g的头孢他啶治疗或每日持续6g的治疗。构建了NONMEM药代动力学模型,并研究了协变量的影响。通过比较预测浓度和观察浓度对模型进行验证。从总体人群中精心构建了最终模型。总清除率(CL)与通过肾病饮食改良(MDRD)计算的肾小球滤过率(GFR)显著相关,中央分布容积(V1)与插管相关,外周分布容积(V2)与入院原因相关。平均药代动力学参数如下:CL为5.48升/小时,变异系数为40%;V1为10.48升,变异系数为34%;V2为32.12升,变异系数为59%;总体积为42.60升,变异系数为45%;以及隔室间清除率为16.19升/小时,变异系数为42%。在多发伤人群(机械通气)中,间断给药时稳态下高于最低抑菌浓度(MIC)的时间从未达到100%,仅对于MDRD<150 ml/min的患者,6g/天的剂量能达到5倍MIC的目标浓度。我们表明,GFR-MDRD、机械通气和入院原因可能会影响头孢他啶的血药浓度。我们的模型允许根据个体患者情况对初始剂量进行调整。

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