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Predicting the dose of vancomycin in ICU patients receiving different types of RRT therapy: a model‐based meta‐analytic approach

机译:预测接受不同类型的RRT治疗的ICU患者的万古霉素剂量:一种基于模型的荟萃分析方法

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Abstract Aim Previous pharmacokinetic (PK) studies have proposed various dosing regimens for vancomycin in intensive care unit (ICU) patients undergoing renal replacement therapy (RRT), but all are restricted to specific RRT modalities. To be useful in practice, a population PK model would need to predict vancomycin clearance during any RRT modality. Development of such a model is feasible using meta‐analysis of published summarized estimates of vancomycin PK parameters. Our aims were: (i) to develop and validate a population PK model for vancomycin that takes into account any RRT modalities, and (ii) to predict vancomycin dosing for RRT patients in ICU. Methods Vancomycin pharmacokinetics were assumed to be two‐compartmental, total body clearance being the sum of non‐RRT clearance and RRT‐induced clearance. Drug disposition and non‐RRT clearance parameters were estimated by systematic review and meta‐analysis of previously published parameter estimates. The relationship between RRT‐induced clearance and RRT flowrate settings was assessed using a model‐based meta‐analysis. Prediction performances of the PK model were assessed using external data. Results The meta‐analyses of disposition parameters, non‐RRT clearance and RRT‐induced clearance included 11, 6 and 38 studies (84 RRT clearance measurements) respectively. The model performed well in predicting external individual PK data. Individual vancomycin concentrations during RRT were accurately predicted using Bayesian estimation based solely on pre‐RRT measurements. Conclusions The PK model allowed accurate prediction of the vancomycin pharmacokinetics during RRT in ICU patients. Based on the model of RRT‐induced clearance, an appropriate adjustment of the vancomycin dosing regimen could be proposed for any kind of flowrate settings.
机译:摘要目的先前的药代动力学(PK)研究提出了在经过肾置换疗法(RRT)的重症监护室(ICU)患者中的万古霉素各种剂量治疗方案,但所有人都仅限于特定的RRT方式。为了在实践中有用,人口PK模型需要在任何RRT模型期间预测万古霉素清除。使用Meta分析的Meta分析,这种模型的开发是可行的,用于发表的Vancomycin PK参数的汇总估计。我们的目标是:(i)开发和验证vancomycin的人口PK模型,考虑到任何RRT方式,以及(ii)预测ICU中RRT患者的万古霉素给药。方法假设万古霉素药代动力学是两室,总体间隙是非RRT间隙和RRT诱导的间隙之和。通过先前公布的参数估计的系统审查和META分析估算了药物处理和非RRT间隙参数。使用基于模型的META分析评估RRT诱导的间隙和RRT流量设置之间的关系。使用外部数据评估PK模型的预测性能。结果分析参数,非RRT间隙和RRT引起的间隙包括11,6和38研究(84 rrt间隙测量)。该模型在预测外部单个PK数据时表现良好。仅使用贝叶斯估计完全基于RRT测量来精确地预测RRT期间的个体万古霉素浓度。结论PK模型允许在ICU患者的RRT中精确预测万古霉素药代动力学。基于RRT诱导的间隙的模型,可以提出适当调整万古霉素给药方案的任何类型的流量设置。

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