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Role of renal function in risk assessment of target non-attainment after standard dosing of meropenem in critically ill patients: a prospective observational study

机译:肾功能在危重患者美罗培南标准剂量给药后靶标未达标风险评估中的作用:一项前瞻性观察研究

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Background: Severe bacterial infections remain a major challenge in intensive care units because of their high prevalence and mortality. Adequate antibiotic exposure has been associated with clinical success in critically ill patients. The objective of this study was to investigate the target attainment of standard meropenem dosing in a heterogeneous critically ill population, to quantify the impact of the full renal function spectrum on meropenem exposure and target attainment, and ultimately to translate the findings into a tool for practical application.\ud\udMethods: A prospective observational single-centre study was performed with critically ill patients with severe infections receiving standard dosing of meropenem. Serial blood samples were drawn over 4 study days to determine meropenem serum concentrations. Renal function was assessed by creatinine clearance according to the Cockcroft and Gault equation (CLCRCG). Variability in meropenem serum concentrations was quantified at the middle and end of each monitored dosing interval. The attainment of two pharmacokinetic/pharmacodynamic targets 100%T >MIC,50%T >4×MIC) was evaluated for minimum inhibitory concentration (MIC) values of 2 mg/L and 8 mg/L and standard meropenem dosing (1000 mg, 30-minute infusion, every 8 h). Furthermore, we assessed the impact of CLCRCG on meropenem concentrations and target attainment and developed a tool for risk assessment of target non-attainment.\ud\udResults: Large inter- and intra-patient variability in meropenem concentrations was observed in the critically ill population (n = 48). Attainment of the target 100%T >MIC was merely 48.4% and 20.6%, given MIC values of 2 mg/L and 8 mg/L, respectively, and similar for the target 50%T >4×MIC. A hyperbolic relationship between CLCRCG (25–255 ml/minute) and meropenem serum concentrations at the end of the dosing interval (C8h) was derived. For infections with pathogens of MIC 2 mg/L, mild renal impairment up to augmented renal function was identified as a risk factor for target non-attainment (for MIC 8 mg/L, additionally, moderate renal impairment).\ud\udConclusions: The investigated standard meropenem dosing regimen appeared to result in insufficient meropenem exposure in a considerable fraction of critically ill patients. An easy- and free-to-use tool (the MeroRisk Calculator) for assessing the risk of target non-attainment for a given renal function and MIC value was developed. Trial registration Clinicaltrials.gov, NCT01793012 . Registered on 24 January 2013.
机译:背景:严重的细菌感染由于其高患病率和高死亡率,仍然是重症监护病房的主要挑战。在重症患者中,充足的抗生素暴露与临床成功相关。这项研究的目的是调查异质危重人群中美罗培南标准剂量的目标达成情况,量化全肾功能谱对美罗培南暴露和目标达成的影响,最终将发现转化为实用的工具方法:采用前瞻性观察性单中心研究,对接受美罗培南标准剂量的重症重症危重患者进行研究。在4个研究日内抽取连续血样以确定美罗培南血清浓度。根据Cockcroft和Gault方程式(CLCRCG)通过肌酐清除率评估肾功能。在每个监测的给药间隔的中间和结束时,定量美罗培南血清浓度的变化。评估两个药代动力学/药效学指标100%T> MIC,50%T> 4×MIC的最低抑菌浓度(MIC)值2 mg / L和8 mg / L,以及标准美罗培南剂量(1000 mg,每8小时输注30分钟)。此外,我们评估了CLCRCG对美罗培南浓度和目标达成的影响,并开发了一种工具,用于评估未达标的风险。\ ud \ ud结果:在危重人群中观察到美罗培南浓度的患者间和患者内差异很大(n = 48)。给定MIC值分别为2 mg / L和8 mg / L,目标100%T> MIC的实现仅为48.4%和20.6%,而目标50%T> 4×MIC的相似。在给药间隔(C8h)结束时得出CLCRCG(25–255 ml /分钟)与美罗培南血清浓度之间的双曲线关系。对于MIC 2 mg / L的病原体感染,轻度的肾功能不全直至肾功能增强被确定为未达到目标的危险因素(对于MIC 8 mg / L,中度肾功能不全)。\ ud \ ud结论:经研究的标准美罗培南给药方案似乎导致相当一部分危重患者的美罗培南暴露不足。开发了一种易于使用且免费的工具(MeroRisk计算器),用于评估给定肾功能和MIC值未达到目标的风险。试用注册Clinicaltrials.gov,NCT01793012。 2013年1月24日注册。

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