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庆大霉素在早产儿和足月儿中的发育药代动力学:一项前瞻性研究的群体建模

Developmental pharmacokinetics of gentamicin in preterm and term neonates: population modelling of a prospective study.

作者信息

Nielsen Elisabet I, Sandström Marie, Honoré Per Hartvig, Ewald Uwe, Friberg Lena E

机构信息

Department of Pharmaceutical Biosciences, Uppsala University, Uppsala, Sweden.

出版信息

Clin Pharmacokinet. 2009;48(4):253-63. doi: 10.2165/00003088-200948040-00003.

Abstract

BACKGROUND AND OBJECTIVE

Preterm and term newborn infants show wide interindividual variability (IIV) in pharmacokinetic parameters of gentamicin. More extensive knowledge and use of predictive covariates could lead to faster attainment of therapeutic concentrations and a reduced need for concentration monitoring. This study was performed to characterize the population pharmacokinetics of gentamicin in preterm and term neonates and to identify and quantify relationships between patient characteristics and IIV. A secondary aim was to evaluate cystatin C as a marker for gentamicin clearance in this patient population.

METHODS

Data were collected in a prospective study performed in the Neonatal Intensive Care Unit at the University Children's Hospital, Uppsala, Sweden. Population pharmacokinetic modelling was performed using nonlinear mixed-effects modelling (NONMEM) software. Bodyweight was included as the primary covariate according to an allometric power model. Other evaluated covariates were age (postmenstrual age, gestational age [GA], postnatal age [PNA]), markers for renal function (serum creatinine, serum cystatin C) and concomitant medication with cefuroxime, vancomycin or indometacin. Covariate-parameter relationships were explored using a stepwise covariate model building procedure. The predictive performance of the developed model was evaluated using an independent external dataset for a similar patient population.

RESULTS

Sixty-one newborn infants (GA range 23.3-42.1 weeks, PNA range 0-45 days) were enrolled in the study. In total, 894 serum gentamicin samples were included in the analysis. The concentration-time profile was described using a three-compartment model. Gentamicin clearance increased with the GA and PNA (included in a nonlinear fashion). The GA was also identified as having a significant influence on the central volume of distribution, with a preterm neonate having a larger central volume of distribution per kilogram of bodyweight than a term neonate. Cystatin C and creatinine were not correlated with gentamicin clearance in this study population. The external dataset was well predicted by the developed model.

CONCLUSION

Bodyweight and age (GA and PNA) were found to be major factors contributing to IIV in gentamicin clearance in neonates. Based on these data, cystatin C and serum creatinine were not correlated with gentamicin clearance and therefore not likely to be predictive markers of renal function in this patient population. Based on predictions from the developed model, preterm neonates do not reach targeted peak and trough gentamicin concentrations after a standard dosage regimen of 4 mg/kg given once daily, suggesting a need for higher loading doses and prolonged dosing intervals in this patient population.

摘要

背景与目的

庆大霉素的药代动力学参数在早产和足月新生儿中存在广泛的个体间差异(IIV)。对预测性协变量有更广泛的了解和应用可能会使治疗浓度更快达到,并减少浓度监测的需求。本研究旨在描述庆大霉素在早产和足月新生儿中的群体药代动力学特征,并确定和量化患者特征与个体间差异之间的关系。次要目的是评估胱抑素C作为该患者群体中庆大霉素清除率标志物的情况。

方法

在瑞典乌普萨拉大学儿童医院新生儿重症监护病房进行的一项前瞻性研究中收集数据。使用非线性混合效应建模(NONMEM)软件进行群体药代动力学建模。根据异速生长幂模型将体重作为主要协变量纳入。其他评估的协变量包括年龄(月经后年龄、胎龄[GA]、出生后年龄[PNA])、肾功能标志物(血清肌酐、血清胱抑素C)以及与头孢呋辛、万古霉素或吲哚美辛的联合用药。使用逐步协变量模型构建程序探索协变量与参数之间的关系。使用针对类似患者群体的独立外部数据集评估所开发模型的预测性能。

结果

61名新生儿(GA范围为23.3 - 42.1周,PNA范围为0 - 45天)纳入研究。分析中总共包括894份血清庆大霉素样本。浓度 - 时间曲线用三室模型描述。庆大霉素清除率随GA和PNA增加(以非线性方式纳入)。GA也被确定对中央分布容积有显著影响,早产新生儿每千克体重的中央分布容积比足月新生儿大。在该研究群体中,胱抑素C和肌酐与庆大霉素清除率无关。所开发的模型对外部数据集预测良好。

结论

发现体重和年龄(GA和PNA)是导致新生儿庆大霉素清除率个体间差异的主要因素。基于这些数据,胱抑素C和血清肌酐与庆大霉素清除率无关,因此不太可能是该患者群体肾功能的预测标志物。根据所开发模型的预测,在每天一次给予4 mg/kg的标准给药方案后,早产新生儿未达到庆大霉素的目标峰浓度和谷浓度,这表明该患者群体需要更高的负荷剂量和更长的给药间隔。

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