新生儿早发性败血症中氨曲南的群体药代动力学和剂量优化:一项真实世界研究。
Population pharmacokinetics and dosing optimization of azlocillin in neonates with early-onset sepsis: a real-world study.
机构信息
Department of Clinical Pharmacy, Key Laboratory of Chemical Biology (Ministry of Education), School of Pharmaceutical Sciences, Cheeloo College of Medicine, Shandong University, Jinan 250012, China.
Department of Pharmacy, Tianjin Central Hospital of Gynecology Obstetrics, Tianjin 300100, China.
出版信息
J Antimicrob Chemother. 2021 Feb 11;76(3):699-709. doi: 10.1093/jac/dkaa468.
OBJECTIVES
Nowadays, real-world data can be used to improve currently available dosing guidelines and to support regulatory approval of drugs for use in neonates by overcoming practical and ethical hurdles. This proof-of-concept study aimed to assess the population pharmacokinetics of azlocillin in neonates using real-world data, to make subsequent dose recommendations and to test these in neonates with early-onset sepsis (EOS).
METHODS
This prospective, open-label, investigator-initiated study of azlocillin in neonates with EOS was conducted using an adaptive two-step design. First, a maturational pharmacokinetic-pharmacodynamic model of azlocillin was developed, using an empirical dosing regimen combined with opportunistic samples resulting from waste material. Second, a Phase II clinical trial (ClinicalTrials.gov: NCT03932123) of this newly developed model-based dosing regimen of azlocillin was conducted to assure optimized target attainment [free drug concentration above MIC during 70% of the dosing interval ('70% fT>MIC')] and to investigate the tolerance and safety in neonates.
RESULTS
A one-compartment model with first-order elimination, using 167 azlocillin concentrations from 95 neonates (31.7-41.6 weeks postmenstrual age), incorporating current weight and renal maturation, fitted the data best. For the second step, 45 neonates (30.3-41.3 weeks postmenstrual age) were subsequently included to investigate target attainment, tolerance and safety of the pharmacokinetic-pharmacodynamic model-based dose regimen (100 mg/kg q8h). Forty-three (95.6%) neonates reached their pharmacokinetic target and only two neonates experienced adverse events (feeding intolerance and abnormal liver function), possibly related to azlocillin.
CONCLUSIONS
Target attainment, tolerance and safety of azlocillin was shown in neonates with EOS using a pharmacokinetic-pharmacodynamic model developed with real-world data.
目的
目前,真实世界的数据可用于改进现有的剂量指南,并通过克服实际和伦理障碍来支持药物在新生儿中的监管批准。本概念验证研究旨在使用真实世界的数据评估氨苄西林在新生儿中的群体药代动力学,提出后续剂量建议,并在患有早发性败血症(EOS)的新生儿中进行测试。
方法
本前瞻性、开放标签、研究者发起的 EOS 新生儿氨苄西林研究采用适应性两步设计进行。首先,使用经验性给药方案结合废物机会样本开发氨苄西林的成熟药代动力学-药效动力学模型。其次,开展一项基于该新开发模型的氨苄西林给药方案的 II 期临床试验(ClinicalTrials.gov:NCT03932123),以确保优化目标达到率(给药间隔的 70%时间内游离药物浓度超过 MIC [‘70%fT>MIC’]),并研究新生儿的耐受性和安全性。
结果
使用来自 95 名新生儿(胎龄 31.7-41.6 周)的 167 个氨苄西林浓度的单室模型,采用一级消除,纳入当前体重和肾功能成熟度,最适合数据。在第二步中,随后纳入 45 名新生儿(胎龄 30.3-41.3 周),以研究基于药代动力学-药效动力学模型的剂量方案的目标达到率、耐受性和安全性(100mg/kg,q8h)。43 名(95.6%)新生儿达到了其药代动力学目标,仅 2 名新生儿发生不良事件(喂养不耐受和肝功能异常),可能与氨苄西林有关。
结论
在 EOS 新生儿中使用基于真实世界数据开发的药代动力学-药效动力学模型,显示了氨苄西林的目标达到率、耐受性和安全性。
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