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澳大利亚重症败血症原住民患者万古霉素的优化剂量

Optimised dosing of vancomycin in critically ill Indigenous Australian patients with severe sepsis.

作者信息

Tsai D, Stewart P C, Hewagama S, Krishnaswamy S, Wallis S C, Lipman J, Roberts J A

机构信息

Burns, Trauma and Critical Care Research Centre, School of Medicine, The University of Queensland, Brisbane, Queensland; Centre for Remote Health, Flinders University, Adelaide, South Australia; Pharmacy Department, Alice Springs Hospital, Alice Springs, Northern Territory.

Specialist, Department of Intensive Care Medicine and Department of Medicine, Alice Springs Hospital, Alice Springs, Northern Territory.

出版信息

Anaesth Intensive Care. 2018 Jul;46(4):374-380. doi: 10.1177/0310057X1804600405.

Abstract

Vancomycin is a commonly used antibiotic due to the high burden of methicillin-resistant infections. This study aimed to describe the pharmacokinetics (PK) of vancomycin in Australian Indigenous patients with severe sepsis, and advise an optimal dosing strategy. A population PK study was conducted in a remote Australian intensive care unit (ICU). Serial plasma samples were collected over one to two dosing intervals and assayed by validated chromatography. Concentration-time data collected were analysed using Pmetrics® software. The final population PK model was then used for Monte Carlo dosing simulations to determine optimal loading and intermittent maintenance doses. Fifteen Indigenous subjects were included for analysis with a median (interquartile range, IQR) age, weight and creatinine clearance (CrCL) of 43 (34-46) years, 73 (66-104) kg and 99 (56-139) ml/minute respectively. A two-compartment model described the data adequately. Vancomycin clearance (CL) and volume of distribution of the central compartment (Vc) were described by CrCL and patient weight respectively. Median (IQR) CL, Vc, distribution rate constants from central to peripheral, and from peripheral to central compartments were 4.6 (3.8-5.6) litres per hour, 25.4 (16.1-31.3) litres, 0.46 (0.28-0.52)/hour and 0.25 (0.12-0.37)/hour respectively. No significant interethnic PK differences were observed in comparison to published data. Therapeutic loading doses were significantly dependent on both weight and CrCL, whereas maintenance doses were dependent on CrCL. In the absence of severe renal impairment, initiation of maintenance dose eight hours post-loading dose achieved higher probability of target attainment at 24 hours. This is the first report of vancomycin PK in this patient group.

摘要

由于耐甲氧西林感染的负担较重,万古霉素是一种常用的抗生素。本研究旨在描述万古霉素在患有严重脓毒症的澳大利亚原住民患者中的药代动力学(PK),并提出最佳给药策略。在澳大利亚一个偏远的重症监护病房(ICU)进行了一项群体PK研究。在一到两个给药间隔内采集系列血浆样本,并通过经过验证的色谱法进行分析。使用Pmetrics®软件对收集到的浓度-时间数据进行分析。然后将最终的群体PK模型用于蒙特卡洛给药模拟,以确定最佳负荷剂量和间歇维持剂量。纳入15名原住民受试者进行分析,其年龄、体重和肌酐清除率(CrCL)的中位数(四分位间距,IQR)分别为43(34-46)岁、73(66-104)kg和99(56-139)ml/分钟。一个二室模型能够充分描述这些数据。万古霉素清除率(CL)和中央室分布容积(Vc)分别由CrCL和患者体重来描述。CL、Vc、从中央室到外周室以及从外周室到中央室的分布速率常数的中位数(IQR)分别为每小时4.6(3.8-5.6)升、25.4(16.1-31.3)升、0.46(0.28-0.52)/小时和0.25(0.12-0.37)/小时。与已发表的数据相比,未观察到显著的种族间PK差异。治疗负荷剂量显著依赖于体重和CrCL,而维持剂量依赖于CrCL。在没有严重肾功能损害的情况下,在负荷剂量后8小时开始给予维持剂量,在24小时时达到目标浓度的概率更高。这是关于该患者群体万古霉素PK的首份报告。

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