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利奈唑胺在重症感染患者中的药动学
引用本文:肖莹,张弋,李淑娟,邢迎红. 利奈唑胺在重症感染患者中的药动学[J]. 中国医院药学杂志, 2016, 36(7): 535-539. DOI: 10.13286/j.cnki.chinhosppharmacyj.2016.07.04
作者姓名:肖莹  张弋  李淑娟  邢迎红
作者单位:1. 天津市第一中心医院药学部, 天津 300192;2. 天津市第一中心医院重症监护室, 天津 300192
基金项目:国家高技术研究发展计划(编号:2012AA021001);国家国际科技合作专项项目(编号:2015DFG31850)
摘    要:
目的:研究重症感染患者静脉滴注和鼻饲2种不同给药途经下利奈唑胺的药动学特点。方法:本研究为前瞻性研究,2013年8月-2014年3月使用利奈唑胺治疗的6例ICU患者,根据给药途径不同,分为静脉滴注组4例,鼻饲管给药组2例,2组均给予利奈唑胺600 mg/q12h,于给药后第5天的0,0.5,1,2,3,4,6,8,12 h采取静脉血1 mL,监测利奈唑胺的血药浓度。结果:6例患者的Cmin变化范围为3.59~19.82 μg·mL-1,其中2例超过了安全临界值10 μg·mL-1,AUC0-12 h变化范围为116.7~305.5 μg·h-1·mL-1,Cmin与AUC0-12 h具有很强的相关性(r=0.997,P=0.001)。结论:重症感染患者利奈唑胺药动学参数个体差异较大,应根据PK/PD相关参数制定合理的给药方案,预防细菌耐药,保证临床治疗效果,减少不良反应。

关 键 词:利奈唑胺  重症感染患者  药动学  
收稿时间:2015-10-08

Pharmacokinetics of linezolid in critically ill patients
XIAO Ying,ZHANG Yi,LI Shu-juan,XING Ying-hong. Pharmacokinetics of linezolid in critically ill patients[J]. Chinese Journal of Hospital Pharmacy, 2016, 36(7): 535-539. DOI: 10.13286/j.cnki.chinhosppharmacyj.2016.07.04
Authors:XIAO Ying  ZHANG Yi  LI Shu-juan  XING Ying-hong
Affiliation:1. Department of Pharmacy, Tianjin First Central Hospital, Tianjin 300192, China;2. Department of Intensive Care Unit, Tianjin First Central Hospital, Tianjin 300192, China
Abstract:
OBJECTIVE To compare pharmacokinetics of linezolid by nasogastric and intravenous administration in critically ill patients from intensive care unit.METHODS A prospective study was conducted between August 2013 and March 2014 and 6 patients administered of linezolid were included. The drug was administered in two patients by nasogastric route and four patients by intravenous route. Patients of both groups were all given 600 mg twice daily, blood specimens were collected at zero (prior to dosing), 0.5, 1, 2, 3, 4, 6, 8, 12 after dosing at day 5. Plasma concentrations of linezolid were monitored.RESULTS Trough concentration range of 6 patients was 3.59-19.82 μg·mL-1, two of them were above the safe value (<10 μg·mL-1). AUC0-12 h range was 116.7-305.5 μg·h-1·mL-1. Trough plasma concentration was positively correlated with AUC0-12 h (r=0.997, P=0.001).CONCLUSION A high variability of linezolid plasma concentrations is observed in intensively cared patients. To prevent bacterial resistance, ensure clinical outcome and reduce adverse reactions, pharmacokinetics/pharmacodynamics of linezolid should be monitored to develop individualized regimen of linezolid in clinical practice.
Keywords:linezolid  intensive care unit  pharmacokinetics  
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