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阿米卡星在脊髓损伤患者血清及与压疮相邻组织中的药代动力学。

Pharmacokinetics of amikacin in serum and in tissue contiguous with pressure sores in humans with spinal cord injury.

作者信息

Segal J L, Brunnemann S R, Eltorai I M

机构信息

Department of Medicine, Veterans Affairs Medical Center, Long Beach, California.

出版信息

Antimicrob Agents Chemother. 1990 Jul;34(7):1422-8. doi: 10.1128/AAC.34.7.1422.

Abstract

Pressure sores are a common occurrence in immobilized patients. They increase morbidity and mortality and impede rehabilitation. Antibiotics are routinely used to assist in effecting a cure when infection is present. Nevertheless, for patients with spinal cord injuries (SCI), strategies for effective therapy with antibiotics based on measurement of concentrations in tissue and pharmacokinetic behavior in extravascular spaces do not exist. By analyzing the concentration-time profile and protein binding of amikacin in the interstitial fluid (IF) in contact with pressure sores, we found that the disposition of amikacin in the tissue contiguous with pressure sores appears to be governed by simultaneous first-order and capacity-limited pharmacokinetic behavior. Amikacin disposition in IF proceeded without a simple relationship to amikacin concentrations in serum, and the time course in IF was not accurately simulated by linear models of amikacin pharmacokinetic behavior. Total amikacin clearance estimated from a pharmacokinetic model using simultaneous first-order and nonlinear intercompartmental transfer of amikacin was not significantly different from clearance calculated by us in a prior study of amikacin pharmacokinetic behavior in patients with SCI. In patients with SCI, optimal use of amikacin in the treatment of infected pressure sores is contingent upon accurate characterization of the pharmacokinetic behavior of this aminoglycoside in serum and in the IF in contact with these lesions. Only methods which quantitate amikacin concentration and protein binding in IF and incorporate a model that can simultaneously simulate nonlinear and linear disposition processes should be relied upon to influence therapeutic decision making.

摘要

压疮在卧床患者中很常见。它们会增加发病率和死亡率,并阻碍康复。当存在感染时,抗生素通常用于协助治愈。然而,对于脊髓损伤(SCI)患者,基于组织浓度测量和血管外间隙药代动力学行为的抗生素有效治疗策略并不存在。通过分析与压疮接触的间质液(IF)中阿米卡星的浓度-时间曲线和蛋白结合情况,我们发现与压疮相邻组织中阿米卡星的处置似乎受同时存在的一级和容量限制药代动力学行为支配。IF中阿米卡星的处置与血清中阿米卡星浓度没有简单的关系,并且阿米卡星药代动力学行为的线性模型不能准确模拟IF中的时间进程。使用阿米卡星同时进行一级和非线性隔室间转移的药代动力学模型估计的总阿米卡星清除率与我们之前在SCI患者中对阿米卡星药代动力学行为的研究中计算的清除率没有显著差异。在SCI患者中,在治疗感染性压疮时优化使用阿米卡星取决于准确描述这种氨基糖苷类药物在血清和与这些损伤接触的IF中的药代动力学行为。只有能够定量IF中阿米卡星浓度和蛋白结合并纳入可同时模拟非线性和线性处置过程模型的方法,才能用于影响治疗决策。

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本文引用的文献

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