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通过微透析法测定健康志愿者肌肉和皮下脂肪组织中头孢地嗪和头孢匹罗的血清浓度与游离组织间液浓度之间的关系。

Relationship between serum and free interstitial concentrations of cefodizime and cefpirome in muscle and subcutaneous adipose tissue of healthy volunteers measured by microdialysis.

作者信息

Müller M, Rohde B, Kovar A, Georgopoulos A, Eichler H G, Derendorf H

机构信息

Department of Clinical Pharmacology, Vienna University School of Medicine, Austria.

出版信息

J Clin Pharmacol. 1997 Dec;37(12):1108-13. doi: 10.1002/j.1552-4604.1997.tb04294.x.

DOI:10.1002/j.1552-4604.1997.tb04294.x
PMID:9506005
Abstract

Microdialysis is a suitable method to monitor unbound concentrations of antimicrobial drugs in the interstitial tissue space which is the site of many infections. The aim of this investigation was to examine whether free tissue levels of cefodizime (81% plasma protein binding) and cefpirome (10% plasma protein binding) in muscle and subcutaneous adipose tissue of healthy volunteers obtained by microdialysis are consistent with the extent of their respective plasma protein binding. Healthy volunteers were given cefodizine and cefpirome at a single intravenous 2-g dose in a randomized crossover design. Microdialysis probes were inserted into a medial vastus muscle and into the periumbilical subcutaneous layer. After calibration of the probe, samples of serum and microdialysis fluid were obtained and drug concentrations were measured using a microagar diffusion-bioassay. There was a reasonable agreement between plasma protein binding data and the tissue penetration of both cephalosporins (AUC0-infinity tissue, free/AUC0-infinity serum, total-ratios) into the interstitial fluid of the muscle tissue, but not for the subcutaneous tissue layer. Furthermore, the serum and tissue concentrations of both drugs were fitted to an open two-compartment body model. The measured free-tissue concentrations were compared with calculated unbound concentrations in the peripheral compartment. Good agreement was observed for the free muscle concentrations, but unbound concentrations in the subcutaneous tissue was somewhat higher (cefpirome) or lower (cefodizime) than predicted. This may be due to the different lipophilicities of the two compounds.

摘要

微透析是一种适用于监测许多感染发生部位——间质组织间隙中抗菌药物游离浓度的方法。本研究的目的是检验通过微透析获得的健康志愿者肌肉和皮下脂肪组织中头孢地嗪(血浆蛋白结合率81%)和头孢匹罗(血浆蛋白结合率10%)的游离组织水平是否与其各自的血浆蛋白结合程度一致。在随机交叉设计中,给健康志愿者单次静脉注射2g剂量的头孢地嗪和头孢匹罗。将微透析探针插入股内侧肌和脐周皮下层。在对探针进行校准后,采集血清和微透析液样本,并使用微量琼脂扩散生物测定法测量药物浓度。血浆蛋白结合数据与两种头孢菌素进入肌肉组织间质液的组织穿透情况(AUC0-无穷大组织,游离/AUC0-无穷大血清,总比值)之间存在合理的一致性,但皮下组织层并非如此。此外,将两种药物的血清和组织浓度拟合到一个开放的二室体内模型。将测得的游离组织浓度与外周室中计算出的游离浓度进行比较。观察到游离肌肉浓度之间有良好的一致性,但皮下组织中的游离浓度比预测值略高(头孢匹罗)或略低(头孢地嗪)。这可能是由于这两种化合物的亲脂性不同。

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