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新生儿头孢唑林分布容积的个体间变化及其基于生理药代动力学概念的预测

Interindividual changes in volume of distribution of cefazolin in newborn infants and its prediction based on physiological pharmacokinetic concepts.

作者信息

Deguchi Y, Koshida R, Nakashima E, Watanabe R, Taniguchi N, Ichimura F, Tsuji A

机构信息

Hospital Pharmacy, University of Kanazawa, Japan.

出版信息

J Pharm Sci. 1988 Aug;77(8):674-8. doi: 10.1002/jps.2600770807.

Abstract

The purpose of this study was to investigate factors affecting the volume of distribution of cefazolin (a beta-lactam antibiotic) in newborn infants with bacterial infections, and to propose a method for predicting the volume of distribution at steady state per body weight (Vdss/BW). Cefazolin and tobramycin (an aminoglycoside) were simultaneously given to newborn infants (aged 2 to 28 d), and plasma concentration-time data were analyzed on the basis of model-independent moment analysis. The Vdss/BW values ranged from 0.212 to 0.373 L/kg for cefazolin and from 0.384 to 0.541 L/kg for tobramycin. The unbound fraction of cefazolin in plasma (fp) fluctuated widely, from 0.22 to 0.83, among patients. The Vdss/BW value for cefazolin was characterized by both large extracellular water volume and a remarkable change in fp, and could be predicted as a function of fp using physiological pharmacokinetic concepts. Moreover, interindividual changes in the unconjugated bilirubin:albumin molar ratio were predominantly responsible for the individual variation in the fp values of cefazolin in newborn infants.

摘要

本研究的目的是调查影响患有细菌感染的新生儿中头孢唑林(一种β-内酰胺类抗生素)分布容积的因素,并提出一种预测每体重稳态分布容积(Vdss/BW)的方法。将头孢唑林和妥布霉素(一种氨基糖苷类抗生素)同时给予新生儿(年龄2至28天),并基于非模型依赖矩分析法分析血浆浓度-时间数据。头孢唑林的Vdss/BW值范围为0.212至0.373 L/kg,妥布霉素的Vdss/BW值范围为0.384至0.541 L/kg。患者之间血浆中头孢唑林的游离分数(fp)波动很大,从0.22至0.83。头孢唑林的Vdss/BW值的特征是细胞外液量较大且fp有显著变化,并且可以使用生理药代动力学概念预测为fp的函数。此外,未结合胆红素与白蛋白摩尔比的个体间变化是新生儿中头孢唑林fp值个体差异的主要原因。

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