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头孢噻肟和头孢唑肟的比较药代动力学以及去乙酰头孢噻肟在头孢噻肟抗菌活性中的作用。

Comparative pharmacokinetics of cefotaxime and ceftizoxime and the role of desacetylcefotaxime in the antibacterial activity of cefotaxime.

作者信息

Quintiliani R, Nightingale C H, Tilton R

出版信息

Diagn Microbiol Infect Dis. 1984 Jun;2(3 Suppl):63S-70S.

PMID:6086220
Abstract

A single 15 mg/kg i.v. dose of cefotaxime (CTX) and ceftizoxime (CTZ) were given to six adult volunteers on two separate occasions in a cross-over experiment to determine the pharmacokinetics of each drug and the desacetyl metabolite of cefotaxime, desacetylcefotaxime (des-CTX). From these data, mock serum samples were prepared in human serum to simulate the concentrations of CTX, CTZ, and des-CTX at the following times postdose: 5, 10, 30, and 45 min; 1, 1.5, 2, 3, 4, 5, 6, 8, and 10 hr. At each of these time periods, serum bacteriostatic and bactericidal assays were performed against selected pathogens (Escherichia coli, Serratia marcescens, Enterobacter species) with similar susceptibilities to CTX and CTZ, but with varying sensitivity to des-CTX, and against one organism (Bacteroides fragilis) toward which CTX and des-CTX exhibited synergistic activity. From these studies, it was found that des-CTX can appreciably lengthen the microbiologic action of CTX when it has a high degree of inherent activity (MIC less than or equal to mcg/ml) against the organism, or when it behaves synergistically with CTX toward the bacterium, or both. It is possible that the major advance of CTX and CTZ pertains to their ability to kill many organisms at extremely low concentrations, allowing for monotherapy with low and infrequent dosing, which is very cost-effective in comparison with high and more frequent dosing required by older agents or with antibiotic combinations.

摘要

在一项交叉实验中,对6名成年志愿者分两次分别静脉注射15 mg/kg的头孢噻肟(CTX)和头孢唑肟(CTZ),以确定每种药物以及头孢噻肟的去乙酰代谢物去乙酰头孢噻肟(des-CTX)的药代动力学。根据这些数据,在人血清中制备模拟血清样本,以模拟给药后以下时间点CTX、CTZ和des-CTX的浓度:5、10、30和45分钟;1、1.5、2、3、4、5、6、8和10小时。在每个时间点,针对对CTX和CTZ敏感性相似但对des-CTX敏感性不同的选定病原体(大肠杆菌、粘质沙雷氏菌、肠杆菌属)以及CTX和des-CTX对其表现出协同活性的一种生物体(脆弱拟杆菌)进行血清抑菌和杀菌试验。从这些研究中发现,当des-CTX对生物体具有高度固有活性(最低抑菌浓度小于或等于微克/毫升),或与CTX对该细菌表现出协同作用,或两者兼有时,des-CTX可显著延长CTX的微生物学作用时间。CTX和CTZ的主要优势可能在于它们能够在极低浓度下杀死多种生物体,从而允许采用低剂量和不频繁给药的单一疗法,与旧药或抗生素联合使用所需的高剂量和更频繁给药相比,这具有很高的成本效益。

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