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大环内酯类药物对麻风分枝杆菌的体外及体内活性

In vitro and in vivo activities of macrolides against Mycobacterium leprae.

作者信息

Franzblau S G, Hastings R C

机构信息

Gillis W. Long Hansen's Disease Center, Carville, Louisiana 70721.

出版信息

Antimicrob Agents Chemother. 1988 Dec;32(12):1758-62. doi: 10.1128/AAC.32.12.1758.

Abstract

We previously demonstrated the potent in vitro activity of erythromycin against Mycobacterium leprae as determined by its effect on ATP pools and rates of palmitate oxidation and phenolic glycolipid I synthesis. In the present study, the relative in vitro activities of a number of new macrolides with superior pharmacokinetic properties were assessed. In addition, for the most active compounds, concentrations in serum were determined by bioassay during continuous administration in the feed of mice, and in vivo activity against M. leprae was assessed by the kinetic mouse footpad technique. Both clarithromycin and roxithromycin were more potent than erythromycin in vitro, with the former showing the highest activity in accelerating rates of ATP decay and reducing rates of palmitate oxidation. In mice, concentrations of clarithromycin in serum were higher than those of roxithromycin and erythromycin, with the latter undetectable even when administered at 0.1% (wt/wt) in the diet. When administered at 0.01% (wt/wt) in the diet, erythromycin and roxithromycin were unable to inhibit growth of M. leprae in mouse footpads whereas clarithromycin demonstrated bactericidal-type activity. On the basis of these data and other properties of macrolides, a clinical trial of clarithromycin in leprosy is warranted.

摘要

我们之前已证明,红霉素对麻风分枝杆菌具有强大的体外活性,这是通过其对三磷酸腺苷(ATP)池、棕榈酸氧化速率以及酚糖脂I合成速率的影响来确定的。在本研究中,我们评估了一些具有更优药代动力学特性的新型大环内酯类药物的相对体外活性。此外,对于活性最强的化合物,在持续经饲料给药的小鼠中,通过生物测定法测定血清浓度,并采用动态小鼠足垫技术评估其对麻风分枝杆菌的体内活性。克拉霉素和罗红霉素在体外均比红霉素更具活性,前者在加速ATP衰减速率和降低棕榈酸氧化速率方面表现出最高活性。在小鼠中,血清中克拉霉素的浓度高于罗红霉素和红霉素,后者即使在饲料中以0.1%(重量/重量)给药时也检测不到。当在饲料中以0.01%(重量/重量)给药时,红霉素和罗红霉素无法抑制小鼠足垫中麻风分枝杆菌的生长,而克拉霉素表现出杀菌型活性。基于这些数据以及大环内酯类药物的其他特性,有必要对克拉霉素治疗麻风病进行临床试验。

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J Infect Dis. 1971 Feb;123(2):216-9. doi: 10.1093/infdis/123.2.216.
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