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克拉霉素治疗鸟分枝杆菌复合群感染

Clarithromycin against Mycobacterium avium complex infections.

作者信息

Heifets L B

机构信息

Department of Microbiology, University of Colorado Health Sciences Center, USA.

出版信息

Tuber Lung Dis. 1996 Feb;77(1):19-26. doi: 10.1016/s0962-8479(96)90070-2.

Abstract

The turning point in antimicrobial therapy of Mycobacterium avium infections came with the development of two new macrolides, clarithromycin and azithromycin. Controlled clinical trials, the first ever conducted with any agent among patients with M. avium infection, indicated the high efficiency of clarithromycin, in either acquired immune deficiency syndrome (AIDS) patients having a disseminated infection or non-AIDS patients with localized pulmonary disease. Monotherapy with clarithromycin resulted in elimination of bacteremia in almost all patients with disseminated infection, which is inevitably followed by a relapse of bacteremia in patients who survived long enough to reach this event. The strains susceptible to clarithromycin isolated before therapy contained 10(-8) or 10(-9) resistant mutants, and the relapses of bacteremia were caused by multiplication of these pre-existing mutants. Clarithromycin-resistance was associated with a mutation in the 23S rRNA gene. Cross-resistance between clarithromycin and azithromycin was confirmed with laboratory mutants and clinical isolates. At least two methods for determining the susceptibility of the M. avium isolates to clarithromycin are available: one is minimum inhibitory concentration (MIC) determination on Mueller-Hinton agar (pH 7.4) supplemented with 10% Oleic acid-albumin-dextrose catalase, the other is MIC determination in 7H12 broth, also at pH 7.4. The breakpoints for 'susceptible' for these methods are < or = 8.0 micrograms/ml and < or = 2.0 micrograms/ml, respectively. The breakpoints for 'resistant' are > 128 micrograms/ml for the agar method and > 32.0 micrograms/ml for the broth method. The predictability value of MIC determination was confirmed by comparing the test results with the patients' clinical and bacteriological response to therapy. The remaining major problem in the therapy of the M. avium infections is a selection of companion drugs to be used in combination with clarithromycin (or azithromycin) to prevent the emergence of the macrolide-resistance. A number of clinical trials are now in progress to find a solution to this problem.

摘要

鸟分枝杆菌感染抗菌治疗的转折点在于两种新型大环内酯类药物——克拉霉素和阿奇霉素的研发。有史以来首次针对鸟分枝杆菌感染患者使用任何药物进行的对照临床试验表明,克拉霉素对患有播散性感染的获得性免疫缺陷综合征(AIDS)患者或患有局限性肺部疾病的非AIDS患者均具有高效性。几乎所有播散性感染患者采用克拉霉素单药治疗后菌血症均得以消除,但存活时间足够长到出现这种情况的患者不可避免地会出现菌血症复发。治疗前分离出的对克拉霉素敏感的菌株含有10^(-8)或10^(-9)的耐药突变体,菌血症复发是由这些预先存在的突变体增殖所致。克拉霉素耐药与23S rRNA基因的突变有关。克拉霉素与阿奇霉素之间的交叉耐药已通过实验室突变体和临床分离株得到证实。目前有至少两种方法可用于测定鸟分枝杆菌分离株对克拉霉素的敏感性:一种是在补充了10%油酸 - 白蛋白 - 葡萄糖过氧化氢酶的穆勒 - 欣顿琼脂(pH 7.4)上测定最低抑菌浓度(MIC),另一种是在pH 7.4的7H12肉汤中测定MIC。这些方法中“敏感”的断点分别为≤8.0微克/毫升和≤2.0微克/毫升。“耐药”的断点对于琼脂法是>128微克/毫升,对于肉汤法是>32.微克/毫升。通过将检测结果与患者对治疗的临床和细菌学反应进行比较,证实了MIC测定的预测价值。鸟分枝杆菌感染治疗中剩下的主要问题是选择与克拉霉素(或阿奇霉素)联合使用的辅助药物以防止大环内酯类耐药的出现。目前正在进行多项临床试验以寻找解决这个问题的方法。

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