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瓣膜病变的发育状态对实验性肠球菌感染中头孢噻肟抗菌活性的影响。

Influence of the developmental state of valvular lesions on the antimicrobial activity of cefotaxime in experimental enterococcal infections.

作者信息

Sullam P M, Drake T A, Täuber M G, Hackbarth C J, Sande M A

出版信息

Antimicrob Agents Chemother. 1985 Mar;27(3):320-3. doi: 10.1128/AAC.27.3.320.

Abstract

Cefotaxime has little antimicrobial activity in vitro against most strains of enterococci, as measured by conventional MICs and MBCs. However, the MICs of cefotaxime against many enterococci are markedly reduced by the addition of serum to the test medium. To assess the relevance of this observation in vivo, we examined the efficacy of cefotaxime in experimental Streptococcus faecalis endocarditis. Since response to antimicrobial agents may vary with the degree of vegetation development, therapeutic efficacy was assessed both in rabbits with newly formed vegetations and in rabbits with well-developed endocardial lesions. Peak serum levels of cefotaxime (50.1 +/- 20.0 micrograms/ml) exceeded the MIC in medium supplemented with serum (4 micrograms/ml), but not in Mueller-Hinton broth alone (greater than 64 micrograms/ml). After 4 days of therapy, animals with newly formed lesions (therapy initiated 1 h after infection, transvalvular catheters removed) had lower mean vegetation bacterial titers than did untreated controls. Among animals with mature vegetations (therapy initiated 12 h after infection, catheters indwelling), the rate of mortality was significantly reduced by cefotaxime therapy. However, no difference in vegetation titers was observed. Thus, cefotaxime demonstrated antienterococcal activity within newly formed vegetations, but did not inhibit bacterial proliferation within well-established vegetations.

摘要

通过传统的最低抑菌浓度(MIC)和最低杀菌浓度(MBC)测定,头孢噻肟对大多数肠球菌菌株在体外几乎没有抗菌活性。然而,在测试培养基中添加血清后,头孢噻肟对许多肠球菌的MIC显著降低。为了评估这一观察结果在体内的相关性,我们研究了头孢噻肟在实验性粪肠球菌心内膜炎中的疗效。由于对抗菌药物的反应可能随赘生物发展程度而变化,因此在有新形成赘生物的兔子和有发育良好的心内膜病变的兔子中均评估了治疗效果。头孢噻肟的血清峰值水平(50.1±20.0微克/毫升)在补充血清的培养基中超过了MIC(4微克/毫升),但在单独的穆勒-欣顿肉汤中未超过(大于64微克/毫升)。治疗4天后,有新形成病变的动物(感染后1小时开始治疗,移除经瓣膜导管)的平均赘生物细菌滴度低于未治疗的对照组。在有成熟赘生物的动物中(感染后12小时开始治疗,导管留置),头孢噻肟治疗显著降低了死亡率。然而,未观察到赘生物滴度有差异。因此,头孢噻肟在新形成的赘生物中显示出抗肠球菌活性,但在已形成的赘生物中并未抑制细菌增殖。

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