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首页> 外文期刊>The Journal of Antimicrobial Chemotherapy >HMR 3647 human-like treatment of experimental pneumonia due to penicillin-resistant and erythromycin-resistant Streptococcus pneumoniae.
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HMR 3647 human-like treatment of experimental pneumonia due to penicillin-resistant and erythromycin-resistant Streptococcus pneumoniae.

机译:HMR 3647对因青霉素耐药和对红霉素耐药的肺炎链球菌引起的实验性肺炎进行人样治疗。

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摘要

An experimental Streptococcus pneumoniae pneumonia model in rabbits was used to assess the efficacy of amoxycillin, erythromycin and a new ketolide, telithromycin (HMR 3647). The MICs of amoxycillin, erythromycin and HMR 3647 for the three clinical S. pneumoniae strains used were, respectively, (mg/L): 0.01, 16 and 0.02 (strain 195); 2, 0.25 and 0.02 (strain 16089); 8, >64 and 0.02 (strain 11724). Antibiotic therapy reproduced human serum pharmacokinetics (amoxycillin 1 g iv tds or erythromycin 500 mg qds or HMR 3647 800 mg bd). Forty-eight hours of therapy with HMR 3647 and amoxycillin resulted in significant bacterial clearance in the lungs and spleen of rabbits infected by S. pneumoniae strain 195 and strain 16089 (at least 3 log(10) cfu/g decrease, P < 0.001). Erythromycin was active against only the erythromycinsusceptible strain (3 log(10) cfu/g decrease at 48 h, P < 0.001). None of the antibiotics showed significant efficacy with strain 11724. All agents produced significant bacterial clearance when time above MBC was >33%, and microbiological failure when it was <25%, whereas MIC was not correlated with microbiological outcome with HMR 3647. Our findings suggest that pharmacodynamic data integrating MBC may be predictive of microbiological success or failure with greater accuracy than with MIC. HMR 3647 produced significant bacterial clearance in both penicillin- and erythromycin-resistant pneumonia, but was less effective against the highly erythromycin-resistant S. pneumoniae strain.
机译:使用兔实验性肺炎链球菌肺炎模型评估阿莫西林,红霉素和新的酮内酯泰利霉素(HMR 3647)的功效。使用的三种临床肺炎链球菌菌株的阿莫西林,红霉素和HMR 3647的MIC分别为(mg / L):0.01、16和0.02(195株); 2、0.25和0.02(应变16089); 8,> 64和0.02(应变11724)。抗生素疗法可复制人血清的药代动力学(阿莫西林1 g iv tds或红霉素500 mg qds或HMR 3647 800 mg bd)。用HMR 3647和阿莫西林治疗48小时导致被肺炎链球菌195株和16089株感染的兔子的肺和脾脏具有明显的细菌清除率(降低至少3 log(10)cfu / g,P <0.001) 。红霉素仅对红霉素敏感菌株具有活性(48小时降低3 log(10)cfu / g,P <0.001)。没有一种抗生素对11724菌株表现出显着的功效。当超过MBC的时间> 33%时,所有药物均产生明显的细菌清除,而当其<25%时,所有微生物均产生微生物衰竭,而MIC与HMR 3647与微生物结果无关。我们的发现提示结合MBC的药效学数据可以比MIC更准确地预测微生物学的成功或失败。 HMR 3647在耐青霉素和红霉素的肺炎中均产生明显的细菌清除作用,但对高度耐红霉素的肺炎链球菌菌株的效果较差。

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