Carumonam体外抗革兰氏阴性菌活性及对其β -内酰胺酶的稳定性。

A Raimondi, R Mattina, C E Cocuzza
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引用次数: 0

摘要

与氨曲南、头孢噻肟、头孢他啶、头孢替坦和头孢曲松比较,对311株革兰氏阴性临床分离株的体外活性进行了评价。Carumonam的抑菌效力等于或高于其他参比化合物;其中对吲哚变形杆菌阳性菌和克雷伯氏菌的抑菌活性与头孢他啶相当,对柠檬酸杆菌、肠杆菌和大肠杆菌的抑菌活性最高。对渗透性改变的生物体进行的最低抑制浓度表明,卡鲁莫南的渗透率与阿曲南相当,高于头孢替坦和头孢曲松。Carumonam对染色体和质粒介导的β -内酰胺酶表现出良好的稳定性,这与其对产菌的抑菌活性和接种量效应有关。
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Carumonam's in-vitro activity against gram-negative bacteria and its stability to their beta-lactamases.

The in vitro activity of the novel monobactam carumonam (RO17-2301) was evaluated on 311 gram-negative clinical isolates in comparison to aztreonam, cefotaxime, ceftazidime, cefotetan and ceftriaxone. Carumonam showed an antibacterial potency equal to or higher than any other reference compound; in particular it was the most effective against Proteus indole positive and Klebsiella sp. Its antipseudomonal activity was comparable to that of ceftazidime and it showed, together with aztreonam, the highest activity against the Citrobacter, Enterobacter and Escherichia coli isolates. The minimal inhibitory concentrations performed on permeability altered organisms indicated that carumonam has a penetration rate comparable to aztreonam and higher than cefotetan and ceftriaxone. Carumonam demonstrated excellent stability to chromosomal and plasmid-mediated beta-lactamases and that correlated with its antibacterial activity against the producing strains and inoculum size effect.

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