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首页> 外文期刊>Antimicrobial agents and chemotherapy. >Potentiation effects of amikacin and fosfomycin against selected amikacin-nonsusceptible gram-negative respiratory tract pathogens
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Potentiation effects of amikacin and fosfomycin against selected amikacin-nonsusceptible gram-negative respiratory tract pathogens

机译:阿米卡星和磷霉素对选定的非阿米卡星敏感性克氏阴性呼吸道病原体的增强作用

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摘要

The amikacin-fosfomycin inhalation system (AFIS) is a combination of 2 antibiotics and an in-line nebulizer delivery system that is being developed for adjunctive treatment of pneumonia caused by Gram-negative organisms in patients on mechanical ventilation. AFIS consists of a combination of amikacin and fosfomycin solutions at a 5:2 ratio (amikacin, 3 ml at 100 mg/ml; fosfomycin, 3 ml at 40 mg/ml) and the PARI Investigational eFlow Inline System. In this antibiotic potentiation study, the antimicrobial activities of amikacin and fosfomycin, alone and in a 5:2 combination, were assessed against 62 Gram-negative pathogens from a worldwide antimicrobial surveillance collection (SENTRY). The amikacin MICs for 62 isolates of Acinetobacter baumannii, Pseudomonas aeruginosa, and Klebsiella pneumoniae were ≥32 μg/ml (intermediate or resistant according to the Clinical and Laboratory Standards Institute [CLSI]; resistant according to the European Committee on Antimicrobial Susceptibility Testing [EUCAST]). Each isolate was tested against amikacin (0.25 to 1,024 μg/ml), fosfomycin (0.1 to 409.6 μg/ml), and amikacin-fosfomycin (at a 5:2 ratio) using CLSI reference agar dilution methods. The median MIC values for amikacin and fosfomycin against the 62 isolates each decreased 2-fold with the amikacin-fosfomycin (5:2) combination from that with either antibiotic alone. Interactions between amikacin and fosfomycin differed by isolate and ranged from no detectable interaction to high potentiation. The amikacin-fosfomycin (5:2) combination reduced the amikacin concentration required to inhibit all 62 isolates from >1,024 to ≤256 μg/ml and reduced the required fosfomycin concentration from 204.8 to 102.4 μg/ml. These results support continued development of the amikacin-fosfomycin combination for aerosolized administration, where high drug levels can be achieved.
机译:阿米卡星-磷霉素吸入系统(AFIS)是两种抗生素和在线雾化器输送系统的组合,该系统正在开发中,用于辅助治疗在机械通气患者中由革兰氏阴性菌引起的肺炎。 AFIS由比例为5:2的阿米卡星和磷霉素溶液(阿米卡星,浓度为100 mg / ml的3 ml;磷磷霉素,浓度为40 mg / ml的3 ml)和PARI研究用eFlow在线系统组成。在这项抗生素增效研究中,评估了阿米卡星和磷霉素的抗菌活性,并以5:2的组合对来自全球抗菌监测收集机构(SENTRY)的62种革兰氏阴性病原体进行了评估。 62个鲍曼不动杆菌,铜绿假单胞菌和肺炎克雷伯菌的分离株的阿米卡星MIC≥32μg/ ml(根据临床和实验室标准协会[CLSI]为中等或耐药;根据欧洲抗菌药物敏感性测试委员会[EUCAST]为耐药])。使用CLSI参考琼脂稀释法对每种分离物进行抗阿米卡星(0.25至1,024μg/ ml),磷霉素(0.1至409.6μg/ ml)和阿米卡星-磷霉素(5:2比例)的测试。阿米卡星-磷霉素(5:2)联合用药时,阿米卡星和磷霉素对62株分离菌的平均MIC值降低了2倍,而单独使用任何一种抗生素的MIC值却降低了2倍。阿米卡星和磷霉素之间的相互作用因分离物而异,范围从无可检测的相互作用到高增强作用。阿米卡星-磷霉素(5:2)的组合将抑制所有62个分离株所需的阿米卡星浓度从> 1,024降低到了≤256μg/ ml,将磷霉素的浓度从204.8降低到102.4μg/ ml。这些结果支持了用于雾化给药的阿米卡星-磷霉素组合的继续开发,其中可以实现高药物水平。

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