Investigation of in vitro efficacy of meropenem/polymyxin B and meropenem/fosfomycin combinations against carbapenem resistant Klebsiella pneumoniae strains.

IF 1.3 4区 医学 Q4 IMMUNOLOGY
Rıza Adaleti, Yaşar Nakipoğlu, Şeyma Çalık, Neslihan Arıcı, Nilgün Kansak, Seniha Şenbayrak, Sebahat Aksaray
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Abstract

The incidence of infections caused by carbapenem-resistant Klebsiella pneumoniae (CRKP) is increasing worldwide, and very limited number of effective antibiotics are available for therapy. In our study, the in vitro efficacy of meropenem/polymyxin B and meropenem/fosfomycin combinations against CRKP strains was investigated. The efficiency of meropenem/polymyxin B and meropenem/fosfomycin combinations was tested by checkerboard microdilution and checkerboard agar dilution methods, respectively, against 21 CRKP strains containing major carbapenem resistant genes (7 blaKPC, 7 blaOXA-48 gene, and 7 blaOXA-48+ blaNDM), and seven additional CRKP strains without carbapenemase genes.Among the 28 CRKP strains, the meropenem/polymyxin B combination was synergistic in ten (35.7%), partially synergistic in 12 (42.8%), and indifferent in six (21.4%) isolates. The meropenem/fosfomycin combination was found to be synergistic in three isolates (10.7%), partially synergistic in 20 (71.4%), and indifferent in five (17.8%). In 21 strains containing carbapenem resistance genes, meropenem/polymyxin B and meropenem/fosfomycin combinations exhibited synergistic/partial synergistic effects in 15 (71.4%) and 16 (76.2%) strains, respectively, compared to 100% synergistic/partial synergistic efficiency in both combinations in seven strains free of carbapenemase genes. No antagonistic effect was detected in either combination.Regardless of presence or absence of carbapenem resistance genes, meropenem/polymyxin B and meropenem/fosfomycin combinations both demonstrated high synergistic and partial synergistic activity against 78.4% and 82.1% of CRKP strains, respectively. Also, they have no antagonistic effects and can be used successfully to prevent therapeutic failure with monotherapy, according to our in vitro studies.

美罗培南/多粘菌素B及美罗培南/磷霉素联合用药对耐碳青霉烯肺炎克雷伯菌的体外疗效观察。
耐碳青霉烯肺炎克雷伯菌(CRKP)引起的感染在世界范围内正在增加,而可用于治疗的有效抗生素数量非常有限。本研究考察了美罗培南/多粘菌素B和美罗培南/磷霉素联合用药对CRKP菌株的体外抑菌效果。采用棋盘格微量稀释法和棋盘格琼脂稀释法分别检测美罗培南/多粘菌素B和美罗培南/磷霉素联合用药对21株含碳青霉烯烯主要耐药基因(7株blaKPC、7株blaOXA-48基因和7株blaNDM基因)的CRKP和另外7株不含碳青霉烯酶基因的CRKP的抑菌效果。在28株CRKP菌株中,美罗培南/多粘菌素B联合增效10株(35.7%),部分增效12株(42.8%),无增效6株(21.4%)。美罗培南/磷霉素联合用药对3株(10.7%)有增效作用,20株(71.4%)有部分增效作用,5株(17.8%)无增效作用。在含有碳青霉烯酶耐药基因的21株菌株中,美罗培南/多粘菌素B联合和美罗培南/磷霉素联合分别有15株(71.4%)和16株(76.2%)具有增效/部分增效作用,而在无碳青霉烯酶基因的7株菌株中,两种组合的增效/部分增效效果为100%。两种组合均无拮抗作用。无论是否存在碳青霉烯类耐药基因,美罗培南/多粘菌素B和美罗培南/磷霉素联合对CRKP菌株分别表现出78.4%和82.1%的高增效和部分增效活性。此外,根据我们的体外研究,它们没有拮抗作用,可以成功地用于预防单药治疗失败。
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来源期刊
CiteScore
2.30
自引率
13.30%
发文量
36
审稿时长
>12 weeks
期刊介绍: AMIH is devoted to the publication of research in all fields of medical microbiology (bacteriology, virology, parasitology, mycology); immunology of infectious diseases and study of the microbiome related to human diseases.
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