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Imipenem reduces the efficacy of vancomycin against Elizabethkingia species

亚胺培南 万古霉素 微生物学 抗生素 生物膜 抗菌剂 生物 抗生素耐药性 细菌 金黄色葡萄球菌 遗传学
作者
Ya‐Sung Yang,Hsing‐Yu Chen,I Chieh Lin,Meng-He Lin,Wei‐Yao Wang,Shu‐Chen Kuo,Wenting Chen,Yun-Hsiang Cheng,Jun‐Ren Sun
出处
期刊:Journal of Antimicrobial Chemotherapy [Oxford University Press]
卷期号:79 (8): 2048-2052
标识
DOI:10.1093/jac/dkae210
摘要

Abstract Background Elizabethkingia spp. are emerging as nosocomial pathogens causing various infections. These pathogens express resistance to a broad range of antibiotics, thus requiring antimicrobial combinations for coverage. However, possible antagonistic interactions between antibiotics have not been thoroughly explored. This study aimed to evaluate the effectiveness of antimicrobial combinations against Elizabethkingia infections, focusing on their impact on pathogenicity, including biofilm production and cell adhesion. Methods Double-disc diffusion, time–kill, and chequerboard assays were used for evaluating the combination effects of antibiotics against Elizabethkingia spp. We further examined the antagonistic effects of antibiotic combinations on biofilm formation and adherence to A549 human respiratory epithelial cells. Further validation of the antibiotic interactions and their implications was performed using ex vivo hamster precision-cut lung sections (PCLSs) to mimic in vivo conditions. Results Antagonistic effects were observed between cefoxitin, imipenem and amoxicillin/clavulanic acid in combination with vancomycin. The antagonism of imipenem toward vancomycin was specific to its effects on the genus Elizabethkingia. Imipenem further hampered the bactericidal effect of vancomycin and impaired its inhibition of biofilm formation and the adhesion of Elizabethkingia meningoseptica ATCC 13253 to human cells. In the ex vivo PCLS model, vancomycin exhibited dose-dependent bactericidal effects; however, the addition of imipenem also reduced the effect of vancomycin. Conclusions Imipenem reduced the bactericidal efficacy of vancomycin against Elizabethkingia spp. and compromised its capacity to inhibit biofilm formation, thereby enhancing bacterial adhesion. Clinicians should be aware of the potential issues with the use of these antibiotic combinations when treating Elizabethkingia infections.
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