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首页> 外文期刊>Frontiers in Microbiology >Relationship between Antibiotic Resistance, Biofilm Formation, and Biofilm-Specific Resistance in Acinetobacter baumannii
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Relationship between Antibiotic Resistance, Biofilm Formation, and Biofilm-Specific Resistance in Acinetobacter baumannii

机译:<斜斜杆菌抗生素抗性,生物膜形成和生物膜特异性抗性的关系

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In this study, we aimed to examine the relationships between antibiotic resistance, biofilm formation, and biofilm-specific resistance in clinical isolates of Acinetobacter baumannii . The tested 272 isolates were collected from several hospitals in China during 2010–2013. Biofilm-forming capacities were evaluated using the crystal violet staining method. Antibiotic resistance/susceptibility profiles to 21 antibiotics were assessed using VITEK 2 system, broth microdilution method or the Kirby-Bauer disc diffusion method. The minimum inhibitory concentration (MIC) and minimum biofilm eradication concentration (MBEC) to cefotaxime, imipenem, and ciprofloxacin were evaluated using micro dilution assays. Genetic relatedness of the isolates was also analyzed by pulsed-field gel electrophoresis (PFGE) and plasmid profile. Among all the 272 isolates, 31 were multidrug-resistant (MDR), and 166 were extensively drug-resistant (XDR). PFGE typing revealed 167 pattern types and 103 clusters with a similarity of 80%. MDR and XDR isolates built up the main prevalent genotypes. Most of the non-MDR isolates were distributed in a scattered pattern. Additionally, 249 isolates exhibited biofilm formation, among which 63 were stronger biofilm formers than type strain ATCC19606. Population that exhibited more robust biofilm formation likely contained larger proportion of non-MDR isolates. Isolates with higher level of resistance tended to form weaker biofilms. The MBECs for cefotaxime, imipenem, and ciprofloxacin showed a positive correlation with corresponding MICs, while the enhancement in resistance occurred independent of the quantity of biofilm biomass produced. Results from this study imply that biofilm acts as a mechanism for bacteria to get a better survival, especially in isolates with resistance level not high enough. Moreover, even though biofilms formed by isolates with high level of resistance are always weak, they could still provide similar level of protection for the isolates. Further explorations genetically would improve our understanding of these processes and provide novel insights in the therapeutics and prevention against A. baumannii biofilm-related infections.
机译:在这项研究中,我们旨在研究抗生素抗性,生物膜形成和临床分离株的抗生素抗性,生物膜形成和生物膜特异性的关系。在2010 - 2013年期间,从中国的几家医院收集了测试的272个分离物。使用晶体紫染色方法评价生物膜形成能力。使用Vitek 2系统,肉汤微泡法或Kirby-Bauer盘扩散法评估抗生素抗性/易感性至21种抗生素的谱。使用微量稀释测定评估最小抑制浓度(MIC)和最小生物膜根除浓度(MBEC)至头孢噻肟,亚胺蛋白和环丙沙星。通过脉冲场凝胶电泳(PFGE)和质粒分析,还分析了分离物的遗传相关性。在所有272个分离物中,31是多药抗性(MDR),166个是广泛的耐药性(XDR)。 PFGE键入显示167种模式类型和103个簇,其相似度为80%。 MDR和XDR分离ates建立了主要的普遍性基因型。大多数非MDR分离株以分散的图案分布。另外,249个分离株表现出生物膜形成,其中63个比菌株ATCC19606的菌株更强的生物膜成型剂。表现出更强大的生物膜形成的人口可能包含较大比例的非MDR分离株。分离含量较高的电阻趋势,形成弱生物膜。 Cefotaxime,ImipeNem和Ciphofloxacin的MBEC与相应的麦克风显示出正相关,而抗性的增强与产生的生物膜生物质的量无关。本研究的结果意味着生物膜作为细菌的机制,以获得更好的生存,特别是在具有足够高的阻力水平的分离物中。此外,即使通过具有高耐受性高水平的分离物形成的生物膜始终弱,它们仍然可以为隔离物提供类似的保护水平。进一步的探索将改善我们对这些过程的理解,并提供对A.Baumannii生物膜相关感染的治疗和预防的新见解。

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