亚抑制剂量抗生素和纳米银颗粒对尿路致病菌的长期暴露影响

M. J. Mbarga, Razan Marouf, I. Podoprigora, Kitio L.D. Anyutoulou, Y. Chapurin, Irina N. Sharova
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引用次数: 0

摘要

相关性。虽然使用抗生素的主要目的是治疗传染病,但滥用抗生素会逐渐导致其效力丧失。本次调查旨在探索尿路致病菌在长期接触抗菌素后发生的变化。材料和方法。我们比较了长期接触氨苄西林、头孢唑啉、卡那霉素和纳米银颗粒(AgNPs)对 4 种临床尿路致病菌(即大肠埃希菌(UPEC)、金黄色葡萄球菌(S. aureus)、粪肠球菌(E. faecalis)和无乳链球菌(St. agalactiae))的敏感性、生物膜形成和浮游细菌的影响。使用微孔板循环稀释法测定最低抑菌浓度(MIC),并将细菌置于脑心输液肉汤中制备的浓度不断增加的每种抗菌剂(从 MIC/2 到 MIC)中 8 天。使用柯比鲍尔盘扩散法评估细菌对抗生素的敏感性,使用水晶紫细菌附着试验评估生物膜的形成。结果与讨论。这项调查的数据突出表明,长期接触抗菌药物可能会导致泌尿系统致病菌株对其他抗生素的敏感性发生变化,并形成生物膜。事实上,接触氨苄西林会使粪肠球菌对头孢唑肟产生抗药性,使痢疾杆菌对四环素、头孢唑肟/克拉维酸和头孢唑肟产生抗药性。暴露于头孢唑啉后,大肠杆菌对头孢他啶/克拉维酸头孢他啶和头孢他啶的敏感性显著下降,而金黄色葡萄球菌对头孢他啶/克拉维酸头孢他啶、头孢他啶和头孢曲松产生了抗药性。阿加拉菌和粪大肠杆菌也出现了类似的变化,除了对上述三种抗生素产生抗药性外,还对四环素产生了抗药性。在接触卡那霉素后,对抗生素的敏感性发生了最明显的变化:大肠杆菌对头孢唑肟产生了抗药性,对头孢唑肟/克拉维酸的敏感性下降,而金黄色葡萄球菌、粪大肠杆菌和无乳酸圣氏菌都对头孢唑肟/克拉维酸和头孢唑肟产生了抗药性。此外,除大肠杆菌外,本次调查中所有在 AgNPs 中连续培养的细菌都对头孢他啶/克拉维酸和头孢唑肟产生了抗药性。与各自的对照组相比,暴露于氨苄西林和头孢唑啉的细菌产生的生物膜更多。结论尿路病原体长期接触抗生素和 AgNPs 会导致对其他抗生素的敏感性和生物膜的形成发生显著变化,因此只有在必要时才能使用抗生素。
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Long exposure impact of antibiotics subinhibitory doses and silver nanoparticles on uropathogenic bacteria
Relevance. Although the primary purpose of using antibiotics is to treat infectious diseases, their misuse gradually leads to loss of their effectiveness. The aim of the current investigation was to explore the changes that occur in uropathogenic bacteria after long exposure to antimicrobials. Materials and Methods. We compared the effects of long-term exposure to ampicillin, cefazoline, kanamycin and silver nanoparticles (AgNPs) on susceptibility, biofilm formation and planktonic bacteria in 4 clinical uropathogenic strains namely Escherichia coli (UPEC), Staphylococcus aureus (S. aureus), Enterococcus faecalis (E. faecalis) and Streptococcus agalactiae (St. agalactiae). The minimum inhibitory concentrations (MIC) were determined using the microplate mircodilution method and bacteria were exposed to increasing concentrations of each antimicrobial (from MIC/2 to MIC) prepared in the brain heart infusion broth for 8 days. The susceptibility of bacteria to antibiotics was assessed using the Kirby Bauer disc diffusion method and the biofilm formation was assessed using crystal violet bacterial attachment assay. Results and Discussion. The data in this investigation highlight that long-term exposure to antimicrobials may induce changes in susceptibility to other antibiotics and biofilm formation in Uropathogenic strains. Indeed, exposure to ampicillin made E. faecalis resistant to ceftazidime and St agalactiae resistant to tetracycline, ceftazidime/clavulanate and ceftazidime. Following exposure to cefazolin, a significant decrease in susceptibility was observed in E. coli to ceftazidime/clavulanate and ceftazidime while S. aureus became resistant to ceftazidime/clavulanate, ceftazidime and to ceftriaxone. Similar variations were observed on St agalactiae and E. faecalis, which in addition to the 3 antibiotics above-mentioned, have become resistant to tetracycline. The most significant variations in susceptibility to antibiotics were observed following exposure to kanamycin: E. coli developed resistance to ceftazidime and a decrease in sensitivity was noted on ceftazidime/clavulanate while S. aureus, E. faecalis and St. agalactiae all 3 became resistant to ceftazidime/clavulanate and ceftazidime. In addition, except for E. coli all the bacteria in this investigation which had undergone successive passages in AgNPs developed resistance to ceftazidime/ clavulanate and ceftazidime. Bacteria exposed to ampicillin and cefazolin produced more biofilms than their respective controls. Conclusion. Long term exposure of uropathogens to antibiotics and AgNPs induces significant changes in susceptibility to other antibiotics and biofilm formation and antibiotics should therefore only be used when necessary.
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