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Clonal Diversity Biofilm Formation and Antimicrobial Resistance among Stenotrophomonas maltophilia Strains from Cystic Fibrosis and Non-Cystic Fibrosis Patients

机译:囊性纤维化和非囊性纤维化患者嗜麦芽窄食单胞菌菌株的克隆多样性生物膜形成和抗菌素耐药性

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摘要

The intrinsic antibiotic resistance of , along with its ability to form biofilm both on abiotic surfaces and host tissues, dramatically affects the efficacy of the antibiotic therapy. In this work, 85 strains isolated in several hospital of central Italy and from several clinical settings were evaluated for their genetic relatedness (by pulsed-field gel electrophoresis, PFGE), biofilm formation (by microtiter plate assay), and planktonic antibiotic resistance (by Kirby–Bauer disk diffusion technique). The population showed a high genetic heterogeneity: 64 different PFGE types were identified, equally distributed in cystic fibrosis (CF) and non-CF strains, and some consisted of multiple strains. Most of the strains (88.2%) were able to form biofilm, although non-CF strains were significantly more efficient than CF strains. CF strains produced lower biofilm amounts than non-CF strains, both those from respiratory tracts and blood. Non-CF PFGE types 3 and 27 consisted of strong-producers only. Cotrimoxazole and levofloxacin were the most effective antibiotics, being active respectively against 81.2% and 72.9% of strains. CF strains were significantly more resistant to piperacillin/tazobactam compared to non-CF strains (90% versus 53.3%), regardless of sample type. Among respiratory strains, cotrimoxazole was more active against non-CF than CF strains (susceptibility rates: 86.7% versus 75%). The multidrug resistant phenotype was significantly more prevalent in CF than non-CF strains (90% versus 66.7%). Overall, the multidrug-resistance level was negatively associated with efficiency in biofilm formation. Our results showed, for the first time, that in both classical planktonic drug resistance and the ability of biofilm formation might favor its dissemination in the hospital setting. Biofilm formation might in fact act as a survival mechanism for susceptible bacteria, suggesting that clinical isolates should be routinely assayed for biofilm formation in diagnostic laboratories.
机译:内在的抗生素抗性及其在非生物表面和宿主组织上形成生物膜的能力极大地影响了抗生素治疗的功效。在这项工作中,评估了意大利中部几家医院和几种临床环境中分离出的85株菌株的遗传相关性(通过脉冲场凝胶电泳,PFGE),生物膜形成(通过微量滴定板测定)和浮游抗生素耐药性(通过Kirby–Bauer磁盘扩散技术)。该种群显示出高度的遗传异质性:鉴定出64种不同的PFGE类型,它们均等地分布在囊性纤维化(CF)和非CF菌株中,其中一些由多种菌株组成。大多数菌株(88.2%)能够形成生物膜,尽管非CF菌株比CF菌株效率更高。 CF菌株产生的生物膜数量低于非CF菌株,无论是呼吸道还是血液。非CF PFGE类型3和27仅由强大的生产者组成。复方新诺明和左氧氟沙星是最有效的抗生素,分别对81.2%和72.9%的菌株具有活性。与非CF菌株相比,CF菌株对哌拉西林/他唑巴坦的耐药性要高得多(无论样品类型如何,其抗性分别为90%和53.3%)。在呼吸道菌株中,cotrimoxazole对非CF的活性高于CF菌株(敏感性:86.7%对75%)。 CF中的多药耐药表型显着高于非CF株(90%对66.7%)。总体而言,多药耐药水平与生物膜形成效率呈负相关。我们的结果首次表明,在经典的浮游药物耐药性和生物膜形成能力方面,都可能有利于其在医院中的传播。实际上,生物膜的形成可能是易感细菌的生存机制,这表明应在诊断实验室中常规检测临床分离株的生物膜形成。

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