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Differential Distribution of Plasmid-Mediated Quinolone Resistance Genes in Clinical Enterobacteria with Unusual Phenotypes of Quinolone Susceptibility from Argentina

机译:来自阿根廷的喹诺酮易感性表型的临床肠杆菌中质粒介导的喹诺酮耐药基因的差异分布

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摘要

We studied a collection of 105 clinical enterobacteria with unusual phenotypes of quinolone susceptibility to analyze the occurrence of plasmid-mediated quinolone resistance (PMQR) and oqx genes and their implications for quinolone susceptibility. The oqxA and oqxB genes were found in 31/34 (91%) Klebsiella pneumoniae and 1/3 Klebsiella oxytoca isolates. However, the oqxA- and oqxB-harboring isolates lacking other known quinolone resistance determinants showed wide ranges of susceptibility to nalidixic acid and ciprofloxacin. Sixty of the 105 isolates (57%) harbored at least one PMQR gene [qnrB19, qnrB10, qnrB2, qnrB1, qnrS1, or aac(6′)-Ib-cr)], belong to 8 enterobacterial species, and were disseminated throughout the country, and most of them were categorized as susceptible by the current clinical quinolone susceptibility breakpoints. We developed a disk diffusion-based method to improve the phenotypic detection of aac(6′)-Ib-cr. The most common PMQR genes in our collection [qnrB19, qnrB10, and aac(6′)-Ib-cr] were differentially distributed among enterobacterial species, and two different epidemiological settings were evident. First, the species associated with community-acquired infections (Salmonella spp. and Escherichia coli) mainly harbored qnrB19 (a unique PMQR gene) located in small ColE1-type plasmids that might constitute its natural reservoirs. qnrB19 was not associated with an extended-spectrum β-lactamase phenotype. Second, the species associated with hospital-acquired infections (Enterobacter spp., Klebsiella spp., and Serratia marcescens) mainly harbored qnrB10 in ISCR1-containing class 1 integrons that may also have aac(6′)-Ib-cr as a cassette within the variable region. These two PMQR genes were strongly associated with an extended-spectrum β-lactamase phenotype. Therefore, this differential distribution of PMQR genes is strongly influenced by their linkage or lack of linkage to integrons.
机译:我们研究了105种临床肠杆菌,它们具有不同的喹诺酮敏感性表型,以分析质粒介导的喹诺酮耐药性(PMQR)和oqx基因的发生及其对喹诺酮敏感性的影响。在31/34(91%)肺炎克雷伯菌和1/3产氧克雷伯菌中发现了oqxA和oqxB基因。但是,缺乏其他已知喹诺酮耐药性决定因素的oqxA和oqxB携带病毒的分离株对萘啶酸和环丙沙星的敏感性范围很广。在105个分离株中,有60个(57%)带有至少一个PMQR基因[qnrB19,qnrB10,qnrB2,qnrB1,qnrS1或aac(6')-Ib-cr)],属于8种肠杆菌种,并在整个细菌中传播。国家/地区,并且大多数人被目前的临床喹诺酮类药物敏感性断点归类为易感者。我们开发了一种基于磁盘扩散的方法,以改善aac( 6 ') -Ib-cr 的表型检测。我们的集合中最常见的PMQR基因[ qnrB19 qnrB10 aac 6 ') -Ib-cr ]在肠细菌种间的分布不同,并且有两种不同的流行病学背景。首先,与社区获得性感染相关的物种(沙门氏菌 spp。和大肠杆菌)主要包含 qnrB19 (一个独特的PMQR基因)位于可能构成其天然贮库的小型ColE1型质粒中。 qnrB19 与超广谱β-内酰胺酶表型无关。其次,与医院获得性感染相关的物种(肠杆菌 spp。, Klebsiella spp。和)主要在包含IS CR1 的1类整形体中包含 qnrB10 ,这些整形体也可能具有 aac 6 ') -Ib-cr 作为可变区中的暗盒。这两个PMQR基因与广谱β-内酰胺酶表型密切相关。因此,PMQR基因的这种差异分布会受到它们与整联蛋白的连锁或连锁缺乏的强烈影响。

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