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首页> 外文期刊>Acta microbiologica et immunologica Hungarica: A quarterly of the Hungarian Academy of Sciences >IDENTIFICATION AND CHARACTERIZATION OF CTX-M-15 PRODUCING KLEBSIELLA PNEUMONIAE CLONE ST101 IN A HUNGARIAN UNIVERSITY TEACHING HOSPITAL
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IDENTIFICATION AND CHARACTERIZATION OF CTX-M-15 PRODUCING KLEBSIELLA PNEUMONIAE CLONE ST101 IN A HUNGARIAN UNIVERSITY TEACHING HOSPITAL

机译:匈牙利大学教学医院中生产的CTX-M-15肺炎克雷伯菌肺炎克隆ST101的鉴定和表征

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We investigated the molecular epidemiology of extended spectrum beta-lactamase (ESBL) producing Klebsiella pneumoniae isolates derived from the teaching hospitals of University of Pecs, Pecs, Hungary in the time period 2004-2008. Molecular typing, antimicrobial susceptibility testing, detection of common beta-lactamase genes (bla(CTX-M), bla(TEM) and bla(SHV)) and virulence associated traits (hypermucoviscosity, magA, k2a, rmpA, siderophores, type 1 and 3 fimbria, biofilm formation, serum resistance) were performed for 102 isolates. The results showed the presence of three major ciprofloxacin resistant CTX-M-15 producing clones (ST15 n = 69, ST101 n = 10, and ST147 n = 9), of which ST15 was predominant and universally widespread. Considering distribution in time and place, ST101 and ST147 were detected at fewer inpatient units and within a narrower time frame, as compared to ST15. Beside major clones, eleven minor clones were identified, and were shown to harbour the following beta-lactamase genes: six clones carried bla(CTX-M), four clones harboured bla(SHV)-5 and one clone possessed both bla(CTX-M) and ESBL type bla(SHV). Among the SHV-5 producing K. pneumoniae clones a novel sequence type was found, namely ST1193, which harboured a unique infB allele. Different virulence factor content and peculiar antimicrobial susceptibility profile were characteristic for each clone. In contrast to major clone isolates, which showed high level resistance to ciprofloxacin, minor clone isolates displayed significantly lower MIC values for ciprofloxacin suggesting a role for fluoroquinolones in the dissemination of the major K. pneumoniae clones. This is the first description of the CTX-M-15 producing K. pneumoniae clone ST101 in Hungary.
机译:我们调查了2004-2008年间从匈牙利佩奇大学教学医院派生的产宽谱β-内酰胺酶(ESBL)肺炎克雷伯菌的分子流行病学。分子分型,抗菌药性测试,常见的β-内酰胺酶基因(bla(CTX-M),bla(TEM)和bla(SHV))的检测以及与毒力相关的特征(高粘黏度,magA,k2a,rmpA,铁载体,1型和对102个分离株进行了3次菌毛,生物膜形成,血清抗性测定。结果表明存在三个主要的耐环丙沙星的CTX-M-15克隆(ST15 n = 69,ST101 n = 10和ST147 n = 9),其中ST15占主导地位,并且普遍存在。考虑到时间和地点的分布,与ST15相比,ST101和ST147在更少的住院单元和更短的时间范围内被检测到。除了主要克隆外,还鉴定出11个次要克隆,并显示它们具有以下β-内酰胺酶基因:六个克隆带有bla(CTX-M),四个克隆带有bla(SHV)-5,一个克隆同时具有bla(CTX-M) M)和ESBL型bla(SHV)。在产生SHV-5的肺炎克雷伯氏菌克隆中,发现了一种新的序列类型,即ST1193,其具有独特的infB等位基因。每个克隆具有不同的毒力因子含量和独特的抗菌药敏性。与对环丙沙星表现出高水平抗药性的主要克隆分离株相比,次要克隆分离株显示出环丙沙星的MIC值显着降低,这表明氟喹诺酮类药物在肺炎克雷伯菌的主要克隆传播中发挥了作用。这是匈牙利生产CTX-M-15的肺炎克雷伯菌克隆ST101的首次描述。

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