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首页> 外文期刊>Microbial drug resistance: MDR : Mechanisms, epidemiology, and disease >Dissemination of International Clone II Acinetobacter baumannii Strains Coproducing OXA-23 Carbapenemase and 16S rRNA Methylase ArmA in Athens, Greece
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Dissemination of International Clone II Acinetobacter baumannii Strains Coproducing OXA-23 Carbapenemase and 16S rRNA Methylase ArmA in Athens, Greece

机译:传播国际克隆II类植物植物植物植物植物植物(烟草)和16S rRNA甲基酶ARMA在雅典,希腊

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摘要

The aim of this study was to study the molecular epidemiology of 16S rRNA-methylase (RMT)-producing clinical Acinetobacter baumannii isolates from hospitals in Athens, Greece. Single-patient A. baumannii clinical isolates, coresistant to amikacin and gentamicin (n = 347), from five tertiary care hospitals, were submitted to minimum inhibitory concentration determination and molecular testing for carbapenemase and RMT genes. A. baumannii, resistant to amikacin and gentamicin, was isolated at participating institutions at a mean rate of 67.8%. Among them 93.7% harbored the armA. The vast majority (98.5%) of armA positive isolates were OXA-23 producers, assigned mainly (99.4%) to sequence group G1, corresponding to international clone (IC) II. Four isolates (all from the same hospital) were OXA-24 producers (1.2%), assigned to G6 corresponding to CC78 and only one isolate was OXA-58-producer, assigned to G2 (IC I). Apramycin was the most active agent inhibiting 99.7% of the isolates at <= 64 mg/L, whereas colistin, trimethoprim/sulfamethoxazole, minocycline, and tigecycline exhibited only sparse activity (S, <18%). RMT production is an emerging mechanism of resistance, capable of compromising the clinical efficacy of aminoglycosides. High prevalence of armA was observed among A. baumannii strains isolated in participating hospitals in Athens, which were mainly OXA-23 producers and belonged to IC II. Apramycin is a structurally unique aminoglycoside, currently used as a veterinary agent. Although it has not been evaluated for clinical use, apramycin appears worthy of further investigation for repurposing as a human therapeutic against difficult-to-treat pathogens.
机译:本研究的目的是研究16S rRNA-甲基酶(RMT)的分子流行病学 - 培养雅典雅典医院的临床传导术株式会生物的分子流行病学。从五个第三张三级护理医院,单患者A.Baumannii临床分离物,insikacin和庆大霉素(n = 347)的insiSistant被提交至碳结构酶和RMT基因的最小抑制浓度测定和分子检测。 A. Baumannii,耐药和庆大霉素,在参与的机构中被分离,平均速度为67.8%。其中93.7%是arma。绝大多数(98.5%)ARMA阳性分离株是牛-23生产商,主要(99.4%)分配给序列组G1,对应于国际克隆(IC)II。四个分离株(来自同一医院)的氧气-24生产商(1.2%),分配给对应于CC78的G6,只有一个分离物是牛-58-生产者,分配给G2(IC I)。 Aparamycin是最活跃的药剂,抑制在<= 64mg / L的分离物中的99.7%,而Colistin,Trimethokim /磺胺甲恶唑,米诺环素和脱癸锌糖蛋白仅表现出稀疏活性(S,<18%)。 RMT生产是一种抗性的新出现机制,能够损害氨基糖苷类的临床疗效。在雅典参与医院隔离的A.Baumannii菌株中观察到arma的高普遍率。主要是牛粪生产商并属于IC II。 Aparamycin是一种结构独特的氨基糖苷,目前用作兽医代理。虽然尚未评估临床用途,但仍然有助于进一步调查将作为难以治疗病原体的人类治疗的进一步调查。

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