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首页> 外文期刊>Antimicrobial agents and chemotherapy. >OXA-163, an OXA-48-related class D beta-lactamase with extended activity toward expanded-spectrum cephalosporins.
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OXA-163, an OXA-48-related class D beta-lactamase with extended activity toward expanded-spectrum cephalosporins.

机译:OXA-163,一种与OXA-48相关的D类β-内酰胺酶,具有对广谱头孢菌素的扩展活性。

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摘要

Two bla(OXA-48)-like-positive isolates (Klebsiella pneumoniae and Enterobacter cloacae) were recovered in Argentina in 2008 as part of a large-scale survey focused on multidrug resistance in Enterobacteriaceae. In both cases, sequencing identified beta-lactamase OXA-163, differing from OXA-48 by a single amino substitution and a 4-amino-acid deletion. OXA-163 hydrolyzed penicillins, ceftazidime, and cefotaxime, whereas OXA-48 did not. However, OXA-163 had a much lower ability to hydrolyze carbapenems than OXA-48, therefore barely being considered a carbapenemase. In both isolates, the bla(OXA-163) gene was located on plasmids that differed in structure and size. However, a detailed genetic analysis revealed a similar genetic context in those isolates, with the bla(OXA-163) gene being bracketed by novel transposase genes, making this genetic environment different from that reported for the bla(OXA-48) gene. This study identified the first class D beta-lactamase compromising both extended-spectrum cephalosporin and carbapenem activities.
机译:作为一项针对肠道杆菌科多药耐药性的大规模调查的一部分,2008年在阿根廷回收了两个bla(OXA-48)样阳性分离株(肺炎克雷伯菌和阴沟肠杆菌)。在两种情况下,测序均鉴定出β-内酰胺酶OXA-163,其与OXA-48的区别在于单个氨基酸取代和4-氨基酸缺失。 OXA-163水解青霉素,头孢他啶和头孢噻肟,而OXA-48没有。但是,OXA-163水解碳青霉烯的能力比OXA-48低得多,因此几乎不被认为是碳青霉烯酶。在两种分离物中,bla(OXA-163)基因均位于结构和大小不同的质粒上。但是,详细的遗传分析显示,这些分离株具有相似的遗传背景,其中bla(OXA-163)基因被新的转座酶基因包围,从而使该遗传环境不同于bla(OXA-48)基因的报道。这项研究确定了一流的D类β-内酰胺酶,可破坏广谱头孢菌素和碳青霉烯的活性。

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