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Genetic and Biochemical Characterization of OXA-405 an OXA-48-Type Extended-Spectrum β-Lactamase without Significant Carbapenemase Activity

机译:OXA-405一种无显着碳青霉烯酶活性的OXA-48型超广谱β-内酰胺酶的遗传和生化特性

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摘要

The epidemiology of carbapenemases worldwide is showing that OXA-48 variants are becoming the predominant carbapenemase type in Enterobacteriaceae in many countries. However, not all OXA-48 variants possess significant activity toward carbapenems (e.g., OXA-163). Two Serratia marcescens isolates with resistance either to carbapenems or to extended-spectrum cephalosporins were successively recovered from the same patient. A genomic comparison using pulsed-field gel electrophoresis and automated Rep-PCR typing identified a 97.8% similarity between the two isolates. Both strains were resistant to penicillins and first-generation cephalosporins. The first isolate was susceptible to expanded-spectrum cephalosporins, was resistant to carbapenems, and had a significant carbapenemase activity (positive Carba NP test) related to the expression of OXA-48. The second isolate was resistant to expanded-spectrum cephalosporins, was susceptible to carbapenems, and did not express a significant imipenemase activity, (negative for the Carba NP test) despite possessing a blaOXA-48-type gene. Sequencing identified a novel OXA-48-type β-lactamase, OXA-405, with a four-amino-acid deletion compared to OXA-48. The blaOXA-405 gene was located on a ca. 46-kb plasmid identical to the prototype IncL/M blaOXA-48-carrying plasmid except for a ca. 16.4-kb deletion in the tra operon, leading to the suppression of self-conjugation properties. Biochemical analysis showed that OXA-405 has clavulanic acid-inhibited activity toward expanded-spectrum activity without significant imipenemase activity. This is the first identification of a successive switch of catalytic activity in OXA-48-like β-lactamases, suggesting their plasticity. Therefore, this report suggests that the first-line screening of carbapenemase producers in Enterobacteriaceae may be based on the biochemical detection of carbapenemase activity in clinical settings.
机译:全世界碳青霉烯酶的流行病学表明,在许多国家中,OXA-48变体正在成为肠杆菌科中主要的碳青霉烯酶类型。但是,并非所有的OXA-48变体都具有对碳青霉烯的显着活性(例如OXA-163)。随后从同一患者中回收了两个对碳青霉烯类或广谱头孢菌素具有抗性的粘质沙雷氏菌。使用脉冲场凝胶电泳和自动Rep-PCR分型的基因组比较确定了两个分离株之间的97.8%相似性。两种菌株均对青霉素和第一代头孢菌素具有抗性。第一个分离株对广谱头孢菌素敏感,对碳青霉烯类有抗性,并且具有与OXA-48表达相关的显着的碳青霉烯酶活性(阳性Carba NP测试)。尽管具有blaOXA-48型基因,第二个分离株对广谱头孢菌素具有抗性,对碳青霉烯类药物敏感,并且不表达显着的亚胺培南酶活性(对Carba NP测试阴性)。测序鉴定出一种新颖的OXA-48型β-内酰胺酶OXA-405,与OXA-48相比,具有四个氨基酸的缺失。 blaOXA-405基因位于一个约。与携带IncL / M blaOXA-48的原型质粒相同的46 kb质粒,除了ca. tra操纵子中16.4kb的缺失,导致自缀合特性的抑制。生化分析表明,OXA-405具有克拉维酸抑制活性,对扩谱活性无明显的亚胺培南酶活性。这是OXA-48-样β-内酰胺酶催化活性连续转换的首次鉴定,表明它们具有可塑性。因此,该报告表明肠杆菌科中碳青霉烯酶生产者的一线筛选可能是基于临床环境中碳青霉烯酶活性的生化检测。

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