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首页> 外文期刊>Antimicrobial agents and chemotherapy. >Clinical and Molecular Correlates of Escherichia coli Bloodstream Infection from Two Geographically Diverse Centers in Rochester, Minnesota, and Singapore
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Clinical and Molecular Correlates of Escherichia coli Bloodstream Infection from Two Geographically Diverse Centers in Rochester, Minnesota, and Singapore

机译:罗切斯特,明尼苏达州两种地理上不同中心的大肠杆菌血流感染的临床和分子相关

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Escherichia coli bacteremia is caused mainly by sequence type complex 131 (STc131) and two clades within its fluoroquinolone-resistance-associated H30 subclone, H30R1 and H30Rx. We examined clinical and molecular correlates of E. coli bacteremia in two geographically distinct centers. We retrospectively studied 251 unique E. coli bloodstream isolates from 246 patients (48 from the Mayo Clinic, Rochester, MN [MN], and 198 from Tan Tock Seng Hospital, Singapore [SG]), from October 2013 through March 2014. Isolates underwent PCR for phylogroup, STc, bla(CTX-M) type, and virulence gene profiles, and medical records were reviewed. Although STc131 accounted for 25 to 27% of all E. coli bacteremia isolates at each site, its extended-spectrum-beta-lactamase (ESBL)-associated H30Rx clade was more prominent in SG than in MN (15% versus 4%; P = 0.04). In SG only, patients with STc131 (versus other E. coli STc isolates) were more likely to receive inactive initial antibiotics (odds ratio, 2.8; P = 0.005); this was true specifically for patients with H30Rx (odds ratio, 7.0; P = 0.005). H30Rx comprised 16% of community-onset bacteremia episodes in SG but none in MN. In SG, virulence scores were higher for H30Rx than for H30R1, non-H30 STc131, and non-STc131 isolates (P 0.02 for all comparisons). At neither site did mortality differ by clonal status. The ESBL-associated H30Rx clade was more prevalent and more often of community onset in SG, where it predicted inactive empirical treatment. The clonal distribution varies geographically and has potentially important clinical implications. Rapid susceptibility testing and clonal diagnostics for H30/H30Rx might facilitate earlier prescribing of active therapy.
机译:大肠杆菌菌血症主要由序列型复合物131(STC131)和其氟喹啉酮抗性相关H30亚克隆,H30R1和H30RX中的两种蛹引起。我们在两个地理上不同的中心检查了大肠杆菌菌血症的临床和分子相关。我们回顾性研究了246名患者的251名独特的大肠杆菌血流分离株(来自Mayo Clinic,罗彻斯特,Mn [Mn],198年,来自2013年10月至2014年3月的Tan Tock Seng Hospital(Tan Tock Seng Hospital)。分离株综述了PROGroup,STC,BLA(CTX-M)和毒力基因谱和病历的PCR。虽然STC131占每个站点的所有大肠杆菌菌血症的25%至27%,但其扩展光谱 - β-内酰胺酶(ESBL) - 分配的H30RX疏水液在SG中比Mn更突出(15%与4%; P = 0.04)。仅在SG中,患有STC131(与其他大肠杆菌STC分离物)的患者更可能获得无活性的初始抗生素(差距,2.8; P = 0.005);对于H30RX患者(差距比,7.0; P = 0.005),这是真的。 H30RX包含16%的SG中的社区发作菌血症,但没有在Mn中。在SG中,H30RX比H30R1,非H30STC131和非STC131分离株为毒力分数比H30R1,非STC131分离物(P <0.02用于所有比较)。在任何网站上都没有受到克隆状态的死亡率。 ESBL相关的H30RX疏水性普遍普遍,更常见于SG中的社区发作,其中预测失真的经验治疗。克隆分布在地理上变化并且具有潜在的重要临床意义。 H30 / H30RX的快速易感性测试和克隆诊断可能促进早期的活动疗法规定。

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