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首页> 外文期刊>Journal of Clinical Microbiology >Molecular Epidemiology over an 11-Year Period (2000 to 2010) of Extended-Spectrum β-Lactamase-Producing Escherichia coli Causing Bacteremia in a Centralized Canadian Region
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Molecular Epidemiology over an 11-Year Period (2000 to 2010) of Extended-Spectrum β-Lactamase-Producing Escherichia coli Causing Bacteremia in a Centralized Canadian Region

机译:在加拿大中部地区造成细菌血症的大范围生产β-内酰胺酶的大肠杆菌的11年期间(2000年至2010年)的分子流行病学

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A study was designed to assess the importance of sequence types among extended-spectrum β-lactamase (ESBL)-producing Escherichia coli isolates causing bacteremia over an 11-year period (2000 to 2010) in a centralized Canadian region. A total of 197 patients with incident infections were identified; the majority presented with community-onset urosepsis, with a significant increase in the prevalence of ESBL-producing E. coli during the later part of the study. The majority of E. coli isolates produced either CTX-M-15 or CTX-M-14. We identified 7 different major sequence types among 91% of isolates (i.e., the ST10 clonal complex, ST38, ST131, ST315, ST393, ST405, and ST648) and provided insight into their clinical and molecular characteristics. ST38 was the most antimicrobial-susceptible sequence type and predominated during 2000 to 2004 but disappeared after 2008. ST131 was the most antimicrobial-resistant sequence type, and the influx of a single pulsotype of this sequence type was responsible for the significant increase of ESBL-producing E. coli strains since 2007. During 2010, 49/63 (78%) of the ESBL-producing E. coli isolates belonged to ST131, and this sequence type had established itself as a major drug-resistant pathogen in Calgary, Alberta, Canada, posing an important new public health threat within our region. We urgently need well-designed epidemiological and molecular studies to understand the dynamics of transmission, risk factors, and reservoirs for E. coli ST131. This will provide insight into the emergence and spread of this multiresistant sequence type.
机译:设计了一项研究,以评估在加拿大中部地区的11年期间(2000年至2010年),产生广谱β-内酰胺酶(ESBL)的大肠埃希菌分离株中引起菌血症的序列类型的重要性。总共确定了197名事件感染患者;大多数人出现社区性尿毒症,在研究后期,ESBL产生大肠杆菌的患病率显着增加。大多数大肠杆菌分离株产生CTX-M-15或CTX-M-14。我们在91%的分离株(即ST10克隆复合物,ST38,ST131,ST315,ST393,ST405和ST648)中鉴定了7种不同的主要序列类型,并提供了对其临床和分子特征的了解。 ST38是最易感微生物的序列类型,在2000年至2004年占主导地位,但在2008年后消失。ST131是最抗微生物的序列类型,这种序列类型的单个脉冲型的涌入导致ESBL-的显着增加。从2007年开始生产E. coli菌株。2010年,有49/63(78%)产ESBL的大肠杆菌分离株属于ST131,并且该序列类型已将其自身确立为阿尔伯塔省卡尔加里市的主要耐药菌加拿大,对我们地区构成了重要的新的公共卫生威胁。我们迫切需要精心设计的流行病学和分子研究,以了解大肠杆菌ST131的传播动态,危险因素和储库。这将提供对这种多抗序列类型的出现和传播的洞察。

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