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澳大利亚人群与海鸥中 CMY-2 型大肠埃希菌 963 型序列株的种间传播

Interspecies Transmission of CMY-2-Producing Escherichia coli Sequence Type 963 Isolates between Humans and Gulls in Australia.

机构信息

Central European Institute of Technology, University of Veterinary Sciences Brno, Brno, Czech Republic.

Department of Chemistry, Faculty of Science, University of Hradec Kralove, Hradec Kralove, Czech Republic.

出版信息

mSphere. 2022 Aug 31;7(4):e0023822. doi: 10.1128/msphere.00238-22. Epub 2022 Jul 5.

Abstract

Escherichia coli sequence type 963 (ST963) is a neglected lineage closely related to ST38, a globally widespread extraintestinal pathogenic ST causing urinary tract infections (UTI) as well as sepsis in humans. Our current study aimed to improve the knowledge of this understudied ST by carrying out a comprehensive comparative analysis of whole-genome sequencing data consisting of 31 isolates from silver gulls in Australia along with another 80 genomes from public resources originating from geographically scattered regions. ST963 was notable for carriage of cephalosporinase gene which was identified in 99 isolates and was generally chromosomally encoded. ST963 isolates showed otherwise low carriage of antibiotic resistance genes, in contrast with the closely related E. coli ST38. We found considerable phylogenetic variability among international ST963 isolates (up to 11,273 single nucleotide polymorphisms [SNPs]), forming three separate clades. A major clade that often differed by 20 SNPs or less consisted of Australian isolates of both human and animal origin, providing evidence of zoonotic or zooanthropogenic transmission. There was a high prevalence of virulence F29:A-:B10 pUTI89-like plasmids within E. coli ST963 ( = 88), carried especially by less variable isolates exhibiting ≤1,154 SNPs. We characterized a novel 115,443-bp pUTI89-like plasmid, pCE2050_A, that carried a :IS insertion absent from pUTI89. Since IS was also present in a transposition unit bearing on chromosomes of ST963 strains, IS insertion into pUTI89 may enable mobilization of the gene from the chromosome/transposition unit to pUTI89 via homologous recombination. We have provided the first comprehensive genomic study of E. coli ST963 by analyzing various genomic and phenotypic data sets of isolates from Australian silver gulls and comparison with genomes from geographically dispersed regions of human and animal origin. Our study suggests the emergence of a specific -carrying E. coli ST963 clone in Australia that is widely spread across the continent by humans and birds. Genomic analysis has revealed that ST963 is a globally dispersed lineage with a remarkable set of virulence genes and virulence plasmids described in uropathogenic E. coli. While ST963 separated into three clusters, a unique specific clade of Australian ST963 isolates harboring a chromosomal copy of AmpC β-lactamase encoding the gene and originating from both humans and wild birds was identified. This phylogenetically close cluster comprised isolates of both animal and human origin, thus providing evidence of interspecies zoonotic transmission. The analysis of the genetic environment of the AmpC β-lactamase-encoding gene highlighted ongoing evolutionary events that shape the carriage of this gene in ST963.

摘要

大肠杆菌序列型 963(ST963)是一个被忽视的谱系,与 ST38 密切相关,ST38 是一种在全球广泛传播的肠道外致病性 ST,可导致尿路感染(UTI)和人类败血症。我们的研究旨在通过对来自澳大利亚银鸥的 31 株分离株以及来自地理分散地区的另外 80 个公共资源基因组的全基因组测序数据进行全面比较分析,来提高对这一研究较少的 ST 的认识。ST963 携带头孢菌素酶基因,该基因在 99 株菌中被鉴定出来,通常是染色体编码的。与密切相关的大肠杆菌 ST38 相比,ST963 分离株携带的抗生素耐药基因数量较少。我们发现国际 ST963 分离株之间存在相当大的系统发育变异(高达 11273 个单核苷酸多态性[SNP]),形成了三个独立的分支。一个主要的分支通常由来自人类和动物来源的澳大利亚分离株组成,差异不超过 20 个 SNP,这提供了人畜共患或动物源人畜共患传播的证据。在大肠杆菌 ST963 中,F29:A-:B10 pUTI89 样质粒的流行率很高( = 88),特别是在携带 ≤1154 SNPs 的变异性较小的分离株中。我们对一种新型的 115443bp pUTI89 样质粒 pCE2050_A 进行了表征,该质粒携带一个缺失于 pUTI89 的插入 :IS。由于 IS 也存在于携带的转座单元中,因此 pUTI89 上的 基因可能通过同源重组从染色体/转座单元插入到 pUTI89 中。我们通过分析来自澳大利亚银鸥的分离株的各种基因组和表型数据集,并与来自人类和动物来源的地理分散地区的基因组进行比较,对大肠杆菌 ST963 进行了首次全面的基因组研究。我们的研究表明,在澳大利亚出现了一个携带特定的 E. coli ST963 克隆,该克隆通过人类和鸟类在整个大陆广泛传播。基因组分析表明,ST963 是一个具有显著一组毒力基因和毒力质粒的全球分布谱系,这些基因和质粒在尿路致病性大肠杆菌中被描述。虽然 ST963 分为三个群,但一个独特的澳大利亚 ST963 分离株特定分支被鉴定出来,该分支携带染色体编码的 AmpC β-内酰胺酶基因 ,并源自人类和野生鸟类。这个系统发育上密切相关的分支包含了动物和人类来源的分离株,因此提供了种间人畜共患传播的证据。对 AmpC β-内酰胺酶基因的遗传环境进行分析,突出了塑造该基因在 ST963 中携带的进化事件。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b151/9429958/e0b493f2ad2f/msphere.00238-22-f001.jpg

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