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短读长读测序揭示了携带和基因的 IncF 质粒在大肠杆菌 ST131 中的存在和进化。

Short- and Long-Read Sequencing Reveals the Presence and Evolution of an IncF Plasmid Harboring and Genes in Escherichia coli ST131.

机构信息

School of Biomedical Sciences, University of West London, London, United Kingdom.

Yerevan State Medical University after M. Heratsi, Faculty of Public Health, Department of Epidemiology, Yerevan, Republic of Armenia.

出版信息

Microbiol Spectr. 2023 Aug 17;11(4):e0035623. doi: 10.1128/spectrum.00356-23. Epub 2023 Jul 19.

Abstract

Escherichia coli sequence type 131 (ST131) has contributed to the spread of extended-spectrum beta-lactamase (ESBL) and has emerged as the dominant cause of hospital- and community-acquired urinary tract infections. Here, we report for the first time an in-depth analysis of whole-genome sequencing (WGS) of 4 ESBL-producing E. coli ST131 isolates recovered from patients in two hospitals in Armenia using Illumina short-read sequencing for accurate base calling to determine their genotype and to infer their phylogeny and using Oxford Nanopore Technologies long-read sequencing to resolve plasmid and chromosomal genetic elements. Genotypically, the four Armenian isolates were identified as part of the 30Rx/clade C2 ( = 2) and 41/clade A ( = 2) lineages and were phylogenetically closely related to isolates from the European Nucleotide Archive (ENA) database previously recovered from patients in the United States, Australia, and New Zealand. The Armenian isolates recovered in this study had chromosomal integration of the gene in the 30Rx isolates and a high number of virulence genes found in the 41 isolates associated with the carriage of a rare genomic island (in the context of E. coli ST131) containing the S fimbrial, salmochelin siderophore, and microcin H47 virulence genes. Furthermore, our data show the evolution of the IncF[2:A2:B20] plasmid harboring both and genes, derived from the recombination of genes from an IncF[F2:A-:B-] -associated plasmid into the IncF[F1:A2:B20] -associated plasmid backbone seen in two genetically closely related 41 Armenian isolates. Combining short and long reads from whole-genome sequencing analysis provided a genetic context for uncommon genes of clinical importance to better understand transmission and evolutionary features of ESBL-producing uropathogenic E. coli (UPEC) ST131 isolates recovered in Armenia. Using hybrid genome assembly in countries lacking genomic surveillance studies can inform us about new lineages not seen in other countries with genes encoding high virulence and antibiotic resistance harbored on mobile genetic elements.

摘要

大肠杆菌序列类型 131(ST131)促进了扩展谱β-内酰胺酶(ESBL)的传播,并已成为医院和社区获得性尿路感染的主要原因。在这里,我们首次报道了对从亚美尼亚两家医院的患者中分离的 4 株产 ESBL 的大肠杆菌 ST131 全基因组测序(WGS)的深入分析,使用 Illumina 短读测序进行准确的碱基调用,以确定其基因型,并推断其系统发育,使用 Oxford Nanopore Technologies 长读测序来解析质粒和染色体遗传元件。从基因型上看,这 4 个亚美尼亚分离株被鉴定为 30Rx/clade C2( = 2)和 41/clade A( = 2)谱系的一部分,在系统发育上与先前从美国、澳大利亚和新西兰的患者中从欧洲核苷酸档案库(ENA)数据库中恢复的分离株密切相关。本研究中恢复的亚美尼亚分离株在 30Rx 分离株中具有 基因的染色体整合,以及在 41 分离株中发现的大量与罕见基因组岛(在大肠杆菌 ST131 背景下)相关的毒力基因,该基因组岛包含 S 菌毛、沙门氏菌铁载体和微菌素 H47 毒力基因。此外,我们的数据显示了携带 和 基因的 IncF[2:A2:B20]质粒的进化,该质粒是通过将 IncF[F2:A-:B-]相关质粒中的基因重组到 IncF[F1:A2:B20]相关质粒骨架中而产生的,这在两个遗传上密切相关的 41 个亚美尼亚分离株中可见。结合全基因组测序分析的短读和长读,为具有临床重要性的罕见基因提供了遗传背景,以更好地了解在亚美尼亚恢复的产 ESBL 尿路致病性大肠杆菌(UPEC)ST131 分离株的传播和进化特征。在缺乏基因组监测研究的国家中使用混合基因组组装可以使我们了解其他国家未发现的具有编码高毒力和抗生素耐药性的基因的新谱系,这些基因存在于移动遗传元件上。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/52a7/10433869/5119424adf73/spectrum.00356-23-f001.jpg

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