Global genomic epidemiology of bla GES-5 carbapenemase-associated integrons.

IF 4 2区 生物学 Q1 GENETICS & HEREDITY Microbial Genomics Pub Date : 2024-12-01 DOI:10.1099/mgen.0.001312
William Matlock, Liam P Shaw, Nicole Stoesser
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Abstract

Antimicrobial resistance (AMR) gene cassettes comprise an AMR gene flanked by short recombination sites (attI and attC or attC and attC). Integrons are genetic elements able to capture, excise and shuffle these cassettes, providing 'adaptation on demand', and can be found on both chromosomes and plasmids. Understanding the patterns of integron diversity may help to understand the epidemiology of AMR genes. As a case study, we examined the clinical resistance gene bla GES-5, an integron-associated class A carbapenemase first reported in Greece in 2004 and since observed worldwide, which to our knowledge has not been the subject of a previous global analysis. Using a dataset comprising all de-duplicated NCBI contigs containing bla GES-5 (n=104), we developed a pangenome graph-based workflow to characterize and cluster the diversity of bla GES-5-associated integrons. We demonstrate that bla GES-5-associated integrons on plasmids are different to those on chromosomes. Chromosomal integrons were almost all identified in Pseudomonas aeruginosa ST235, with a consistent gene cassette content and order. We observed instances where insertion sequence IS110 disrupted attC sites, which might immobilize the gene cassettes and explain the conserved integron structure despite the presence of intI1 integrase promoters, which would typically facilitate capture or excision and rearrangement. The plasmid-associated integrons were more diverse in their gene cassette content and order, which could be an indication of greater integrase activity and 'shuffling' of integrons on plasmids.

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bla GES-5碳青霉烯酶相关整合子的全球基因组流行病学研究
抗菌素耐药性(AMR)基因盒包括AMR基因两侧的短重组位点(attI和attC或attC和attC)。整合子是一种能够捕获、切除和打乱这些磁带的遗传元素,提供“随需应变”,可以在染色体和质粒上找到。了解整合子多样性的模式可能有助于了解AMR基因的流行病学。作为一个案例研究,我们研究了临床耐药基因bla GES-5,这是一种整合子相关的a类碳青霉烯酶,于2004年首次在希腊报道,此后在全球范围内观察到,据我们所知,此前尚未有全球分析的主题。利用包含bla GES-5的所有去重复NCBI contigs (n=104)的数据集,我们开发了一个基于泛基因组图的工作流程,以表征和聚类bla GES-5相关整合子的多样性。我们证明质粒上的bla ges -5相关整合子与染色体上的整合子不同。铜绿假单胞菌ST235几乎全部鉴定出染色体整合子,且基因盒数和顺序一致。我们观察到插入序列IS110破坏了attC位点的情况,这可能会固定基因盒,并解释了尽管存在intI1整合酶启动子,但保守的整合子结构,这通常会促进捕获或切除和重排。质粒相关的整合子在其基因盒内容和顺序上更加多样化,这可能表明质粒上整合酶活性和整合子的“洗牌”。
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来源期刊
Microbial Genomics
Microbial Genomics Medicine-Epidemiology
CiteScore
6.60
自引率
2.60%
发文量
153
审稿时长
12 weeks
期刊介绍: Microbial Genomics (MGen) is a fully open access, mandatory open data and peer-reviewed journal publishing high-profile original research on archaea, bacteria, microbial eukaryotes and viruses.
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