Comprehensive investigation of antibiotic resistance gene content in cfiA-harboring Bacteroides fragilis isolates of human and animal origins by whole genome sequencing

IF 4.5 3区 医学 Q1 MICROBIOLOGY
Huiluo Cao , Melissa Chun-Jiao Liu , Man-Ki Tong , Shuo Jiang , Kin-Hung Chow , Kelvin Kai-Wang To , Cindy Wing-Sze Tse , Pak-Leung Ho
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引用次数: 6

Abstract

Introduction

The emergence of multidrug resistance in Bacteroides fragilis, especially the phylogenetic lineage carrying the carbapenemase gene cfiA, represents an increasing threat to human health. However, knowledge on the diversity of the multidrug-resistant strains and the genetic elements carrying the antibiotic resistance genes (ARGs) remains limited.

Aim

The objective of the study was to describe the resistome in cfiA-positive B. fragilis.

Methods

A collection of cfiA-positive B. fragilis from diverse human (8 bacteremias, 15 wound infections) and animal (2 chickens, 2 pigs, 6 dogs, 3 cats) sources in Hong Kong, 2015–2017 was analysed by whole genome sequencing.

Results

In the 36 isolates, 13 distinct ARGs (total number 83, median 2, range 0–7 per isolate) other than cfiA were detected. ARGs encoding resistance to aminoglycosides, β-lactams, macrolides, sulphonamides and tetracyclines were carried by CTn341-like, CTnHyb-like, Tn5220-like, Tn4555-like and Tn613-like transposons and were detected in phylogenetically diverse isolates of different host sources. Only few ARGs encoding resistance to metronidazole and tetracyclines were localized on plasmids. In two chicken isolates, a novel transposon (designated as Tn6994) was found to be involved in the dissemination of multiple ARGs mediating resistance to multiple antibiotics, including metronidazole and linezolid that are critically important for treatment of anaerobic infections. In mating experiments, Tn6994 and the associated phenotypic resistance could be transferred to Bacteroides nordii recipient.

Conclusion

This study illustrates the importance of transposons in the dissemination of ARGs in the cfiA-positive division of B. fragilis. One Health approach is necessary to track the dissemination of ARGs.

利用全基因组测序技术对含cfia的脆弱拟杆菌(Bacteroides fragile)人、动物分离株抗生素耐药基因含量进行综合研究
脆弱拟杆菌(Bacteroides fragile)多药耐药的出现,特别是携带碳青霉烯酶基因cfiA的系统发育谱系,对人类健康的威胁日益严重。然而,对多重耐药菌株的多样性和携带抗生素耐药基因(ARGs)的遗传元件的了解仍然有限。目的研究cfia阳性脆弱芽孢杆菌的抗性组。方法采用全基因组测序方法,对2015-2017年香港地区不同来源的人(8例菌血症,15例伤口感染)和动物(2例鸡、2例猪、6例狗、3例猫)采集的cfia阳性脆弱贝氏杆菌进行分析。结果36株分离株除cfiA外,共检出13种不同的ARGs(总数83株,中位数2株,范围0 ~ 7株)。编码氨基糖苷类、β-内酰胺类、大环内酯类、磺胺类和四环素类抗性的ARGs由ctn341样、ctnhyb样、tn5220样、tn4555样和tn613样转座子携带,并在不同宿主来源的分离株中检测到系统发育差异。只有少数编码甲硝唑和四环素耐药的ARGs定位在质粒上。在两个鸡分离株中,发现了一个新的转座子(命名为Tn6994)参与多种ARGs的传播,介导对多种抗生素的耐药性,包括对治疗厌氧感染至关重要的甲硝唑和利奈唑胺。在交配实验中,Tn6994和相关的表型抗性可以转移给诺氏拟杆菌受体。结论本研究说明了转座子在脆弱贝氏杆菌cfia阳性分裂中ARGs传播的重要性。跟踪ARGs的传播需要一种卫生方法。
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来源期刊
CiteScore
9.70
自引率
0.00%
发文量
18
审稿时长
45 days
期刊介绍: Pathogen genome sequencing projects have provided a wealth of data that need to be set in context to pathogenicity and the outcome of infections. In addition, the interplay between a pathogen and its host cell has become increasingly important to understand and interfere with diseases caused by microbial pathogens. IJMM meets these needs by focussing on genome and proteome analyses, studies dealing with the molecular mechanisms of pathogenicity and the evolution of pathogenic agents, the interactions between pathogens and host cells ("cellular microbiology"), and molecular epidemiology. To help the reader keeping up with the rapidly evolving new findings in the field of medical microbiology, IJMM publishes original articles, case studies and topical, state-of-the-art mini-reviews in a well balanced fashion. All articles are strictly peer-reviewed. Important topics are reinforced by 2 special issues per year dedicated to a particular theme. Finally, at irregular intervals, current opinions on recent or future developments in medical microbiology are presented in an editorial section.
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