International High-Risk Clones Among Extended-Spectrum β-Lactamase-Producing Escherichia coli in Dhaka, Bangladesh

孟加拉国达卡产超广谱 β-内酰胺酶大肠杆菌中发现国际高风险克隆

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作者:Razib Mazumder, Arif Hussain, Ahmed Abdullah, Md Nazrul Islam, Md Tuhin Sadique, S M Muniruzzaman, Anika Tabassum, Farhana Halim, Nasrin Akter, Dilruba Ahmed, Dinesh Mondal

Background

Escherichia coli is a major extended-spectrum β-lactamase (ESBL)-producing organism responsible for the rapid spread of antimicrobial resistance (AMR) that has compromised our ability to treat infections. Baseline data on population structure, virulence, and resistance mechanisms in E. coli lineages from developing countries such as Bangladesh are lacking.

Conclusion

Our study reveals a high diversity of E. coli lineages among ESBL-producing E. coli from Dhaka. This study suggests ongoing circulation of ST131 and all major non-ST131 high-risk clones that are strongly associated with cephalosporin resistance and virulence genes. These findings warrant prospective monitoring of high-risk clones, which would otherwise worsen the AMR crises.

Methods

Whole-genome sequencing was performed for 46 ESBL-E. coli isolates cultured from patient samples at the International Centre for Diarrhoeal Disease Research, Bangladesh (icddr,b)-Dhaka. Sequence data were analyzed to glean details of AMR, virulence, and phylogenetic and molecular markers of E. coli lineages.

Results

Genome comparison revealed presence of all major high-risk clones including sequence type 131 (ST131) (46%), ST405 (13%), ST648 (7%), ST410 (4.3%), ST38 (2%), ST73 (2%), and ST1193 (2%). The predominant ESBL gene and plasmid combination were bla CTX - M - 15 and FII-FIA-FIB detected in diverse E. coli phylogroups and STs. The bla NDM - 5 (9%) gene was present in prominent E. coli STs. One (2%) mcr-1-positive ST1011 E. coli, coharboring bla CTXM - 55 gene, was detected. The extraintestinal pathogenic E. coli genotype was associated with specific E. coli lineages. The single nucleotide polymorphism (SNP)-based genome phylogeny largely showed correlation with phylogroups, serogroups, and fimH types. Majority of these isolates were susceptible to amikacin (93%), imipenem (93%), and nitrofurantoin (83%).

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