AI Article Synopsis

  • The study explores the worsening threat of carbapenem-resistant Klebsiella pneumoniae (CRKP) in healthcare, focusing on the evolutionary pathways of pKPC-2-bearing plasmids, which are crucial for antibiotic resistance.
  • Researchers collected 237 CRKP strains and performed advanced sequencing and bioinformatics analyses to categorize the plasmids into three subgroups based on their unique evolutionary events and resistance mechanisms.
  • The findings highlight a high incidence of multicopy antibiotic resistance genes, which significantly affect treatment outcomes, especially in reducing sensitivity to ceftazidime/avibactam, ultimately underscoring the complex dynamics of resistance in hospital settings.

Article Abstract

The threat posed by in healthcare settings has worsened due to the evolutionary advantages conferred by -harboring plasmids (pKPC-2). However, the specific evolutionary pathway of nosocomial carrying pKPC-2 and its transmission between patients and healthcare environments are not yet well understood. Between 1 August and 31 December 2019, 237 ST11 KPC-2-producing-carbapenem-resistant (CRKP) (KPC-2-CRKP) were collected from patient or ward environments in an intensive care unit and subjected to Illumina sequencing, of which 32 strains were additionally selected for Nanopore sequencing to obtain complete plasmid sequences. Bioinformatics analysis, conjugation experiments, antimicrobial susceptibility tests, and virulence assays were performed to identify the evolutionary characteristics of pKPC-2. The pKPC-2 plasmids were divided into three subgroups with distinct evolutionary events, including Tn-mediated plasmid homologous recombination, ISmediated horizontal gene transfer, and dynamic duplications of antibiotic resistance genes (ARGs). Surprisingly, the incidence rates of multicopy , , and were quite high (ranging from 27.43% to 67.01%), and strains negative for extended-spectrum β-lactamase tended to develop multicopy . Notably, the presence of multicopy reduced sensitivity to ceftazidime/avibactam (CZA), and the relative expression level of in the CZA-resistant group was 6.12 times higher than that in the sensitive group. Furthermore, a novel hybrid pKPC-2 was identified, presenting enhanced virulence levels and decreased susceptibility to CZA. This study emphasizes the notable prevalence of multicopy ARGs and provides a comprehensive insight into the intricate and diverse evolutionary pathways of resistant plasmids that disseminate among patients and healthcare environments.IMPORTANCEThis study is based on a CRKP screening program between patients and ward environments in an intensive care unit, describing the pKPC-2 (-harboring plasmids) population structure and evolutionary characteristics in clinical settings. Long-read sequencing was performed in genetically closely related strains, enabling the high-resolution analysis of evolution pathway between or within pKPC-2 subgroups. We revealed the extremely high rates of multicopy antibiotic resistance genes (ARGs) in clinical settings and its effect on resistance profile toward novel β-lactam/β-lactamase inhibitor combinations, which belongs to the last line treatment choices toward CRKP infection. A novel hybrid pKPC-2 carrying CRKP with enhanced resistance and virulence level was captured during its clonal spread between patients and ward environment. These evidences highlight the threat of pKPC-2 to CRKP treatment and control. Thus, surveillance and timely disinfection in clinical settings should be practiced to prevent transmission of CRKP carrying threatful pKPC-2. And rational use of antibiotics should be called for to prevent inducing of pKPC-2 evolution, especially the multicopy ARGs.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10878039PMC
http://dx.doi.org/10.1128/msystems.00924-23DOI Listing

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