Genomic epidemiology of global Klebsiella pneumoniae carbapenemase (KPC)-producing Escherichia coli

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作者
N. Stoesser
A. E. Sheppard
G. Peirano
L. W. Anson
L. Pankhurst
R. Sebra
H. T. T. Phan
A. Kasarskis
A. J. Mathers
T. E. A. Peto
P. Bradford
M. R. Motyl
A. S. Walker
D. W. Crook
J. D. Pitout
机构
[1] Modernising Medical Microbiology Consortium,Department of Pathology and Laboratory Medicine
[2] Nuffield Department of Medicine,Department of Microbiology
[3] John Radcliffe Hospital,Department of Medical Microbiology
[4] University of Oxford,undefined
[5] Division of Microbiology,undefined
[6] Calgary Laboratory Services,undefined
[7] University of Calgary,undefined
[8] Icahn Institute and Department of Genetics and Genomic Sciences,undefined
[9] Icahn School of Medicine,undefined
[10] National Institute for Health Research (NIHR) Health Protection Research Unit (NIHR HPRU) in Healthcare Associated Infections and Antimicrobial Resistance,undefined
[11] University of Oxford,undefined
[12] Division of Infectious Diseases and International Health,undefined
[13] Department of Medicine,undefined
[14] University of Virginia Health System,undefined
[15] Office of Hospital Epidemiology,undefined
[16] University of Virginia Health System,undefined
[17] AstraZeneca Pharmaceuticals LP,undefined
[18] Clinical Microbiology,undefined
[19] Merck and Co Inc.,undefined
[20] Rahway,undefined
[21] Immunology and Infectious diseases,undefined
[22] University of Calgary,undefined
[23] Snyder Institute for Chronic diseases,undefined
[24] University of Calgary,undefined
[25] University of Pretoria,undefined
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摘要
The dissemination of carbapenem resistance in Escherichia coli has major implications for the management of common infections. blaKPC, encoding a transmissible carbapenemase (KPC), has historically largely been associated with Klebsiella pneumoniae, a predominant plasmid (pKpQIL), and a specific transposable element (Tn4401, ~10 kb). Here we characterize the genetic features of blaKPC emergence in global E. coli, 2008–2013, using both long- and short-read whole-genome sequencing. Amongst 43/45 successfully sequenced blaKPC-E. coli strains, we identified substantial strain diversity (n = 21 sequence types, 18% of annotated genes in the core genome); substantial plasmid diversity (≥9 replicon types); and substantial blaKPC-associated, mobile genetic element (MGE) diversity (50% not within complete Tn4401 elements). We also found evidence of inter-species, regional and international plasmid spread. In several cases blaKPC was found on high copy number, small Col-like plasmids, previously associated with horizontal transmission of resistance genes in the absence of antimicrobial selection pressures. E. coli is a common human pathogen, but also a commensal in multiple environmental and animal reservoirs, and easily transmissible. The association of blaKPC with a range of MGEs previously linked to the successful spread of widely endemic resistance mechanisms (e.g. blaTEM, blaCTX-M) suggests that it may become similarly prevalent.
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