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KPC-49 的表型和遗传分析,KPC-2 变体赋予对头孢他啶-阿维巴坦的抗性并维持对亚胺培南和美罗培南的抗性
Authors Yu M, Wei Q, Song W, Yuan J
Received 29 January 2023
Accepted for publication 18 April 2023
Published 27 April 2023 Volume 2023:16 Pages 2477—2485
DOI https://doi.org/10.2147/IDR.S406319
Checked for plagiarism Yes
Review by Single anonymous peer review
Peer reviewer comments 2
Editor who approved publication: Prof. Dr. Héctor M Mora-Montes
Purpose: Klebsiella pneumoniae , a gram-negative bacterium, poses a severe hazard to public health, with many bacterial hosts having developed resistance to most antibiotics in clinical use. The goal of this study was to look into the development of resistance to both ceftazidime–avibactam and carbapenems, including imipenem and meropenem, in a K. pneumonia strain expressing a novel K. pneumoniae carbapenemase-2 (KPC-2) variant, referred to as KPC-49.
Methods: After 1 day of incubation of K1 on agar containing ceftazidime–avibactam (MIC = 16/4 mg/L), a second KPC-producing K. pneumoniae strain (K2) was recovered. Antimicrobial susceptibility assays, cloning assays, and whole genome sequencing were performed to analyse and evaluate antibiotic resistance phenotypes and genotypes.
Results: K. pneumoniae strain (K1), that produced KPC-2, was susceptible to ceftazidime–avibactam but resistant to carbapenems. The K2 isolate harboured a novel blaKPC-49 variant, which differs from blaKPC-2 by a single nucleotide (C487A), and results in an arginine-serine substitution at amino acid position 163 (R163S). The mutant K2 strain was resistant to both ceftazidime–avibactam and carbapenems. We demonstrated the ability of KPC-49 to hydrolyse carbapenems, which may be attributed to high KPC-49 expression or presence of an efflux pump and/or absence of membrane pore proteins in K2. Furthermore, blaKPC-like was carried on an IncFII (pHN7A8)/IncR-type plasmid within a TnAs1 -orf-orf-orf-orf-orf-orf-ISKpn6-blaKPC-ISKpn27 structure. The blaKPC-like gene was flanked by various insertion sequences and transposon elements, including the Tn3 family transposon, such as TnAs1 , TnAs3 , IS 26 , and IS 481-ISKpn27 .
Conclusion: New KPC variants are emerging owing to sustained exposure to antimicrobials and modifications in their amino acid sequences. We demonstrated the drug resistance mechanisms of the new mutant strains through experimental whole genome sequencing combined with bioinformatics analysis. Enhanced understanding of laboratory and clinical features of infections due to K. pneumoniae of the new KPC subtype is key to early and accurate anti-infective therapy.
Keywords: KPC, antibiotic resistance, whole genome sequencing, ceftazidime–avibactam, susceptibility testing