Outbreak report of polymyxin-carbapenem-resistant Klebsiella pneumoniae causing untreatable infections evidenced by synergy tests and bacterial genomes

Author:

Gomes Marisa Zenaide Ribeiro,de Lima Elisangela Martins,Martins Aires Caio Augusto,Pereira Polyana Silva,Yim Juwon,Silva Fernando Henrique,Rodrigues Caio Augusto Santos,Oliveira Thamirys Rachel Tavares e,da Silva Priscila Pinho,Eller Cristiane Monteiro,de Souza Claudio Marcos Rocha,Rybak Michael J.,Albano Rodolpho Mattos,de Miranda Antonio Basílio,Machado Edson,Catanho Marcos,Dutra Vitoria Pinson Ruggi,de Mello Luciana Sênos,Tonhá João Pedro Silva,Castro Murillo Marçal,da Silva Machado Amanda Aparecida,da Silva Maxuel Cassiano,Mathuiy Yann Rodrigues,Tozo Thaisa Medeiros,

Abstract

AbstractPolymyxin-carbapenem-resistant Klebsiella pneumoniae (PCR-Kp) with pan (PDR)- or extensively drug-resistant phenotypes has been increasingly described worldwide. Here, we report a PCR-Kp outbreak causing untreatable infections descriptively correlated with bacterial genomes. Hospital-wide surveillance of PCR-Kp was initiated in December-2014, after the first detection of a K. pneumoniae phenotype initially classified as PDR, recovered from close spatiotemporal cases of a sentinel hospital in Rio de Janeiro. Whole-genome sequencing of clinical PCR-Kp was performed to investigate similarities and dissimilarities in phylogeny, resistance and virulence genes, plasmid structures and genetic polymorphisms. A target phenotypic profile was detected in 10% (12/117) of the tested K. pneumoniae complex bacteria recovered from patients (8.5%, 8/94) who had epidemiological links and were involved in intractable infections and death, with combined therapeutic drugs failing to meet synergy. Two resistant bacterial clades belong to the same transmission cluster (ST437) or might have different sources (ST11). The severity of infection was likely related to patients’ comorbidities, lack of antimicrobial therapy and predicted bacterial genes related to high resistance, survival, and proliferation. This report contributes to the actual knowledge about the natural history of PCR-Kp infection, while reporting from a time when there were no licensed drugs in the world to treat some of these infections. More studies comparing clinical findings with bacterial genetic markers during clonal spread are needed.

Funder

National Council for Scientific and Technological Development

Publisher

Springer Science and Business Media LLC

Subject

Multidisciplinary

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