Polymyxin Resistance in Clinical Isolates of K. pneumoniae in Brazil: Update on Molecular Mechanisms, Clonal Dissemination and Relationship With KPC-Producing Strains

In Brazil, the production of KPC-type carbapenemases in Enterobacteriales is endemic, leading to widespread use of polymyxins. In the present study, 502 Klebsiella pneumoniae isolates were evaluated for resistance to polymyxins, their genetic determinants and clonality, in addition to the presence o...

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Autores principales: Conceição-Neto, Orlando C., da Costa, Bianca Santos, Pontes, Leilane da Silva, Silveira, Melise Chaves, Justo-da-Silva, Lívia Helena, de Oliveira Santos, Ivson Cassiano, Teixeira, Camila Bastos Tavares, Tavares e Oliveira, Thamirys Rachel, Hermes, Fernanda Stephens, Galvão, Teca Calcagno, Antunes, L. Caetano M., Rocha-de-Souza, Cláudio Marcos, Carvalho-Assef, Ana P. D.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Cellular and Infection Microbiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9334684/
https://www.ncbi.nlm.nih.gov/pubmed/35909953
http://dx.doi.org/10.3389/fcimb.2022.898125
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author Conceição-Neto, Orlando C.
da Costa, Bianca Santos
Pontes, Leilane da Silva
Silveira, Melise Chaves
Justo-da-Silva, Lívia Helena
de Oliveira Santos, Ivson Cassiano
Teixeira, Camila Bastos Tavares
Tavares e Oliveira, Thamirys Rachel
Hermes, Fernanda Stephens
Galvão, Teca Calcagno
Antunes, L. Caetano M.
Rocha-de-Souza, Cláudio Marcos
Carvalho-Assef, Ana P. D.
author_facet Conceição-Neto, Orlando C.
da Costa, Bianca Santos
Pontes, Leilane da Silva
Silveira, Melise Chaves
Justo-da-Silva, Lívia Helena
de Oliveira Santos, Ivson Cassiano
Teixeira, Camila Bastos Tavares
Tavares e Oliveira, Thamirys Rachel
Hermes, Fernanda Stephens
Galvão, Teca Calcagno
Antunes, L. Caetano M.
Rocha-de-Souza, Cláudio Marcos
Carvalho-Assef, Ana P. D.
author_sort Conceição-Neto, Orlando C.
collection PubMed
description In Brazil, the production of KPC-type carbapenemases in Enterobacteriales is endemic, leading to widespread use of polymyxins. In the present study, 502 Klebsiella pneumoniae isolates were evaluated for resistance to polymyxins, their genetic determinants and clonality, in addition to the presence of carbapenem resistance genes and evaluation of antimicrobial resistance. Resistance to colistin (polymyxin E) was evaluated through initial selection on EMB agar containing 4% colistin sulfate, followed by Minimal Inhibitory Concentration (MIC) determination by broth microdilution. The susceptibility to 17 antimicrobials was assessed by disk diffusion. The presence of bla (KPC), bla (NDM) and bla (OXA-48-like) carbapenemases was investigated by phenotypic methods and conventional PCR. Molecular typing was performed by PFGE and MLST. Allelic variants of the mcr gene were screened by PCR and chromosomal mutations in the pmrA, pmrB, phoP, phoQ and mgrB genes were investigated by sequencing. Our work showed a colistin resistance frequency of 29.5% (n = 148/502) in K. pneumoniae isolates. Colistin MICs from 4 to >128 µg/mL were identified (MIC(50) = 64 µg/mL; MIC(90) >128 µg/mL). All isolates were considered MDR, with the lowest resistance rates observed for amikacin (34.4%), and 19.6% of the isolates were resistant to all tested antimicrobials. The bla (KPC) gene was identified in 77% of the isolates, in consonance with the high rate of resistance to polymyxins related to its use as a therapeutic alternative. Through XbaI-PFGE, 51 pulsotypes were identified. MLST showed 21 STs, with ST437, ST258 and ST11 (CC11) being the most prevalent, and two new STs were determined: ST4868 and ST4869. The mcr-1 gene was identified in 3 K. pneumoniae isolates. Missense mutations in chromosomal genes were identified, as well as insertion sequences in mgrB. Furthermore, the identification of chromosomal mutations in K. pneumoniae isolates belonging from CC11 ensures its success as a high-risk epidemic clone in Brazil and worldwide.
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spelling pubmed-93346842022-07-30 Polymyxin Resistance in Clinical Isolates of K. pneumoniae in Brazil: Update on Molecular Mechanisms, Clonal Dissemination and Relationship With KPC-Producing Strains Conceição-Neto, Orlando C. da Costa, Bianca Santos Pontes, Leilane da Silva Silveira, Melise Chaves Justo-da-Silva, Lívia Helena de Oliveira Santos, Ivson Cassiano Teixeira, Camila Bastos Tavares Tavares e Oliveira, Thamirys Rachel Hermes, Fernanda Stephens Galvão, Teca Calcagno Antunes, L. Caetano M. Rocha-de-Souza, Cláudio Marcos Carvalho-Assef, Ana P. D. Front Cell Infect Microbiol Cellular and Infection Microbiology In Brazil, the production of KPC-type carbapenemases in Enterobacteriales is endemic, leading to widespread use of polymyxins. In the present study, 502 Klebsiella pneumoniae isolates were evaluated for resistance to polymyxins, their genetic determinants and clonality, in addition to the presence of carbapenem resistance genes and evaluation of antimicrobial resistance. Resistance to colistin (polymyxin E) was evaluated through initial selection on EMB agar containing 4% colistin sulfate, followed by Minimal Inhibitory Concentration (MIC) determination by broth microdilution. The susceptibility to 17 antimicrobials was assessed by disk diffusion. The presence of bla (KPC), bla (NDM) and bla (OXA-48-like) carbapenemases was investigated by phenotypic methods and conventional PCR. Molecular typing was performed by PFGE and MLST. Allelic variants of the mcr gene were screened by PCR and chromosomal mutations in the pmrA, pmrB, phoP, phoQ and mgrB genes were investigated by sequencing. Our work showed a colistin resistance frequency of 29.5% (n = 148/502) in K. pneumoniae isolates. Colistin MICs from 4 to >128 µg/mL were identified (MIC(50) = 64 µg/mL; MIC(90) >128 µg/mL). All isolates were considered MDR, with the lowest resistance rates observed for amikacin (34.4%), and 19.6% of the isolates were resistant to all tested antimicrobials. The bla (KPC) gene was identified in 77% of the isolates, in consonance with the high rate of resistance to polymyxins related to its use as a therapeutic alternative. Through XbaI-PFGE, 51 pulsotypes were identified. MLST showed 21 STs, with ST437, ST258 and ST11 (CC11) being the most prevalent, and two new STs were determined: ST4868 and ST4869. The mcr-1 gene was identified in 3 K. pneumoniae isolates. Missense mutations in chromosomal genes were identified, as well as insertion sequences in mgrB. Furthermore, the identification of chromosomal mutations in K. pneumoniae isolates belonging from CC11 ensures its success as a high-risk epidemic clone in Brazil and worldwide. Frontiers Media S.A. 2022-07-15 /pmc/articles/PMC9334684/ /pubmed/35909953 http://dx.doi.org/10.3389/fcimb.2022.898125 Text en Copyright © 2022 Conceição-Neto, da Costa, Pontes, Silveira, Justo-da-Silva, de Oliveira Santos, Teixeira, Tavares e Oliveira, Hermes, Galvão, Antunes, Rocha-de-Souza and Carvalho-Assef https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Cellular and Infection Microbiology
Conceição-Neto, Orlando C.
da Costa, Bianca Santos
Pontes, Leilane da Silva
Silveira, Melise Chaves
Justo-da-Silva, Lívia Helena
de Oliveira Santos, Ivson Cassiano
Teixeira, Camila Bastos Tavares
Tavares e Oliveira, Thamirys Rachel
Hermes, Fernanda Stephens
Galvão, Teca Calcagno
Antunes, L. Caetano M.
Rocha-de-Souza, Cláudio Marcos
Carvalho-Assef, Ana P. D.
Polymyxin Resistance in Clinical Isolates of K. pneumoniae in Brazil: Update on Molecular Mechanisms, Clonal Dissemination and Relationship With KPC-Producing Strains
title Polymyxin Resistance in Clinical Isolates of K. pneumoniae in Brazil: Update on Molecular Mechanisms, Clonal Dissemination and Relationship With KPC-Producing Strains
title_full Polymyxin Resistance in Clinical Isolates of K. pneumoniae in Brazil: Update on Molecular Mechanisms, Clonal Dissemination and Relationship With KPC-Producing Strains
title_fullStr Polymyxin Resistance in Clinical Isolates of K. pneumoniae in Brazil: Update on Molecular Mechanisms, Clonal Dissemination and Relationship With KPC-Producing Strains
title_full_unstemmed Polymyxin Resistance in Clinical Isolates of K. pneumoniae in Brazil: Update on Molecular Mechanisms, Clonal Dissemination and Relationship With KPC-Producing Strains
title_short Polymyxin Resistance in Clinical Isolates of K. pneumoniae in Brazil: Update on Molecular Mechanisms, Clonal Dissemination and Relationship With KPC-Producing Strains
title_sort polymyxin resistance in clinical isolates of k. pneumoniae in brazil: update on molecular mechanisms, clonal dissemination and relationship with kpc-producing strains
topic Cellular and Infection Microbiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9334684/
https://www.ncbi.nlm.nih.gov/pubmed/35909953
http://dx.doi.org/10.3389/fcimb.2022.898125
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