Novel Conserved Genotypes Correspond to Antibiotic Resistance Phenotypes of E. coli Clinical Isolates

Current efforts to understand antibiotic resistance on the whole genome scale tend to focus on known genes even as high throughput sequencing strategies uncover novel mechanisms. To identify genomic variations associated with antibiotic resistance, we employed a modified genome-wide association stud...

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Autores principales: Swick, Michelle C., Evangelista, Michael A., Bodine, Truston J., Easton-Marks, Jeremy R., Barth, Patrick, Shah, Minita J., Bormann Chung, Christina A., Stanley, Sarah, McLaughlin, Stephen F., Lee, Clarence C., Sheth, Vrunda, Doan, Quynh, Hamill, Richard J., Steffen, David, Becnel, Lauren B., Sucgang, Richard, Zechiedrich, Lynn
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3688849/
https://www.ncbi.nlm.nih.gov/pubmed/23824211
http://dx.doi.org/10.1371/journal.pone.0065961
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author Swick, Michelle C.
Evangelista, Michael A.
Bodine, Truston J.
Easton-Marks, Jeremy R.
Barth, Patrick
Shah, Minita J.
Bormann Chung, Christina A.
Stanley, Sarah
McLaughlin, Stephen F.
Lee, Clarence C.
Sheth, Vrunda
Doan, Quynh
Hamill, Richard J.
Steffen, David
Becnel, Lauren B.
Sucgang, Richard
Zechiedrich, Lynn
author_facet Swick, Michelle C.
Evangelista, Michael A.
Bodine, Truston J.
Easton-Marks, Jeremy R.
Barth, Patrick
Shah, Minita J.
Bormann Chung, Christina A.
Stanley, Sarah
McLaughlin, Stephen F.
Lee, Clarence C.
Sheth, Vrunda
Doan, Quynh
Hamill, Richard J.
Steffen, David
Becnel, Lauren B.
Sucgang, Richard
Zechiedrich, Lynn
author_sort Swick, Michelle C.
collection PubMed
description Current efforts to understand antibiotic resistance on the whole genome scale tend to focus on known genes even as high throughput sequencing strategies uncover novel mechanisms. To identify genomic variations associated with antibiotic resistance, we employed a modified genome-wide association study; we sequenced genomic DNA from pools of E. coli clinical isolates with similar antibiotic resistance phenotypes using SOLiD technology to uncover single nucleotide polymorphisms (SNPs) unanimously conserved in each pool. The multidrug-resistant pools were genotypically similar to SMS-3-5, a previously sequenced multidrug-resistant isolate from a polluted environment. The similarity was evenly spread across the entire genome and not limited to plasmid or pathogenicity island loci. Among the pools of clinical isolates, genomic variation was concentrated adjacent to previously reported inversion and duplication differences between the SMS-3-5 isolate and the drug-susceptible laboratory strain, DH10B. SNPs that result in non-synonymous changes in gyrA (encoding the well-known S83L allele associated with fluoroquinolone resistance), mutM, ligB, and recG were unanimously conserved in every fluoroquinolone-resistant pool. Alleles of the latter three genes are tightly linked among most sequenced E. coli genomes, and had not been implicated in antibiotic resistance previously. The changes in these genes map to amino acid positions in alpha helices that are involved in DNA binding. Plasmid-encoded complementation of null strains with either allelic variant of mutM or ligB resulted in variable responses to ultraviolet light or hydrogen peroxide treatment as markers of induced DNA damage, indicating their importance in DNA metabolism and revealing a potential mechanism for fluoroquinolone resistance. Our approach uncovered evidence that additional DNA binding enzymes may contribute to fluoroquinolone resistance and further implicate environmental bacteria as a reservoir for antibiotic resistance.
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spelling pubmed-36888492013-07-02 Novel Conserved Genotypes Correspond to Antibiotic Resistance Phenotypes of E. coli Clinical Isolates Swick, Michelle C. Evangelista, Michael A. Bodine, Truston J. Easton-Marks, Jeremy R. Barth, Patrick Shah, Minita J. Bormann Chung, Christina A. Stanley, Sarah McLaughlin, Stephen F. Lee, Clarence C. Sheth, Vrunda Doan, Quynh Hamill, Richard J. Steffen, David Becnel, Lauren B. Sucgang, Richard Zechiedrich, Lynn PLoS One Research Article Current efforts to understand antibiotic resistance on the whole genome scale tend to focus on known genes even as high throughput sequencing strategies uncover novel mechanisms. To identify genomic variations associated with antibiotic resistance, we employed a modified genome-wide association study; we sequenced genomic DNA from pools of E. coli clinical isolates with similar antibiotic resistance phenotypes using SOLiD technology to uncover single nucleotide polymorphisms (SNPs) unanimously conserved in each pool. The multidrug-resistant pools were genotypically similar to SMS-3-5, a previously sequenced multidrug-resistant isolate from a polluted environment. The similarity was evenly spread across the entire genome and not limited to plasmid or pathogenicity island loci. Among the pools of clinical isolates, genomic variation was concentrated adjacent to previously reported inversion and duplication differences between the SMS-3-5 isolate and the drug-susceptible laboratory strain, DH10B. SNPs that result in non-synonymous changes in gyrA (encoding the well-known S83L allele associated with fluoroquinolone resistance), mutM, ligB, and recG were unanimously conserved in every fluoroquinolone-resistant pool. Alleles of the latter three genes are tightly linked among most sequenced E. coli genomes, and had not been implicated in antibiotic resistance previously. The changes in these genes map to amino acid positions in alpha helices that are involved in DNA binding. Plasmid-encoded complementation of null strains with either allelic variant of mutM or ligB resulted in variable responses to ultraviolet light or hydrogen peroxide treatment as markers of induced DNA damage, indicating their importance in DNA metabolism and revealing a potential mechanism for fluoroquinolone resistance. Our approach uncovered evidence that additional DNA binding enzymes may contribute to fluoroquinolone resistance and further implicate environmental bacteria as a reservoir for antibiotic resistance. Public Library of Science 2013-06-18 /pmc/articles/PMC3688849/ /pubmed/23824211 http://dx.doi.org/10.1371/journal.pone.0065961 Text en © 2013 Swick et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Swick, Michelle C.
Evangelista, Michael A.
Bodine, Truston J.
Easton-Marks, Jeremy R.
Barth, Patrick
Shah, Minita J.
Bormann Chung, Christina A.
Stanley, Sarah
McLaughlin, Stephen F.
Lee, Clarence C.
Sheth, Vrunda
Doan, Quynh
Hamill, Richard J.
Steffen, David
Becnel, Lauren B.
Sucgang, Richard
Zechiedrich, Lynn
Novel Conserved Genotypes Correspond to Antibiotic Resistance Phenotypes of E. coli Clinical Isolates
title Novel Conserved Genotypes Correspond to Antibiotic Resistance Phenotypes of E. coli Clinical Isolates
title_full Novel Conserved Genotypes Correspond to Antibiotic Resistance Phenotypes of E. coli Clinical Isolates
title_fullStr Novel Conserved Genotypes Correspond to Antibiotic Resistance Phenotypes of E. coli Clinical Isolates
title_full_unstemmed Novel Conserved Genotypes Correspond to Antibiotic Resistance Phenotypes of E. coli Clinical Isolates
title_short Novel Conserved Genotypes Correspond to Antibiotic Resistance Phenotypes of E. coli Clinical Isolates
title_sort novel conserved genotypes correspond to antibiotic resistance phenotypes of e. coli clinical isolates
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3688849/
https://www.ncbi.nlm.nih.gov/pubmed/23824211
http://dx.doi.org/10.1371/journal.pone.0065961
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