IS1-related large-scale deletion of chromosomal regions harbouring the oxygen-insensitive nitroreductase gene nfsB causes nitrofurantoin heteroresistance in Escherichia coli

Nitrofurantoin is a broad-spectrum first-line antimicrobial used for managing uncomplicated urinary tract infection (UTI). Loss-of-function mutations in chromosomal genes nfsA, nfsB and ribE of Escherichia coli are known to reduce nitrofurantoin susceptibility. Here, we report the discovery of nitro...

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Autores principales: Wan, Yu, Sabnis, Akshay, Mumin, Zaynab, Potterill, Isabelle, Jauneikaite, Elita, Brown, Colin S., Ellington, Matthew J., Edwards, Andrew, Sriskandan, Shiranee
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Microbiology Society 2023
Materias:
Short Communications
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10569738/
https://www.ncbi.nlm.nih.gov/pubmed/37672334
http://dx.doi.org/10.1099/mgen.0.001102
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author Wan, Yu
Sabnis, Akshay
Mumin, Zaynab
Potterill, Isabelle
Jauneikaite, Elita
Brown, Colin S.
Ellington, Matthew J.
Edwards, Andrew
Sriskandan, Shiranee
author_facet Wan, Yu
Sabnis, Akshay
Mumin, Zaynab
Potterill, Isabelle
Jauneikaite, Elita
Brown, Colin S.
Ellington, Matthew J.
Edwards, Andrew
Sriskandan, Shiranee
author_sort Wan, Yu
collection PubMed
description Nitrofurantoin is a broad-spectrum first-line antimicrobial used for managing uncomplicated urinary tract infection (UTI). Loss-of-function mutations in chromosomal genes nfsA, nfsB and ribE of Escherichia coli are known to reduce nitrofurantoin susceptibility. Here, we report the discovery of nitrofurantoin heteroresistance in E. coli clinical isolates and a novel genetic mechanism associated with this phenomenon. Subpopulations with lower nitrofurantoin susceptibility than major populations (hereafter, nitrofurantoin-resistant subpopulations) in two E. coli blood isolates (previously whole-genome sequenced) were identified using population analysis profiling. Each isolate was known to have a loss-of-function mutation in nfsA. From each isolate, four nitrofurantoin-resistant isolates were derived at a nitrofurantoin concentration of 32 mg l(−1), and a comparator isolate was obtained without any nitrofurantoin exposure. Genomes of derived isolates were sequenced on Illumina and Nanopore MinION systems. Genetic variation between isolates was determined based on genome assemblies and read mapping. Nitrofurantoin minimum inhibitory concentrations (MICs) of both blood isolates were 64 mg l(−1), with MICs of major nitrofurantoin-susceptible populations varying from 4 to 8 mg l(−1). Two to 99 c.f.u. per million demonstrated growth at the nitrofurantoin concentration of 32 mg l(−1), which is distinct from that of a homogeneously susceptible or resistant isolate. Derived nitrofurantoin-resistant isolates had 11–66 kb deletions in chromosomal regions harbouring nfsB, and all deletions were immediately adjacent to IS1-family insertion sequences. Our findings demonstrate that the IS1-associated large-scale genetic deletion is a hitherto unrecognized mechanism of nitrofurantoin heteroresistance and could compromise UTI management. Further, frequencies of resistant subpopulations from nitrofurantoin-heteroresistant isolates may challenge conventional nitrofurantoin susceptibility testing in clinical settings.
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spelling pubmed-105697382023-10-13 IS1-related large-scale deletion of chromosomal regions harbouring the oxygen-insensitive nitroreductase gene nfsB causes nitrofurantoin heteroresistance in Escherichia coli Wan, Yu Sabnis, Akshay Mumin, Zaynab Potterill, Isabelle Jauneikaite, Elita Brown, Colin S. Ellington, Matthew J. Edwards, Andrew Sriskandan, Shiranee Microb Genom Short Communications Nitrofurantoin is a broad-spectrum first-line antimicrobial used for managing uncomplicated urinary tract infection (UTI). Loss-of-function mutations in chromosomal genes nfsA, nfsB and ribE of Escherichia coli are known to reduce nitrofurantoin susceptibility. Here, we report the discovery of nitrofurantoin heteroresistance in E. coli clinical isolates and a novel genetic mechanism associated with this phenomenon. Subpopulations with lower nitrofurantoin susceptibility than major populations (hereafter, nitrofurantoin-resistant subpopulations) in two E. coli blood isolates (previously whole-genome sequenced) were identified using population analysis profiling. Each isolate was known to have a loss-of-function mutation in nfsA. From each isolate, four nitrofurantoin-resistant isolates were derived at a nitrofurantoin concentration of 32 mg l(−1), and a comparator isolate was obtained without any nitrofurantoin exposure. Genomes of derived isolates were sequenced on Illumina and Nanopore MinION systems. Genetic variation between isolates was determined based on genome assemblies and read mapping. Nitrofurantoin minimum inhibitory concentrations (MICs) of both blood isolates were 64 mg l(−1), with MICs of major nitrofurantoin-susceptible populations varying from 4 to 8 mg l(−1). Two to 99 c.f.u. per million demonstrated growth at the nitrofurantoin concentration of 32 mg l(−1), which is distinct from that of a homogeneously susceptible or resistant isolate. Derived nitrofurantoin-resistant isolates had 11–66 kb deletions in chromosomal regions harbouring nfsB, and all deletions were immediately adjacent to IS1-family insertion sequences. Our findings demonstrate that the IS1-associated large-scale genetic deletion is a hitherto unrecognized mechanism of nitrofurantoin heteroresistance and could compromise UTI management. Further, frequencies of resistant subpopulations from nitrofurantoin-heteroresistant isolates may challenge conventional nitrofurantoin susceptibility testing in clinical settings. Microbiology Society 2023-09-06 /pmc/articles/PMC10569738/ /pubmed/37672334 http://dx.doi.org/10.1099/mgen.0.001102 Text en © 2023 The Authors https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License. This article was made open access via a Publish and Read agreement between the Microbiology Society and the corresponding author’s institution.
spellingShingle Short Communications
Wan, Yu
Sabnis, Akshay
Mumin, Zaynab
Potterill, Isabelle
Jauneikaite, Elita
Brown, Colin S.
Ellington, Matthew J.
Edwards, Andrew
Sriskandan, Shiranee
IS1-related large-scale deletion of chromosomal regions harbouring the oxygen-insensitive nitroreductase gene nfsB causes nitrofurantoin heteroresistance in Escherichia coli
title IS1-related large-scale deletion of chromosomal regions harbouring the oxygen-insensitive nitroreductase gene nfsB causes nitrofurantoin heteroresistance in Escherichia coli
title_full IS1-related large-scale deletion of chromosomal regions harbouring the oxygen-insensitive nitroreductase gene nfsB causes nitrofurantoin heteroresistance in Escherichia coli
title_fullStr IS1-related large-scale deletion of chromosomal regions harbouring the oxygen-insensitive nitroreductase gene nfsB causes nitrofurantoin heteroresistance in Escherichia coli
title_full_unstemmed IS1-related large-scale deletion of chromosomal regions harbouring the oxygen-insensitive nitroreductase gene nfsB causes nitrofurantoin heteroresistance in Escherichia coli
title_short IS1-related large-scale deletion of chromosomal regions harbouring the oxygen-insensitive nitroreductase gene nfsB causes nitrofurantoin heteroresistance in Escherichia coli
title_sort is1-related large-scale deletion of chromosomal regions harbouring the oxygen-insensitive nitroreductase gene nfsb causes nitrofurantoin heteroresistance in escherichia coli
topic Short Communications
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10569738/
https://www.ncbi.nlm.nih.gov/pubmed/37672334
http://dx.doi.org/10.1099/mgen.0.001102
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