Virulence of Mycobacterium tuberculosis after Acquisition of Isoniazid Resistance: Individual Nature of katG Mutants and the Possible Role of AhpC.

Virulence of Mycobacterium tuberculosis after Acquisition of Isoniazid Resistance: Individual Nature of katG Mutants and the Possible Role of AhpC.

In the last decade, there were 10 million new tuberculosis cases per year globally. Around 9.5% of these cases were caused by isoniazid resistant (INHr) Mycobacterium tuberculosis (Mtb) strains. Although isoniazid resistance in Mtb is multigenic, mutations in the catalase-peroxidase (katG) gene pred...

Full description

Bibliographic Details
Main Authors: Luisa Maria Nieto R, Carolina Mehaffy, Elizabeth Creissen, JoLynn Troudt, Amber Troy, Helle Bielefeldt-Ohmann, Marcos Burgos, Angelo Izzo, Karen M Dobos
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2016-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC5125630?pdf=render
_version_ 1818244815627747328
author Luisa Maria Nieto R
Carolina Mehaffy
Elizabeth Creissen
JoLynn Troudt
Amber Troy
Helle Bielefeldt-Ohmann
Marcos Burgos
Angelo Izzo
Karen M Dobos
author_facet Luisa Maria Nieto R
Carolina Mehaffy
Elizabeth Creissen
JoLynn Troudt
Amber Troy
Helle Bielefeldt-Ohmann
Marcos Burgos
Angelo Izzo
Karen M Dobos
author_sort Luisa Maria Nieto R
collection DOAJ
description In the last decade, there were 10 million new tuberculosis cases per year globally. Around 9.5% of these cases were caused by isoniazid resistant (INHr) Mycobacterium tuberculosis (Mtb) strains. Although isoniazid resistance in Mtb is multigenic, mutations in the catalase-peroxidase (katG) gene predominate among the INHr strains. The effect of these drug-resistance-conferring mutations on Mtb fitness and virulence is variable. Here, we assessed differences in bacterial growth, immune response and pathology induced by Mtb strains harboring mutations at the N-terminus of the katG gene. We studied one laboratory and one clinically isolated Mtb clonal pair from different genetic lineages. The INHr strain in each pair had one and two katG mutations with significantly reduced levels of the enzyme and peroxidase activity. Both strains share the V1A mutation, while the double mutant clinical INHr had also the novel E3V katG mutation. Four groups of C57BL/6 mice were infected with one of the Mtb strains previously described. We observed a strong reduction in virulence (reduced bacterial growth), lower induction of proinflammatory cytokines and significantly reduced pathology scores in mice infected with the clinical INHr strain compared to the infection caused by its INHs progenitor strain. On the other hand, there was a subtle reduction of bacteria growth without differences in the pathology scores in mice infected with the laboratory INHr strain. Our results also showed distinct alkyl-hydroperoxidase C (AhpC) levels in the katG mutant strains, which could explain the difference in the virulence profile observed. The difference in the AhpC levels between clonal strains was not related to a genetic defect in the gene or its promoter. Cumulatively, our results indicate that the virulence, pathology and fitness of INHr strains could be negatively affected by multiple mutations in katG, lack of the peroxidase activity and reduced AhpC levels.
first_indexed 2024-12-12T14:23:01Z
format Article
id doaj.art-d24921853bcd45b3a3cd8ffb7d30dc1a
institution Directory Open Access Journal
issn 1932-6203
language English
last_indexed 2024-12-12T14:23:01Z
publishDate 2016-01-01
publisher Public Library of Science (PLoS)
record_format Article
series PLoS ONE
spelling doaj.art-d24921853bcd45b3a3cd8ffb7d30dc1a2022-12-22T00:21:45ZengPublic Library of Science (PLoS)PLoS ONE1932-62032016-01-011111e016680710.1371/journal.pone.0166807Virulence of Mycobacterium tuberculosis after Acquisition of Isoniazid Resistance: Individual Nature of katG Mutants and the Possible Role of AhpC.Luisa Maria Nieto RCarolina MehaffyElizabeth CreissenJoLynn TroudtAmber TroyHelle Bielefeldt-OhmannMarcos BurgosAngelo IzzoKaren M DobosIn the last decade, there were 10 million new tuberculosis cases per year globally. Around 9.5% of these cases were caused by isoniazid resistant (INHr) Mycobacterium tuberculosis (Mtb) strains. Although isoniazid resistance in Mtb is multigenic, mutations in the catalase-peroxidase (katG) gene predominate among the INHr strains. The effect of these drug-resistance-conferring mutations on Mtb fitness and virulence is variable. Here, we assessed differences in bacterial growth, immune response and pathology induced by Mtb strains harboring mutations at the N-terminus of the katG gene. We studied one laboratory and one clinically isolated Mtb clonal pair from different genetic lineages. The INHr strain in each pair had one and two katG mutations with significantly reduced levels of the enzyme and peroxidase activity. Both strains share the V1A mutation, while the double mutant clinical INHr had also the novel E3V katG mutation. Four groups of C57BL/6 mice were infected with one of the Mtb strains previously described. We observed a strong reduction in virulence (reduced bacterial growth), lower induction of proinflammatory cytokines and significantly reduced pathology scores in mice infected with the clinical INHr strain compared to the infection caused by its INHs progenitor strain. On the other hand, there was a subtle reduction of bacteria growth without differences in the pathology scores in mice infected with the laboratory INHr strain. Our results also showed distinct alkyl-hydroperoxidase C (AhpC) levels in the katG mutant strains, which could explain the difference in the virulence profile observed. The difference in the AhpC levels between clonal strains was not related to a genetic defect in the gene or its promoter. Cumulatively, our results indicate that the virulence, pathology and fitness of INHr strains could be negatively affected by multiple mutations in katG, lack of the peroxidase activity and reduced AhpC levels.http://europepmc.org/articles/PMC5125630?pdf=render
spellingShingle Luisa Maria Nieto R
Carolina Mehaffy
Elizabeth Creissen
JoLynn Troudt
Amber Troy
Helle Bielefeldt-Ohmann
Marcos Burgos
Angelo Izzo
Karen M Dobos
Virulence of Mycobacterium tuberculosis after Acquisition of Isoniazid Resistance: Individual Nature of katG Mutants and the Possible Role of AhpC.
PLoS ONE
title Virulence of Mycobacterium tuberculosis after Acquisition of Isoniazid Resistance: Individual Nature of katG Mutants and the Possible Role of AhpC.
title_full Virulence of Mycobacterium tuberculosis after Acquisition of Isoniazid Resistance: Individual Nature of katG Mutants and the Possible Role of AhpC.
title_fullStr Virulence of Mycobacterium tuberculosis after Acquisition of Isoniazid Resistance: Individual Nature of katG Mutants and the Possible Role of AhpC.
title_full_unstemmed Virulence of Mycobacterium tuberculosis after Acquisition of Isoniazid Resistance: Individual Nature of katG Mutants and the Possible Role of AhpC.
title_short Virulence of Mycobacterium tuberculosis after Acquisition of Isoniazid Resistance: Individual Nature of katG Mutants and the Possible Role of AhpC.
title_sort virulence of mycobacterium tuberculosis after acquisition of isoniazid resistance individual nature of katg mutants and the possible role of ahpc
url http://europepmc.org/articles/PMC5125630?pdf=render
work_keys_str_mv AT luisamarianietor virulenceofmycobacteriumtuberculosisafteracquisitionofisoniazidresistanceindividualnatureofkatgmutantsandthepossibleroleofahpc
AT carolinamehaffy virulenceofmycobacteriumtuberculosisafteracquisitionofisoniazidresistanceindividualnatureofkatgmutantsandthepossibleroleofahpc
AT elizabethcreissen virulenceofmycobacteriumtuberculosisafteracquisitionofisoniazidresistanceindividualnatureofkatgmutantsandthepossibleroleofahpc
AT jolynntroudt virulenceofmycobacteriumtuberculosisafteracquisitionofisoniazidresistanceindividualnatureofkatgmutantsandthepossibleroleofahpc
AT ambertroy virulenceofmycobacteriumtuberculosisafteracquisitionofisoniazidresistanceindividualnatureofkatgmutantsandthepossibleroleofahpc
AT hellebielefeldtohmann virulenceofmycobacteriumtuberculosisafteracquisitionofisoniazidresistanceindividualnatureofkatgmutantsandthepossibleroleofahpc
AT marcosburgos virulenceofmycobacteriumtuberculosisafteracquisitionofisoniazidresistanceindividualnatureofkatgmutantsandthepossibleroleofahpc
AT angeloizzo virulenceofmycobacteriumtuberculosisafteracquisitionofisoniazidresistanceindividualnatureofkatgmutantsandthepossibleroleofahpc
AT karenmdobos virulenceofmycobacteriumtuberculosisafteracquisitionofisoniazidresistanceindividualnatureofkatgmutantsandthepossibleroleofahpc

Similar Items