Rifampicin exposure reveals within-host Mycobacterium tuberculosis diversity in patients with delayed culture conversion

Mycobacterium tuberculosis (Mtb) genetic micro-diversity in clinical isolates may underline mycobacterial adaptation to tuberculosis (TB) infection and provide insights to anti-TB treatment response and emergence of resistance. Herein we followed within-host evolution of Mtb clinical isolates in two...

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Autores principales: Genestet, Charlotte, Hodille, Elisabeth, Barbry, Alexia, Berland, Jean-Luc, Hoffmann, Jonathan, Westeel, Emilie, Bastian, Fabiola, Guichardant, Michel, Venner, Samuel, Lina, Gérard, Ginevra, Christophe, Ader, Florence, Goutelle, Sylvain, Dumitrescu, Oana
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2021
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8224949/
https://www.ncbi.nlm.nih.gov/pubmed/34166469
http://dx.doi.org/10.1371/journal.ppat.1009643
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author Genestet, Charlotte
Hodille, Elisabeth
Barbry, Alexia
Berland, Jean-Luc
Hoffmann, Jonathan
Westeel, Emilie
Bastian, Fabiola
Guichardant, Michel
Venner, Samuel
Lina, Gérard
Ginevra, Christophe
Ader, Florence
Goutelle, Sylvain
Dumitrescu, Oana
author_facet Genestet, Charlotte
Hodille, Elisabeth
Barbry, Alexia
Berland, Jean-Luc
Hoffmann, Jonathan
Westeel, Emilie
Bastian, Fabiola
Guichardant, Michel
Venner, Samuel
Lina, Gérard
Ginevra, Christophe
Ader, Florence
Goutelle, Sylvain
Dumitrescu, Oana
author_sort Genestet, Charlotte
collection PubMed
description Mycobacterium tuberculosis (Mtb) genetic micro-diversity in clinical isolates may underline mycobacterial adaptation to tuberculosis (TB) infection and provide insights to anti-TB treatment response and emergence of resistance. Herein we followed within-host evolution of Mtb clinical isolates in two cohorts of TB patients, either with delayed Mtb culture conversion (> 2 months), or with fast culture conversion (< 2 months). We captured the genetic diversity of Mtb isolates obtained in each patient, by focusing on minor variants detected as unfixed single nucleotide polymorphisms (SNPs). To unmask antibiotic tolerant sub-populations, we exposed these isolates to rifampicin (RIF) prior to whole genome sequencing (WGS) analysis. Thanks to WGS, we detected at least 1 unfixed SNP within the Mtb isolates for 9/15 patients with delayed culture conversion, and non-synonymous (ns) SNPs for 8/15 patients. Furthermore, RIF exposure revealed 9 additional unfixed nsSNP from 6/15 isolates unlinked to drug resistance. By contrast, in the fast culture conversion cohort, RIF exposure only revealed 2 unfixed nsSNP from 2/20 patients. To better understand the dynamics of Mtb micro-diversity, we investigated the variant composition of a persistent Mtb clinical isolate before and after controlled stress experiments mimicking the course of TB disease. A minor variant, featuring a particular mycocerosates profile, became enriched during both RIF exposure and macrophage infection. The variant was associated with drug tolerance and intracellular persistence, consistent with the pharmacological modeling predicting increased risk of treatment failure. A thorough study of such variants not necessarily linked to canonical drug-resistance, but which are prone to promote anti-TB drug tolerance, may be crucial to prevent the subsequent emergence of resistance. Taken together, the present findings support the further exploration of Mtb micro-diversity as a promising tool to detect patients at risk of poorly responding to anti-TB treatment, ultimately allowing improved and personalized TB management.
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spelling pubmed-82249492021-07-19 Rifampicin exposure reveals within-host Mycobacterium tuberculosis diversity in patients with delayed culture conversion Genestet, Charlotte Hodille, Elisabeth Barbry, Alexia Berland, Jean-Luc Hoffmann, Jonathan Westeel, Emilie Bastian, Fabiola Guichardant, Michel Venner, Samuel Lina, Gérard Ginevra, Christophe Ader, Florence Goutelle, Sylvain Dumitrescu, Oana PLoS Pathog Research Article Mycobacterium tuberculosis (Mtb) genetic micro-diversity in clinical isolates may underline mycobacterial adaptation to tuberculosis (TB) infection and provide insights to anti-TB treatment response and emergence of resistance. Herein we followed within-host evolution of Mtb clinical isolates in two cohorts of TB patients, either with delayed Mtb culture conversion (> 2 months), or with fast culture conversion (< 2 months). We captured the genetic diversity of Mtb isolates obtained in each patient, by focusing on minor variants detected as unfixed single nucleotide polymorphisms (SNPs). To unmask antibiotic tolerant sub-populations, we exposed these isolates to rifampicin (RIF) prior to whole genome sequencing (WGS) analysis. Thanks to WGS, we detected at least 1 unfixed SNP within the Mtb isolates for 9/15 patients with delayed culture conversion, and non-synonymous (ns) SNPs for 8/15 patients. Furthermore, RIF exposure revealed 9 additional unfixed nsSNP from 6/15 isolates unlinked to drug resistance. By contrast, in the fast culture conversion cohort, RIF exposure only revealed 2 unfixed nsSNP from 2/20 patients. To better understand the dynamics of Mtb micro-diversity, we investigated the variant composition of a persistent Mtb clinical isolate before and after controlled stress experiments mimicking the course of TB disease. A minor variant, featuring a particular mycocerosates profile, became enriched during both RIF exposure and macrophage infection. The variant was associated with drug tolerance and intracellular persistence, consistent with the pharmacological modeling predicting increased risk of treatment failure. A thorough study of such variants not necessarily linked to canonical drug-resistance, but which are prone to promote anti-TB drug tolerance, may be crucial to prevent the subsequent emergence of resistance. Taken together, the present findings support the further exploration of Mtb micro-diversity as a promising tool to detect patients at risk of poorly responding to anti-TB treatment, ultimately allowing improved and personalized TB management. Public Library of Science 2021-06-24 /pmc/articles/PMC8224949/ /pubmed/34166469 http://dx.doi.org/10.1371/journal.ppat.1009643 Text en © 2021 Genestet et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Genestet, Charlotte
Hodille, Elisabeth
Barbry, Alexia
Berland, Jean-Luc
Hoffmann, Jonathan
Westeel, Emilie
Bastian, Fabiola
Guichardant, Michel
Venner, Samuel
Lina, Gérard
Ginevra, Christophe
Ader, Florence
Goutelle, Sylvain
Dumitrescu, Oana
Rifampicin exposure reveals within-host Mycobacterium tuberculosis diversity in patients with delayed culture conversion
title Rifampicin exposure reveals within-host Mycobacterium tuberculosis diversity in patients with delayed culture conversion
title_full Rifampicin exposure reveals within-host Mycobacterium tuberculosis diversity in patients with delayed culture conversion
title_fullStr Rifampicin exposure reveals within-host Mycobacterium tuberculosis diversity in patients with delayed culture conversion
title_full_unstemmed Rifampicin exposure reveals within-host Mycobacterium tuberculosis diversity in patients with delayed culture conversion
title_short Rifampicin exposure reveals within-host Mycobacterium tuberculosis diversity in patients with delayed culture conversion
title_sort rifampicin exposure reveals within-host mycobacterium tuberculosis diversity in patients with delayed culture conversion
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8224949/
https://www.ncbi.nlm.nih.gov/pubmed/34166469
http://dx.doi.org/10.1371/journal.ppat.1009643
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