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The changes in mycolic acid structures caused by hadC mutation have a dramatic effect on the virulence of Mycobacterium tuberculosis

Identifieur interne : 000603 ( Hal/Corpus ); précédent : 000602; suivant : 000604

The changes in mycolic acid structures caused by hadC mutation have a dramatic effect on the virulence of Mycobacterium tuberculosis

Auteurs : Nawel Slama ; Stevie Jamet ; Wafa Frigui ; Alexandre Pawlik ; Daria Bottai ; Françoise Laval ; Patricia Constant ; Anne Lemassu ; Kaymeuang Cam ; Mamadou Daffé ; Roland Brosch ; Nathalie Eynard ; Annaïk Quémard

Source :

RBID : Hal:pasteur-02618562

Abstract

Understanding the molecular strategies used by Mycobacterium tuberculosis to invade and persist within the host is of paramount importance to tackle the tuberculosis pandemic. Comparative genomic surveys have revealed that hadC, encoding a subunit of the HadBC dehydratase, is mutated in the avirulent M. tuberculosis H37Ra strain. We show here that mutation or deletion of hadC affects the biosynthesis of oxygenated mycolic acids, substantially reducing their production level. Additionally, it causes the loss of atypical extra-long mycolic acids, demonstrating the involvement of HadBC in the late elongation steps of mycolic acid biosynthesis. These events have an impact on the morphotype, cording capacity and biofilm growth of the bacilli as well as on their sensitivity to agents such as rifampicin. Furthermore, deletion of hadC leads to a dramatic loss of virulence: an almost 4-log drop of the bacterial load in the lungs and spleens of infected immunodeficient mice. Both its unique function and importance for M. tuberculosis virulence make HadBC an attractive therapeutic target for tuberculosis drug development.


Url:
DOI: 10.1111/mmi.13266

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Hal:pasteur-02618562

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<idno type="DOI">10.1111/mmi.13266</idno>
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<title level="j">Molecular Microbiology</title>
<idno type="ISSN">0950-382X</idno>
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<date type="datePub">2016-02</date>
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<p>Understanding the molecular strategies used by Mycobacterium tuberculosis to invade and persist within the host is of paramount importance to tackle the tuberculosis pandemic. Comparative genomic surveys have revealed that hadC, encoding a subunit of the HadBC dehydratase, is mutated in the avirulent M. tuberculosis H37Ra strain. We show here that mutation or deletion of hadC affects the biosynthesis of oxygenated mycolic acids, substantially reducing their production level. Additionally, it causes the loss of atypical extra-long mycolic acids, demonstrating the involvement of HadBC in the late elongation steps of mycolic acid biosynthesis. These events have an impact on the morphotype, cording capacity and biofilm growth of the bacilli as well as on their sensitivity to agents such as rifampicin. Furthermore, deletion of hadC leads to a dramatic loss of virulence: an almost 4-log drop of the bacterial load in the lungs and spleens of infected immunodeficient mice. Both its unique function and importance for M. tuberculosis virulence make HadBC an attractive therapeutic target for tuberculosis drug development.</p>
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<title xml:lang="en">The changes in mycolic acid structures caused by hadC mutation have a dramatic effect on the virulence of Mycobacterium tuberculosis</title>
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<forename type="first">Nawel</forename>
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<forename type="first">Stevie</forename>
<surname>Jamet</surname>
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<forename type="first">Daria</forename>
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<forename type="first">Kaymeuang</forename>
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<forename type="first">Mamadou</forename>
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<forename type="first">Nathalie</forename>
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<forename type="first">Annaïk</forename>
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<forename>Alexandre</forename>
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<funder ref="#projanr-41026"></funder>
<funder>This study was supported by grants from the European Union (LSHP‐CT‐2005‐018923 and 260872), the EU‐EFPIA Innovative Medicines Initiative (grant agreement 115337), the Agence Nationale de la Recherche (FASMY, grant ANR‐14‐CE16‐0012). RB acknowledges support by the Fondation pour la Recherche Médicale (DEQ20130326471).</funder>
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<date type="whenSubmitted">2020-05-25 15:00:50</date>
<date type="whenModified">2020-05-27 15:22:05</date>
<date type="whenReleased">2020-05-26 12:49:23</date>
<date type="whenProduced">2016-02</date>
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<idno type="halRefHtml">Molecular Microbiology, Wiley, 2016, 99 (4), pp.794-807. ⟨10.1111/mmi.13266⟩</idno>
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<idno type="stamp" n="PASTEUR">Institut Pasteur</idno>
<idno type="stamp" n="UNIV-TLSE3">Université Paul Sabatier - Toulouse III</idno>
<idno type="stamp" n="CNRS">CNRS - Centre national de la recherche scientifique</idno>
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<title xml:lang="en">The changes in mycolic acid structures caused by hadC mutation have a dramatic effect on the virulence of Mycobacterium tuberculosis</title>
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<persName>
<forename type="first">Nawel</forename>
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<author role="aut">
<persName>
<forename type="first">Alexandre</forename>
<surname>Pawlik</surname>
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<email type="domain">pasteur.fr</email>
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<author role="aut">
<persName>
<forename type="first">Daria</forename>
<surname>Bottai</surname>
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<author role="aut">
<persName>
<forename type="first">Françoise</forename>
<surname>Laval</surname>
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<forename type="first">Patricia</forename>
<surname>Constant</surname>
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<persName>
<forename type="first">Anne</forename>
<surname>Lemassu</surname>
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<forename type="first">Kaymeuang</forename>
<surname>Cam</surname>
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<persName>
<forename type="first">Mamadou</forename>
<surname>Daffé</surname>
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<forename type="first">Roland</forename>
<surname>Brosch</surname>
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<forename type="first">Nathalie</forename>
<surname>Eynard</surname>
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<email type="domain">ipbs.fr</email>
<idno type="halauthorid">11854475</idno>
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<author role="crp">
<persName>
<forename type="first">Annaïk</forename>
<surname>Quémard</surname>
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<idno type="halJournalId" status="VALID">11010</idno>
<idno type="issn">0950-382X</idno>
<idno type="eissn">1365-2958</idno>
<title level="j">Molecular Microbiology</title>
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<biblScope unit="issue">4</biblScope>
<biblScope unit="pp">794-807</biblScope>
<date type="datePub">2016-02</date>
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<idno type="doi">10.1111/mmi.13266</idno>
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<langUsage>
<language ident="en">English</language>
</langUsage>
<textClass>
<classCode scheme="mesh">Animals</classCode>
<classCode scheme="mesh">Antitubercular Agents / pharmacology</classCode>
<classCode scheme="mesh">Mycobacterium tuberculosis / chemistry</classCode>
<classCode scheme="mesh">Mycobacterium tuberculosis / enzymology</classCode>
<classCode scheme="mesh">Mycobacterium tuberculosis / genetics*</classCode>
<classCode scheme="mesh">Mycobacterium tuberculosis / pathogenicity*</classCode>
<classCode scheme="mesh">Mycolic Acids / chemistry*</classCode>
<classCode scheme="mesh">Mycolic Acids / metabolism</classCode>
<classCode scheme="mesh">Spleen / microbiology</classCode>
<classCode scheme="mesh">Tuberculosis / microbiology*</classCode>
<classCode scheme="mesh">Virulence / genetics</classCode>
<classCode scheme="mesh">Bacterial Load</classCode>
<classCode scheme="mesh">Bacterial Proteins / genetics*</classCode>
<classCode scheme="mesh">Bacterial Proteins / metabolism</classCode>
<classCode scheme="mesh">Biofilms / growth & development</classCode>
<classCode scheme="mesh">Gene Deletion</classCode>
<classCode scheme="mesh">Lung / microbiology</classCode>
<classCode scheme="mesh">Mice</classCode>
<classCode scheme="mesh">Mutation</classCode>
<classCode scheme="halDomain" n="sdv.bbm.bc">Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biomolecules [q-bio.BM]</classCode>
<classCode scheme="halDomain" n="sdv.bbm.gtp">Life Sciences [q-bio]/Biochemistry, Molecular Biology/Genomics [q-bio.GN]</classCode>
<classCode scheme="halDomain" n="sdv.mhep.mi">Life Sciences [q-bio]/Human health and pathology/Infectious diseases</classCode>
<classCode scheme="halTypology" n="ART">Journal articles</classCode>
</textClass>
<abstract xml:lang="en">
<p>Understanding the molecular strategies used by Mycobacterium tuberculosis to invade and persist within the host is of paramount importance to tackle the tuberculosis pandemic. Comparative genomic surveys have revealed that hadC, encoding a subunit of the HadBC dehydratase, is mutated in the avirulent M. tuberculosis H37Ra strain. We show here that mutation or deletion of hadC affects the biosynthesis of oxygenated mycolic acids, substantially reducing their production level. Additionally, it causes the loss of atypical extra-long mycolic acids, demonstrating the involvement of HadBC in the late elongation steps of mycolic acid biosynthesis. These events have an impact on the morphotype, cording capacity and biofilm growth of the bacilli as well as on their sensitivity to agents such as rifampicin. Furthermore, deletion of hadC leads to a dramatic loss of virulence: an almost 4-log drop of the bacterial load in the lungs and spleens of infected immunodeficient mice. Both its unique function and importance for M. tuberculosis virulence make HadBC an attractive therapeutic target for tuberculosis drug development.</p>
</abstract>
<particDesc>
<org type="consortium">We wish to thank Lucie Spina and Dr. Emilie Huc for their help during some MS analyses, Wladimir Malaga for the generous gift of modified versions of plasmids pMV361 and pJV53, Fabien Le Chevalier for help with bacterial staining and Dr. Marie‐Antoinette Lanéelle for helpful discussions. The NMR data were collected on the PICT‐IbiSA facility; NMR experiments were performed on the PICT‐Genotoul platform of Toulouse funded by CNRS, Université de Toulouse‐UPS, Ibisa, European structural funds and the Midi‐Pyrénées region.</org>
</particDesc>
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