Disruption of an M. tuberculosis Membrane Protein Causes a Magnesium-dependent Cell Division Defect and Failure to Persist in Mice

The identification of Mycobacterium tuberculosis genes necessary for persistence in vivo provides insight into bacterial biology as well as host defense strategies. We show that disruption of M. tuberculosis membrane protein PerM (Rv0955) resulted in an IFN-γ-dependent persistence defect in chronic...

Descripción completa

Detalles Bibliográficos
Autores principales: Goodsmith, Nichole, Guo, Xinzheng V., Vandal, Omar H., Vaubourgeix, Julien, Wang, Ruojun, Botella, Hélène, Song, Shuang, Bhatt, Kamlesh, Liba, Amir, Salgame, Padmini, Schnappinger, Dirk, Ehrt, Sabine
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4450064/
https://www.ncbi.nlm.nih.gov/pubmed/25658098
http://dx.doi.org/10.1371/journal.ppat.1004645
_version_ 1782373961555771392
author Goodsmith, Nichole
Guo, Xinzheng V.
Vandal, Omar H.
Vaubourgeix, Julien
Wang, Ruojun
Botella, Hélène
Song, Shuang
Bhatt, Kamlesh
Liba, Amir
Salgame, Padmini
Schnappinger, Dirk
Ehrt, Sabine
author_facet Goodsmith, Nichole
Guo, Xinzheng V.
Vandal, Omar H.
Vaubourgeix, Julien
Wang, Ruojun
Botella, Hélène
Song, Shuang
Bhatt, Kamlesh
Liba, Amir
Salgame, Padmini
Schnappinger, Dirk
Ehrt, Sabine
author_sort Goodsmith, Nichole
collection PubMed
description The identification of Mycobacterium tuberculosis genes necessary for persistence in vivo provides insight into bacterial biology as well as host defense strategies. We show that disruption of M. tuberculosis membrane protein PerM (Rv0955) resulted in an IFN-γ-dependent persistence defect in chronic mouse infection despite the mutant’s near normal growth during acute infection. The perM mutant required increased magnesium for replication and survival; incubation in low magnesium media resulted in cell elongation and lysis. Transcriptome analysis of the perM mutant grown in reduced magnesium revealed upregulation of cell division and cell wall biosynthesis genes, and live cell imaging showed PerM accumulation at the division septa in M. smegmatis. The mutant was acutely sensitive to β-lactam antibiotics, including specific inhibitors of cell division-associated peptidoglycan transpeptidase FtsI. Together, these data implicate PerM as a novel player in mycobacterial cell division and pathogenesis, and are consistent with the hypothesis that immune activation deprives M. tuberculosis of magnesium.
format Online
Article
Text
id pubmed-4450064
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-44500642015-06-23 Disruption of an M. tuberculosis Membrane Protein Causes a Magnesium-dependent Cell Division Defect and Failure to Persist in Mice Goodsmith, Nichole Guo, Xinzheng V. Vandal, Omar H. Vaubourgeix, Julien Wang, Ruojun Botella, Hélène Song, Shuang Bhatt, Kamlesh Liba, Amir Salgame, Padmini Schnappinger, Dirk Ehrt, Sabine PLoS Pathog Research Article The identification of Mycobacterium tuberculosis genes necessary for persistence in vivo provides insight into bacterial biology as well as host defense strategies. We show that disruption of M. tuberculosis membrane protein PerM (Rv0955) resulted in an IFN-γ-dependent persistence defect in chronic mouse infection despite the mutant’s near normal growth during acute infection. The perM mutant required increased magnesium for replication and survival; incubation in low magnesium media resulted in cell elongation and lysis. Transcriptome analysis of the perM mutant grown in reduced magnesium revealed upregulation of cell division and cell wall biosynthesis genes, and live cell imaging showed PerM accumulation at the division septa in M. smegmatis. The mutant was acutely sensitive to β-lactam antibiotics, including specific inhibitors of cell division-associated peptidoglycan transpeptidase FtsI. Together, these data implicate PerM as a novel player in mycobacterial cell division and pathogenesis, and are consistent with the hypothesis that immune activation deprives M. tuberculosis of magnesium. Public Library of Science 2015-02-06 /pmc/articles/PMC4450064/ /pubmed/25658098 http://dx.doi.org/10.1371/journal.ppat.1004645 Text en © 2015 Goodsmith 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
Goodsmith, Nichole
Guo, Xinzheng V.
Vandal, Omar H.
Vaubourgeix, Julien
Wang, Ruojun
Botella, Hélène
Song, Shuang
Bhatt, Kamlesh
Liba, Amir
Salgame, Padmini
Schnappinger, Dirk
Ehrt, Sabine
Disruption of an M. tuberculosis Membrane Protein Causes a Magnesium-dependent Cell Division Defect and Failure to Persist in Mice
title Disruption of an M. tuberculosis Membrane Protein Causes a Magnesium-dependent Cell Division Defect and Failure to Persist in Mice
title_full Disruption of an M. tuberculosis Membrane Protein Causes a Magnesium-dependent Cell Division Defect and Failure to Persist in Mice
title_fullStr Disruption of an M. tuberculosis Membrane Protein Causes a Magnesium-dependent Cell Division Defect and Failure to Persist in Mice
title_full_unstemmed Disruption of an M. tuberculosis Membrane Protein Causes a Magnesium-dependent Cell Division Defect and Failure to Persist in Mice
title_short Disruption of an M. tuberculosis Membrane Protein Causes a Magnesium-dependent Cell Division Defect and Failure to Persist in Mice
title_sort disruption of an m. tuberculosis membrane protein causes a magnesium-dependent cell division defect and failure to persist in mice
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4450064/
https://www.ncbi.nlm.nih.gov/pubmed/25658098
http://dx.doi.org/10.1371/journal.ppat.1004645
work_keys_str_mv AT goodsmithnichole disruptionofanmtuberculosismembraneproteincausesamagnesiumdependentcelldivisiondefectandfailuretopersistinmice
AT guoxinzhengv disruptionofanmtuberculosismembraneproteincausesamagnesiumdependentcelldivisiondefectandfailuretopersistinmice
AT vandalomarh disruptionofanmtuberculosismembraneproteincausesamagnesiumdependentcelldivisiondefectandfailuretopersistinmice
AT vaubourgeixjulien disruptionofanmtuberculosismembraneproteincausesamagnesiumdependentcelldivisiondefectandfailuretopersistinmice
AT wangruojun disruptionofanmtuberculosismembraneproteincausesamagnesiumdependentcelldivisiondefectandfailuretopersistinmice
AT botellahelene disruptionofanmtuberculosismembraneproteincausesamagnesiumdependentcelldivisiondefectandfailuretopersistinmice
AT songshuang disruptionofanmtuberculosismembraneproteincausesamagnesiumdependentcelldivisiondefectandfailuretopersistinmice
AT bhattkamlesh disruptionofanmtuberculosismembraneproteincausesamagnesiumdependentcelldivisiondefectandfailuretopersistinmice
AT libaamir disruptionofanmtuberculosismembraneproteincausesamagnesiumdependentcelldivisiondefectandfailuretopersistinmice
AT salgamepadmini disruptionofanmtuberculosismembraneproteincausesamagnesiumdependentcelldivisiondefectandfailuretopersistinmice
AT schnappingerdirk disruptionofanmtuberculosismembraneproteincausesamagnesiumdependentcelldivisiondefectandfailuretopersistinmice
AT ehrtsabine disruptionofanmtuberculosismembraneproteincausesamagnesiumdependentcelldivisiondefectandfailuretopersistinmice

Ejemplares similares