Mycobacterium tuberculosis arrests host cycle at the G1/S transition to establish long term infection.

Mycobacterium tuberculosis arrests host cycle at the G1/S transition to establish long term infection.

Signals modulating the production of Mycobacterium tuberculosis (Mtb) virulence factors essential for establishing long-term persistent infection are unknown. The WhiB3 redox regulator is known to regulate the production of Mtb virulence factors, however the mechanisms of this modulation are unknown...

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Main Authors: Bridgette M Cumming, Md Aejazur Rahman, Dirk A Lamprecht, Kyle H Rohde, Vikram Saini, John H Adamson, David G Russell, Adrie J C Steyn
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2017-05-01
Series:PLoS Pathogens
Online Access:https://doi.org/10.1371/journal.ppat.1006389
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spelling doaj-bbe88887c055490abf4056eb3e684a742021-06-19T04:32:27ZengPublic Library of Science (PLoS)PLoS Pathogens1553-73661553-73742017-05-01135e100638910.1371/journal.ppat.1006389Mycobacterium tuberculosis arrests host cycle at the G1/S transition to establish long term infection.Bridgette M CummingMd Aejazur RahmanDirk A LamprechtKyle H RohdeVikram SainiJohn H AdamsonDavid G RussellAdrie J C SteynSignals modulating the production of Mycobacterium tuberculosis (Mtb) virulence factors essential for establishing long-term persistent infection are unknown. The WhiB3 redox regulator is known to regulate the production of Mtb virulence factors, however the mechanisms of this modulation are unknown. To advance our understanding of the mechanisms involved in WhiB3 regulation, we performed Mtb in vitro, intraphagosomal and infected host expression analyses. Our Mtb expression analyses in conjunction with extracellular flux analyses demonstrated that WhiB3 maintains bioenergetic homeostasis in response to available carbon sources found in vivo to establish Mtb infection. Our infected host expression analysis indicated that WhiB3 is involved in regulation of the host cell cycle. Detailed cell-cycle analysis revealed that Mtb infection inhibited the macrophage G1/S transition, and polyketides under WhiB3 control arrested the macrophages in the G0-G1 phase. Notably, infection with the Mtb whiB3 mutant or polyketide mutants had little effect on the macrophage cell cycle and emulated the uninfected cells. This suggests that polyketides regulated by Mtb WhiB3 are responsible for the cell cycle arrest observed in macrophages infected with the wild type Mtb. Thus, our findings demonstrate that Mtb WhiB3 maintains bioenergetic homeostasis to produce polyketide and lipid cyclomodulins that target the host cell cycle. This is a new mechanism whereby Mtb modulates the immune system by altering the host cell cycle to promote long-term persistence. This new knowledge could serve as the foundation for new host-directed therapeutic discovery efforts that target the host cell cycle.https://doi.org/10.1371/journal.ppat.1006389
collection DOAJ
language English
format Article
sources DOAJ
author Bridgette M Cumming
Md Aejazur Rahman
Dirk A Lamprecht
Kyle H Rohde
Vikram Saini
John H Adamson
David G Russell
Adrie J C Steyn
spellingShingle Bridgette M Cumming
Md Aejazur Rahman
Dirk A Lamprecht
Kyle H Rohde
Vikram Saini
John H Adamson
David G Russell
Adrie J C Steyn
Mycobacterium tuberculosis arrests host cycle at the G1/S transition to establish long term infection.
PLoS Pathogens
author_facet Bridgette M Cumming
Md Aejazur Rahman
Dirk A Lamprecht
Kyle H Rohde
Vikram Saini
John H Adamson
David G Russell
Adrie J C Steyn
author_sort Bridgette M Cumming
title Mycobacterium tuberculosis arrests host cycle at the G1/S transition to establish long term infection.
title_short Mycobacterium tuberculosis arrests host cycle at the G1/S transition to establish long term infection.
title_full Mycobacterium tuberculosis arrests host cycle at the G1/S transition to establish long term infection.
title_fullStr Mycobacterium tuberculosis arrests host cycle at the G1/S transition to establish long term infection.
title_full_unstemmed Mycobacterium tuberculosis arrests host cycle at the G1/S transition to establish long term infection.
title_sort mycobacterium tuberculosis arrests host cycle at the g1/s transition to establish long term infection.
publisher Public Library of Science (PLoS)
series PLoS Pathogens
issn 1553-7366
1553-7374
publishDate 2017-05-01
description Signals modulating the production of Mycobacterium tuberculosis (Mtb) virulence factors essential for establishing long-term persistent infection are unknown. The WhiB3 redox regulator is known to regulate the production of Mtb virulence factors, however the mechanisms of this modulation are unknown. To advance our understanding of the mechanisms involved in WhiB3 regulation, we performed Mtb in vitro, intraphagosomal and infected host expression analyses. Our Mtb expression analyses in conjunction with extracellular flux analyses demonstrated that WhiB3 maintains bioenergetic homeostasis in response to available carbon sources found in vivo to establish Mtb infection. Our infected host expression analysis indicated that WhiB3 is involved in regulation of the host cell cycle. Detailed cell-cycle analysis revealed that Mtb infection inhibited the macrophage G1/S transition, and polyketides under WhiB3 control arrested the macrophages in the G0-G1 phase. Notably, infection with the Mtb whiB3 mutant or polyketide mutants had little effect on the macrophage cell cycle and emulated the uninfected cells. This suggests that polyketides regulated by Mtb WhiB3 are responsible for the cell cycle arrest observed in macrophages infected with the wild type Mtb. Thus, our findings demonstrate that Mtb WhiB3 maintains bioenergetic homeostasis to produce polyketide and lipid cyclomodulins that target the host cell cycle. This is a new mechanism whereby Mtb modulates the immune system by altering the host cell cycle to promote long-term persistence. This new knowledge could serve as the foundation for new host-directed therapeutic discovery efforts that target the host cell cycle.
url https://doi.org/10.1371/journal.ppat.1006389
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