(13)C Metabolic Flux Analysis Identifies an Unusual Route for Pyruvate Dissimilation in Mycobacteria which Requires Isocitrate Lyase and Carbon Dioxide Fixation

Mycobacterium tuberculosis requires the enzyme isocitrate lyase (ICL) for growth and virulence in vivo. The demonstration that M. tuberculosis also requires ICL for survival during nutrient starvation and has a role during steady state growth in a glycerol limited chemostat indicates a function for...

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Autores principales: Beste, Dany J. V., Bonde, Bhushan, Hawkins, Nathaniel, Ward, Jane L., Beale, Michael H., Noack, Stephan, Nöh, Katharina, Kruger, Nicholas J., Ratcliffe, R. George, McFadden, Johnjoe
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3141028/
https://www.ncbi.nlm.nih.gov/pubmed/21814509
http://dx.doi.org/10.1371/journal.ppat.1002091
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author Beste, Dany J. V.
Bonde, Bhushan
Hawkins, Nathaniel
Ward, Jane L.
Beale, Michael H.
Noack, Stephan
Nöh, Katharina
Kruger, Nicholas J.
Ratcliffe, R. George
McFadden, Johnjoe
author_facet Beste, Dany J. V.
Bonde, Bhushan
Hawkins, Nathaniel
Ward, Jane L.
Beale, Michael H.
Noack, Stephan
Nöh, Katharina
Kruger, Nicholas J.
Ratcliffe, R. George
McFadden, Johnjoe
author_sort Beste, Dany J. V.
collection PubMed
description Mycobacterium tuberculosis requires the enzyme isocitrate lyase (ICL) for growth and virulence in vivo. The demonstration that M. tuberculosis also requires ICL for survival during nutrient starvation and has a role during steady state growth in a glycerol limited chemostat indicates a function for this enzyme which extends beyond fat metabolism. As isocitrate lyase is a potential drug target elucidating the role of this enzyme is of importance; however, the role of isocitrate lyase has never been investigated at the level of in vivo fluxes. Here we show that deletion of one of the two icl genes impairs the replication of Mycobacterium bovis BCG at slow growth rate in a carbon limited chemostat. In order to further understand the role of isocitrate lyase in the central metabolism of mycobacteria the effect of growth rate on the in vivo fluxes was studied for the first time using (13)C-metabolic flux analysis (MFA). Tracer experiments were performed with steady state chemostat cultures of BCG or M. tuberculosis supplied with (13)C labeled glycerol or sodium bicarbonate. Through measurements of the (13)C isotopomer labeling patterns in protein-derived amino acids and enzymatic activity assays we have identified the activity of a novel pathway for pyruvate dissimilation. We named this the GAS pathway because it utilizes the Glyoxylate shunt and Anapleurotic reactions for oxidation of pyruvate, and Succinyl CoA synthetase for the generation of succinyl CoA combined with a very low flux through the succinate – oxaloacetate segment of the tricarboxylic acid cycle. We confirm that M. tuberculosis can fix carbon from CO(2) into biomass. As the human host is abundant in CO(2) this finding requires further investigation in vivo as CO(2) fixation may provide a point of vulnerability that could be targeted with novel drugs. This study also provides a platform for further studies into the metabolism of M. tuberculosis using (13)C-MFA.
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spelling pubmed-31410282011-08-03 (13)C Metabolic Flux Analysis Identifies an Unusual Route for Pyruvate Dissimilation in Mycobacteria which Requires Isocitrate Lyase and Carbon Dioxide Fixation Beste, Dany J. V. Bonde, Bhushan Hawkins, Nathaniel Ward, Jane L. Beale, Michael H. Noack, Stephan Nöh, Katharina Kruger, Nicholas J. Ratcliffe, R. George McFadden, Johnjoe PLoS Pathog Research Article Mycobacterium tuberculosis requires the enzyme isocitrate lyase (ICL) for growth and virulence in vivo. The demonstration that M. tuberculosis also requires ICL for survival during nutrient starvation and has a role during steady state growth in a glycerol limited chemostat indicates a function for this enzyme which extends beyond fat metabolism. As isocitrate lyase is a potential drug target elucidating the role of this enzyme is of importance; however, the role of isocitrate lyase has never been investigated at the level of in vivo fluxes. Here we show that deletion of one of the two icl genes impairs the replication of Mycobacterium bovis BCG at slow growth rate in a carbon limited chemostat. In order to further understand the role of isocitrate lyase in the central metabolism of mycobacteria the effect of growth rate on the in vivo fluxes was studied for the first time using (13)C-metabolic flux analysis (MFA). Tracer experiments were performed with steady state chemostat cultures of BCG or M. tuberculosis supplied with (13)C labeled glycerol or sodium bicarbonate. Through measurements of the (13)C isotopomer labeling patterns in protein-derived amino acids and enzymatic activity assays we have identified the activity of a novel pathway for pyruvate dissimilation. We named this the GAS pathway because it utilizes the Glyoxylate shunt and Anapleurotic reactions for oxidation of pyruvate, and Succinyl CoA synthetase for the generation of succinyl CoA combined with a very low flux through the succinate – oxaloacetate segment of the tricarboxylic acid cycle. We confirm that M. tuberculosis can fix carbon from CO(2) into biomass. As the human host is abundant in CO(2) this finding requires further investigation in vivo as CO(2) fixation may provide a point of vulnerability that could be targeted with novel drugs. This study also provides a platform for further studies into the metabolism of M. tuberculosis using (13)C-MFA. Public Library of Science 2011-07-21 /pmc/articles/PMC3141028/ /pubmed/21814509 http://dx.doi.org/10.1371/journal.ppat.1002091 Text en Beste 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
Beste, Dany J. V.
Bonde, Bhushan
Hawkins, Nathaniel
Ward, Jane L.
Beale, Michael H.
Noack, Stephan
Nöh, Katharina
Kruger, Nicholas J.
Ratcliffe, R. George
McFadden, Johnjoe
(13)C Metabolic Flux Analysis Identifies an Unusual Route for Pyruvate Dissimilation in Mycobacteria which Requires Isocitrate Lyase and Carbon Dioxide Fixation
title (13)C Metabolic Flux Analysis Identifies an Unusual Route for Pyruvate Dissimilation in Mycobacteria which Requires Isocitrate Lyase and Carbon Dioxide Fixation
title_full (13)C Metabolic Flux Analysis Identifies an Unusual Route for Pyruvate Dissimilation in Mycobacteria which Requires Isocitrate Lyase and Carbon Dioxide Fixation
title_fullStr (13)C Metabolic Flux Analysis Identifies an Unusual Route for Pyruvate Dissimilation in Mycobacteria which Requires Isocitrate Lyase and Carbon Dioxide Fixation
title_full_unstemmed (13)C Metabolic Flux Analysis Identifies an Unusual Route for Pyruvate Dissimilation in Mycobacteria which Requires Isocitrate Lyase and Carbon Dioxide Fixation
title_short (13)C Metabolic Flux Analysis Identifies an Unusual Route for Pyruvate Dissimilation in Mycobacteria which Requires Isocitrate Lyase and Carbon Dioxide Fixation
title_sort (13)c metabolic flux analysis identifies an unusual route for pyruvate dissimilation in mycobacteria which requires isocitrate lyase and carbon dioxide fixation
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3141028/
https://www.ncbi.nlm.nih.gov/pubmed/21814509
http://dx.doi.org/10.1371/journal.ppat.1002091
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