Evolution of Helicobacter: Acquisition by Gastric Species of Two Histidine-Rich Proteins Essential for Colonization

Metal acquisition and intracellular trafficking are crucial for all cells and metal ions have been recognized as virulence determinants in bacterial pathogens. Virulence of the human gastric pathogen Helicobacter pylori is dependent on nickel, cofactor of two enzymes essential for in vivo colonizati...

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Autores principales: Vinella, Daniel, Fischer, Frédéric, Vorontsov, Egor, Gallaud, Julien, Malosse, Christian, Michel, Valérie, Cavazza, Christine, Robbe-Saule, Marie, Richaud, Pierre, Chamot-Rooke, Julia, Brochier-Armanet, Céline, De Reuse, Hilde
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4671568/
https://www.ncbi.nlm.nih.gov/pubmed/26641249
http://dx.doi.org/10.1371/journal.ppat.1005312
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author Vinella, Daniel
Fischer, Frédéric
Vorontsov, Egor
Gallaud, Julien
Malosse, Christian
Michel, Valérie
Cavazza, Christine
Robbe-Saule, Marie
Richaud, Pierre
Chamot-Rooke, Julia
Brochier-Armanet, Céline
De Reuse, Hilde
author_facet Vinella, Daniel
Fischer, Frédéric
Vorontsov, Egor
Gallaud, Julien
Malosse, Christian
Michel, Valérie
Cavazza, Christine
Robbe-Saule, Marie
Richaud, Pierre
Chamot-Rooke, Julia
Brochier-Armanet, Céline
De Reuse, Hilde
author_sort Vinella, Daniel
collection PubMed
description Metal acquisition and intracellular trafficking are crucial for all cells and metal ions have been recognized as virulence determinants in bacterial pathogens. Virulence of the human gastric pathogen Helicobacter pylori is dependent on nickel, cofactor of two enzymes essential for in vivo colonization, urease and [NiFe] hydrogenase. We found that two small paralogous nickel-binding proteins with high content in Histidine (Hpn and Hpn-2) play a central role in maintaining non-toxic intracellular nickel content and in controlling its intracellular trafficking. Measurements of metal resistance, intracellular nickel contents, urease activities and interactomic analysis were performed. We observed that Hpn acts as a nickel-sequestration protein, while Hpn-2 is not. In vivo, Hpn and Hpn-2 form homo-multimers, interact with each other, Hpn interacts with the UreA urease subunit while Hpn and Hpn-2 interact with the HypAB hydrogenase maturation proteins. In addition, Hpn-2 is directly or indirectly restricting urease activity while Hpn is required for full urease activation. Based on these data, we present a model where Hpn and Hpn-2 participate in a common pathway of controlled nickel transfer to urease. Using bioinformatics and top-down proteomics to identify the predicted proteins, we established that Hpn-2 is only expressed by H. pylori and its closely related species Helicobacter acinonychis. Hpn was detected in every gastric Helicobacter species tested and is absent from the enterohepatic Helicobacter species. Our phylogenomic analysis revealed that Hpn acquisition was concomitant with the specialization of Helicobacter to colonization of the gastric environment and the duplication at the origin of hpn-2 occurred in the common ancestor of H. pylori and H. acinonychis. Finally, Hpn and Hpn-2 were found to be required for colonization of the mouse model by H. pylori. Our data show that during evolution of the Helicobacter genus, acquisition of Hpn and Hpn-2 by gastric Helicobacter species constituted a decisive evolutionary event to allow Helicobacter to colonize the hostile gastric environment, in which no other bacteria persistently thrives. This acquisition was key for the emergence of one of the most successful bacterial pathogens, H. pylori.
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spelling pubmed-46715682015-12-10 Evolution of Helicobacter: Acquisition by Gastric Species of Two Histidine-Rich Proteins Essential for Colonization Vinella, Daniel Fischer, Frédéric Vorontsov, Egor Gallaud, Julien Malosse, Christian Michel, Valérie Cavazza, Christine Robbe-Saule, Marie Richaud, Pierre Chamot-Rooke, Julia Brochier-Armanet, Céline De Reuse, Hilde PLoS Pathog Research Article Metal acquisition and intracellular trafficking are crucial for all cells and metal ions have been recognized as virulence determinants in bacterial pathogens. Virulence of the human gastric pathogen Helicobacter pylori is dependent on nickel, cofactor of two enzymes essential for in vivo colonization, urease and [NiFe] hydrogenase. We found that two small paralogous nickel-binding proteins with high content in Histidine (Hpn and Hpn-2) play a central role in maintaining non-toxic intracellular nickel content and in controlling its intracellular trafficking. Measurements of metal resistance, intracellular nickel contents, urease activities and interactomic analysis were performed. We observed that Hpn acts as a nickel-sequestration protein, while Hpn-2 is not. In vivo, Hpn and Hpn-2 form homo-multimers, interact with each other, Hpn interacts with the UreA urease subunit while Hpn and Hpn-2 interact with the HypAB hydrogenase maturation proteins. In addition, Hpn-2 is directly or indirectly restricting urease activity while Hpn is required for full urease activation. Based on these data, we present a model where Hpn and Hpn-2 participate in a common pathway of controlled nickel transfer to urease. Using bioinformatics and top-down proteomics to identify the predicted proteins, we established that Hpn-2 is only expressed by H. pylori and its closely related species Helicobacter acinonychis. Hpn was detected in every gastric Helicobacter species tested and is absent from the enterohepatic Helicobacter species. Our phylogenomic analysis revealed that Hpn acquisition was concomitant with the specialization of Helicobacter to colonization of the gastric environment and the duplication at the origin of hpn-2 occurred in the common ancestor of H. pylori and H. acinonychis. Finally, Hpn and Hpn-2 were found to be required for colonization of the mouse model by H. pylori. Our data show that during evolution of the Helicobacter genus, acquisition of Hpn and Hpn-2 by gastric Helicobacter species constituted a decisive evolutionary event to allow Helicobacter to colonize the hostile gastric environment, in which no other bacteria persistently thrives. This acquisition was key for the emergence of one of the most successful bacterial pathogens, H. pylori. Public Library of Science 2015-12-07 /pmc/articles/PMC4671568/ /pubmed/26641249 http://dx.doi.org/10.1371/journal.ppat.1005312 Text en © 2015 Vinella 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
Vinella, Daniel
Fischer, Frédéric
Vorontsov, Egor
Gallaud, Julien
Malosse, Christian
Michel, Valérie
Cavazza, Christine
Robbe-Saule, Marie
Richaud, Pierre
Chamot-Rooke, Julia
Brochier-Armanet, Céline
De Reuse, Hilde
Evolution of Helicobacter: Acquisition by Gastric Species of Two Histidine-Rich Proteins Essential for Colonization
title Evolution of Helicobacter: Acquisition by Gastric Species of Two Histidine-Rich Proteins Essential for Colonization
title_full Evolution of Helicobacter: Acquisition by Gastric Species of Two Histidine-Rich Proteins Essential for Colonization
title_fullStr Evolution of Helicobacter: Acquisition by Gastric Species of Two Histidine-Rich Proteins Essential for Colonization
title_full_unstemmed Evolution of Helicobacter: Acquisition by Gastric Species of Two Histidine-Rich Proteins Essential for Colonization
title_short Evolution of Helicobacter: Acquisition by Gastric Species of Two Histidine-Rich Proteins Essential for Colonization
title_sort evolution of helicobacter: acquisition by gastric species of two histidine-rich proteins essential for colonization
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4671568/
https://www.ncbi.nlm.nih.gov/pubmed/26641249
http://dx.doi.org/10.1371/journal.ppat.1005312
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