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Microevolution of Virulence-Related Genes in Helicobacter pylori Familial Infection

Helicobacter pylori, a bacterial pathogen that can infect human stomach causing gastritis, ulcers and cancer, is known to have a high degree of genome/epigenome diversity as the result of mutation and recombination. The bacteria often infect in childhood and persist for the life of the host. One of...

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Autores principales: Furuta, Yoshikazu, Konno, Mutsuko, Osaki, Takako, Yonezawa, Hideo, Ishige, Taichiro, Imai, Misaki, Shiwa, Yuh, Shibata-Hatta, Mari, Kanesaki, Yu, Yoshikawa, Hirofumi, Kamiya, Shigeru, Kobayashi, Ichizo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4433339/
https://www.ncbi.nlm.nih.gov/pubmed/25978460
http://dx.doi.org/10.1371/journal.pone.0127197
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author Furuta, Yoshikazu
Konno, Mutsuko
Osaki, Takako
Yonezawa, Hideo
Ishige, Taichiro
Imai, Misaki
Shiwa, Yuh
Shibata-Hatta, Mari
Kanesaki, Yu
Yoshikawa, Hirofumi
Kamiya, Shigeru
Kobayashi, Ichizo
author_facet Furuta, Yoshikazu
Konno, Mutsuko
Osaki, Takako
Yonezawa, Hideo
Ishige, Taichiro
Imai, Misaki
Shiwa, Yuh
Shibata-Hatta, Mari
Kanesaki, Yu
Yoshikawa, Hirofumi
Kamiya, Shigeru
Kobayashi, Ichizo
author_sort Furuta, Yoshikazu
collection PubMed
description Helicobacter pylori, a bacterial pathogen that can infect human stomach causing gastritis, ulcers and cancer, is known to have a high degree of genome/epigenome diversity as the result of mutation and recombination. The bacteria often infect in childhood and persist for the life of the host. One of the reasons of the rapid evolution of H. pylori is that it changes its genome drastically for adaptation to a new host. To investigate microevolution and adaptation of the H. pylori genome, we undertook whole genome sequencing of the same or very similar sequence type in multi-locus sequence typing (MLST) with seven genes in members of the same family consisting of parents and children in Japan. Detection of nucleotide substitutions revealed likely transmission pathways involving children. Nonsynonymous (amino acid changing) mutations were found in virulence-related genes (cag genes, vacA, hcpDX, tnfα, ggt, htrA and the collagenase gene), outer membrane protein (OMP) genes and other cell surface-related protein genes, signal transduction genes and restriction-modification genes. We reconstructed various pathways by which H. pylori can adapt to a new human host, and our results raised the possibility that the mutational changes in virulence-related genes have a role in adaptation to a child host. Changes in restriction-modification genes might remodel the methylome and transcriptome to help adaptation. This study has provided insights into H. pylori transmission and virulence and has implications for basic research as well as clinical practice.
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spelling pubmed-44333392015-05-27 Microevolution of Virulence-Related Genes in Helicobacter pylori Familial Infection Furuta, Yoshikazu Konno, Mutsuko Osaki, Takako Yonezawa, Hideo Ishige, Taichiro Imai, Misaki Shiwa, Yuh Shibata-Hatta, Mari Kanesaki, Yu Yoshikawa, Hirofumi Kamiya, Shigeru Kobayashi, Ichizo PLoS One Research Article Helicobacter pylori, a bacterial pathogen that can infect human stomach causing gastritis, ulcers and cancer, is known to have a high degree of genome/epigenome diversity as the result of mutation and recombination. The bacteria often infect in childhood and persist for the life of the host. One of the reasons of the rapid evolution of H. pylori is that it changes its genome drastically for adaptation to a new host. To investigate microevolution and adaptation of the H. pylori genome, we undertook whole genome sequencing of the same or very similar sequence type in multi-locus sequence typing (MLST) with seven genes in members of the same family consisting of parents and children in Japan. Detection of nucleotide substitutions revealed likely transmission pathways involving children. Nonsynonymous (amino acid changing) mutations were found in virulence-related genes (cag genes, vacA, hcpDX, tnfα, ggt, htrA and the collagenase gene), outer membrane protein (OMP) genes and other cell surface-related protein genes, signal transduction genes and restriction-modification genes. We reconstructed various pathways by which H. pylori can adapt to a new human host, and our results raised the possibility that the mutational changes in virulence-related genes have a role in adaptation to a child host. Changes in restriction-modification genes might remodel the methylome and transcriptome to help adaptation. This study has provided insights into H. pylori transmission and virulence and has implications for basic research as well as clinical practice. Public Library of Science 2015-05-15 /pmc/articles/PMC4433339/ /pubmed/25978460 http://dx.doi.org/10.1371/journal.pone.0127197 Text en © 2015 Furuta 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
Furuta, Yoshikazu
Konno, Mutsuko
Osaki, Takako
Yonezawa, Hideo
Ishige, Taichiro
Imai, Misaki
Shiwa, Yuh
Shibata-Hatta, Mari
Kanesaki, Yu
Yoshikawa, Hirofumi
Kamiya, Shigeru
Kobayashi, Ichizo
Microevolution of Virulence-Related Genes in Helicobacter pylori Familial Infection
title Microevolution of Virulence-Related Genes in Helicobacter pylori Familial Infection
title_full Microevolution of Virulence-Related Genes in Helicobacter pylori Familial Infection
title_fullStr Microevolution of Virulence-Related Genes in Helicobacter pylori Familial Infection
title_full_unstemmed Microevolution of Virulence-Related Genes in Helicobacter pylori Familial Infection
title_short Microevolution of Virulence-Related Genes in Helicobacter pylori Familial Infection
title_sort microevolution of virulence-related genes in helicobacter pylori familial infection
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4433339/
https://www.ncbi.nlm.nih.gov/pubmed/25978460
http://dx.doi.org/10.1371/journal.pone.0127197
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