American Society for Microbiology
Infection and Immunity
volume 93 issue 4

Helicobacter pylori CagA and Cag type IV secretion system activity have key roles in triggering gastric transcriptional and proteomic alterations

Jennifer H B Shuman 1
Aung Soe Lin 1
Mandy D. Westland 1
Kaeli N. Bryant 1
Gabrielle E. Fortier 1
M. Blanca Piazuelo 2
Michelle L Reyzer 3, 4
Audra M Judd 3, 4
Tina Tsui 3
W. Hayes McDonald 3
Mark S. McClain 2, 5
Kevin L. Schey 3, 4
Holly Algood 1, 2, 5, 6
Timothy L. Cover 1, 2, 5, 6
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Veterans Affairs Tennessee Valley Healthcare System
Publication typeJournal Article
Publication date2025-04-08
American Society for Microbiology
scimago Q1
wos Q2
SJR1.054
CiteScore5.9
Impact factor2.8
ISSN00199567, 10985522
Abstract
ABSTRACT

Colonization of the human stomach with cag pathogenicity island (PAI)-positive Helicobacter pylori strains is associated with increased gastric cancer risk compared to colonization with cag PAI-negative strains. To evaluate the contributions of the Cag type IV secretion system (T4SS) and CagA (a secreted bacterial oncoprotein) to gastric molecular alterations relevant for carcinogenesis, we infected Mongolian gerbils with a Cag T4SS-positive wild-type (WT) H. pylori strain, one of two Cag T4SS mutant strains (∆ cagT or ∆ cagY ), or a ∆ cagA mutant for 12 weeks. Histologic staining revealed a biphasic distribution of gastric inflammation severity in WT-infected animals and minimal inflammation in animals infected with mutant strains. Atrophic gastritis (a premalignant condition), dysplasia, and gastric adenocarcinoma were only detected in WT-infected animals with high inflammation scores. Transcriptional profiling, liquid chromatography-tandem mass spectrometry analysis of micro-extracted tryptic peptides, and imaging mass spectrometry revealed more than a thousand molecular alterations in gastric tissues from WT-infected animals with high inflammation scores compared to uninfected tissues and few alterations in tissues from other groups of infected animals. Proteins with altered abundance in animals with severe Cag T4SS-induced inflammation mapped to multiple pathways, including the complement/coagulation cascade and proteasome pathway. Proteins exhibiting markedly increased abundance in tissues from H. pylori -infected animals with severe inflammation included calprotectin components, proteins involved in proteasome activation, polymeric immunoglobulin receptor (PIGR), interferon-inducible guanylate-binding protein (GBP2), lactoferrin, lysozyme, superoxide dismutase, and eosinophil peroxidase. These results demonstrate key roles for CagA and Cag T4SS activity in promoting gastric mucosal inflammation, transcriptional alterations, and proteomic alterations relevant to gastric carcinogenesis.

IMPORTANCE

Helicobacter pylori colonizes the stomachs of about half of humans worldwide, and its presence is the primary risk factor for the development of stomach cancer. H. pylori strains isolated from humans can be broadly classified into two groups based on whether they contain a chromosomal cag pathogenicity island, which encodes a secreted effector protein (CagA) and components of a type IV secretion system (T4SS). In experiments using a Mongolian gerbil model, we found that severe gastric inflammation and gastric transcriptional and proteomic alterations related to gastric cancer development were detected only in animals infected with a wild-type H. pylori strain containing CagA and an intact Cag T4SS . Mutant strains lacking CagA or Cag T4SS activity successfully colonized the stomach without inducing detectable pathologic host responses. These findings illustrate two different patterns of H. pylori -host interaction.

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Shuman J. H. B. et al. Helicobacter pylori CagA and Cag type IV secretion system activity have key roles in triggering gastric transcriptional and proteomic alterations // Infection and Immunity. 2025. Vol. 93. No. 4.
GOST all authors (up to 50) Copy
Shuman J. H. B., Lin A. S., Westland M. D., Bryant K. N., Fortier G. E., Piazuelo M. B., Reyzer M. L., Judd A. M., Tsui T., McDonald W. H., McClain M. S., Schey K. L., Algood H., Cover T. L. Helicobacter pylori CagA and Cag type IV secretion system activity have key roles in triggering gastric transcriptional and proteomic alterations // Infection and Immunity. 2025. Vol. 93. No. 4.
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TY - JOUR
DO - 10.1128/iai.00595-24
UR - https://journals.asm.org/doi/10.1128/iai.00595-24
TI - Helicobacter pylori CagA and Cag type IV secretion system activity have key roles in triggering gastric transcriptional and proteomic alterations
T2 - Infection and Immunity
AU - Shuman, Jennifer H B
AU - Lin, Aung Soe
AU - Westland, Mandy D.
AU - Bryant, Kaeli N.
AU - Fortier, Gabrielle E.
AU - Piazuelo, M. Blanca
AU - Reyzer, Michelle L
AU - Judd, Audra M
AU - Tsui, Tina
AU - McDonald, W. Hayes
AU - McClain, Mark S.
AU - Schey, Kevin L.
AU - Algood, Holly
AU - Cover, Timothy L.
PY - 2025
DA - 2025/04/08
PB - American Society for Microbiology
IS - 4
VL - 93
SN - 0019-9567
SN - 1098-5522
ER -
BibTex
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BibTex (up to 50 authors) Copy
@article{2025_Shuman,
author = {Jennifer H B Shuman and Aung Soe Lin and Mandy D. Westland and Kaeli N. Bryant and Gabrielle E. Fortier and M. Blanca Piazuelo and Michelle L Reyzer and Audra M Judd and Tina Tsui and W. Hayes McDonald and Mark S. McClain and Kevin L. Schey and Holly Algood and Timothy L. Cover},
title = {Helicobacter pylori CagA and Cag type IV secretion system activity have key roles in triggering gastric transcriptional and proteomic alterations},
journal = {Infection and Immunity},
year = {2025},
volume = {93},
publisher = {American Society for Microbiology},
month = {apr},
url = {https://journals.asm.org/doi/10.1128/iai.00595-24},
number = {4},
doi = {10.1128/iai.00595-24}
}