<i>Helicobacter pylori</i>
            Infection Targets Adherens Junction Regulatory Proteins and Results in Increased Rates of Migration in Human Gastric Epithelial Cells

Conlin, Victoria S.; Curtis, Susan B.; Zhao, Ying; Moore, Edwin D.W.; Smith, Valerie C.; Meloche, R. M.; Finlay, B. Brett; Buchan, A.M.J.

doi:10.1128/iai.72.9.5181-5192.2004

Cited by 52 publications

(41 citation statements)

References 34 publications

(36 reference statements)

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“…However, it is becoming clear that H. pylori can also have more-direct effects on the AJ. Indeed, in vitro H. pylori can rapidly disrupt the integrity of the AJ without affecting E-cadherin and ␤-catenin expression (10,45). Our results also indicate that H. pylori disrupts AJs at an intracellular level via activation of the host cell protease calpain.…”

Section: Discussionsupporting

confidence: 58%

“…␤-Catenin is aberrantly activated in gastric cancer precursor lesions (40), suggesting that AJ modifications precede adenocarcinoma development. Studies using a gerbil-adapted strain of H. pylori in an in vivo model of disease have shown that ␤-catenin activation plays a role in gastric tumorigenesis (14), and AJ disruption has been linked to increased cell migration (10,45) and cellular transdifferentiation from a gastric to an intestinal phenotype in vitro (29). However, despite advances in this area, the mechanisms whereby persistent H. pylori infection alters gastric epithelial AJs remain incompletely understood.…”

Section: Discussionmentioning

confidence: 99%

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Helicobacter pylori Activates Calpain via Toll-Like Receptor 2 To Disrupt Adherens Junctions in Human Gastric Epithelial Cells

et al. 2011

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Helicobacter pylori is a risk factor for the development of gastritis, gastroduodenal ulcers, and gastric adenocarcinoma. H. pylori-induced disruption of epithelial adherens junctions (AJs) is thought to promote the development of severe disease; however, the mechanisms whereby H. pylori alters AJ structure remain incompletely understood. The present study demonstrates that H. pylori infection in human patients is associated with elevated serum levels of an 80-kDa E-cadherin ectodomain, whose presence is independent of the presence of serum antibodies against CagA. In vitro, a heat-labile H. pylori surface component activates the host protease calpain in human gastric MKN45 cells independently of the virulence factors CagA and VacA. H. pylori-induced calpain activation results in cleavage of E-cadherin to produce a 100-kDa truncated form and induce relocalization of E-cadherin and ␤-catenin. Stimulation of MKN45 cells with the toll-like receptor 2 (TLR2) ligand P3C activated calpain and disrupted E-cadherin and ␤-catenin in a pattern similar to that induced by H. pylori. Inhibition of TLR2 prevented H. pylori-induced calpain activation and AJ disassembly. Together, these findings identify a novel pathway whereby H. pylori activates calpain via TLR2 to disrupt gastric epithelial AJ structure.

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Section: Discussionsupporting

confidence: 58%

Section: Discussionmentioning

confidence: 99%

Helicobacter pylori Activates Calpain via Toll-Like Receptor 2 To Disrupt Adherens Junctions in Human Gastric Epithelial Cells

et al. 2011

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“…In a recent study, normal and gastric cancer cells were infected with H. pylori and differential expression of genes and proteins measured (133). H. pylori infection consistently up-regulated Annexin II, S100A7 and the Rho-GTP protein and significantly altered the location of E-cadherin from plasma membrane to intra-cellular vesicles (133).. Based on the results, the authors suggested that H. pylori infection results in destabilizing epithelial cell adherence via the up-regulation of specific membrane associated proteins such as Annexin II and S100A7, which may play a role in increasing the risk of gastric carcinogenesis (133).…”

Section: A Role Of Anx-ii In Gi Cancersmentioning

confidence: 99%

Role of Annexin-II in GI cancers: Interaction with gastrins/progastrins

Singh

2007

Cancer Letters

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The role of the gastrin peptide hormones (G17, G34) and their precursors (progastrins, PG; glyextended gastrin, G-gly), in gastrointestinal (GI) cancers has been extensively reviewed in recent years (1-3). A possible important role of progastrin peptides in colon carcinogenesis has become evident from experiments with transgenic mouse models (1;3). It is now known that growth stimulatory and co-carcinogenic effects of gastrin/PG peptides are mediated by both proliferative and anti-apoptotic effects of the peptides on target cells (4;5). Several receptor subtypes have been described that mediate growth effects of gastrin peptides (1;2). Recently, we identified Annexin II as a high affinity binding protein for gastrin/PG peptides (6). Importantly, the expression of Annexin II was required for mediating growth stimulatory effects of gastrin and PG peptides on intestinal epithelial and colon cancer cells (6), suggesting that Annexin II may represent the elusive novel receptor for gastrin/PG peptides. The importance of this finding in relation to the structure and function of Annexin II, especially in GI cancers, is described below. Since this surprising finding represents a new front in our understanding of the mechanisms involved in mediating growth effects of gastrin/PG peptides in GI cancers, our current understanding of the role of Annexin II in proliferation and metastasis of cancer cells is additionally reviewed.

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“…AGS (ATCC CRL-1739 [56]) or NCI-N87 (CRL-5822 [13]) human gastric epithelial cells were cultured according to the ATCC guidelines in Dulbecco's modified Eagle's medium (DMEM). To assay cytokine and chemokine production, cells were seeded at 2 ϫ 10 5 cells/well in 24-well tissue culture plates and incubated for 24 h. After this time, H. pylori, cultured for 24 h on CHBA, was scraped from a plate and resuspended in sterile DMEM or phosphate-buffered saline.…”

Section: Methodsmentioning

confidence: 99%

Helicobacter pyloriChemotaxis Modulates Inflammation and Bacterium-Gastric Epithelium Interactions in Infected Mice

et al. 2007

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The ulcer-causing pathogen Helicobacter pylori uses directed motility, or chemotaxis, to both colonize the stomach and promote disease development. Previous work showed that mutants lacking the TlpB chemoreceptor, one of the receptors predicted to drive chemotaxis, led to less inflammation in the gerbil stomach than did the wild type. Here we expanded these findings and examined the effects on inflammation of completely nonchemotactic mutants and mutants lacking each chemoreceptor. Of note, all mutants colonized mice to the same levels as did wild-type H. pylori. Infection by completely nonchemotactic mutants (cheW or cheY) resulted in significantly less inflammation after both 3 and 6 months of infection. Mutants lacking either the TlpA or TlpB H. pylori chemotaxis receptors also had alterations in inflammation severity, while mutants lacking either of the other two chemoreceptors (TlpC and HylB) behaved like the wild type. Fully nonchemotactic and chemoreceptor mutants adhered to cultured gastric epithelial cells and caused cellular release of the chemokine interleukin-8 in vitro similar to the release caused by the wild type. The situation appeared to be different in the stomach. Using silver-stained histological sections, we found that nonchemotactic cheY or cheW mutants were less likely than the wild type to be intimately associated with the cells of the gastric mucosa, although there was not a strict correlation between intimate association and inflammation. Because others have shown that in vivo adherence promotes inflammation, we propose a model in which H. pylori uses chemotaxis to guide it to a productive interaction with the stomach epithelium.

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Helicobacter pylori Infection Targets Adherens Junction Regulatory Proteins and Results in Increased Rates of Migration in Human Gastric Epithelial Cells

Cited by 52 publications

References 34 publications

Helicobacter pylori Activates Calpain via Toll-Like Receptor 2 To Disrupt Adherens Junctions in Human Gastric Epithelial Cells

Helicobacter pylori Activates Calpain via Toll-Like Receptor 2 To Disrupt Adherens Junctions in Human Gastric Epithelial Cells

Role of Annexin-II in GI cancers: Interaction with gastrins/progastrins

Helicobacter pyloriChemotaxis Modulates Inflammation and Bacterium-Gastric Epithelium Interactions in Infected Mice

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