Abstract

Helicobacter pylori and its sequelae of peptic ulcer disease and gastric cancer remain substantial health concerns for our Veterans. H. pylori infects half of the world's population, causes peptic ulcers in 10% and gastric cancer in 1-3% of those infected, and it is the third leading cause of cancer death worldwide. American Servicemen/women are exposed to H. pylori in regions where infection rates are very high and strains associated with high cancer risk are prevalent. For disease progression, chronic inflammation and epithelial events are necessary. We have identified mechanisms underlying inflammation and carcinogenesis. This includes induction of futile, dysregulated, innate and adaptive immune responses leading to inflammation; and molecular signatures of carcinogenesis. Antibiotics do not uniformly eradicate the infection, and do not reduce cancer risk if preneoplastic lesions have developed, thus there is a great need to establish strategies for prevention of disease progression. Risk for cancer remains a major issue in Veterans particularly those that are Hispanic, whose numbers are increasing. We have implicated the biogenic polyamines (putrescine, spermidine, and spermine), derived from the rate-limiting enzyme ornithine decarboxylase (ODC), in gastric inflammation and carcinogenesis, and shown that DNA damage is due to induction of spermine oxidase (SMOX), which is downstream of ODC and generates H2O2. We have reported that H. pylori strains from Veterans induced SMOX expression and oxidative DNA damage in vitro and in tissues. Our goal is to find new strategies for intervention. Polyamine generation is downstream of the amino acid L-arginine (L-Arg). We have shown that cellular uptake of L-Arg is regulated by cationic amino acid transporter 2 (CAT2; solute carrier family 7, member 2, or SLC7A2), and is induced by H. pylori infection. We have key new evidence that SLC7A2 is a key player in gastric epithelial cells, and that it is upregulated in gastric cancer. We have recently implicated the cytoskeletal protein Talin-1 in the pathogenesis of infectious colitis, and now show that it may link L-Arg and H. pylori-induced immune dysregulation. Talin-1 is upregulated in macrophages with H. pylori infection, including in gastric cancer. We will further pursue targets for intervention in the L-Arg/polyamine pathway by investigating SMOX and oxidative stress derived from epithelial cells vs. macrophages, and by utilizing a novel inhibitor of SMOX. We hypothesize that arginine availability and metabolism, including polyamine synthesis and oxidation, are key events that lead to H. pylori-associated gastric inflammation, injury, DNA damage, and risk for carcinogenesis.
Our specific aims are: 1) To determine the myeloid and epithelial components related to SLC7A2-mediated effects on gastric inflammation and damage. We will utilize H. pylori strains and tissues from Veterans and from subjects at high and low cancer risk, and study cell-specific responses: A) Induction and role of SLC7A2 in gastric epithelial cells, gastric organoids, and gastric tissues; B) Bone marrow chimeras using Slc7a2-/- mice. 2) To determine if Talin-1 is a key regulator of responses to H. pylori infection. We will assess Talin-1 expression and function in vitro and in vivo: A) Talin-1 expression and function in epithelial cells and macrophages, and effect of L-Arg availability; B) Role of Talin-1 n vivo, including studies in human tissues from Veterans, in mice with altered L-Arg availability and with myeloid-specific deletion of Tln1. 3) To determine effects of epithelial cells and immune cells in SMOX- mediated gastric inflammation and carcinogenesis. We will utilize mouse and gerbil models and assess: A) Effects of bone marrow chimeras using Smox-/- mice; B) Effect of a novel SMOX inhibitor on inflammation and carcinogenesis in mice and gerbils. These studies will have a major impact on our understanding of H. pylori immunopathogenesis and progression to gastric carcinogenesis, and will lead to new approaches for risk assessment and treatment.

Public Health Relevance

The gastric bacterial pathogen Helicobacter pylori infects half of the world's population. It causes peptic ulcer disease in 10% and gastric carcinoma in 1-3% of those infected. Stomach cancer is the third leading cause of cancer-related deaths worldwide. American servicemen/women are frequently exposed to H. pylori at sites of duty where prevalence of this infection is high, and they are at risk of acquiring virulent strains that are harder to treat and associated with carcinogenesis. Antibiotics are not useful if precancerous lesions have occurred. Our studies will investigate mechanisms by which H. pylori causes a futile inflammatory response that leads to ongoing tissue injury and DNA damage that can progress to cancer. We will focus on how alterations in the metabolism of the amino acid arginine leads to pathologic events, including immune dysfunction and aberrant epithelial cell responses. Our studies will lead to new understanding of H. pylori-induced disease and rational strategies for intervention, including future chemopreventive therapies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Veterans Affairs (VA)
Type
Non-HHS Research Projects (I01)
Project #
5I01BX001453-06
Application #
9269883
Study Section
Gastroenterology (GAST)
Project Start
2012-04-01
Project End
2020-03-31
Budget Start
2017-04-01
Budget End
2018-03-31
Support Year
6
Fiscal Year
2017
Total Cost
Indirect Cost

  Institution

Name
Veterans Health Administration
Department
Type
DUNS #
156385783
City
Nashville
State
TN
Country
United States
Zip Code
37212

  Publications

Singh, Kshipra; Coburn, Lori A; Asim, Mohammad et al. (2018) Ornithine Decarboxylase in Macrophages Exacerbates Colitis and Promotes Colitis-Associated Colon Carcinogenesis by Impairing M1 Immune Responses. Cancer Res 78:4303-4315
Gobert, Alain P; Al-Greene, Nicole T; Singh, Kshipra et al. (2018) Distinct Immunomodulatory Effects of Spermine Oxidase in Colitis Induced by Epithelial Injury or Infection. Front Immunol 9:1242
Choksi, Yash A; Reddy, Vishruth K; Singh, Kshipra et al. (2018) BVES is required for maintenance of colonic epithelial integrity in experimental colitis by modifying intestinal permeability. Mucosal Immunol 11:1363-1374
Scoville, Elizabeth A; Allaman, Margaret M; Brown, Caroline T et al. (2018) Alterations in Lipid, Amino Acid, and Energy Metabolism Distinguish Crohn's Disease from Ulcerative Colitis and Control Subjects by Serum Metabolomic Profiling. Metabolomics 14:
Sierra, Johanna C; Asim, Mohammad; Verriere, Thomas G et al. (2018) Epidermal growth factor receptor inhibition downregulates Helicobacter pylori-induced epithelial inflammatory responses, DNA damage and gastric carcinogenesis. Gut 67:1247-1260
Means, Anna L; Freeman, Tanner J; Zhu, Jing et al. (2018) Epithelial Smad4 Deletion Up-Regulates Inflammation and Promotes Inflammation-Associated Cancer. Cell Mol Gastroenterol Hepatol 6:257-276
Blosse, Alice; Lehours, Philippe; Wilson, Keith T et al. (2018) Helicobacter: Inflammation, immunology, and vaccines. Helicobacter 23 Suppl 1:e12517
Coburn, Lori A; Singh, Kshipra; Asim, Mohammad et al. (2018) Loss of solute carrier family 7 member 2 exacerbates inflammation-associated colon tumorigenesis. Oncogene :
Noto, Jennifer M; Chopra, Abha; Loh, John T et al. (2018) Pan-genomic analyses identify key Helicobacter pylori pathogenic loci modified by carcinogenic host microenvironments. Gut 67:1793-1804
Mera, Robertino M; Bravo, Luis E; Camargo, M Constanza et al. (2018) Dynamics of Helicobacter pylori infection as a determinant of progression of gastric precancerous lesions: 16-year follow-up of an eradication trial. Gut 67:1239-1246

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