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Home Gastroenterology Genetic study links H. pylori susceptibility to HLA and innate immunity genes, suggests causal disease relationships

Genetic study links H. pylori susceptibility to HLA and innate immunity genes, suggests causal disease relationshipsLarge genetic study finds links between H. pylori infection susceptibility and autoimmune diseases

medRxiv Published April 2, 2026 Study authors: Kyosaka, T.; Narita, A.; Kulski, J. K.; Minn, A. K. K.; Miyake, A.; Kotsar, Y.; Hiraide, K.; Ojima, … DOI ↗ Editorial oversight: Dr. Amelia Tan, PhD · Internal Medicine & Chronic Disease

AI-generated summary of the cited source, checked by automated accuracy review. How we work

Key Takeaway
Consider genetic susceptibility to H. pylori in autoimmune disease contexts, but causal links remain unquantified.

This meta-analysis examined genetic factors for Helicobacter pylori infection susceptibility and potential causal links to diseases using genome-wide association studies (GWAS) and Mendelian randomization. The study included up to 140,863 individuals from Japanese and European cohorts, using anti-H. pylori IgG antibody titers as a surrogate marker for infection. Researchers analyzed genetic liability to H. pylori infection as the exposure, with genome-wide associations for antibody titers as the primary outcome, along with gene-based, pathway, and Mendelian randomization analyses for causal relationships with diseases.

The analysis identified significant genetic associations for H. pylori infection susceptibility in the HLA class II region (MHC) and several other genes including CCDC80, NFKBIZ, TIFA, PSCA, and TRAF3. Mendelian randomization analyses suggested that genetic liability to H. pylori infection has both positive and negative causal relationships with various diseases and traits, specifically mentioning type 1 diabetes, Hashimoto's disease, atopic dermatitis, body height, and body weight. However, the source did not provide specific effect sizes, p-values, confidence intervals, or absolute numbers for these associations or causal estimates.

No safety or tolerability data were reported as this was a genetic association study rather than an interventional trial. Key limitations were not explicitly detailed in the provided information. The study's practice relevance is restrained to providing insights for public health strategies and personalized medicine approaches, though clinical application remains speculative. The validation of the surrogate marker (anti-H. pylori IgG antibody titers) was described as correlation with clinical traits, but specific details were not provided.

Researchers conducted a large genetic study to understand why some people are more susceptible to infection with H. pylori, a common stomach bacteria. They analyzed genetic data from up to 140,863 people of Japanese and European ancestry, looking for links between a person's genes and their levels of antibodies against H. pylori.

The study found that certain genetic regions, particularly those involved in the immune system, are associated with a person's susceptibility to H. pylori. Using a statistical method called Mendelian randomization, the analysis also suggested possible genetic links between susceptibility to H. pylori and other conditions, including type 1 diabetes, Hashimoto's disease, atopic dermatitis, and body height.

It is important to be careful with these results. The study used antibody levels as a marker for infection, not direct infection tests. The suggested links to other diseases are based on genetic modeling and do not prove that H. pylori infection causes these conditions. The researchers did not report specific numbers on how strong these links are. This research provides clues for future studies on personalized medicine and public health, but it is not yet ready to change medical practice.

What this means for you:
A large genetic study found links between susceptibility to H. pylori and other conditions, but more research is needed to understand what it means.

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Study Details

Study typeMeta analysis
EvidenceLevel 1
PublishedMar 2026
View Original Abstract ↓
Helicobacter pylori (H. pylori) infects the gastric epithelium of approximately half of the global population, and is a well-known risk factor for developing gastric cancer. Despite the clinical significance of H. pylori infection, many genetic factors that contribute to susceptibility remain unidentified. While it is well-established that H. pylori infection can result in gastritis and peptic ulcers, which may progress to gastric cancer, its causal link to other diseases remains unclear. We performed the genome-wide association study (GWAS) for anti-H. pylori IgG antibody titers, which were validated as a surrogate marker for H. pylori infection by the correlation with clinical traits, followed by gene-based and pathway analyses, involving up to 140,863 individuals. This included 56,967 in the discovery phase, and 68,211 in the replication phase from Japanese cohorts, and an additional 15,685 from European populations in a cross-ancestry meta-analysis. We reveal significant associations between H. pylori infection and polymorphisms in the Human Leukocyte Antigen (HLA) class II region within the Major Histocompatibility Complex (MHC), as well as genes related to innate immunity, including CCDC80, NFKBIZ, TIFA, PSCA, and TRAF3. Mendelian randomization (MR) analysis revealed that genetic liability to H. pylori infection has both positive and negative causal relationships with a variety of diseases, including autoimmune-related diseases such as Type 1 diabetes, Hashimotos disease, atopic dermatitis, as well as traits like body height and weight. These genetic findings strongly support the notion that genetic liability to H. pylori infection influences not only gastrointestinal diseases, but also a broader spectrum of health issues, thereby providing valuable insights for public health strategies and personalized medicine approaches.
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