Genome‐wide association study of Helicobacter pylori serological status in Latin American children

Author:

Lima Iasmin Souza1,da Silva Thiago Magalhães2ORCID,Weiss Stefan34ORCID,Homuth Georg3,Lerch Markus M.4,Figueiredo Camila A.5,Alcantara‐Neves Neuza Maria5,Barreto Maurício Lima6,Marques Cintia Rodrigues1

Affiliation:

1. Multidisciplinary Institute in Health Federal University of Bahia Vitória da Conquista Brazil

2. Department of Biological Sciences State University of Southwest Bahia Jequié Brazil

3. Department of Functional Genomics, Interfaculty Institute for Genetics and Functional Genomics University Medicine Greifswald Greifswald Germany

4. Department of Medicine A University Medicine Greifswald Greifswald Germany

5. Institute of Health Sciences, Federal University of Bahia Salvador Brazil

6. Center of Data and Knowledge Integration for Health Instituto Gonçalo Muniz, Fundação Osvaldo Cruz Salvador Brazil

Abstract

AbstractBackgroundFew genome‐wide association studies (GWAS) on Helicobacter pylori infection susceptibility have been conducted for admixed populations from developing countries. Here, we performed a GWAS to identify genetic factors associated with H. pylori serostatus in a cohort of admixed children from a large Latin American urban center.MethodsA cross‐sectional study involving 1161 children from 4 to 11 years old living in poor areas of Salvador, in northeastern Brazil. Logistic regression analysis was performed to detect associations between single‐nucleotide variants (SNVs) and H. pylori seropositivity, assuming an additive genetic model. Enrichment analyses were conducted using the MAGMA v1.10 software.ResultsWe found 22 SNVs to be suggestively associated (p < 10−5) with H. pylori seropositivity. The most suggestive SNV was the rs77955022 (p = 4.83e‐07) located in an intronic region of EXOC3 at 5p15.33. The second most suggestively associated SNV was rs10914996 (p = 8.97e‐07), located in an intergenic region at 1p34.3. Furthermore, we were able to replicate three SNVs (p < 0.05) in the Study of Health in Pomerania (SHIP) cohort: the rs2339212 and rs4795970, both located at 17q12 near TMEM132E, as well as the rs6595814, an intronic variant of FBN2 at 5q23.3. The enrichment analysis indicated the participation of genes and metabolic pathways related to the regulation of the digestive system and gastric acid secretion in the risk of seropositivity for H. pylori.ConclusionsAdditional studies are required to validate these association findings in larger population samples and to get insight into the underlying physiological mechanisms.

Publisher

Wiley

Subject

Infectious Diseases,Gastroenterology,General Medicine

Reference46 articles.

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