Genome-wide DNA methylation profiling identifies epigenetic signatures of gastric cardiac intestinal metaplasia

Runhua Lin; Chenxi Li; Zhaohui Liu; Ruinuan Wu; Jianghong Lu

doi:10.1186/s12967-020-02453-2

Genome-wide DNA methylation profiling identifies epigenetic signatures of gastric cardiac intestinal metaplasia

J Transl Med. 2020 Jul 31;18(1):292. doi: 10.1186/s12967-020-02453-2.

Authors

Runhua Lin¹, Chenxi Li², Zhaohui Liu³, Ruinuan Wu³, Jianghong Lu²

Affiliations

¹ Department of Pathology, Shantou University Medical College, Shantou, 515041, China. rhlin2010@163.com.
² Department of Pathology, Shantou University Medical College, Shantou, 515041, China.
³ The Second People's Hospital of Shenzhen/The First Affiliated Hospital of Shenzhen University, Shenzhen, China.

Abstract

Background: Measuring the DNA methylome may offer the opportunity to identify novel disease biomarkers and insights into disease mechanisms. Although aberrant DNA methylation has been investigated in many human cancers and precancerous lesions, the DNA methylation landscape of gastric cardiac intestinal metaplasia (IM) remains unknown. Therefore, we aimed to investigate the genome-wide DNA methylation landscape and to search for potential epigenetic biomarkers of gastric cardiac IM.

Methods: Histopathologic profiling was performed on a total of 118 gastric cardiac biopsies from cancer-free individuals. Genome-wide DNA methylation analysis was performed on 11 gastric cardiac mucosal biopsies (IM = 7; normal = 4) using Illumina 850K microarrays. Transcriptional relevance of any candidate epigenetic biomarker was validated by qRT-PCR.

Results: The detection rate of gastric cardiac IM was 23% (27/118) in cancer-free individuals. Genome-wide DNA methylation profiling showed a global decrease in methylation in IM compared with normal tissues (median methylation = 0.64 and 0.70 for gastric cardiac IM and normal tissues, respectively). Differential methylation analysis between gastric cardiac IM and normal tissues identified 38,237 differentially methylated probes (DMPs) with a majority of sites showing hypermethylation in IM compared with normal tissues (56.3% vs. 43.7%). Subsequent analysis revealed a significant enrichment of hypermethylated DMPs in promoter and CpG islands (p < 0.001 for both, Pearson χ² test). For DMPs located in promoter CpG islands showing extreme hypermethylation, the candidate gene with the largest number of DMPs (n = 7) was mapped to HOXA5. Accordingly, mRNA expression of HOXA5 was significantly reduced in IM compared to normal tissue.

Conclusions: Our results suggest the implication of alterations in DNA methylation in gastric cardiac IM and highlight that HOXA5 hypermethylation may be a promising epigenetic biomarker, emphasizing the role of aberrant HOXA5 expression in the pathogenesis of gastric cardiac IM.

Keywords: Gastric cardia; Genome-wide DNA methylation; Intestinal metaplasia.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

CpG Islands / genetics
DNA Methylation* / genetics
Epigenesis, Genetic / genetics
Genes, Homeobox
Humans
Metaplasia / genetics
Precancerous Conditions*
Stomach Neoplasms