Author:
Tian Bowen,Xu Xiaogang,Li Lin,Tian Yan,Liu Yanqing,Mu Yide,Lu Jieting,Song Kai,lv Junjian,He Qiuming,Zhong Wei,Xia Huimin,Lan Chaoting
Abstract
AbstractNecrotizing enterocolitis (NEC) is a multifactorial gastrointestinal disease with high morbidity and mortality among premature infants. This study aimed to identify novel methylation-regulated biomarkers in NEC intestinal tissue through multiomics analysis. We analyzed DNA methylation and transcriptome datasets from ileum and colon tissues of patients with NEC. We identify methylation-related differential genes (MrDEGs) based on the rule that the degree of methylation in the promoter region is inversely proportional to RNA transcription. These MrDEGs included ADAP1, GUCA2A, BCL2L14, FUT3, MISP, USH1C, ITGA3, UNC93A and IL22RA1. Single-cell data revealed that MrDEGs were mainly located in the intestinal epithelial part of intestinal tissue. These MrDEGs were verified through Target gene bisulfite sequencing and RT-qPCR. We successfully identified and verified the ADAP1, GUCA2A, IL22RA1 and MISP, primarily expressed in intestinal epithelial villus cells through single-cell data. Through single-gene gene set enrichment analysis, we found that these genes participate mainly in the pathological process of T-cell differentiation and the suppression of intestinal inflammation in NEC. This study enhances our understanding of the pathogenesis of NEC and may promote the development of new precision medicine methods for NEC prediction and diagnosis.
Funder
Scienceand Technology Research Project of Education Department of Jiangxi Province
National Natural Science Foundation of China
Research Foundation of Guangzhou Women and Children’s Medical Center for Clinical Doctor
China Postdoctor Science Foundation
Science and Technology Project of Guangzhou
Publisher
Springer Science and Business Media LLC