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Lee, SangJoon
Viral Immunology Lab.
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Identification of reactive CpGs and RNA expression in early COVID-19 through cis-eQTM analysis reflecting disease severity and recovery

Author(s)
Ryu, HyojungAn, KyungwhanKwon, YoonsungJeon, YeonsuJeon, SungwonChoi, HansolKim, Yeo JinKim, SunhwaSul, Ok JooLee, SangJoonChun, Asaph YoungShin, Eun-SeokRa, Seung WonBhak, Jong
Issued Date
2025-08
DOI
10.1038/s42003-025-08609-4
URI
https://scholarworks.unist.ac.kr/handle/201301/87729
Citation
COMMUNICATIONS BIOLOGY, v.8, no.1, pp.1174
Abstract
Multi-omics analyses of severe COVID-19 cases are crucial in deciphering the complex interplay between genetic and epigenetic factors. Here, we present an analysis of Expression Quantitative Trait Methylation (eQTM) to investigate the complex interplay of methylation and gene expression pattern during the acute phase of severe COVID-19. We identified 16 differentially expressed genes and 30 nearby differentially methylated CpG sites. Six key genes-SRXN1, FURIN, IL18RAP, FOXO3, GCNT4, and FKBP5-were either up-regulated or down-regulated near hypomethylated CpG sites. These genes are associated with viral infiltration, immune activation, lung damage, and oxidative stress-related multi-organ failure, which are the hallmarks of severe COVID-19. Interestingly, during the recovery phase, methylation and gene expression levels returned to baseline, underscoring the rapid and reversible nature of these molecular changes. These findings provide insight into the dynamics of epigenetic and transcriptomic shifts according to the infectious stage, supporting potential prognostic and therapeutic approaches for severe COVID-19.
Publisher
NATURE PORTFOLIO
ISSN
2399-3642

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