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Gene Body Methylation of the Lymphocyte-Specific Gene

Authors :
Michael H, McGuire
Santosh K, Dasari
Hui, Yao
Yunfei, Wen
Lingegowda S, Mangala
Emine, Bayraktar
Wencai, Ma
Cristina, Ivan
Einav, Shoshan
Sherry Y, Wu
Eric, Jonasch
Menashe, Bar-Eli
Jing, Wang
Keith A, Baggerly
Anil K, Sood
Source :
Mol Cancer Res
Publication Year :
2020

Abstract

Investigations into the function of non-promoter DNA methylation have yielded new insights into epigenetic regulation of gene expression. Previous studies have highlighted the importance of distinguishing between DNA methylation in discrete functional regions; however, integrated non-promoter DNA methylation and gene expression analyses across a wide number of tumor types and corresponding normal tissues have not been performed. Through integrated analysis of gene expression and DNA methylation profiles, we examined 32 tumor types and identified 57 tumor suppressors and oncogenes out of 260 genes exhibiting a correlation of > 0.5 between gene body methylation and gene expression in at least 1 tumor type. The lymphocyte-specific gene CARD11 exhibits robust association between gene body methylation and expression across 19 of 32 tumor types examined. It is significantly overexpressed in kidney renal cell carcinoma (KIRC) and lung adenocarcinoma (LUAD) tumor tissues in comparison to respective control samples; and is significantly associated with lower overall survival in KIRC. Contrary to its canonical function in lymphocyte NF-kB activation, CARD11 activates the mTOR pathway in KIRC and LUAD, resulting in suppressed autophagy. Furthermore, demethylation of a CpG island within the gene body of CARD11 decreases gene expression. Collectively, our study highlights how DNA methylation outside the promoter region can impact tumor progression.

Details

ISSN :
15573125
Volume :
19
Issue :
11
Database :
OpenAIRE
Journal :
Molecular cancer research : MCR
Accession number :
edsair.pmid..........3ddcd803feff6dd202539128c5dc4e39