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Hypermethylation of PDX1, EN2, and MSX1 predicts the prognosis of colorectal cancer.


ABSTRACT: Despite numerous observations regarding the relationship between DNA methylation changes and cancer progression, only a few genes have been verified as diagnostic biomarkers of colorectal cancer (CRC). To more practically detect methylation changes, we performed targeted bisulfite sequencing. Through co-analysis of RNA-seq, we identified cohort-specific DNA methylation markers: CpG islands of the intragenic regions of PDX1, EN2, and MSX1. We validated that these genes have oncogenic features in CRC and that their expression levels are increased in correlation with the hypermethylation of intragenic regions. The reliable depth of the targeted bisulfite sequencing data enabled us to design highly optimized quantitative methylation-specific PCR primer sets that can successfully detect subtle changes in the methylation levels of candidate regions. Furthermore, these methylation levels can divide CRC patients into two groups denoting good and poor prognoses. In this study, we present a streamlined workflow for screening clinically significant differentially methylated regions. Our discovery of methylation markers in the PDX1, EN2, and MSX1 genes suggests their promising performance as prognostic markers and their clinical application in CRC patients.

SUBMITTER: Lee Y 

PROVIDER: S-EPMC8894425 | biostudies-literature | 2022 Feb

REPOSITORIES: biostudies-literature

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Hypermethylation of PDX1, EN2, and MSX1 predicts the prognosis of colorectal cancer.

Lee Yeongun Y   Dho So Hee SH   Lee Jiyeon J   Hwang Ji-Hyun JH   Kim Minjung M   Choi Won-Young WY   Lee Jin-Young JY   Lee Jongwon J   Chang Woochul W   Lee Min Young MY   Choi Jungmin J   Kim Tae-You TY   Kim Lark Kyun LK  

Experimental & molecular medicine 20220215 2


Despite numerous observations regarding the relationship between DNA methylation changes and cancer progression, only a few genes have been verified as diagnostic biomarkers of colorectal cancer (CRC). To more practically detect methylation changes, we performed targeted bisulfite sequencing. Through co-analysis of RNA-seq, we identified cohort-specific DNA methylation markers: CpG islands of the intragenic regions of PDX1, EN2, and MSX1. We validated that these genes have oncogenic features in  ...[more]

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