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  5. Comparative genome-wide DNA methylation analysis of colorectal tumor and matched normal tissues

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Article
en
2012

Comparative genome-wide DNA methylation analysis of colorectal tumor and matched normal tissues

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en
2012
Vol 7 (12)
Vol. 7
DOI: 10.4161/epi.22562

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Manel Esteller
Manel Esteller

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Femke Simmer
Arie B. Brinkman
Yassen Assenov
+11 more

Abstract

Aberrant DNA methylation often occurs in colorectal cancer (CRC). In our study we applied a genome-wide DNA methylation analysis approach, MethylCap-seq, to map the differentially methylated regions (DMRs) in 24 tumors and matched normal colon samples. In total, 2687 frequently hypermethylated and 468 frequently hypomethylated regions were identified, which include potential biomarkers for CRC diagnosis. Hypermethylation in the tumor samples was enriched at CpG islands and gene promoters, while hypomethylation was distributed throughout the genome. Using epigenetic data from human embryonic stem cells, we show that frequently hypermethylated regions coincide with bivalent loci in human embryonic stem cells. DNA methylation is commonly thought to lead to gene silencing; however, integration of publically available gene expression data indicates that 75% of the frequently hypermethylated genes were most likely already lowly or not expressed in normal tissue. Collectively, our study provides genome-wide DNA methylation maps of CRC, comprehensive lists of DMRs, and gives insights into the role of aberrant DNA methylation in CRC formation.

How to cite this publication

Femke Simmer, Arie B. Brinkman, Yassen Assenov, Filomena Matarese, Anita Kaan, Lina Sabatino, Alberto Villanueva, Dori Huertas, Manel Esteller, Thomas Lengauer, Christoph Bock, Vittorio Colantuoni, Lucia Altucci, Hendrik G. Stunnenberg (2012). Comparative genome-wide DNA methylation analysis of colorectal tumor and matched normal tissues. , 7(12), DOI: https://doi.org/10.4161/epi.22562.

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Publication Details

Type

Article

Year

2012

Authors

14

Datasets

0

Total Files

0

Language

en

DOI

https://doi.org/10.4161/epi.22562

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