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  5. A DNA methylation map of human cancer at single base-pair resolution

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Article
en
2017

A DNA methylation map of human cancer at single base-pair resolution

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en
2017
Vol 36 (40)
Vol. 36
DOI: 10.1038/onc.2017.176

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Manel Esteller
Manel Esteller

University of Barcelona

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Enrique Vidal
Sergi Sayols
Sebastián Morán
+9 more

Abstract

Although single base-pair resolution DNA methylation landscapes for embryonic and different somatic cell types provided important insights into epigenetic dynamics and cell-type specificity, such comprehensive profiling is incomplete across human cancer types. This prompted us to perform genome-wide DNA methylation profiling of 22 samples derived from normal tissues and associated neoplasms, including primary tumors and cancer cell lines. Unlike their invariant normal counterparts, cancer samples exhibited highly variable CpG methylation levels in a large proportion of the genome, involving progressive changes during tumor evolution. The whole-genome sequencing results from selected samples were replicated in a large cohort of 1112 primary tumors of various cancer types using genome-scale DNA methylation analysis. Specifically, we determined DNA hypermethylation of promoters and enhancers regulating tumor-suppressor genes, with potential cancer-driving effects. DNA hypermethylation events showed evidence of positive selection, mutual exclusivity and tissue specificity, suggesting their active participation in neoplastic transformation. Our data highlight the extensive changes in DNA methylation that occur in cancer onset, progression and dissemination.

How to cite this publication

Enrique Vidal, Sergi Sayols, Sebastián Morán, Amy Guillaumet-Adkins, M. Schroeder, Romina Royo, Modesto Orozco, Marta Gut, Marta Gut, Núria López-Bigas, Holger Heyn, Manel Esteller (2017). A DNA methylation map of human cancer at single base-pair resolution. , 36(40), DOI: https://doi.org/10.1038/onc.2017.176.

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Publication Details

Type

Article

Year

2017

Authors

12

Datasets

0

Total Files

0

Language

en

DOI

https://doi.org/10.1038/onc.2017.176

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