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DNA methylation of intragenic CpG islands depends on their transcriptional activity during differentiation and disease

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journal contribution
posted on 2020-11-19, 16:37 authored by Danuta M Jeziorska, Robert JS Murray, Marco De Gobbi, Ricarda Gaentzsch, David Garrick, Helena Ayyub, Taiping Chen, En Li, Jelena Telenius, Magnus Lynch, Bryony Graham, Andrew JH Smith, Jonathan N Lund, Jim R Hughes, Douglas R Higgs, Cristina Tufarelli
The human genome contains ~30,000 CpG islands (CGIs). While CGIs associated with promoters nearly always remain unmethylated, many of the ~9,000 CGIs lying within gene bodies become methylated during development and differentiation. Both promoter and intragenic CGIs may also become abnormally methylated as a result of genome rearrangements and in malignancy. The epigenetic mechanisms by which some CGIs become methylated but others, in the same cell, remain unmethylated in these situations are poorly understood. Analyzing specific loci and using a genome-wide analysis, we show that transcription running across CGIs, associated with specific chromatin modifications, is required for DNA methyltransferase 3B (DNMT3B)-mediated DNA methylation of many naturally occurring intragenic CGIs. Importantly, we also show that a subgroup of intragenic CGIs is not sensitive to this process of transcription-mediated methylation and that this correlates with their individual intrinsic capacity to initiate transcription in vivo. We propose a general model of how transcription could act as a primary determinant of the patterns of CGI methylation in normal development and differentiation, and in human disease.

History

Citation

PNAS September 5, 2017 114 (36) E7526-E7535

Version

  • AM (Accepted Manuscript)

Published in

Proceedings of the National Academy of Sciences (PNAS)

Volume

114

Issue

36

Pagination

E7526 - E7535 (10)

Publisher

National Academy of Sciences

issn

0027-8424

eissn

1091-6490

Copyright date

2017

Spatial coverage

United States

Language

English