Universitat de Barcelona
Lee, Seung-Tae
Muench, Marcus O.
Fomin, Marina E.
Xiao, Jianqiao
Zhou, Mi
Smith, Adam de
Martín-Subero, José Ignacio
Heath, Simon C.
Houseman, E.Andres
Roy, Ritu
Wrensch, Margaret
Wiencke, John K.
Metayer, Catherine
Wiemels, Joseph L.
2018-01-12T15:12:21Z
2018-01-12T15:12:21Z
2015-03-11
2018-01-12T15:12:21Z
We investigated DNA methylomes of pediatric B-cell acute lymphoblastic leukemias (B-ALLs) using whole-genome bisulfite sequencing and high-definition microarrays, along with RNA expression profiles. Epigenetic alteration of B-ALLs occurred in two tracks: de novo methylation of small functional compartments and demethylation of large inter-compartmental backbones. The deviations were exaggerated in lamina-associated domains, with differences corresponding to methylation clusters and/or cytogenetic groups. Our data also suggested a pivotal role of polycomb and CTBP2 in de novo methylation, which may be traced back to bivalency status of embryonic stem cells. Driven by these potent epigenetic modulations, suppression of polycomb target genes was observed along with disruption of developmental fate and cell cycle and mismatch repair pathways and altered activities of key upstream regulators.
Anglès
Leucèmia; Epigenètica; Cèl·lules mare embrionàries; Leukemia; Epigenetics; Embryonic stem cells
Oxford University Press
Reproducció del document publicat a: https://doi.org/10.1093/nar/gkv103
Nucleic Acids Research, 2015, vol. 43, num. 5, p. 2590-2602
https://doi.org/10.1093/nar/gkv103
cc-by-nc (c) Lee, Seung-Tae et al., 2015
http://creativecommons.org/licenses/by-nc/3.0/es
