PLoS ONE (Jan 2014)

Genome-wide binding of MBD2 reveals strong preference for highly methylated loci.

  • Roberta Menafra,
  • Arie B Brinkman,
  • Filomena Matarese,
  • Gianluigi Franci,
  • Stefanie J J Bartels,
  • Luan Nguyen,
  • Takashi Shimbo,
  • Paul A Wade,
  • Nina C Hubner,
  • Hendrik G Stunnenberg

DOI
https://doi.org/10.1371/journal.pone.0099603
Journal volume & issue
Vol. 9, no. 6
p. e99603

Abstract

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MBD2 is a subunit of the NuRD complex that is postulated to mediate gene repression via recruitment of the complex to methylated DNA. In this study we adopted an MBD2 tagging-approach to study its genome wide binding characteristics. We show that in vivo MBD2 is mainly recruited to CpG island promoters that are highly methylated. Interestingly, MBD2 binds around 1 kb downstream of the transcription start site of a subset of ∼ 400 CpG island promoters that are characterized by the presence of active histone marks, RNA polymerase II (Pol2) and low to medium gene expression levels and H3K36me3 deposition. These tagged-MBD2 binding sites in MCF-7 show increased methylation in a cohort of primary breast cancers but not in normal breast samples, suggesting a putative role for MBD2 in breast cancer.