4.8 Article

Transient DNMT1 suppression reveals hidden heritable marks in the genome

Journal

NUCLEIC ACIDS RESEARCH
Volume 43, Issue 3, Pages 1485-1497

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/nar/gku1386

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Funding

  1. Canadian Institute of Health Research [110987]
  2. National Institutes of Health [R01 HD044133]
  3. Fonds de la Recherche Quebec-Sante and Montreal Children's Hospital Research Institute fellowships
  4. Fonds de la Recherche Quebec-Sante
  5. Canadian Institute of Health Research

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Genome-wide demethylation and remethylation of DNA during early embryogenesis is essential for development. Imprinted germline differentially methylated domains (gDMDs) established by sex-specific methylation in either male or female germ cells, must escape these dynamic changes and sustain precise inheritance of both methylated and unmethylated parental alleles. To identify other, gDMD-like sequences with the same epigenetic inheritance properties, we used a modified embryonic stem (ES) cell line that emulates the early embryonic demethylation and remethylation waves. Transient DNMT1 suppression revealed gDMD-like sequences requiring continuous DNMT1 activity to sustain a highly methylated state. Remethylation of these sequences was also compromised in vivo in a mouse model of transient DNMT1 loss in the preimplantation embryo. These novel regions, possessing heritable epigenetic features similar to imprinted-gDMDs are required for normal physiological and developmental processes and when disrupted are associated with disorders such as cancer and autism spectrum disorders. This study presents new perspectives on DNA methylation heritability during early embryo development that extend beyond conventional imprinted-gDMDs.

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