4.5 Article

Developmental profile of H19 differentially methylated domain (DMD) deletion alleles reveals multiple roles of the DMD in regulating allelic expression and DNA methylation at the imprinted H19/Igf2 locus

Journal

MOLECULAR AND CELLULAR BIOLOGY
Volume 26, Issue 4, Pages 1245-1258

Publisher

AMER SOC MICROBIOLOGY
DOI: 10.1128/MCB.26.4.1245-1258.2006

Keywords

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Funding

  1. NICHD NIH HHS [T32 HD-07516, T32 HD007516] Funding Source: Medline
  2. NIGMS NIH HHS [R01 GM051279, GM51279, R37 GM051279] Funding Source: Medline

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The differentially methylated domain (DMD) of the mouse H19 gene is a methylation-sensitive insulator that blocks access of the Igf2 gene to shared enhancers on the maternal allele and inactivates H19 expression on the methylated paternal allele. By analyzing H19 DMD deletion alleles H19(Delta DMD) and H19(Delta 3.8kb-5'H19) in pre- and postimplantation embryos, we show that the DMD exhibits positive transcriptional activity and is required for H19 expression in blastocysts and full activation of H19 during subsequent development. We also show that the DMD is required to establish Igf2 imprinting by blocking access to shared enhancers when Igf2 monoallelic expression is initiated in postimplantation embryos and that the single remaining CTCF site of the H19(Delta DMD) allele is unable to provide this function. Furthermore, our data demonstrate that sequence outside of the DMD can attract some paternal-allele-specific CpG methylation 5' of H19 in preimplantation embryos, although this methylation is not maintained during postimplantation in the absence of the DMD. Finally, we report a conditional allele floxing the 1.6-kb sequence deleted from the H19(Delta DMD) allele and demonstrate that the DMD is required to maintain repression of the maternal Igf2 allele and the full activity of the paternal Igf2 allele in neonatal liver.

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