Literature DB >> 18311137

PRC1 and Suv39h specify parental asymmetry at constitutive heterochromatin in early mouse embryos.

Mareike Puschendorf1, Rémi Terranova, Erwin Boutsma, Xiaohong Mao, Kyo-ichi Isono, Urszula Brykczynska, Carolin Kolb, Arie P Otte, Haruhiko Koseki, Stuart H Orkin, Maarten van Lohuizen, Antoine H F M Peters.   

Abstract

In eukaryotes, Suv39h H3K9 trimethyltransferases are required for pericentric heterochromatin formation and function. In early mouse preimplantation embryos, however, paternal pericentric heterochromatin lacks Suv39h-mediated H3K9me3 and downstream marks. Here we demonstrate Ezh2-independent targeting of maternally provided polycomb repressive complex 1 (PRC1) components to paternal heterochromatin. In Suv39h2 maternally deficient zygotes, PRC1 also associates with maternal heterochromatin lacking H3K9me3, thereby revealing hierarchy between repressive pathways. In Rnf2 maternally deficient zygotes, the PRC1 complex is disrupted, and levels of pericentric major satellite transcripts are increased at the paternal but not the maternal genome. We conclude that in early embryos, Suv39h-mediated H3K9me3 constitutes the dominant maternal transgenerational signal for pericentric heterochromatin formation. In absence of this signal, PRC1 functions as the default repressive back-up mechanism. Parental epigenetic asymmetry, also observed along cleavage chromosomes, is resolved by the end of the 8-cell stage--concurrent with blastomere polarization--marking the end of the maternal-to-embryonic transition.

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Year:  2008        PMID: 18311137     DOI: 10.1038/ng.99

Source DB:  PubMed          Journal:  Nat Genet        ISSN: 1061-4036            Impact factor:   38.330


  137 in total

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4.  Two-step imprinted X inactivation: repeat versus genic silencing in the mouse.

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5.  Distinct histone modifications in stem cell lines and tissue lineages from the early mouse embryo.

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6.  Repressive and active histone methylation mark distinct promoters in human and mouse spermatozoa.

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7.  Targets and dynamics of promoter DNA methylation during early mouse development.

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8.  Ring1B and Suv39h1 delineate distinct chromatin states at bivalent genes during early mouse lineage commitment.

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Journal:  Brief Funct Genomics       Date:  2010-12-23       Impact factor: 4.241

Review 10.  Histone variants in metazoan development.

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