Ring1B Compacts Chromatin Structure and Represses Gene Expression Independent of Histone Ubiquitination

Eskeland, Ragnhild; Leeb, Martin; Grimes, Graeme R.; Kress, Clémence; Boyle, Shelagh; Sproul, Duncan; Gilbert, Nick; Fan, Yuhong; Skoultchi, Arthur I.; Wutz, Anton; Bickmore, Wendy A.

doi:10.1016/j.molcel.2010.02.032

Cited by 492 publications

(569 citation statements)

References 62 publications

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“…Indeed, our observations that both L3MBTL2 and L3MBTL1 are expressed throughout pre-implantation development could provide more versatile actions of polycomb-related function at specific genome locations at a given developmental time. While it is known that the catalytic, ubiquitylation activity of PRC1 is not necessary to compact chromatin at the time of gastrulation in vivo 9,17 whether catalytic activity per se of PRC1 is necessary after fertilization, has not been addressed.…”

Section: Discussionmentioning

confidence: 99%

“…PRC2 displays its main catalytic activity toward H3K27me3 while the main catalytic activity of PRC1 is monoubiquitylation of H2A at lysine 119 (K119), although PRC1 has also been shown to be able to compact chromatin independently of H2AK119ub in vitro and in vivo. 9,12,17 Genetically and biochemically, a role for PRC1 in transcriptional repression has been clearly demonstrated. 33 The initial model for PcG repression posited that PRC1 recruitment depends upon previously established H3K27me3 domains by the action of PRC2.…”

Section: Introductionmentioning

confidence: 99%

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Characterization of non-canonical Polycomb Repressive Complex 1 subunits during early mouse embryogenesis

Eid

Torres-Padilla

2016

Epigenetics

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An intense period of chromatin remodeling takes place after fertilization in mammals, which is thought necessary for epigenetic reprogramming to start a new developmental program. While much attention has been given to the role of Polycomb Repressive Complex 2 (PRC2) and to canonical PRC1 complexes during this process, little is known as to whether there is any contribution of non-canonical PRC1 in shaping the chromatin landscape after fertilization. Here, we first describe in detail the temporal dynamics and abundance of H2A ubiquitylation (H2AK119ub), a histone modification catalyzed by PRC1, during preimplantation mouse development. In addition, we have analyzed the presence of the 2 characteristic subunits of non-canonical PRC1 complexes, RYBP and its homolog YAF-2. Our results indicate that H2AK119ub is inherited from the sperm, rapidly removed from the paternal chromatin after fertilization, but detected again prior to the first mitosis, suggesting that PRC1 activity occurs as early as the zygotic stage. RYBP and YAF-2, together with the non-canonical subunit L3MBTL2, are all present during preimplantation development but show different temporal dynamics. While RYBP is absent in the zygote, it is strongly induced from the 4-cell stage onwards. YAF-2 is inherited maternally and localizes to the pericentromeric regions in the zygote, is strongly induced between the 2-and 4-cell stages but then remains weak to undetectable subsequently. All together, our data suggest that non-canonical PRC1 is active during pre-implantation development and should be regarded as an additional component during epigenetic reprogramming and in the establishment of cellular plasticity of the early embryo.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Characterization of non-canonical Polycomb Repressive Complex 1 subunits during early mouse embryogenesis

Eid

Torres-Padilla

2016

Epigenetics

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“…13 Further, transcriptional repression by PRC1 is likely independent of the H2AK119ub mark and rather a function of chromatin condensation. [14][15][16][17] PRC1 is dislocated from chromatin by Zrf1, which tethers to H2AK119ub via a specific ubiquitin-binding domain. 18 Hence, PRC1-mediated ubiquitylation of H2A is a prerequisite for Zrf1 recruitment and thereby PRC1 dislocation.…”

Section: Introductionmentioning

confidence: 99%

Dual role of Med12 in PRC1-dependent gene repression and ncRNA-mediated transcriptional activation

et al. 2016

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Mediator is considered an enhancer of RNA-Polymerase II dependent transcription but its function and regulation in pluripotent mouse embryonic stem cells (mESCs) remains unresolved. One means of controlling the function of Mediator is provided by the binding of the Cdk8 module (Med12, Cdk8, Ccnc and Med13) to the core Mediator. Here we report that Med12 operates together with PRC1 to silence key developmental genes in pluripotency. At the molecular level, while PRC1 represses genes it is also required to assemble ncRNA containing Med12-Mediator complexes. In the course of cellular differentiation the H2A ubiquitin binding protein Zrf1 abrogates PRC1-Med12 binding and facilitates the association of Cdk8 with Mediator. This remodeling of Mediator-associated protein complexes converts Mediator from a transcriptional repressor to a transcriptional enhancer, which then mediates ncRNA-dependent activation of Polycomb target genes. Altogether, our data reveal how the interplay of PRC1, ncRNA and Mediator complexes controls pluripotency and cellular differentiation.

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“…Ring1 mediates the ubiquitylation of histone H2A (de Napoles et al, 2004) (for a review, see Martinez and Cavalli, 2006). PRC1 recognizes H3K27me3 to inhibit transcriptional elongation through H2A ubiquitylation (Zhou et al, 2008) and to compact the chromatin structure (Eskeland et al, 2010). PRC2 methylates H3K27 (a key chromatin mark), a main feature of chromatin silencing mediated by PcG proteins.…”

Section: Components Of Polycomb Complexesmentioning

confidence: 99%

“…PRC2 catalyzes the methylation of H3K27; the methylation of H3K27, particularly trimethylation, is the main hallmark of PcG-mediated silencing (Levine et al, 2004;Ringrose et al, 2003), which occurs through enzymatic activity (in association with PRC1). In addition to the nonenzymatic chromatin-compacting regulatory effect of PRC1 (Eskeland et al, 2010), this Pc complex is able to ubiquitylate histone H2A through Ring1A and Ring1B (for reviews, see Eckert et al, 2011;Richly et al, 2011;Vidal, 2009).…”

Section: Golbabapour Et Almentioning

confidence: 99%

Gene Silencing and Polycomb Group Proteins: An Overview of their Structure, Mechanisms and Phylogenetics

Golbabapour

Majid²,

Hassandarvish³

et al. 2013

OMICS: A Journal of Integrative Biology

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DNA methylation, histone modifications, and chromatin configuration are crucially important in the regulation of gene expression. Among these epigenetic mechanisms, silencing the expression of certain genes depending on developmental stage and tissue specificity is a key repressive system in genome programming. Polycomb (Pc) proteins play roles in gene silencing through different mechanisms. These proteins act in complexes and govern the histone methylation profiles of a large number of genes that regulate various cellular pathways. This review focuses on two main Pc complexes, Pc repressive complexes 1 and 2, and their phylogenetic relationship, structures, and function. The dynamic roles of these complexes in silencing will be discussed herein, with a focus on the recruitment of Pc complexes to target genes and the key factors involved in their recruitment.

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Ring1B Compacts Chromatin Structure and Represses Gene Expression Independent of Histone Ubiquitination

Cited by 492 publications

References 62 publications

Characterization of non-canonical Polycomb Repressive Complex 1 subunits during early mouse embryogenesis

Characterization of non-canonical Polycomb Repressive Complex 1 subunits during early mouse embryogenesis

Dual role of Med12 in PRC1-dependent gene repression and ncRNA-mediated transcriptional activation

Gene Silencing and Polycomb Group Proteins: An Overview of their Structure, Mechanisms and Phylogenetics

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