Phase separation by the polyhomeotic sterile alpha motif compartmentalizes Polycomb Group proteins and enhances their activity

Seif, Elias; Kang, Jaw Jou; Sasseville, Charles; Senkovich, Olga; Kaltashov, Alexander; Boulier, Elodie L.; Kapur, Ibani; Kim, Chongwoo A.; Francis, Nicole J.

doi:10.1038/s41467-020-19435-z

Cited by 90 publications

(124 citation statements)

References 97 publications

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“…Considering the existence of cPRC1 and recent identification of BAHCC1 BAH as H3K27me3-specific readers (17), the chromodomain (cPRC1)- and BAH-mediated functional readout of H3K27me3 can coexist in mammalian cells, imparting their respective gene-silencing effects through distinctive molecular pathways. Besides a catalytic function for inducing H2AK119ub1, cPRC1 induces chromatin compaction via cofactor-mediated phase separation and condensation formation (12–14). On the other hand, BAHCC1 (17) and BAHD1 both interact with HDACs, thus linking H3K27me3 together with histone deacetylation, an integral step of gene repression.…”

Section: Discussionmentioning

confidence: 99%

“…As a support, mutation of the histone H3K27 site or its modifying enzymes occur recurrently in a range of human diseases, such as cancer and developmental syndrome (6–9). A prevalent model for functional transduction of H3K27me3 in mammals is that H3K27me3 is read and bound by chromodomain harbored within the chromobox (CBX) component of canonical Polycomb repressive complex 1 (cPRC1), which can induce gene silencing at least partly through mono-ubiquitination of histone H2A lysine 119 (H2AK119ub1) (2,3,10,11) and/or a phase separation-mediated chromatin compaction mechanism (12–14). However, emerging evidence has shown that, in mammalian cells, H3K27me3 is also ‘sensed’ and bound by a second class of “reader” modules termed Bromo-Adjacent Homology (BAH), which exist within chromatin regulators such as BAH D omain Containing 1 (BAHD1) (15,16) and BAH and C oiled- c oil Domain-containing Protein 1 (BAHCC1) (17).…”

Section: Introductionmentioning

confidence: 99%

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A conserved BAH module within mammalian BAHD1 connects H3K27me3 to Polycomb gene silencing

Fan

Guo

Tsai

et al. 2021

Preprint

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Trimethylation of histone H3 lysine 27 (H3K27me3) is important for gene silencing and imprinting, (epi)genome organization and organismal development. In a prevalent model, the functional readout of H3K27me3 in mammalian cells is achieved through the H3K27me3-recognizing chromodomain harbored within the chromobox (CBX) component of canonical Polycomb repressive complex 1 (cPRC1), which induces chromatin compaction and gene repression. Here, we report that binding of H3K27me3 by a Bromo Adjacent Homology (BAH) domain harbored within BAH domain-containing protein 1 (BAHD1) is required for overall BAHD1 targeting to chromatin and for optimal repression of the H3K27me3-demarcated genes in mammalian cells. Disruption of direct interaction between BAHD1BAH and H3K27me3 by point mutagenesis leads to chromatin remodeling, notably, increased histone acetylation, at its Polycomb gene targets. Mice carrying an H3K27me3-interaction-defective mutation of Bahd1BAH causes marked embryonic lethality, showing a requirement of this pathway for normal development. Altogether, this work demonstrates an H3K27me3-initiated signaling cascade that operates through a conserved BAH 'reader' module within BAHD1 in mammals.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

A conserved BAH module within mammalian BAHD1 connects H3K27me3 to Polycomb gene silencing

Fan

Guo

Tsai

et al. 2021

Preprint

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“…PcG proteins can directly silence transcription by, for example, preventing the binding of chromatin remodeling complexes [ 117 ]. In addition, polycomb proteins can indirectly block transcription through a combination of local chromatin compaction [ 118 , 119 , 120 , 121 ], loop formation [ 106 , 107 ], as well as phase separation [ 24 , 28 , 122 ].…”

Section: Facultative Heterochromatinmentioning

confidence: 99%

The Sound of Silence: How Silenced Chromatin Orchestrates the Repair of Double-Strand Breaks

Kendek

Wensveen

Janssen

2021

Genes

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The eukaryotic nucleus is continuously being exposed to endogenous and exogenous sources that cause DNA breaks, whose faithful repair requires the activity of dedicated nuclear machineries. DNA is packaged into a variety of chromatin domains, each characterized by specific molecular properties that regulate gene expression and help maintain nuclear structure. These different chromatin environments each demand a tailored response to DNA damage. Silenced chromatin domains in particular present a major challenge to the cell’s DNA repair machinery due to their specific biophysical properties and distinct, often repetitive, DNA content. To this end, we here discuss the interplay between silenced chromatin domains and DNA damage repair, specifically double-strand breaks, and how these processes help maintain genome stability.

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“…In this work, we assumed that such contacts were dependent only on the genomic distance and were not affected by the local epigenetic landscape. However, PRC1 that binds to H3K27me3 may form condensate (45,(76)(77)(78) , the so-called Polycomb bodies, and may subsequently impact the local 3D organization of the locus (79,80), an increase compaction may in turn facilitate spreading (81)(82)(83). Accounting for this positive feedback loop between longrange spreading and 3D chromosome organization may allow a better characterization of the role of genome folding in epigenetic regulation (84,85).…”

Section: Discussionmentioning

confidence: 99%

Dynamical modeling of the H3K27 epigenetic landscape in mouse embryonic stem cells

Newar

Fanchon

Jost³

2021

Preprint

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The Polycomb system via the methylation of the lysine 27 of histone H3 (H3K27) plays central roles in the silencing of many lineage-specific genes during development. Recent experimental evidence suggested that the recruitment of histone modifying enzymes like the Polycomb repressive complex 2 (PRC2) at specific sites and their spreading capacities from these sites are key to the establishment and maintenance of a proper epigenomic landscape around Polycomb-target genes. Here, based on previous biochemical knowledge, we turned this hypothesis into a mathematical model that can predict the locus-specific distributions of H3K27 modifications. Within the biological context of mouse embryonic stem cells, our model showed quantitative agreement with experimental profiles of H3K27 acetylation and methylation around Polycomb-target genes in wild-type and mutants. In particular, we demonstrated the key role of the reader-writer module of PRC2 and of the competition between the binding of activating and repressing enzymes in shaping the H3K27 landscape around transcriptional start sites. The predicted dynamics of establishment and maintenance of the repressive trimethylated H3K27 state suggest a slow accumulation, in perfect agreement with experiments. Our approach represents a first step towards a quantitative description of PcG regulation in various cellular contexts and provides a generic framework to better characterize epigenetic regulation in normal or disease situations.

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Phase separation by the polyhomeotic sterile alpha motif compartmentalizes Polycomb Group proteins and enhances their activity

Cited by 90 publications

References 97 publications

A conserved BAH module within mammalian BAHD1 connects H3K27me3 to Polycomb gene silencing

A conserved BAH module within mammalian BAHD1 connects H3K27me3 to Polycomb gene silencing

The Sound of Silence: How Silenced Chromatin Orchestrates the Repair of Double-Strand Breaks

Dynamical modeling of the H3K27 epigenetic landscape in mouse embryonic stem cells

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