| Literature DB >> 33494958 |
Yiran Guo1, Shuai Zhao2, Gang Greg Wang3.
Abstract
Modulation of chromatin structure and/or modification by Polycomb repressive complexes (PRCs) provides an important means to partition the genome into functionally distinct subdomains and to regulate the activity of the underlying genes. Both the enzymatic activity of PRC2 and its chromatin recruitment, spreading, and eviction are exquisitely regulated via interactions with cofactors and DNA elements (such as unmethylated CpG islands), histones, RNA (nascent mRNA and long noncoding RNA), and R-loops. PRC2-catalyzed histone H3 lysine 27 trimethylation (H3K27me3) is recognized by distinct classes of effectors such as canonical PRC1 and BAH module-containing proteins (notably BAHCC1 in human). These effectors mediate gene silencing by different mechanisms including phase separation-related chromatin compaction and histone deacetylation. We discuss recent advances in understanding the structural architecture of PRC2, the regulation of its activity and chromatin recruitment, and the molecular mechanisms underlying Polycomb-mediated gene silencing. Because PRC deregulation is intimately associated with the development of diseases, a better appreciation of Polycomb-based (epi)genomic regulation will have far-reaching implications in biology and medicine.Entities:
Keywords: BAH; CpG island; H3K27me3; PRC1; PRC2; Polycomb; R-loop; RNA; allosteric activation; chromatin; chromodomain; histone; methylation; phase separation; transcription
Year: 2021 PMID: 33494958 PMCID: PMC8119337 DOI: 10.1016/j.tig.2020.12.006
Source DB: PubMed Journal: Trends Genet ISSN: 0168-9525 Impact factor: 11.639