AI Article Synopsis

  • The process of repairing UV-induced DNA damage involves changes in chromatin structure, which is not fully understood yet.
  • Researchers have identified specific genomic regions where global genome-nucleotide excision repair (GG-NER) starts, known as GG-NER complex binding sites (GCBSs).
  • They found that in response to DNA damage, the GG-NER complex disrupts nucleosomes at these sites, initiating the repair process and revealing a connection between these binding sites and chromatin organization.

Article Abstract

Repair of UV-induced DNA damage requires chromatin remodeling. How repair is initiated in chromatin remains largely unknown. We recently demonstrated that global genome-nucleotide excision repair (GG-NER) in chromatin is organized into domains in relation to open reading frames. Here, we define these domains, identifying the genomic locations from which repair is initiated. By examining DNA damage-induced changes in the linear structure of nucleosomes at these sites, we demonstrate how chromatin remodeling is initiated during GG-NER. In undamaged cells, we show that the GG-NER complex occupies chromatin, establishing the nucleosome structure at these genomic locations, which we refer to as GG-NER complex binding sites (GCBSs). We demonstrate that these sites are frequently located at genomic boundaries that delineate chromosomally interacting domains (CIDs). These boundaries define domains of higher-order nucleosome-nucleosome interaction. We demonstrate that initiation of GG-NER in chromatin is accompanied by the disruption of dynamic nucleosomes that flank GCBSs by the GG-NER complex.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6314166PMC
http://dx.doi.org/10.1101/gr.237198.118DOI Listing

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