AI Article Synopsis

  • * Researchers identified the association dynamics of 3,995 proteins, finding that certain replication and chromatin factors are enriched in nascent chromatin, while others exhibit delayed association during the replication process.
  • * The study not only highlights changes in specific protein modifications associated with chromatin during replication but also predicts the functions of 93 uncharacterized proteins, revealing FAM111A as a crucial factor for PCNA loading in the replication process.

Article Abstract

To maintain genome function and stability, DNA sequence and its organization into chromatin must be duplicated during cell division. Understanding how entire chromosomes are copied remains a major challenge. Here, we use nascent chromatin capture (NCC) to profile chromatin proteome dynamics during replication in human cells. NCC relies on biotin-dUTP labelling of replicating DNA, affinity purification and quantitative proteomics. Comparing nascent chromatin with mature post-replicative chromatin, we provide association dynamics for 3,995 proteins. The replication machinery and 485 chromatin factors such as CAF-1, DNMT1 and SUV39h1 are enriched in nascent chromatin, whereas 170 factors including histone H1, DNMT3, MBD1-3 and PRC1 show delayed association. This correlates with H4K5K12diAc removal and H3K9me1 accumulation, whereas H3K27me3 and H3K9me3 remain unchanged. Finally, we combine NCC enrichment with experimentally derived chromatin probabilities to predict a function in nascent chromatin for 93 uncharacterized proteins, and identify FAM111A as a replication factor required for PCNA loading. Together, this provides an extensive resource to understand genome and epigenome maintenance.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4283098PMC
http://dx.doi.org/10.1038/ncb2918DOI Listing

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