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RNA polymerase II promotes the organization of chromatin following DNA replication.

EMBO reports (2024-02-13)
Susanne Bandau, Vanesa Alvarez, Hao Jiang, Sarah Graff, Ramasubramanian Sundaramoorthy, Marek Gierlinski, Matt Toman, Tom Owen-Hughes, Simone Sidoli, Angus Lamond, Constance Alabert
RESUMEN

Understanding how chromatin organisation is duplicated on the two daughter strands is a central question in epigenetics. In mammals, following the passage of the replisome, nucleosomes lose their defined positioning and transcription contributes to their re-organisation. However, whether transcription plays a greater role in the organization of chromatin following DNA replication remains unclear. Here we analysed protein re-association with newly replicated DNA upon inhibition of transcription using iPOND coupled to quantitative mass spectrometry. We show that nucleosome assembly and the re-establishment of most histone modifications are uncoupled from transcription. However, RNAPII acts to promote the re-association of hundreds of proteins with newly replicated chromatin via pathways that are not observed in steady-state chromatin. These include ATP-dependent remodellers, transcription factors and histone methyltransferases. We also identify a set of DNA repair factors that may handle transcription-replication conflicts during normal transcription in human non-transformed cells. Our study reveals that transcription plays a greater role in the organization of chromatin post-replication than previously anticipated.

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5,6-Dichlorobenzimidazole 1-β-D-ribofuranoside
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Anti-ZNF462 antibody produced in rabbit, Prestige Antibodies® Powered by Atlas Antibodies, affinity isolated antibody, buffered aqueous glycerol solution