Your search keyword '"Alabert C"' showing total 2 results

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

Author

Bandau S, Alvarez V, Jiang H, Graff S, Sundaramoorthy R, Gierlinski M, Toman M, Owen-Hughes T, Sidoli S, Lamond A, and Alabert C

Subjects

Animals, Humans, DNA Replication, Nucleosomes, Transcription Factors metabolism, Chromatin Assembly and Disassembly, Mammals genetics, Mammals metabolism, Chromatin, RNA Polymerase II metabolism

Abstract

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., (© 2024. The Author(s).)

Published

2024

2. DONSON is required for CMG helicase assembly in the mammalian cell cycle.

Author

Evrin C, Alvarez V, Ainsworth J, Fujisawa R, Alabert C, and Labib KP

Subjects

Mice, Animals, Humans, Cell Cycle, DNA Replication, Minichromosome Maintenance Proteins metabolism, Mammals metabolism, Cell Cycle Proteins genetics, Cell Cycle Proteins metabolism, Chromosome Duplication

Abstract

DONSON is one of 13 genes mutated in a form of primordial microcephalic dwarfism known as Meier-Gorlin syndrome. The other 12 encode components of the CDC45-MCM-GINS helicase, around which the eukaryotic replisome forms, or are factors required for helicase assembly during DNA replication initiation. A role for DONSON in CDC45-MCM-GINS assembly was unanticipated, since DNA replication initiation can be reconstituted in vitro with purified proteins from budding yeast, which lacks DONSON. Using mouse embryonic stem cells as a model for the mammalian helicase, we show that DONSON binds directly but transiently to CDC45-MCM-GINS during S-phase and is essential for chromosome duplication. Rapid depletion of DONSON leads to the disappearance of the CDC45-MCM-GINS helicase from S-phase cells and our data indicate that DONSON is dispensable for loading of the MCM2-7 helicase core onto chromatin during G1-phase, but instead is essential for CDC45-MCM-GINS assembly during S-phase. These data identify DONSON as a missing link in our understanding of mammalian chromosome duplication and provide a molecular explanation for why mutations in human DONSON are associated with Meier-Gorlin syndrome., (© 2023 The Authors. Published under the terms of the CC BY 4.0 license.)

Published

2023