Your search keyword '"Courbet S"' showing total 3 results

1. Nucleotide supply, not local histone acetylation, sets replication origin usage in transcribed regions.

Author

Gay S, Lachages AM, Millot GA, Courbet S, Letessier A, Debatisse M, and Brison O

Subjects

Acetylation, Animals, Cells, Cultured, Fibroblasts cytology, Fibroblasts physiology, Histone Deacetylase Inhibitors metabolism, Histone Deacetylases metabolism, Humans, Hydroxamic Acids metabolism, Transcription, Genetic, DNA Replication, Histones metabolism, Nucleotides metabolism, Replication Origin

Abstract

In eukaryotes, only a fraction of replication origins fire at each S phase. Local histone acetylation was proposed to control firing efficiency of origins, but conflicting results were obtained. We report that local histone acetylation does not reflect origin efficiencies along the adenosine monophosphate deaminase 2 locus in mammalian fibroblasts. Reciprocally, modulation of origin efficiency does not affect acetylation. However, treatment with a deacetylase inhibitor changes the initiation pattern. We demonstrate that this treatment alters pyrimidine biosynthesis and decreases fork speed, which recruits latent origins. Our findings reconcile results that seemed inconsistent and reveal an unsuspected effect of deacetylase inhibitors on replication dynamics.

Published

2010

2. Replication fork movement sets chromatin loop size and origin choice in mammalian cells.

Author

Courbet S, Gay S, Arnoult N, Wronka G, Anglana M, Brison O, and Debatisse M

Subjects

Animals, Cell Line, Chromatin genetics, Cricetinae, Cricetulus, DNA biosynthesis, DNA genetics, G1 Phase, Nuclear Matrix metabolism, S Phase, Time Factors, Chromatin metabolism, DNA Replication physiology, Movement, Replication Origin genetics

Abstract

Genome stability requires one, and only one, DNA duplication at each S phase. The mechanisms preventing origin firing on newly replicated DNA are well documented, but much less is known about the mechanisms controlling the spacing of initiation events(2,3), namely the completion of DNA replication. Here we show that origin use in Chinese hamster cells depends on both the movement of the replication forks and the organization of chromatin loops. We found that slowing the replication speed triggers the recruitment of latent origins within minutes, allowing the completion of S phase in a timely fashion. When slowly replicating cells are shifted to conditions of fast fork progression, although the decrease in the overall number of active origins occurs within 2 h, the cells still have to go through a complete cell cycle before the efficiency specific to each origin is restored. We observed a strict correlation between replication speed during a given S phase and the size of chromatin loops in the next G1 phase. Furthermore, we found that origins located at or near sites of anchorage of chromatin loops in G1 are activated preferentially in the following S phase. These data suggest a mechanism of origin programming in which replication speed determines the spacing of anchorage regions of chromatin loops, that, in turn, controls the choice of initiation sites.

Published

2008

3. A homologous recombination defect affects replication-fork progression in mammalian cells.

Author

Daboussi F, Courbet S, Benhamou S, Kannouche P, Zdzienicka MZ, Debatisse M, and Lopez BS

Subjects

Animals, BRCA2 Protein biosynthesis, Cell Line, Cell Line, Tumor, Cell Separation, Cricetinae, DNA-Binding Proteins metabolism, Flow Cytometry, Humans, Models, Biological, Models, Genetic, Rad51 Recombinase biosynthesis, DNA Repair, DNA Replication, Recombination, Genetic

Abstract

Faithful genome transmission requires a network of pathways coordinating DNA replication to DNA repair and recombination. Here, we used molecular combing to measure the impact of homologous recombination (HR) on the velocity of DNA replication forks. We used three hamster cell lines defective in HR either by overexpression of a RAD51 dominant-negative form, or by a defect in the RAD51 paralogue XRCC2 or the breast tumor suppressor BRCA2. Irrespectively of the type or extent of HR alteration, all three cell lines exhibited a similar reduction in the rate of replication-fork progression, associated with an increase in the density of replication forks. Importantly, this phenotype was completely reversed in complemented derivatives of Xrcc2 and Brca2 mutants. These data reveal a novel role for HR, different from the reactivation of stalled replication forks, which may play an important role in genome stability and thus in tumor protection.

Published

2008