M. Gerbault-Seureau scite author profile

Various studies suggest a tight relationship between chromosome rearrangements driving tumor progression and breaks at loci called common fragile sites. Most of these sites are induced after perturbation of the replication dynamics, notably by aphidicolin treatment. We have mapped the majority of these sites to the interface of R and G bands, which calls into question the previous assignment of aphidicolin-sensitive sites to R bands. This observation suggests that most of them correspond to loci that ensure the transition between early and late replicating domains. We show that calyculin A, which triggers chromosome condensation at any phase of the cell cycle but does not markedly impair replication, induces damage in the chromosomes of human lymphocytes treated in G 2 but not in G1 phase. We demonstrate that these lesions colocalize with those induced by aphidicolin treatment. Hence, common fragile site stability is compromised, whether aphidicolin delays replication or calyculin A advances condensation. We also show that, in cells that go through an unperturbed S phase, completion of their replication and͞or replication-associated chromatin reorganization occur all along the G2 phase, which may explain their inability to condense properly after calyculin A treatment during this phase of the cell cycle.genome instability ͉ DNA damage ͉ calyculin A ͉ aphidicolin ͉ cell cycle

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DNA hypomethylation in breast cancer: An independent parameter of tumor progression?

Bernardino

Roux

Almeida

et al. 1997

Cancer Genetics and Cytogenetics

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M. Gerbault-Seureau

Premature condensation induces breaks at the interface of early and late replicating chromosome bands bearing common fragile sites

DNA hypomethylation in breast cancer: An independent parameter of tumor progression?

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