Permanent cell cycle exit in G2 phase after DNA damage in normal human fibroblasts - Université de Montpellier
Article Dans Une Revue EMBO Journal Année : 2003

Permanent cell cycle exit in G2 phase after DNA damage in normal human fibroblasts

Résumé

Although the Cdk inhibitor p21(Waf1/Cip1), one of the transcriptional targets of p53, has been implicated in the maintenance of G(2) arrest after DNA damage, its function at this stage of the cell cycle is not really understood. Here, we show that the exposure of normal human fibroblasts (NHFs) to genotoxic agents provokes permanent cell cycle exit in G(2) phase, whereas mouse embryo fibroblasts and transformed human cells progress through mitosis and arrest in G(1) without intervening cytokinesis. p21(Waf1/Cip1) exerts a key role in driving this G(2) exit both by inhibiting cyclin B1-Cdk1 and cyclin A-Cdk1/2 complexes, which control G(2)/M progression, and by blocking the phosphorylation of pRb family proteins. NHFs with compromised pRb proteins could still efficiently arrest in G(2) but were unable to exit the cell cycle, resulting in cell death. Our experiments show that, when under continuous genotoxic stress, normal cells can reverse their commitment to mitotic progression due to passage through the restriction point and that mechanisms involving p21(Waf1/Cip1) and pocket proteins can induce exit in G(2) and G(1).

Dates et versions

hal-03763240 , version 1 (29-08-2022)

Identifiants

Citer

Fabienne Baus, Véronique Gire, Daniel Fisher, Jacques Piette, Vjekoslav Dulic. Permanent cell cycle exit in G2 phase after DNA damage in normal human fibroblasts. EMBO Journal, 2003, 22 (15), pp.3992-4002. ⟨10.1093/emboj/cdg387⟩. ⟨hal-03763240⟩
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