Role of wild type p53 in the G2 phase: regulation of the γirradiation-induced delay and DNA repair (original) (raw)

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• Published: 20 November 1997

Oncogene volume 15, pages 2597–2607 (1997)Cite this article

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Abstract

Up-regulation of the p53 protein was found to induce cell cyle arrest at the G1/S border and in some cases at the G2/M border. Futhermore, it was suggested that p53 is associated with the induction of the various DNA repair pathways. Previously, we demonstrated that cells coexpressing endogenous wild type p53 protein, together with dominant negative mutant p53, exhibit deregulation of apoptosis, G1 arrest and delay in G2 following γ-irradiation. IN the present study, we investigated the role of p53 protein in the DNA damage response at the G2 phase. Using p53-null, wild type p53 and mutant p53-producer cell lines, we found that the two C-terminally spliced p53 forms could prevent γ-irradiation induced muatgenesis prior to mitosis, at the G2/M checkpoint. We found that at the G2 phase, p53 may facilitate repair of DNA breaks giving rise to micronuclei, and regulate the exit from the G2 checkpoint. At the G1 phase, only the regularly spliced form of p53 caused growth arrrest. In contrast, both the regularly and the alternatively spliced p53 forms directed postmitotic micronucleated cells towards apoptosis. These results provide a functional explanation for the cell cycle-independent expression of p53 in mnormal cycling cells, as well as in cells where p53 is up-regulated, following DNA damage.

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Authors and Affiliations

1. Department of Molecular Cell Biology, Weizmann Institute of Science, Rehevot, Israel
   Dov Schwartz, Nava Almog, Amnon Peled, Naomi Goldfinger & Varda Rotter

Authors

1. Dov Schwartz
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2. Nava Almog
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3. Amnon Peled
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4. Naomi Goldfinger
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5. Varda Rotter
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Schwartz, D., Almog, N., Peled, A. et al. Role of wild type p53 in the G2 phase: regulation of the γirradiation-induced delay and DNA repair.Oncogene 15, 2597–2607 (1997). https://doi.org/10.1038/sj.onc.1201436

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• Received: 29 April 1997
• Revised: 18 July 1997
• Accepted: 21 July 1997
• Issue Date: 20 November 1997
• DOI: https://doi.org/10.1038/sj.onc.1201436

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