Outcomes of p53 activation - spoilt for choice
Author:
Affiliation:
1. Beatson Institute for Cancer Research, Garscube Estate, Switchback Road, Bearsden, Glasgow G61 1BD, UK
Abstract
Publisher
The Company of Biologists
Subject
Cell Biology
Link
http://journals.biologists.com/jcs/article-pdf/119/24/5015/1513607/5015.pdf
Reference54 articles.
1. Bensaad, K., Tsuruta, A., Selak, M. A., Vidal, M. N., Nakano, K., Bartrons, R., Gottlieb, E. and Vousden, K. H. (2006). TIGAR, a p53-inducible regulator of glycolysis and apoptosis. Cell126, 107-120.
2. Bergamaschi, D., Samuels-Lev, Y., O'Neil, N. J., Trigiante, G., Crook, T., Hseih, J. K., O'Conner, D. J., Zhong, S., Compargue, I., Tomlinson, M. L. et al. (2003). iASPP oncoprotein is a key inhibitor of p53 conserved from worms to humans. Nat. Genet.33, 162-167.
3. Bergamaschi, D., Samuels, Y., Jin, B., Duraisingham, S., Crook, T. and Lu, X. (2004). ASPP1 and ASPP2: common activators of p53 family members. Mol. Cell. Biol.24, 1341-1350.
4. Blattner, C., Sparks, A. and Lane, D. (1999). Transcription factor E2F-1 is upregulated in response to DNA damage in a manner analogous to that of p53. Mol. Cell. Biol.19, 3704-3713.
5. Budanov, A. V., Sablina, A. A., Feinstein, E., Koonin, E. V. and Chumakov, P. M. (2004). Regeneration of peroxiredoxins by p53-regulated sestrins, homologs of bacterial AhpD. Science304, 596-600.
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