p63 and p73: p53 mimics, menaces and more
- 1 December 2000
- journal article
- review article
- Published by Springer Science and Business Media LLC in Nature Reviews Molecular Cell Biology
- Vol. 1 (3), 199-207
- https://doi.org/10.1038/35043127
Abstract
Inactivation of the tumour suppressor p53 is the most common defect in cancer cells. The discovery of its two close relatives, p63 and p73, was therefore both provocative and confounding. Were these new genes tumour suppressors, p53 regulators, or evolutionary spin-offs? Both oncogenic and tumour-suppressor properties have now been attributed to the p53 homologues, perhaps reflecting the complex, often contradictory, protein products encoded by these genes. p63 and p73 are further implicated in many p53-independent pathways, including stem-cell regeneration, neurogenesis and sensory processes.Keywords
This publication has 49 references indexed in Scilit:
- Physical Interaction between Wilms Tumor 1 and p73 Proteins Modulates Their FunctionsJournal of Biological Chemistry, 2000
- Adenovirus‐mediated Transfer of p53‐related Genes Induces Apoptosis of Human Cancer CellsJapanese Journal of Cancer Research, 2000
- Mdm2 binds p73α without targeting degradationOncogene, 1999
- Infrequent somatic mutations of thep73genein various human cancersEuropean Journal of Surgical Oncology, 1999
- The p53 tumour suppressor geneBritish Journal of Surgery, 1998
- Cajal—Retzius cells, Reelin, and the formation of layersCurrent Opinion in Neurobiology, 1998
- Epidermal stem cells: markers, patterning and the control of stem cell fatePhilosophical Transactions Of The Royal Society B-Biological Sciences, 1998
- Tumor spectrum analysis in p53-mutant miceCurrent Biology, 1994
- Mice deficient for p53 are developmentally normal but susceptible to spontaneous tumoursNature, 1992
- Three clonal types of keratinocyte with different capacities for multiplication.Proceedings of the National Academy of Sciences, 1987