Signalling to p53: where does it all start?
- 1 August 1996
- Vol. 18 (8), 617-619
- https://doi.org/10.1002/bies.950180804
Abstract
Alterations in the p53 gene product appear to be a major factor in human tumorigenesis and may influence the responses of many human tumors to therapy. Much effort has focused on understanding the signals which normally initiate p53 growth‐suppressive functions. Though it has been known that DNA damage can induce p53, a recent publication reports data which suggest that p53 can be induced by depletion of ribonucleotide pools, even in the absence of detectable DNA damage(1). These observations provide new ideas about how cells utilize the p53 signal and open up new avenues of investigation for manipulating p53 function.Keywords
This publication has 26 references indexed in Scilit:
- Hypoxia-mediated selection of cells with diminished apoptotic potential in solid tumoursNature, 1996
- Activation of p53 sequence-specific DNA bindingby short single strands of DNA requires the p53 C-terminusCell, 1995
- Deficiency of p53 accelerates mammary tumorigenesis in Wnt-1 transgenic mice and promotes chromosomal instability.Genes & Development, 1995
- p53-deficient mice are extremely susceptible to radiation-induced tumorigenesisNature Genetics, 1994
- p53-Dependent apoptosis suppresses tumor growth and progression in vivoCell, 1994
- Differential induction of transcriptionally active p53 following UV or lonizing radiation: Defects in chromosome instability syndromes?Cell, 1993
- Thymocyte apoptosis induced by p53-dependent and independent pathwaysNature, 1993
- p53 is required for radiation-induced apoptosis in mouse thymocytesNature, 1993
- Mice deficient for p53 are developmentally normal but susceptible to spontaneous tumoursNature, 1992
- Participation of p53 cellular tumour antigen in transformation of normal embryonic cellsNature, 1984