The p53 family: same response, different signals?

Chen X

doi:10.1016/s1357-4310(99)01545-2

Abstract

TP53, the gene that encodes p53, is a well-defined tumor suppressor gene that is frequently mutated in human cancers. Recently, two proteins homologous to p53, termed p73 and p63, were identified. Current data indicate that both p73 and p63, like p53, can induce cell-cycle arrest and apoptosis, suggesting that they might also be tumor suppressors. However, the physiological signals that can regulate p53, for example, DNA damage, have no effect on p73, as tested in several cell lines. Furthermore, the signaling pathways by which p73 (and possibly p63) induces cell-cycle arrest and apoptosis appear to be similar to those of p53, but also have important differences. Thus, the p53 family proteins are closely related but might have distinct physiological functions.

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References

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NCI NIH HHS (1)

Grant ID: CA81237
3 publications

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The p53 family: same response, different signals?

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Abstract

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References

Monoallelically expressed gene related to p53 at 1p36, a region frequently deleted in neuroblastoma and other human cancers.

p63, a p53 homolog at 3q27-29, encodes multiple products with transactivating, death-inducing, and dominant-negative activities.

A new human p53 homologue.

Cloning and functional analysis of human p51, which structurally and functionally resembles p53.

Cloning and chromosomal mapping of the human p53-related KET gene to chromosome 3q27 and its murine homolog Ket to mouse chromosome 16.

A second p53-related protein, p73L, with high homology to p73.

Lee, L.A. et al. Characterization of an autoantigen associated with chronic ulcerative stomatitis: the CUSP autoantigen is a member of the p53 family, J. Invest. Dermatol. (in press)

p53CP, a putative p53 competing protein that specifically binds to the consensus p53 DNA binding sites: a third member of the p53 family?

Non-p53 p53RE binding protein, a human transcription factor functionally analogous to P53.

The human tumour suppressor gene p53 is alternatively spliced in normal cells.

Citations & impact

Impact metrics

Citations of article over time

Smart citations by scite.ai
Explore citation contexts and check if this article has been supported or disputed.
https://scite.ai/reports/10.1016/s1357-4310(99)01545-2

Article citations

Differential targeting of the cyclin-dependent kinase inhibitor, p21CIP1/WAF1, by chelators with anti-proliferative activity in a range of tumor cell-types.

Transcriptional activity of TAp63 promoter is regulated by c-jun.

NSP 5a3a: a potential novel cancer target in head and neck carcinoma.

Cancer biomarker discovery: the entropic hallmark.

Radiation biology of Caenorhabditis elegans: germ cell response, aging and behavior.

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Search life-sciences literature (45,105,671 articles, preprints and more)

The p53 family: same response, different signals?

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References

Lee, L.A. et al. Characterization of an autoantigen associated with chronic ulcerative stomatitis: the CUSP autoantigen is a member of the p53 family, J. Invest. Dermatol. (in press)

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NCI NIH HHS (1)﻿

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NCI NIH HHS (1)