Gene/Protein
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Drug
Enzyme
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Pivot Concepts:
Gene/Protein
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Target Concepts:
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Query: UNIPROT:P04637 (
p53
)
77,613
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Clone 112 cells, a rat embryo fibroblast cell line cotransfected by an activated ras gene and a temperature-sensitive mutant p53 gene (p53val135) grow well at 37 degrees C but cease DNA synthesis and cell division when shifted to 32 degrees C (Michalovitz, D., Halevy, O., and Oren, M. (1990) Cell 62, 671-680). Characterization of the
p53 protein
in exponentially growing
clone 112
cells at 37 degrees C revealed that both wild-type (reactive with the monoclonal antibody PAb 246) and mutant (reactive with PAb 240)
p53
conformational forms are co-expressed. These results indicate that in
clone 112
cells the growth suppressor activity of the wild-type
p53
species is inactivated at 37 degrees C. We show that
clone 112
cells grown at 37 degrees C elicits specific growth inhibition response to stimulation by the tumor promoter phorbol ester, phorbol 12-myristate 13-acetate (PMA). At 37 degrees C, PMA induced nuclear accumulation of the
p53 protein
, a behavior that is also observed in growth-arrested cells at 32 degrees C. Furthermore, when cells are growth arrested at 32 degrees C, PMA prevented the cells from re-entering the cell cycle when they are shifted back to 37 degrees C. All these observations suggest that PMA can cooperate with the wild-type
p53
in cell growth arrest. At 37 and 32 degrees C, PMA stimulation of
clone 112
cells resulted in specific enhancement of phosphorylation of the wild-type
p53
species but not of the mutant form. We also demonstrate that the growth arrest of
clone 112
cells at 37 degrees C is correlated with stimulation of the nuclear wild-type
p53
-DNA binding activities. The PMA-mediated increase in
p53
DNA binding activity coincides with the loss of the PAb 421 epitope on the
p53
.DNA complex. PAb 421 non-reactivity with
p53
has been shown by others to occur in growth-arrested cells and upon phosphorylation of
p53
by protein kinase C. We also provide evidence that, in vitro, the protein kinase C mode of phosphorylation stimulates DNA binding activities of purified recombinant wild-type
p53
and that in a mutant conformation
p53
is not a substrate for protein kinase C. We propose that wild-type
p53
and protein kinase C, the cellular receptor of phorbol ester, could participate in the negative feedback controls associated with the phosphoinositide-derived signals common to a number of mitogenic stimulations.
...
PMID:The protein kinase C activator, phorbol ester, cooperates with the wild-type p53 species of Ras-transformed embryo fibroblasts growth arrest. 796 44
