Abstract
Identification and characterization of p53 target genes would lead to a better understanding of p53 functions and p53-mediated signaling pathways. Two putative p53 binding sites were identified in the promoter of a gene encoding PTGF-β, a type β transforming growth factor (TGF-β) superfamily member. Gel shift assay showed that p53 bound to both sites. Luciferase-coupled transactivation assay revealed that the gene promoter was activated in a p53 dose- as well as p53 binding site-dependent manner by wild-type p53 but not by several p53 mutants. The p53 binding and transactivation of the PTGF-β promoter was enhanced by etoposide, a p53 activator, and was largely blocked by a dominant negative p53 mutant. Furthermore, expression of endogenous PTGF-β was remarkably induced by etoposide in p53-positive, but not in p53-negative, cell lines. Finally, the conditioned medium collected from PTGF-β-overexpressing cells, but not from the control cells, suppressed tumor cell growth. Growth suppression was not, however, seen in cells that lack functional TGF-β receptors or Smad4, suggesting that PTGF-β acts through the TGF-β signaling pathway. Thus, PTGF-β, a secretory protein, is a p53 target that could mediate p53-induced growth suppression in autocrinal as well as paracrinal fashions. The finding made a vertical connection between p53 and TGF-β signaling pathways in controlling cell growth and implied a potential important role of p53 in inflammation regulation via PTGF-β.
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Dates
Type | When |
---|---|
Created | 23 years, 1 month ago (July 26, 2002, 10:38 a.m.) |
Deposited | 3 years, 4 months ago (April 13, 2022, 5:19 p.m.) |
Indexed | 1 week, 5 days ago (Aug. 20, 2025, 8:40 a.m.) |
Issued | 25 years, 7 months ago (Jan. 4, 2000) |
Published | 25 years, 7 months ago (Jan. 4, 2000) |
Published Online | 25 years, 7 months ago (Jan. 4, 2000) |
Published Print | 25 years, 7 months ago (Jan. 4, 2000) |
@article{Tan_2000, title={PTGF-β , a type β transforming growth factor (TGF-β) superfamily member, is a p53 target gene that inhibits tumor cell growth via TGF-β signaling pathway}, volume={97}, ISSN={1091-6490}, url={http://dx.doi.org/10.1073/pnas.97.1.109}, DOI={10.1073/pnas.97.1.109}, number={1}, journal={Proceedings of the National Academy of Sciences}, publisher={Proceedings of the National Academy of Sciences}, author={Tan, Mingjia and Wang, Yixin and Guan, Kunliang and Sun, Yi}, year={2000}, month=jan, pages={109–114} }