| Literature DB >> 25454946 |
Giulio Di Minin1, Arianna Bellazzo2, Marco Dal Ferro2, Giulia Chiaruttini3, Simona Nuzzo4, Silvio Bicciato4, Silvano Piazza1, Damiano Rami5, Roberta Bulla5, Roberta Sommaggio6, Antonio Rosato7, Giannino Del Sal2, Licio Collavin8.
Abstract
Inflammation is a significant factor in cancer development, and a molecular understanding of the parameters dictating the impact of inflammation on cancers could significantly improve treatment. The tumor suppressor p53 is frequently mutated in cancer, and p53 missense mutants (mutp53) can acquire oncogenic properties. We report that cancer cells with mutp53 respond to inflammatory cytokines increasing their invasive behavior. Notably, this action is coupled to expression of chemokines that can expose the tumor to host immunity, potentially affecting response to therapy. Mechanistically, mutp53 fuels NF-κB activation while it dampens activation of ASK1/JNK by TNFα, and this action depends on mutp53 binding and inhibiting the tumor suppressor DAB2IP in the cytoplasm. Interfering with such interaction reduced aggressiveness of cancer cells in xenografts. This interaction is an unexplored mechanism by which mutant p53 can influence tumor evolution, with implications for our understanding of the complex role of inflammation in cancer.Entities:
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Year: 2014 PMID: 25454946 DOI: 10.1016/j.molcel.2014.10.013
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 17.970