Title of article
Non-Cell-Autonomous Tumor Suppression by p53
Author/Authors
Amaia Lujambio، نويسنده , , Leila Akkari، نويسنده , , Janelle Simon، نويسنده , , Danielle Grace، نويسنده , , Darjus F. Tschaharganeh، نويسنده , , Jessica E. Bolden، نويسنده , , Zhen Zhao، نويسنده , , Vishal Thapar، نويسنده , , Johanna A. Joyce، نويسنده , , Valery Krizhanovsky، نويسنده , , Scott W. Lowe، نويسنده ,
Issue Information
هفته نامه با شماره پیاپی سال 2013
Pages
12
From page
449
To page
460
Abstract
The p53 tumor suppressor can restrict malignant transformation by triggering cell-autonomous programs of cell-cycle arrest or apoptosis. p53 also promotes cellular senescence, a tumor-suppressive program that involves stable cell-cycle arrest and secretion of factors that modify the tissue microenvironment. In the presence of chronic liver damage, we show that ablation of a p53-dependent senescence program in hepatic stellate cells increases liver fibrosis and cirrhosis associated with reduced survival and enhances the transformation of adjacent epithelial cells into hepatocellular carcinoma. p53-expressing senescent stellate cells release factors that skew macrophage polarization toward a tumor-inhibiting M1-state capable of attacking senescent cells in culture, whereas proliferating p53-deficient stellate cells secrete factors that stimulate polarization of macrophages into a tumor-promoting M2-state and enhance the proliferation of premalignant cells. Hence, p53 can act non-cell autonomously to suppress tumorigenesis by promoting an antitumor microenvironment, in part, through secreted factors that modulate macrophage function.
Journal title
CELL
Serial Year
2013
Journal title
CELL
Record number
1021669
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