Title of article
Mutant p53 Drives Invasion by Promoting Integrin Recycling
Author/Authors
Patricia A.J. Muller، نويسنده , , Patrick T. Caswell، نويسنده , , Brendan Doyle، نويسنده , , Marcin P. Iwanicki، نويسنده , , Ee H. Tan، نويسنده , , Saadia Karim، نويسنده , , Natalia Lukashchuk، نويسنده , , David A. Gillespie، نويسنده , , Robert L. Ludwig، نويسنده , , Pauline Gosselin، نويسنده , , Anne Cromer، نويسنده , , Joan S. Brugge، نويسنده , , Owen J. Sansom، نويسنده , , Jim C. Norman، نويسنده , , Karen H. Vousden، نويسنده ,
Issue Information
هفته نامه با شماره پیاپی سال 2009
Pages
15
From page
1327
To page
1341
Abstract
p53 is a tumor suppressor protein whose function is frequently lost in cancers through missense mutations within the Tp53 gene. This results in the expression of point-mutated p53 proteins that have both lost wild-type tumor suppressor activity and show gain of functions that contribute to transformation and metastasis. Here, we show that mutant p53 expression can promote invasion, loss of directionality of migration, and metastatic behavior. These activities of p53 reflect enhanced integrin and epidermal growth factor receptor (EGFR) trafficking, which depends on Rab-coupling protein (RCP) and results in constitutive activation of EGFR/integrin signaling. We provide evidence that mutant p53 promotes cell invasion via the inhibition of TAp63, and simultaneous loss of p53 and TAp63 recapitulates the phenotype of mutant p53 in cells. These findings open the possibility that blocking alpha5/beta1-integrin and/or the EGF receptor will have therapeutic benefit in mutant p53-expressing cancers.
Journal title
CELL
Serial Year
2009
Journal title
CELL
Record number
1020140
Link To Document