Title of article
p53-Dependent repression of focal adhesion kinase in response to estradiol in breast cancer cell-lines
Author/Authors
Anaganti، نويسنده , , Suresh and Fernلndez-Cuesta، نويسنده , , Lynnette and Langerّd، نويسنده , , Anita and Hainaut، نويسنده , , Pierre and Olivier، نويسنده , , Magali، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2011
Pages
10
From page
215
To page
224
Abstract
Mutations in the TP53 suppressor gene are frequent in breast cancers. These mutations are associated with poor prognosis, thought to be due to proliferative advantage and poor response to chemotherapy associated with loss of p53 function. The focal adhesion kinase (FAK/PTK2), a tyrosine kinase, is over-expressed in a variety of human tumors including breast cancers. FAK is a critical regulator of adhesion and motility and its over-expression is associated with increased metastatic potential. Recently, FAK promoter has been shown to contain p53 responsive elements and to be down-regulated by DNA-damage in a p53-dependent manner. Here, we have used five estrogen-dependent breast cancer cells lines with different p53 status, including an isogenic model, to show that FAK expression was regulated in a p53-dependent manner in response to estradiol. FAK protein and mRNA expression were down-regulated by estradiol in wild-type but not mutant p53 cells. Moreover, silencing wild-type p53 increased FAK expression, while over expressing p53 repressed FAK expression. ChIP experiment showed that p53 bound to FAK promoter in the presence of estradiol in p53 wild-type but not in mutant p53 cells, suggesting a direct role of p53 in down regulating FAK mRNA expression. FAK mRNA expression was also found to correlate with TP53 mutation status in a series of breast tumors. Finally, loss of FAK down-regulation in p53 mutant cells was correlated with increased proliferation and invasion upon estradiol stimulation, while FAK silencing reduced invasion. These results suggest that p53 is an important down regulator of FAK and that loss of p53 function in breast cancer may contribute to the metastatic potential of estrogen-responsive tumors through uncontrolled FAK expression upon estrogens stimulation.
Keywords
PTK2 , FAK , transcriptional repression , p53 , breast cancer , Mutation , Estrogens
Journal title
Cancer Letters
Serial Year
2011
Journal title
Cancer Letters
Record number
1819490
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