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ER? decreases the invasiveness of triple-negative breast cancer cells by regulating mutant p53 oncogenic function.


ABSTRACT: Most (80%) of the triple-negative breast cancers (TNBCs) express mutant p53 proteins that acquire oncogenic activities including promoting metastasis. We previously showed that wild-type ER? (ER?1) impedes epithelial to mesenchymal transition (EMT) and decreases the invasiveness of TNBC cells. In the present study we searched for signaling pathways that ER?1 uses to inhibit EMT and invasion in TNBC cells. We show that ER?1 binds to and opposes the transcriptional activity of mutant p53 at the promoters of genes that regulate metastasis. p63 that transcriptionally cooperates with mutant p53 also binds to ER?1. Downregulation of p63 represses the epithelial phenotype of ER?1-expressing cells and alters the expression of mutant p53 target genes. These results describe a novel mechanism through which ER?1 can disturb oncogenic signals to inhibit aggressiveness in TNBCs.

SUBMITTER: Bado I 

PROVIDER: S-EPMC4924664 | biostudies-literature | 2016 Mar

REPOSITORIES: biostudies-literature

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ERβ decreases the invasiveness of triple-negative breast cancer cells by regulating mutant p53 oncogenic function.

Bado Igor I   Nikolos Fotis F   Rajapaksa Gayani G   Gustafsson Jan-Åke JÅ   Thomas Christoforos C  

Oncotarget 20160301 12


Most (80%) of the triple-negative breast cancers (TNBCs) express mutant p53 proteins that acquire oncogenic activities including promoting metastasis. We previously showed that wild-type ERβ (ERβ1) impedes epithelial to mesenchymal transition (EMT) and decreases the invasiveness of TNBC cells. In the present study we searched for signaling pathways that ERβ1 uses to inhibit EMT and invasion in TNBC cells. We show that ERβ1 binds to and opposes the transcriptional activity of mutant p53 at the pr  ...[more]

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