Tamoxifen treatment promotes phosphorylation of the adhesion molecules, p130Cas BCAR1, FAK and Src, via an adhesion-dependent pathway

Tamoxifen treatment promotes phosphorylation of the adhesion molecules, p130Cas BCAR1, FAK and Src, via an adhesion-dependent pathway

Reports that the adhesion-associated molecule p130Cas/BCAR1 promotes resistance to tamoxifen suggested that adhesion-mediated signalling may be altered by tamoxifen treatment. We find that p130Cas/BCAR1 phosphorylation is enhanced in tamoxifen-treated estrogen receptor (ER)-positive MCF-7 breast can...

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Veröffentlicht in:Oncogene 2006-12, Vol.25 (58), p.7597-7607
Hauptverfasser: Cowell, L N, Graham, J D, Bouton, A H, Clarke, C L, O'Neill, G M
Format: Artikel
Sprache:eng
Schlagworte:
Adhesion
AKT protein
Antiestrogens
Antineoplastic Agents, Hormonal - pharmacology
Apoptosis
Biological and medical sciences
Breast cancer
Cell Adhesion Molecules - metabolism
Cell Biology
Cell Line, Tumor
Cell migration
Cell physiology
Cell survival
Cell Survival - drug effects
Cell transformation and carcinogenesis. Action of oncogenes and antioncogenes
Cell viability
Crk-Associated Substrate Protein - metabolism
Estrogen receptors
Estrogens
Focal adhesion kinase
Focal Adhesion Protein-Tyrosine Kinases - metabolism
Fundamental and applied biological sciences. Psychology
Gynecology. Andrology. Obstetrics
Human Genetics
Humans
Internal Medicine
Kinases
Mammary gland diseases
Medical sciences
Medical treatment
Medicine
Medicine & Public Health
Molecular and cellular biology
Oncology
original-article
Phenotypes
Phosphorylation
Phosphorylation - drug effects
Proto-Oncogene Proteins c-akt - metabolism
Proto-Oncogene Proteins pp60(c-src) - metabolism
Receptors, Estrogen - metabolism
Signal transduction
Signal Transduction - drug effects
src-Family Kinases - metabolism
Tamoxifen
Tamoxifen - pharmacology
Tumors
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Zusammenfassung:Reports that the adhesion-associated molecule p130Cas/BCAR1 promotes resistance to tamoxifen suggested that adhesion-mediated signalling may be altered by tamoxifen treatment. We find that p130Cas/BCAR1 phosphorylation is enhanced in tamoxifen-treated estrogen receptor (ER)-positive MCF-7 breast cancer cells. The effects of estrogen and tamoxifen were assessed independently and in combination, and the results demonstrate that tamoxifen antagonizes estrogen regulation of p130Cas/BCAR1 phosphorylation. Phosphorylation correlates with tamoxifen ER antagonist effects, as phosphorylation effects are replicated by the pure antiestrogen ICI 182, 780. Correspondingly, phosphorylation is not changed in ER-negative cells exposed to tamoxifen. We show that deletion of the p130Cas/BCAR1 substrate domain substantially reduces tamoxifen-induced phosphorylation of p130Cas/BCAR1 and confers enhanced sensitivity to tamoxifen. P130Cas/BCAR1 forms a phosphorylation-dependent signalling complex with focal adhesion kinase (FAK) and Src kinase that promotes adhesion-mediated cell survival. Therefore, we examined the kinetics of p130Cas/BCAR1, Src and FAK phosphorylation over a 14-day time course and find sustained phosphorylation of these molecules after 7 days exposure to tamoxifen. Inhibition of Src kinase is shown to reduce tamoxifen-promoted p130Cas/BCAR1 phosphorylation and reduce cell viability. Stimulation of the Src/FAK/p130Cas/BCAR1 adhesion signalling pathway in tamoxifen-treated MCF-7 cells does not cause increased migration; however, there is Src-dependent phosphorylation of the cell survival molecule Akt. Correspondingly, Akt inhibition reduces cell viability in cells treated with tamoxifen. We propose that prolonged activation of adhesion-dependent signalling may confer a survival advantage in response to additional cellular insults or alternatively, may poise cells to develop a migratory phenotype in response to additional cellular cues.
ISSN:0950-9232
1476-5594
DOI:10.1038/sj.onc.1209747