Src Drives Growth of Antiestrogen Resistant Breast Cancer Cell Lines and Is a Marker for Reduced Benefit of Tamoxifen Treatment

The underlying mechanisms leading to antiestrogen resistance in estrogen-receptor α (ER)-positive breast cancer is still poorly understood. The aim of this study was therefore to identify biomarkers and novel treatments for antiestrogen resistant breast cancer. We performed a kinase inhibitor screen...

Descripción completa

Detalles Bibliográficos
Autores principales: Larsen, Sarah L., Laenkholm, Anne-Vibeke, Duun-Henriksen, Anne Katrine, Bak, Martin, Lykkesfeldt, Anne E., Kirkegaard, Tove
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4338193/
https://www.ncbi.nlm.nih.gov/pubmed/25706943
http://dx.doi.org/10.1371/journal.pone.0118346
_version_ 1782481164941918208
author Larsen, Sarah L.
Laenkholm, Anne-Vibeke
Duun-Henriksen, Anne Katrine
Bak, Martin
Lykkesfeldt, Anne E.
Kirkegaard, Tove
author_facet Larsen, Sarah L.
Laenkholm, Anne-Vibeke
Duun-Henriksen, Anne Katrine
Bak, Martin
Lykkesfeldt, Anne E.
Kirkegaard, Tove
author_sort Larsen, Sarah L.
collection PubMed
description The underlying mechanisms leading to antiestrogen resistance in estrogen-receptor α (ER)-positive breast cancer is still poorly understood. The aim of this study was therefore to identify biomarkers and novel treatments for antiestrogen resistant breast cancer. We performed a kinase inhibitor screen on antiestrogen responsive T47D breast cancer cells and T47D-derived tamoxifen and fulvestrant resistant cell lines. We found that dasatinib, a broad-spectrum kinase inhibitor, inhibited growth of the antiestrogen resistant cells compared to parental T47D cells. Furthermore western blot analysis showed increased expression and phosphorylation of Src in the resistant cells and that dasatinib inhibited phosphorylation of Src and also signaling via Akt and Erk in all cell lines. Immunoprecipitation revealed Src: ER complexes only in the parental T47D cells. In fulvestrant resistant cells, Src formed complexes with the Human Epidermal growth factor Receptor (HER)1 and HER2. Neither HER receptors nor ER were co-precipitated with Src in the tamoxifen resistant cell lines. Compared to treatment with dasatinib alone, combined treatment with dasatinib and fulvestrant had a stronger inhibitory effect on tamoxifen resistant cell growth, whereas dasatinib in combination with tamoxifen had no additive inhibitory effect on fulvestrant resistant growth. When performing immunohistochemical staining on 268 primary tumors from breast cancer patients who had received tamoxifen as first line endocrine treatment, we found that membrane expression of Src in the tumor cells was significant associated with reduced disease-free and overall survival. In conclusion, Src was identified as target for treatment of antiestrogen resistant T47D breast cancer cells. For tamoxifen resistant T47D cells, combined treatment with dasatinib and fulvestrant was superior to treatment with dasatinib alone. Src located at the membrane has potential as a new biomarker for reduced benefit of tamoxifen.
format Online
Article
Text
id pubmed-4338193
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-43381932015-03-04 Src Drives Growth of Antiestrogen Resistant Breast Cancer Cell Lines and Is a Marker for Reduced Benefit of Tamoxifen Treatment Larsen, Sarah L. Laenkholm, Anne-Vibeke Duun-Henriksen, Anne Katrine Bak, Martin Lykkesfeldt, Anne E. Kirkegaard, Tove PLoS One Research Article The underlying mechanisms leading to antiestrogen resistance in estrogen-receptor α (ER)-positive breast cancer is still poorly understood. The aim of this study was therefore to identify biomarkers and novel treatments for antiestrogen resistant breast cancer. We performed a kinase inhibitor screen on antiestrogen responsive T47D breast cancer cells and T47D-derived tamoxifen and fulvestrant resistant cell lines. We found that dasatinib, a broad-spectrum kinase inhibitor, inhibited growth of the antiestrogen resistant cells compared to parental T47D cells. Furthermore western blot analysis showed increased expression and phosphorylation of Src in the resistant cells and that dasatinib inhibited phosphorylation of Src and also signaling via Akt and Erk in all cell lines. Immunoprecipitation revealed Src: ER complexes only in the parental T47D cells. In fulvestrant resistant cells, Src formed complexes with the Human Epidermal growth factor Receptor (HER)1 and HER2. Neither HER receptors nor ER were co-precipitated with Src in the tamoxifen resistant cell lines. Compared to treatment with dasatinib alone, combined treatment with dasatinib and fulvestrant had a stronger inhibitory effect on tamoxifen resistant cell growth, whereas dasatinib in combination with tamoxifen had no additive inhibitory effect on fulvestrant resistant growth. When performing immunohistochemical staining on 268 primary tumors from breast cancer patients who had received tamoxifen as first line endocrine treatment, we found that membrane expression of Src in the tumor cells was significant associated with reduced disease-free and overall survival. In conclusion, Src was identified as target for treatment of antiestrogen resistant T47D breast cancer cells. For tamoxifen resistant T47D cells, combined treatment with dasatinib and fulvestrant was superior to treatment with dasatinib alone. Src located at the membrane has potential as a new biomarker for reduced benefit of tamoxifen. Public Library of Science 2015-02-23 /pmc/articles/PMC4338193/ /pubmed/25706943 http://dx.doi.org/10.1371/journal.pone.0118346 Text en © 2015 Larsen et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Larsen, Sarah L.
Laenkholm, Anne-Vibeke
Duun-Henriksen, Anne Katrine
Bak, Martin
Lykkesfeldt, Anne E.
Kirkegaard, Tove
Src Drives Growth of Antiestrogen Resistant Breast Cancer Cell Lines and Is a Marker for Reduced Benefit of Tamoxifen Treatment
title Src Drives Growth of Antiestrogen Resistant Breast Cancer Cell Lines and Is a Marker for Reduced Benefit of Tamoxifen Treatment
title_full Src Drives Growth of Antiestrogen Resistant Breast Cancer Cell Lines and Is a Marker for Reduced Benefit of Tamoxifen Treatment
title_fullStr Src Drives Growth of Antiestrogen Resistant Breast Cancer Cell Lines and Is a Marker for Reduced Benefit of Tamoxifen Treatment
title_full_unstemmed Src Drives Growth of Antiestrogen Resistant Breast Cancer Cell Lines and Is a Marker for Reduced Benefit of Tamoxifen Treatment
title_short Src Drives Growth of Antiestrogen Resistant Breast Cancer Cell Lines and Is a Marker for Reduced Benefit of Tamoxifen Treatment
title_sort src drives growth of antiestrogen resistant breast cancer cell lines and is a marker for reduced benefit of tamoxifen treatment
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4338193/
https://www.ncbi.nlm.nih.gov/pubmed/25706943
http://dx.doi.org/10.1371/journal.pone.0118346
work_keys_str_mv AT larsensarahl srcdrivesgrowthofantiestrogenresistantbreastcancercelllinesandisamarkerforreducedbenefitoftamoxifentreatment
AT laenkholmannevibeke srcdrivesgrowthofantiestrogenresistantbreastcancercelllinesandisamarkerforreducedbenefitoftamoxifentreatment
AT duunhenriksenannekatrine srcdrivesgrowthofantiestrogenresistantbreastcancercelllinesandisamarkerforreducedbenefitoftamoxifentreatment
AT bakmartin srcdrivesgrowthofantiestrogenresistantbreastcancercelllinesandisamarkerforreducedbenefitoftamoxifentreatment
AT lykkesfeldtannee srcdrivesgrowthofantiestrogenresistantbreastcancercelllinesandisamarkerforreducedbenefitoftamoxifentreatment
AT kirkegaardtove srcdrivesgrowthofantiestrogenresistantbreastcancercelllinesandisamarkerforreducedbenefitoftamoxifentreatment

Ejemplares similares