Abstract
Background: We have previously shown that overexpression of RANK-c in ER-negative breast cancer cell lines attenuates aggressive properties of cancer cells, partially through a RANK-c/EGFR interaction. EGFR inhibition through TKIs in breast cancer has been tested in triple-negative disease settings with limited clinical benefit for patients. Here we test if expression of RANK-c in ER-negative breast cancer cells in conjunction with treatment with TK inhibitors (erlotinib or gefitinib) can affect survival and colony-forming capacity of cancer cells. Methods: Stably expressing MDA-MB-231-RANK-c and SKBR3-RANK-c cells were employed to test proliferation and colony formation in the presence of TKIs. In addition, Western blot analysis was performed to dissect EGFR related signaling cascades upon TK inhibition in the presence of RANK-c. Results: Interestingly the two RANK-c expressing, ER-negative cells lines presented with a distinct phenotype concerning TKI sensitivity upon treatment. MDA-MB-231-RANK-c cells had a higher sensitivity upon gefitinib treatment, while erlotinib decreased the proliferation rate of SKBR3-RANK-c cells. Further, colony formation assays for MDA-MB-231-RANK-c cells showed a decrease in the number and size of colonies developed in the presence of erlotinib. In addition, RANK-c seems to alter signaling through EGFR after TKI treatment in a cell type-specific manner. Conclusions: Our results indicate that ER-negative breast cancer cells that express RANK-c alter their sensitivity profile against tyrosine kinase inhibitors (erlotinib and gefitinib) in a cell type-specific and culture substrate-dependent manner.
Highlights
Breast cancer is a leading cause of death in women and almost one out of 8 will develop a breast malignancy through their lifetime [1]
The 3-(4,5-dimethylthiazol-2-yl)-2,5-dimethyltetrazolium bromide (MTT) assay and manual cell counting were performed in order to determine whether erlotinib or gefitinib affects the proliferation of RANK isoform c (RANK-c) expressing MDA-MB-231 and SKBR3 cells
We showed that RANK-c interacts with epidermal growth factor receptor (EGFR) receptor in breast cancer cells affecting EGFR phosphorylation status and downstream signaling [10]
Summary
Breast cancer is a leading cause of death in women and almost one out of 8 will develop a breast malignancy through their lifetime [1]. Estrogen receptor (ER) expression divides malignant breast tumors in ER-positive and ER-negative disease groups and these two entities present with fundamentally different biology, clinical course, and response to therapy [2]. EGF receptor can be targeted by multiple tyrosine kinase inhibitors (TKIs) such as erlotinib and gefitinib and by monoclonal antibodies such as cetuximab and panitumumab [7]. Both targeted pharmaceutical approaches have significant clinical results in lung and colon cancer. With the above in mind, in this work we sought to test the response of ER-negative, RANK-c expressing breast cancer cells under EGFR TKI treatment in respect to cell proliferation, colony formation and downstream EGF-related signaling
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