Article

Effects of EpCAM overexpression on human breast cancer cell lines

BMC Cancer 01/2011; DOI:http://www.doaj.org/doaj?func=openurl&genre=article&issn=14712407&date=2011&volume=11&issue=1&spage=45
Source: DOAJ

ABSTRACT Abstract Background Recently, EpCAM has attracted major interest as a target for antibody- and vaccine-based cancer immunotherapies. In breast cancer, the EpCAM antigen is overexpressed in 30-40% of all cases and this increased expression correlates with poor prognosis. The use of EpCAM-specific monoclonal antibodies is a promising treatment approach in these patients. Methods In order to explore molecular changes following EpCAM overexpression, we investigated changes of the transcriptome upon EpCAM gene expression in commercially available human breast cancer cells lines Hs578T and MDA-MB-231. To assess cell proliferation, a tetrazolium salt based assay was performed. A TCF/LEF Reporter Kit was used to measure the transcriptional activity of the Wnt/β-catenin pathway. To evaluate the accumulation of β-catenin in the nucleus, a subcellular fractionation assay was performed. Results For the first time we could show that expression profiling data of EpCAM transfected cell lines Hs578TEpCAM and MDA-MB-231EpCAM indicate an association of EpCAM overexpression with the downregulation of the Wnt signaling inhibitors SFRP1 and TCF7L2. Confirmation of increased Wnt signaling was provided by a TCF/LEF reporter kit and by the finding of the nuclear accumulation of ß-catenin for MDA-MB-231EpCAM but not Hs578TEpCAM cells. In Hs578T cells, an increase of proliferation and chemosensitivity to Docetaxel was associated with EpCAM overexpression. Conclusions These data show a cell type dependent modification of Wnt signaling components after EpCAM overexpression in breast cancer cell lines, which results in marginal functional changes. Further investigations on the interaction of EpCAM with SFRP1 and TCF7L2 and on additional factors, which may be causal for changes upon EpCAM overexpression, will help to characterize unique molecular properties of EpCAM-positive breast cancer cells.

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Keywords

Abstract Background
 
breast cancer
 
breast cancer cell lines
 
cell type dependent modification
 
EpCAM gene expression
 
EpCAM overexpression
 
EpCAM transfected cell lines Hs578TEpCAM
 
EpCAM-positive breast cancer cells
 
EpCAM-specific monoclonal antibodies
 
expression profiling data
 
increased expression correlates
 
marginal functional changes
 
promising treatment approach
 
subcellular fractionation assay
 
TCF/LEF reporter kit
 
unique molecular properties
 
vaccine-based cancer immunotherapies
 
Wnt signaling components
 
Wnt signaling inhibitors SFRP1
 
Wnt/β-catenin pathway