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Blogger's Note: the EpCAM gene is also tested in Lynch Syndrome patients/families
Abstract:
Background:
The epithelial cell
adhesion molecule (EpCAM) is overexpressed on most carcinomas. Dependent
on the tumour type, its overexpression is either associated with
improved or worse patient survival. For ovarian cancer, however, the
role of EpCAM remains unclear.
Conclusion:
The
bidirectional ATF-based approach is uniquely suited to study
cell-type-specific biological effects of EpCAM expression. Using this
approach, the oncogenic function of EpCAM in breast cancer was
confirmed. Despite its value as a diagnostic marker and for
immunotherapy, EpCAM does not seem to represent a therapeutic target for
gene expression silencing in ovarian cancer.
Methods:
Cell survival of ovarian cancer cell lines was studied after induction or repression of endogenous EpCAM expression using siRNA/cDNA
or artificial transcription factors (ATF) consisting of engineered
zinc-fingers fused to either a transcriptional activator or repressor
domain.
Results:
Two ATFs
were selected as the most potent down- and upregulator, showing at least
a two-fold alteration of EpCAM protein expression compared with
control. Downregulation of EpCAM expression resulted in growth
inhibition in breast cancer, but showed no effect on cell growth in
ovarian cancer. Induction or further upregulation of EpCAM expression
decreased ovarian cancer cell survival.
Conclusion:
The
bidirectional ATF-based approach is uniquely suited to study
cell-type-specific biological effects of EpCAM expression. Using this
approach, the oncogenic function of EpCAM in breast cancer was
confirmed. Despite its value as a diagnostic marker and for
immunotherapy, EpCAM does not seem to represent a therapeutic target for
gene expression silencing in ovarian cancer.
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