Retinoic acid receptor ? (RAR?) is a transcription factor that plays an
essential role in tumor progression. Triple-negative breast cancer (TNBC) is
a subtype of breast carcinoma with a poor prognosis due to early therapeutic
escape from conventional treatments and aggressive metastatic relapse by the
occurrence of an epithelial-mesenchymal transition (EMT). However, as the
expression level of RAR? does not correlate with the overall survival of
TNBC patients, we speculate that post-translational modification such as
phosphorylation of RAR? may be involved in EMT and TNBC metastasis. After
overexpressing a phosphorylation-defective mutant of RAR? at serine 77
residue (RAR?S77A), we found that RAR? hypophosphorylation inhibited
MDA-MB-231 cell motility and migration in vitro while reducing the lung
metastatic potential in vivo. This was accompanied by increased expression
of the epithelial marker E-cadherin and decreased expression of the
mesenchymal markers ?-catenin and zinc finger E-box-binding homeobox 1
(ZEB1) in agreement with the suppression of EMT. Interestingly, the
overexpression of wild-type RAR? in the presence of the RAR? agonist AM580
failed to suppress EMT and cell migration. These results indicate that
hypophosphorylated RAR?S77 can directly mimic activated RAR? to inhibit EMT
and migration/invasion of cells, thus providing a novel target in the
therapeutic intervention of TNBC.
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