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Post‐transcriptional regulation controlled by E‐cadherin is important for c‐Jun activity in melanoma
Author(s) -
Spangler B.,
Vardimon L.,
Bosserhoff A. K.,
Kuphal S.
Publication year - 2011
Publication title -
pigment cell and melanoma research
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.618
H-Index - 105
eISSN - 1755-148X
pISSN - 1755-1471
DOI - 10.1111/j.1755-148x.2010.00787.x
Subject(s) - cadherin , melanoma , cancer research , c jun , transcriptional activity , microbiology and biotechnology , transcription factor , biology , genetics , gene , cell
Summary A central event in the development of malignant melanoma is the loss of the tumor‐suppressor protein E‐cadherin. Here, we report that this loss is linked to the activation of the proto‐oncogene c‐Jun, a key player in tumorigenesis. In vivo , malignant melanomas show strong expression of the c‐Jun protein in contrast to melanocytes. Interestingly, c‐Jun mRNA levels did not differ in the melanoma cell lines when compared to melanocytes, suggesting that c‐Jun could be regulated at the post‐transcriptional level. To uncover the link between E‐cadherin and c‐Jun, we re‐expressed E‐cadherin in melanoma cells and detected decreased protein expression and activity of c‐Jun. Furthermore, c‐Jun accumulation is dependent on active E‐cadherin‐mediated cell–cell adhesion and regulated via the cytoskeleton. Additionally, we determined that, with respect to c‐Jun regulation, there are two melanoma subgroups. One subgroup regulates c‐Jun expression via the newly discovered E‐cadherin‐dependent signaling pathway, whereas the other subgroup uses the MAPKinases to regulate its expression. In summary, our data provide novel insights into the tumor‐suppressor function of E‐cadherin, which contributes to the suppression of c‐Jun protein translation and transcriptional activity independent of MAPKinases.