| Literature DB >> 25341426 |
Susanne Knoll1, Katharina Fürst1, Bhavani Kowtharapu1, Ulf Schmitz2, Stephan Marquardt1, Olaf Wolkenhauer2, Hubert Martin3, Brigitte M Pützer4.
Abstract
Malignant melanoma is highly lethal due to its aggressive invasive properties and metastatic dissemination. The transcription factor E2F1 is crucial for melanoma progression through poorly understood mechanisms. Here, we show that the miR-224/miR-452 cluster is significantly increased in advanced melanoma and invasive/metastatic cell lines that express high levels of E2F1. miR-224/miR-452 expression is directly activated by E2F1 through transactivation of the GABRE gene. Ectopic expression of miR-224/miR-452 in less aggressive cells induces EMT and cytoskeletal rearrangements and enhances migration/invasion. Conversely, miR-224/miR-452 depletion in metastatic cells induces the reversal of EMT, inhibition of motility, loss of the invasive phenotype and an absence of lung metastases in mice. We identify the metastasis suppressor TXNIP as new target of miR-224/miR-452 that induces feedback inhibition of E2F1 and show that miR-224/452-mediated downregulation of TXNIP is essential for E2F1-induced EMT and invasion. The E2F1-miR-224/452-TXNIP axis constitutes a molecular signature that predicts patient survival and may help to set novel therapies.Entities:
Keywords: E2F1 transcription factor; epithelial‐mesenchymal transition; melanoma metastasis; miRNA cluster; thioredoxin‐interacting protein
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Year: 2014 PMID: 25341426 PMCID: PMC4264934 DOI: 10.15252/embr.201439392
Source DB: PubMed Journal: EMBO Rep ISSN: 1469-221X Impact factor: 8.807