Oncogene, 2021-02, Vol.40 (6), p.1091-1105
- Swoboda, Alexander
- Soukup, Robert
- Eckel, Oliver
- Kinslechner, Katharina
- Wingelhofer, Bettina
- Schörghofer, David
- Sternberg, Christina
- Pham, Ha T T
- Vallianou, Maria
- Horvath, Jaqueline
- Stoiber, Dagmar
- Kenner, Lukas
- Larue, Lionel
- Poli, Valeria
- Beermann, Friedrich
- Yokota, Takashi
- Kubicek, Stefan
- Krausgruber, Thomas
- Rendeiro, André F
- Bock, Christoph
- Zenz, Rainer
- Kovacic, Boris
- Aberger, Fritz
- Hengstschläger, Markus
- Petzelbauer, Peter
- Mikula, Mario
- Moriggl, Richard
2021
Details
- Autor(en) / Beteiligte
- Swoboda, Alexander
- Soukup, Robert
- Eckel, Oliver
- Kinslechner, Katharina
- Wingelhofer, Bettina
- Schörghofer, David
- Sternberg, Christina
- Pham, Ha T T
- Vallianou, Maria
- Horvath, Jaqueline
- Stoiber, Dagmar
- Kenner, Lukas
- Larue, Lionel
- Poli, Valeria
- Beermann, Friedrich
- Yokota, Takashi
- Kubicek, Stefan
- Krausgruber, Thomas
- Rendeiro, André F
- Bock, Christoph
- Zenz, Rainer
- Kovacic, Boris
- Aberger, Fritz
- Hengstschläger, Markus
- Petzelbauer, Peter
- Mikula, Mario
- Moriggl, Richard
- Titel
- STAT3 promotes melanoma metastasis by CEBP-induced repression of the MITF pathway
- Ist Teil von
- Oncogene, 2021-02, Vol.40 (6), p.1091-1105
- Ort / Verlag
- England: Nature Publishing Group
- Erscheinungsjahr
- 2021
- Link zum Volltext
- Quelle
- Alma/SFX Local Collection
- Beschreibungen/Notizen
- Metastatic melanoma is hallmarked by its ability of phenotype switching to more slowly proliferating, but highly invasive cells. Here, we tested the impact of signal transducer and activator of transcription 3 (STAT3) on melanoma progression in association with melanocyte inducing transcription factor (MITF) expression levels. We established a mouse melanoma model for deleting Stat3 in melanocytes with specific expression of human hyperactive NRAS in an Ink4a-deficient background, two frequent driver mutations in human melanoma. Mice devoid of Stat3 showed early disease onset with higher proliferation in primary tumors, but displayed significantly diminished lung, brain, and liver metastases. Whole-genome expression profiling of tumor-derived cells also showed a reduced invasion phenotype, which was further corroborated by 3D melanoma model analysis. Notably, loss or knockdown of STAT3 in mouse or human cells resulted in the upregulation of MITF and induction of cell proliferation. Mechanistically we show that STAT3-induced CAAT Box Enhancer Binding Protein (CEBP) expression was sufficient to suppress MITF transcription. Epigenetic analysis by ATAC-seq confirmed that CEBPa/b binding to the MITF enhancer region silenced the MITF locus. Finally, by classification of patient-derived melanoma samples, we show that STAT3 and MITF act antagonistically and hence contribute differentially to melanoma progression. We conclude that STAT3 is a driver of the metastatic process in melanoma and able to antagonize MITF via direct induction of CEBP family member transcription.
- Sprache
- Englisch
- Identifikatoren
- ISSN: 0950-9232eISSN: 1476-5594DOI: 10.1038/s41388-020-01584-6Titel-ID: cdi_pubmedcentral_primary_oai_pubmedcentral_nih_gov_7116782
- Format
- –
- Schlagworte
- Analysis, Care and treatment, Cell proliferation, Cells, Cyclin-dependent kinase inhibitors, Development and progression, Epigenetic inheritance, Epigenetics, Gene expression, Genetic aspects, Genomes, Health aspects, INK4 protein, Melanocytes, Melanoma, Metastases, Metastasis, Microphthalmia-associated transcription factor, Phenotypes, Protein binding, Stat3 protein, Tumors