miR-638 promotes melanoma metastasis and protects melanoma cells from apoptosis and autophagy

نویسندگان

  • Animesh Bhattacharya
  • Ulf Schmitz
  • Yvonne Raatz
  • Madeleine Schönherr
  • Tina Kottek
  • Marianne Schauer
  • Sandra Franz
  • Anja Saalbach
  • Ulf Anderegg
  • Olaf Wolkenhauer
  • Dirk Schadendorf
  • Jan C. Simon
  • Thomas Magin
  • Julio Vera
  • Manfred Kunz
چکیده

The present study identified miR-638 as one of the most significantly overexpressed miRNAs in metastatic lesions of melanomas compared with primary melanomas. miR-638 enhanced the tumorigenic properties of melanoma cells in vitro and lung colonization in vivo. mRNA expression profiling identified new candidate genes including TP53INP2 as miR-638 targets, the majority of which are involved in p53 signalling. Overexpression of TP53INP2 severely attenuated proliferative and invasive capacity of melanoma cells which was reversed by miR-638. Depletion of miR-638 stimulated expression of p53 and p53 downstream target genes and induced apoptosis and autophagy. miR-638 promoter analysis identified the miR-638 target transcription factor associated protein 2α (TFAP2A/AP-2α) as a direct negative regulator of miR-638, suggestive for a double-negative regulatory feedback loop. Taken together, miR-638 supports melanoma progression and suppresses p53-mediated apoptosis pathways, autophagy and expression of the transcriptional repressor TFAP2A/AP-2α.

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عنوان ژورنال:

دوره 6  شماره 

صفحات  -

تاریخ انتشار 2015