| Literature DB >> 32060259 |
Maria Grazia Tupone1,2, Simona D'Aguanno1, Marta Di Martile1, Elisabetta Valentini1, Marianna Desideri1, Daniela Trisciuoglio1,3, Sara Donzelli4, Andrea Sacconi5, Simonetta Buglioni6, Cristiana Ercolani6, Alessio Biagioni7, Gabriella Fibbi7, Luigi Fattore8, Rita Mancini9, Gennaro Ciliberto10, Giovanni Blandino4, Donatella Del Bufalo11.
Abstract
Evaluating the expression levels of miR-378a-5p both in a large melanoma patient cohort from The Cancer Genome Atlas database and in melanoma patients from our Institute, we found that miR-378a-5p is upregulated in metastatic melanoma specimens. miR-378a-5p expression was also increased in melanoma cells resistant to target therapy, and decreased in response to drug treatment. We also demonstrated that overexpression of miR-378a-5p enhances in vitro cell invasion and migration, and facilitates the ability of melanoma cells to form de novo vasculogenic structures. While performing downstream targeting studies, we confirmed the ability of miR-378a-5p to modulate the expression of known target genes, such as SUFU, FUS-1, and KLF9. Luciferase-3'UTR experiments also identified STAMBP and HOXD10 as new miR-378a-5p target genes. MMP2 and uPAR, two HOXD10 target genes, were positively regulated by miR-378a-5p. Genetic and pharmacologic approaches inhibiting uPAR expression and activity evidenced that the in vitro tumor-promoting functions of miR-378a-5p, were in part mediated by uPAR. Of note miR-378a-5p was also able to increase VEGF, as well as in vitro and in vivo angiogenesis. Finally, genetic and pharmacologic modulation of Bcl-2 evidenced Bcl-2 ability to regulate miR-378a-5p expression. In conclusion, to the best of our knowledge, this is the first study demonstrating that miR-378a-5p acts as an oncogenic microRNA in melanoma.Entities:
Year: 2020 PMID: 32060259 PMCID: PMC7021836 DOI: 10.1038/s41389-020-0203-6
Source DB: PubMed Journal: Oncogenesis ISSN: 2157-9024 Impact factor: 7.485