Runx2 stimulates neoangiogenesis through the Runt domain in melanoma

Daniela Cecconi, Jessica Brandi, Marcello Manfredi, Michela Serena, Luca Dalle Carbonare, Michela Deiana, Samuele Cheri, Francesca Parolini, Alberto Gandini, Giulia Marchetto, Giulio Innamorati, Francesco Avanzi, Franco Antoniazzi, Emilio Marengo, Natascia Tiso, Monica Mottes, Donato Zipeto, Maria Teresa Valenti

Risultato della ricerca: Contributo su rivistaArticolo in rivistapeer review

Abstract

Runx2 is a transcription factor involved in melanoma cell migration and proliferation. Here, we extended the analysis of Runt domain of Runx2 in melanoma cells to deepen understanding of the underlying mechanisms. By the CRISPR/Cas9 system we generated the Runt KO melanoma cells 3G8. Interestingly, the proteome analysis showed a specific protein signature of 3G8 cells related to apoptosis and migration, and pointed out the involvement of Runt domain in the neoangiogenesis process. Among the proteins implicated in angiogenesis we identified fatty acid synthase, chloride intracellular channel protein-4, heat shock protein beta-1, Rho guanine nucleotide exchange factor 1, D-3-phosphoglycerate dehydrogenase, myosin-1c and caveolin-1. Upon querying the TCGA provisional database for melanoma, the genes related to these proteins were found altered in 51.36% of total patients. In addition, VEGF gene expression was reduced in 3G8 as compared to A375 cells; and HUVEC co-cultured with 3G8 cells expressed lower levels of CD105 and CD31 neoangiogenetic markers. Furthermore, the tube formation assay revealed down-regulation of capillary-like structures in HUVEC co-cultured with 3G8 in comparison to those with A375 cells. These findings provide new insight into Runx2 molecular details which can be crucial to possibly propose it as an oncotarget of melanoma.

Lingua originaleInglese
Numero di articolo8052
RivistaScientific Reports
Volume9
Numero di pubblicazione1
DOI
Stato di pubblicazionePubblicato - 1 dic 2019

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