| Literature DB >> 33707612 |
Balázs Döme1,2,3, Viktória László4,5, Judit Berta6, Szilvia Török6, Júlia Tárnoki-Zách7, Orsolya Drozdovszky6, József Tóvári8, Sándor Paku9, Ildikó Kovács6, András Czirók7,10,11, Bernard Masri12, Zsolt Megyesfalvi6,13,14, Henriett Oskolás15, Johan Malm16, Christian Ingvar17, György Markó-Varga15.
Abstract
Apelin, a ligand of the APJ receptor, is overexpressed in several human cancers and plays an important role in tumor angiogenesis and growth in various experimental systems. We investigated the role of apelin signaling in the malignant behavior of cutaneous melanoma. Murine B16 and human A375 melanoma cell lines were stably transfected with apelin encoding or control vectors. Apelin overexpression significantly increased melanoma cell migration and invasion in vitro, but it had no impact on its proliferation. In our in vivo experiments, apelin significantly increased the number and size of lung metastases of murine melanoma cells. Melanoma cell proliferation rates and lymph and blood microvessel densities were significantly higher in the apelin-overexpressing pulmonary metastases. APJ inhibition by the competitive APJ antagonist MM54 significantly attenuated the in vivo pro-tumorigenic effects of apelin. Additionally, we detected significantly elevated circulating apelin and VEGF levels in patients with melanoma compared to healthy controls. Our results show that apelin promotes blood and lymphatic vascularization and the growth of pulmonary metastases of skin melanoma. Further studies are warranted to validate apelin signaling as a new potential therapeutic target in this malignancy.Entities:
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Year: 2021 PMID: 33707612 PMCID: PMC7952702 DOI: 10.1038/s41598-021-85162-0
Source DB: PubMed Journal: Sci Rep ISSN: 2045-2322 Impact factor: 4.379