Current Oncology (Feb 2022)

Anti-Metastatic Function of Extracellular Vesicles Derived from <i>Nanog</i>-Overexpressing Melanoma

  • Tomohiro Hatakenaka,
  • Nahoko Matsuki,
  • Seiya Minagawa,
  • Celine Swee May Khoo,
  • Mikako Saito

DOI
https://doi.org/10.3390/curroncol29020088
Journal volume & issue
Vol. 29, no. 2
pp. 1029 – 1046

Abstract

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A metastatic melanoma cell line B16-F10 (F10) was modified to a more undifferentiated state by Nanog overexpression. The produced cell line Nanog+F10 showed a higher metastatic potential than F10. Instead of whole cells, the extracellular vesicles (EVs) therefrom were investigated about their possible role as an autovaccine against metastasis. EVs from Nanog+F10 cells (Nanog+F10-EVs) could suppress the metastasis, contrasting the EVs from less metastatic F10 cells (F10-EVs) enhanced metastasis. The involvement of TGF-β1 in the role of Nanog+F10-EVs was analyzed, as TGF-β1 was a secretory cytokine being affected most intensively by Nanog overexpression. It was suggested to be crucial that the TGF-β1 concentration in Nanog+F10-EVs should be as low as 1.6 pg/μg for its metastasis-suppressive role. In response to Nanog+F10-EVs, immunoreaction was observed in liver, indicating the specific decrease in the number of tumor-promotive CD163-positive macrophages. These indicate a possibility of Nanog+F10-EVs as a novel autovaccine candidate against melanoma metastasis.

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