| Literature DB >> 29580188 |
Ilaria Giusti1, Marianna Di Francesco1, Sandra D'Ascenzo1, Maria Grazia Palmerini1, Guido Macchiarelli1, Gaspare Carta1, Vincenza Dolo1.
Abstract
It has become clear that non-tumor cells in the microenvironment, especially fibroblasts, actively participate in tumor progression. Fibroblasts conditioned by tumor cells become "activated" and, as such, are identified as CAFs (cancer-associated fibroblasts). These CAFs remodel the tumor stroma to make it more favourable for cancer progression. The aim of this work was to verify whether EVs (extracellular vesicles - whose role as mediators of information between tumor and stromal cells is well known) released from human ovarian cancer cells were able to activate fibroblasts. EVs isolated from SKOV3 (more aggressive) and CABA I (less aggressive) cells were administered to fibroblasts. The consequent activation was supported by morphological and molecular changes in treated fibroblasts; XTT assays, zymographies, wound healing tests and invasion assays also highlighted higher proliferation, motility, invasiveness and enzyme expression. The secretome of these "activated" fibroblasts was, in turn, able to modulate the responses (proliferation, motility and invasion) of fibroblasts, and of tumor and endothelial cells. These findings support the idea that ovarian cancer cells can modulate fibroblast behaviour through the release of EVs, activating them to a CAFs-like state; the latter are able, in turn, to stimulate the surrounding cells. EVs from SKOV3 rather than from CABA I seem to be more efficient in some processes.Entities:
Keywords: CAFs; Cancer Biology; EVs; cancer associated fibroblasts; endothelial cells; extracellular vesicles; ovarian cancer; tumor microenvironment
Mesh:
Year: 2018 PMID: 29580188 PMCID: PMC6067870 DOI: 10.1080/15384047.2018.1451286
Source DB: PubMed Journal: Cancer Biol Ther ISSN: 1538-4047 Impact factor: 4.742