Lucia Languino,
Professor of Cancer Biology,
Thomas Jefferson University
Dr. Languino investigates the role of cell adhesion receptors in phenotypic changes of prostate cancer cells. A strong research focus is being devoted to the study of the cross-talk between cell adhesion molecules, extracellular matrix proteins and growth factor receptors in vitro and in vivo systems and how this cross-talk affects intracellular signal transduction, cell survival, cell migration and cell division. Dr. Languino's research interests also focus on the cellular and molecular characterization of the metastatic process of prostate cancer with particular emphasis on the signals directing distant localization of prostate cancer cells
Welcome and Introduction by Conference Co-Chairperson and an Overview of the Conference
Tuesday, 13 September 2022 at 09:00
Add to Calendar ▼2022-09-14 11:00:002022-09-14 12:00:00Europe/LondonExtracellular Vesicles in Cancer ProgressionExtracellular Vesicles 2022: Biology, Disease and Medicine in SeattleSeattleSELECTBIOenquiries@selectbiosciences.com
Extracellular Vesicles in Cancer Progression
Wednesday, 14 September 2022 at 11:00
Add to Calendar ▼2022-09-14 11:00:002022-09-14 12:00:00Europe/LondonExtracellular Vesicles in Cancer ProgressionExtracellular Vesicles 2022: Biology, Disease and Medicine in SeattleSeattleSELECTBIOenquiries@selectbiosciences.com
Cancer cells crosstalk with the tumor microenvironment (TME) by releasing small extracellular vesicles (sEVs). sEVs are enriched in integrins, cell surface receptors for extracellular matrix proteins. We have shown that alphaV integrins are markers for prostate cancer cell sEVs, which were isolated by density gradients, and characterized by electron microscopy, NTA and immunoblotting analysis, as per MISEV2018 guidelines. These sEVs were also characterized for integrin and tetraspanin colocalization by ExoView analysis. We show now that some alphaV integrins promote the formation of unique, low density sEVs and bind a soluble ligand, as quantified using ExoView. sEV integrins, upon release, are then transferred to microvascular endothelial cells and macrophages in the TME. In functional assays using prostate cancer cells, we provide evidence that sEV integrins, upon transfer, modulate recipient cell proliferation and migration. We also describe, as evaluated by our proteomic and immunoblotting analyses, alterations of signaling pathways in recipient microvascular endothelial cells and macrophages upon transfer of cancer cell derived sEVs. Finally, alphaV integrins’ expression in donor cancer cells reduces sEV levels of molecules that have a tumor suppressive role, or promotes enrichment of effectors that support cancer cell differentiation into aggressive metastatic phenotypes. Overall, our studies show that sEVs from cancer cells may contribute to a horizontal propagation of integrin-activated pathways from cancer cells to the neighboring cells to promote a pro-tumorigenic TME.
Add to Calendar ▼2022-09-13 00:00:002022-09-14 00:00:00Europe/LondonExtracellular Vesicles 2022: Biology, Disease and MedicineExtracellular Vesicles 2022: Biology, Disease and Medicine in SeattleSeattleSELECTBIOenquiries@selectbiosciences.com
Add to Calendar ▼2022-09-14 11:00:002022-09-14 12:00:00Europe/LondonExtracellular Vesicles in Cancer ProgressionExtracellular Vesicles 2022: Biology, Disease and Medicine in SeattleSeattleSELECTBIOenquiries@selectbiosciences.com
