Abstract
Exosomes, extracellular nanovesicles that carry nucleic acids, lipids, and proteins, have been the subject of several studies to assess their ability to transfer functional cargoes to cells. We recently characterized extracellular nanovesicles released from glioblastoma cells that carry active Ras in complex with proteins regulating exosome biogenesis. Here, we investigated whether a functional transfer of Ras from exosomes to other cells can initiate intercellular signaling. We observed that treatment of serum-starved, cultured glioblastoma cells with exogenous glioblastoma exosomes caused a significant increase in cellular viability over time. Moreover, we detected fluorescent signal transfer from lipophilic dye-labeled exogenous glioblastoma exosomes into cultured glioblastoma cells. To probe possible signaling from cell-to-cell, we utilized bimolecular luciferase complementation to examine the ability of K-Ras in exosomes to interact with the Raf-Ras Binding domain (Raf-RBD) expressed in a recipient cell line. Although the K-Ras/Raf-RBD interaction was readily detectable upon co-expression in a single cell line, or following lysis of co-cultured cell lines separately expressing K-Ras and RBD, bearing in mind the limitations of our assay, we were unable to detect the interaction in the intact, co-cultured cell lines or upon treatment of the Raf-RBD-expressing cells with exosomes containing K-Ras. Furthermore, HA-Tag-BFP fused to the K-Ras hypervariable region and CAAX sequence failed to be transferred at significant levels from extracellular vesicles into recipient cells, but remained detectable in the cell supernatants even after 96 hours of culture of naïve cells with extracellular vesicles. We conclude that if transfer of functional K-Ras from extracellular vesicles into the cytoplasm of recipient cells occurs, it must do so at an extremely low efficiency and therefore is unlikely to initiate Ras-ERK MAP kinase pathway signaling. These results suggest that studies claiming functional transfer of protein cargoes from exosomes should be interpreted with caution.
Highlights
Exosomes are tiny (50-150nm) extracellular vesicles (EVs) implicated in cell-to-cell communication
We demonstrated that GBM exosomes are enriched for signaling proteins and contain active GTP-bound Ras, and that active Ras interacts with exosome proteins based on GST-Raf-Ras Binding domain (Raf-Ras binding domain (RBD)) pulldown data [1]
Over the course of 30 min, a period sufficient to detect the peak of luminescence for cells co-expressing cLuc-Flag-Raf-RBD with nLuc-HA-K-Ras wild-type or G12D controls, we found that lysates from co-cultured cells exhibited luminescence in a manner dependent on an intact effector domain, since no luminescence was observed for cells co-cultured with the nLuc-HA-K-Ras Y40C effector domain mutant (Fig 4B)
Summary
Exosomes are tiny (50-150nm) extracellular vesicles (EVs) implicated in cell-to-cell communication. No functional transfer of active K-Ras protein from extracellular vesicles into recipient cells in culture collection and analysis, decision to publish, or preparation of the manuscript
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