2016
DOI: 10.18632/oncotarget.10627
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Barriers to horizontal cell transformation by extracellular vesicles containing oncogenic H-ras

Abstract: Extracellular vesicles (EVs) enable the exit of regulatory, mutant and oncogenic macromolecules (proteins, RNA and DNA) from their parental tumor cells and uptake of this material by unrelated cellular populations. Among the resulting biological effects of interest is the notion that cancer-derived EVs may mediate horizontal transformation of normal cells through transfer of mutant genes, including mutant ras. Here, we report that H-ras-mediated transformation of intestinal epithelial cells (IEC-18) results in… Show more

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Cited by 74 publications
(110 citation statements)
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“…S6). Nonetheless, the cumulative ability to uptake EVs was greater in the case of EGFRvIII-transformed glioma cells, which is consistent with the role of oncogeneses in regulating EV uptake (58,59). Thus, EGFRvIIImediated oncogenic transformation alters the magnitude and specificity of the EV internalization by changing the surface properties of both EVs and cellular recipients.…”
Section: Lamc1) Collagens (Col5a1 Col18a1) Basement Membrane Protesupporting
confidence: 78%
See 1 more Smart Citation
“…S6). Nonetheless, the cumulative ability to uptake EVs was greater in the case of EGFRvIII-transformed glioma cells, which is consistent with the role of oncogeneses in regulating EV uptake (58,59). Thus, EGFRvIIImediated oncogenic transformation alters the magnitude and specificity of the EV internalization by changing the surface properties of both EVs and cellular recipients.…”
Section: Lamc1) Collagens (Col5a1 Col18a1) Basement Membrane Protesupporting
confidence: 78%
“…Genetic and epigenetic driver events have already been implicated by us and others as regulators of the EV release and intercellular communication in cancer, including intercellular trafficking of transforming mutant macromolecules, such as HRAS, EGFR and EGFRvIII (12,17,18,58,62).…”
Section: Discussionmentioning
confidence: 99%
“…EVs isolated from cells were labelled with PKH26 (#MINI26, Sigma-Aldrich) red fluorescent dye as described earlier [33,34]. Briefly, EVs were re-suspended in 250 μL of 2× Diluent C. The 2 × Dye Solution (4 × 10 –6  M) in Diluent C is prepared by adding 1 μL of the PKH26 ethanolic dye solution (# P9691) to 250 mL of Diluent C in a polypropylene centrifuge tube and mixed well to disperse.…”
Section: Methodsmentioning
confidence: 99%
“…Interestingly, the interaction and uptake of EVs by recipient cells may be dependent on the specific properties of the recipient cells. For example, epithelial cells and astrocytes were unable to internalize EVs from transformed cells [43]. However, when the same cell types were transformed through ectopic expression of oncogenic forms of Ras or c-Src, they efficiently internalized the EVs [43].…”
Section: Ev Targeting and Docking On Cellsmentioning
confidence: 99%