Oncogenic ras-driven cancer cell vesiculation leads to emission of double-stranded DNA capable of interacting with target cells

Lee, Tae Hoon; Chennakrishnaiah, Shilpa; Audemard, Eric; Montermini, Laura; Meehan, Brian; Rak, Janusz

doi:10.1016/J.BBRC.2014.07.109

Title: Oncogenic ras-driven cancer cell vesiculation leads to emission of double-stranded DNA capable of interacting with target cells

Journal Article · Fri Aug 22 00:00:00 EDT 2014 · Biochemical and Biophysical Research Communications

DOI:https://doi.org/10.1016/J.BBRC.2014.07.109· OSTI ID:22416720

Lee, Tae Hoon; Chennakrishnaiah, Shilpa ^[1]; Audemard, Eric ^[2]; Montermini, Laura; Meehan, Brian ^[1]; Rak, Janusz ^[1]

Montreal Children’s Hospital, Research Institute of McGill University Health Centre, McGill University, Montreal, Quebec (Canada)
McGill University and Genome Quebec Innovation Centre, Montreal, Quebec (Canada)

Highlights: • Oncogenic H-ras stimulates emission of extracellular vesicles containing double-stranded DNA. • Vesicle-associated extracellular DNA contains mutant N-ras sequences. • Vesicles mediate intercellular transfer of mutant H-ras DNA to normal fibroblasts where it remains for several weeks. • Fibroblasts exposed to vesicles containing H-ras DNA exhibit increased proliferation. - Abstract: Cell free DNA is often regarded as a source of genetic cancer biomarkers, but the related mechanisms of DNA release, composition and biological activity remain unclear. Here we show that rat epithelial cell transformation by the human H-ras oncogene leads to an increase in production of small, exosomal-like extracellular vesicles by viable cancer cells. These EVs contain chromatin-associated double-stranded DNA fragments covering the entire host genome, including full-length H-ras. Oncogenic N-ras and SV40LT sequences were also found in EVs emitted from spontaneous mouse brain tumor cells. Disruption of acidic sphingomyelinase and the p53/Rb pathway did not block emission of EV-related oncogenic DNA. Exposure of non-transformed RAT-1 cells to EVs containing mutant H-ras DNA led to the uptake and retention of this material for an extended (30 days) but transient period of time, and stimulated cell proliferation. Thus, our study suggests that H-ras-mediated transformation stimulates vesicular emission of this histone-bound oncogene, which may interact with non-transformed cells.

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OSTI ID:: 22416720

Journal Information:: Biochemical and Biophysical Research Communications, Vol. 451, Issue 2; Other Information: Copyright (c) 2014 Elsevier Science B.V., Amsterdam, The Netherlands, All rights reserved.; Country of input: International Atomic Energy Agency (IAEA); ISSN 0006-291X

Country of Publication:: United States

Language:: English

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Related Subjects

60 APPLIED LIFE SCIENCES
BIOLOGICAL MARKERS
BRAIN
CELL PROLIFERATION
CHROMATIN
DNA
EV RANGE
FIBROBLASTS
HUMAN POPULATIONS
MICE
MUTANTS
NEOPLASMS
ONCOGENES
RATS
RETENTION
TRANSIENTS
TUMOR CELLS
UPTAKE

Title: Oncogenic ras-driven cancer cell vesiculation leads to emission of double-stranded DNA capable of interacting with target cells

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