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Abstract
We hereby report studies that suggest a role for serum exosomes in the anchorage-independent
growth (AIG) of tumor cells. In AIG assays, fetal bovine serum is one of the critical
ingredients. We therefore purified exosomes from fetal bovine serum and examined their
potential to promote growth of breast carcinoma cells in soft agar and Matrigel after
reconstituting them into growth medium (EEM). In all the assays, viable colonies were
formed only in the presence of exosomes. Some of the exosomal proteins we identified,
have been documented by others and could be considered exosomal markers. Labeled purified
exosomes were up-taken by the tumor cells, a process that could be competed out with
excess unlabeled vesicles. Our data also suggested that once endocytosed by a cell,
the exosomes could be recycled back to the conditioned medium from where they can
be up-taken by other cells. We also demonstrated that low concentrations of exosomes
activate MAP kinases, suggesting a mechanism by which they maintain the growth of
the tumor cells in soft agar. Taken together, our data demonstrate that serum exosomes
form a growth promoting platform for AIG of tumor cells and may open a new vista into
cancer cell growth in vivo.