AI Article Synopsis

  • Exosomes from SW480 colorectal cancer cells were found to be taken up by HepG2 liver cancer cells via a specific cellular process called dynamin-dependent endocytosis, and they localized to the lysosomes of these recipient cells.
  • After uptake, these exosomes triggered the activation of a signaling pathway known as ERK1/2 phosphorylation in the HepG2 cells, indicating a quick response to the exosome treatment.
  • The SW480-derived exosomes also increased the migration of HepG2 cells in a wound-healing experiment, and this migration could be inhibited by using a drug (U0126) that blocks the ERK1/2 pathway, highlighting the role of exosomes in enhancing cellular movement.

Article Abstract

Exosomes are membrane-derived extracellular vesicles that have recently been recognized as important mediators of intercellular communication. In the present study, we investigated the effects of exosomes derived from SW480 colorectal cancer cells in recipient HepG2 hepatocellular cancer cells. We demonstrated that SW480-derived exosomes were taken up by the recipient HepG2 cells via dynamin-dependent endocytosis and were localized to the HepG2 lysosomes. In addition, SW480-derived exosomes induced the phosphorylation of extracellular signal-regulated kinase (ERK)1/2 following their uptake into HepG2 cells. Of note, these changes occurred during the early phase after exosome treatment. Furthermore, SW480-derived exosomes promoted the migration of recipient HepG2 cells in a wound-healing assay, which was suppressed by pretreatment with U0126, an upstream inhibitor of ERK1/2. These results indicated that SW480-derived exosomes activated a classical mitogen-activated protein kinase pathway in recipient HepG2 cells via dynamin-dependent endocytosis and subsequently enhanced cell migration by ERK1/2 activation. Our results provide new insights into the regulation of cellular functions by exosomes.

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Source
http://dx.doi.org/10.3892/ijo.2015.3255DOI Listing

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