FEBS Open Bio (Mar 2021)

Uptake of circulating extracellular vesicles from rectal cancer patients and differential responses by human monocyte cultures

  • Tonje Bjørnetrø,
  • Lilly Alice Steffensen,
  • Beate Vestad,
  • Berit Sletbakk Brusletto,
  • Ole Kristoffer Olstad,
  • Anne‐Marie Trøseid,
  • Hans Christian Dalsbotten Aass,
  • Kari Bente Foss Haug,
  • Alicia Llorente,
  • Stig Ove Bøe,
  • Anna Lång,
  • Rampradeep Samiappan,
  • Kathrine Røe Redalen,
  • Reidun Øvstebø,
  • Anne Hansen Ree

DOI
https://doi.org/10.1002/2211-5463.13098
Journal volume & issue
Vol. 11, no. 3
pp. 724 – 740

Abstract

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Extracellular vesicles (EVs) released by tumor cells can directly or indirectly modulate the phenotype and function of the immune cells of the microenvironment locally or at distant sites. The uptake of circulating EVs and the responses by human monocytes in vitro may provide new insights into the underlying biology of the invasive and metastatic processes in cancer. Although a mixed population of vesicles is obtained with most isolation techniques, we predominantly isolated exosomes (small EVs) and microvesicles (medium EVs) from the SW480 colorectal cancer cell line (established from a primary adenocarcinoma of the colon) by sequential centrifugation and ultrafiltration, and plasma EVs were prepared from 22 patients with rectal adenoma polyps or invasive adenocarcinoma by size‐exclusion chromatography. The EVs were thoroughly characterized. The uptake of SW480 EVs was analyzed, and small SW480 EVs were observed to be more potent than medium SW480 EVs in inducing monocyte secretion of cytokines. The plasma EVs were also internalized by monocytes; however, their cytokine‐releasing potency was lower than that of the cell line‐derived vesicles. The transcriptional changes in the monocytes highlighted differences between adenoma and adenocarcinoma patient EVs in their ability to regulate biological functions, whereas the most intriguing changes were found in monocytes receiving EVs from patients with metastatic compared with localized cancer.

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