4.8 Article

Chemotherapy elicits pro-metastatic extracellular vesicles in breast cancer models

Journal

NATURE CELL BIOLOGY
Volume 21, Issue 2, Pages 190-+

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/s41556-018-0256-3

Keywords

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Categories

Funding

  1. Swiss Cancer League [KFS-3007-08-2012]
  2. Swiss National Science Foundation [SNF 31003A-165963]
  3. European Research Council [ERC EVOLVE-72505]
  4. NIH [KL2 TR001100, NCI 1R01CA197943]
  5. Cancer Research UK [C11712/A13028]
  6. Yorkshire Cancer Research [S382]
  7. Breast Cancer Now [2016MayPR746, 2016NovPCC003]
  8. DOD BCRP Era of Hope Scholar Expansion Award [W81XWH-08-PRMRP-IIRA]
  9. Susan B Komen Foundation [KG110560, CCR15224703]
  10. Breast Cancer Research Foundation
  11. Ludwig Center at Harvard
  12. National Foundation for Cancer Research
  13. NCI [R35CA197743]
  14. Wellcome Trust [101067/Z/13/Z]
  15. MRC [MR/N022556/1]
  16. MRC [MR/N022556/1] Funding Source: UKRI

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Cytotoxic chemotherapy is an effective treatment for invasive breast cancer. However, experimental studies in mice also suggest that chemotherapy has pro-metastatic effects. Primary tumours release extracellular vesicles (EVs), including exosomes, that can facilitate the seeding and growth of metastatic cancer cells in distant organs, but the effects of chemotherapy on tumour-derived EVs remain unclear. Here we show that two classes of cytotoxic drugs broadly employed in pre-operative (neoadjuvant) breast cancer therapy, taxanes and anthracyclines, elicit tumour-derived EVs with enhanced pro-metastatic capacity. Chemotherapy-elicited EVs are enriched in annexin A6 (ANXA6), a Ca2+-dependent protein that promotes NF-kappa B-dependent endothelial cell activation, Ccl2 induction and Ly6C(+)CCR2(+) monocyte expansion in the pulmonary pre-metastatic niche to facilitate the establishment of lung metastasis. Genetic inactivation of Anxa6 in cancer cells or Ccr2 in host cells blunts the pro-metastatic effects of chemotherapy-elicited EVs. ANXA6 is detected, and potentially enriched, in the circulating EVs of breast cancer patients undergoing neoadjuvant chemotherapy.

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