Nature Communications (May 2024)

Platelets favor the outgrowth of established metastases

  • Maria J. Garcia-Leon,
  • Cristina Liboni,
  • Vincent Mittelheisser,
  • Louis Bochler,
  • Gautier Follain,
  • Clarisse Mouriaux,
  • Ignacio Busnelli,
  • Annabel Larnicol,
  • Florent Colin,
  • Marina Peralta,
  • Naël Osmani,
  • Valentin Gensbittel,
  • Catherine Bourdon,
  • Rafael Samaniego,
  • Angélique Pichot,
  • Nicodème Paul,
  • Anne Molitor,
  • Raphaël Carapito,
  • Martine Jandrot-Perrus,
  • Olivier Lefebvre,
  • Pierre H. Mangin,
  • Jacky G. Goetz

DOI
https://doi.org/10.1038/s41467-024-47516-w
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 19

Abstract

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Abstract Despite abundant evidence demonstrating that platelets foster metastasis, anti-platelet agents have low therapeutic potential due to the risk of hemorrhages. In addition, whether platelets can regulate metastasis at the late stages of the disease remains unknown. In this study, we subject syngeneic models of metastasis to various thrombocytopenic regimes to show that platelets provide a biphasic contribution to metastasis. While potent intravascular binding of platelets to tumor cells efficiently promotes metastasis, platelets further support the outgrowth of established metastases via immune suppression. Genetic depletion and pharmacological targeting of the glycoprotein VI (GPVI) platelet-specific receptor in humanized mouse models efficiently reduce the growth of established metastases, independently of active platelet binding to tumor cells in the bloodstream. Our study demonstrates therapeutic efficacy when targeting animals bearing growing metastases. It further identifies GPVI as a molecular target whose inhibition can impair metastasis without inducing collateral hemostatic perturbations.