PLoS ONE (Jan 2014)

P-selectin-mediated platelet adhesion promotes the metastasis of murine melanoma cells.

  • Cui-Ling Qi,
  • Bo Wei,
  • Jie Ye,
  • Yang Yang,
  • Bin Li,
  • Qian-Qian Zhang,
  • Jiang-Chao Li,
  • Xiao-Dong He,
  • Tian Lan,
  • Li-Jing Wang

DOI
https://doi.org/10.1371/journal.pone.0091320
Journal volume & issue
Vol. 9, no. 3
p. e91320

Abstract

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Studies have indicated that the aggregation of activated platelets with cancer cells facilitates tumor metastasis; the adhesion molecule P-selectin may be an important mediator of this process, but the detailed mechanism is unclear. In the current study, we established a B16F10 (B16) cell metastatic model in P-selectin knockout (P-sel-/-) mice to determine the effect of P-selectin-mediated platelet adhesion on metastasis. Compared with C57 mice, P-sel-/- mice developed fewer metastatic foci, and cell proliferation within the metastatic tumors was inhibited by P-selectin deficiency. The platelet refusion assay demonstrated that mice with P-sel-/- platelets developed fewer lung metastatic foci (P<0.01) with a lower microvascular density (MVD) than mice with wild-type platelets. A co-culture model of platelets and B16 cells was utilized to determine the difference in VEGF concentration in the supernatants. The results demonstrated that the supernatant from the P-sel-/- platelet/B16 co-culture had a lower concentration of VEGF. Therefore, our findings indicated that P-selectin deficiency inhibited the metastasis of B16 cells and that wild-type platelet refusion reversed this inhibition. The P-selectin-mediated interaction between platelets and B16 cells promoted angiogenesis by up-regulating VEGF.