Molecular mechanisms of platelet activation and aggregation induced by breast cancer cells

Tumor cell-induced platelet aggregation represents a critical process both for successful metastatic spread of the tumor and for the development of thrombotic complications in cancer patients. To get further insights into this process, we investigated and compared the molecular mechanisms of platele...

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Bibliographic Details
Published in:Cellular signalling 2018-08, Vol.48, p.45-53
Main Authors: Zarà, Marta, Canobbio, Ilaria, Visconte, Caterina, Canino, Jessica, Torti, Mauro, Guidetti, Gianni Francesco
Format: Article
Language:English
Subjects:
Breast cancer cells
Calcium signaling
P2Y12 receptor
Phospholipase C
Platelets
Rap1
TCIPA
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Summary:Tumor cell-induced platelet aggregation represents a critical process both for successful metastatic spread of the tumor and for the development of thrombotic complications in cancer patients. To get further insights into this process, we investigated and compared the molecular mechanisms of platelet aggregation induced by two different breast cancer cell lines (MDA-MB-231 and MCF7) and a colorectal cancer cell line (Caco-2). All the three types of cancer cells were able to induce comparable platelet aggregation, which, however, was observed exclusively in the presence of CaCl2 and autologous plasma. Aggregation was supported both by fibrinogen binding to integrin αIIbβ3 as well as by fibrin formation, and was completely prevented by the serine protease inhibitor PPACK. Platelet aggregation was preceded by generation of low amounts of thrombin, possibly through tumor cells-expressed tissue factor, and was supported by platelet activation, as revealed by stimulation of phospholipase C, intracellular Ca2+ increase and activation of Rap1b GTPase. Pharmacological inhibition of phospholipase C, but not of phosphatidylinositol 3-kinase or Src family kinases prevented tumor cell-induced platelet aggregation. Tumor cells also induced dense granule secretion, and the stimulation of the P2Y12 receptor by released ADP was found to be necessary for complete platelet aggregation. By contrast, prevention of thromboxane A2 synthesis by aspirin did not alter the ability of all the cancer cell lines analyzed to induce platelet aggregation. These results indicate that tumor cell-induced platelet aggregation is not related to the type of the cancer cells or to their metastatic potential, and is triggered by platelet activation and secretion driven by the generation of small amount of thrombin from plasma and supported by the positive feedback signaling through secreted ADP. •Platelet aggregation induced by breast cancer cells requires traces amount of plasma•Both thrombin generation and ADP-mediated P2Y12 receptor stimulation are essential mediators of TCIPA•Breast cancer cell-induced platelet aggregation is supported by phospholipase C, but is independent of Src kinases or PI3K.
ISSN:0898-6568
1873-3913
DOI:10.1016/j.cellsig.2018.04.008