In order to investigate the role of the platelet P2Y1 receptor in several aspects of platelet activation and thrombosis, transgenic (TG) mice overexpressing this receptor specifically in the megakaryocytic/platelet lineage were generated using the promoter of the tissue-specific platelet factor 4 gene. Studies of the saturation binding of [ 33P]2MeSADP in the presence or absence of the selective P2Y 1 antagonist MRS2179 indicated that wild-type (WT) mouse platelets bore 150±31 P2Y 1 receptors and TG platelets 276±34, representing an 84% increase in P2Y 1 receptor density. This led to a well defined phenotype of platelet hyper-reactivity in vitro, as shown by increased aggregations in response to adenosine 50-diphosphate (ADP) and low concentration of collagen in TG as compared with WT platelets. Moreover, overexpression of the P2Y 1 receptor enabled ADP to induce granule secretion, unlike in WT platelets, which suggests that the level of P2Y 1 expression is critical for this event. Our results further suggest that the weak responses of normal platelets to ADP are due to a limited number of P2Y 1 receptors rather than to activation of a specific transduction pathway. TG mice displayed a shortened bleeding time and an increased sensitivity to in vivo platelet aggregation induced by infusion of a mixture of collagen and epinephrine. Overall, these findings emphasize the importance of the P2Y 1 receptor in hemostasis and thrombosis and suggest that variable expression levels of this receptor on platelets might play a role in thrombotic states in human, which remains to be assessed. © 2003 International Society on Thrombosis and Haemostasis.
CITATION STYLE
Hechler, B., Zhang, Y., Eckly, A., Cazenave, J. P., Gachet, C., & Ravid, K. (2003). Lineage-specific overexpression of the P2Y 1 receptor induces platelet hyper-reactivity in transgenic mice. Journal of Thrombosis and Haemostasis, 1(1), 155–163. https://doi.org/10.1046/j.1538-7836.2003.00003.x
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