P2X7 receptor signaling contributes to tissue factor–dependent thrombosis in mice
Christian Furlan-Freguia, … , Zaverio M. Ruggeri, Wolfram Ruf
Christian Furlan-Freguia, … , Zaverio M. Ruggeri, Wolfram Ruf
Published June 13, 2011
Citation Information: J Clin Invest. 2011;121(7):2932-2944. https://doi.org/10.1172/JCI46129.
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P2X7 receptor signaling contributes to tissue factor–dependent thrombosis in mice

Abstract

Thrombosis is initiated by tissue factor (TF), a coagulation cofactor/receptor expressed in the vessel wall, on myeloid cells, and on microparticles (MPs) with variable procoagulant activity. However, the molecular pathways that generate prothrombotic TF in vivo are poorly defined. The oxidoreductase protein disulfide isomerase (PDI) is thought to be involved in the activation of TF. Here, we found that in mouse myeloid cells, ATP-triggered signaling through purinergic receptor P2X, ligand-gated ion channel, 7 (P2X7 receptor; encoded by P2rx7) induced activation (decryption) of TF procoagulant activity and promoted release of TF+ MPs from macrophages and SMCs. The generation of prothrombotic MPs required P2X7 receptor–dependent production of ROS leading to increased availability of solvent-accessible extracellular thiols. An antibody to PDI with antithrombotic activity in vivo attenuated the release of procoagulant MPs. In addition, P2rx7–/– mice were protected from TF-dependent FeCl3-induced carotid artery thrombosis. BM chimeras revealed that P2X7 receptor prothrombotic function was present in both hematopoietic and vessel wall compartments. In contrast, an alternative anti-PDI antibody showed activities consistent with cellular activation typically induced by P2X7 receptor signaling. This anti-PDI antibody restored TF-dependent thrombosis in P2rx7–/– mice. These data suggest that PDI regulates a critical P2X7 receptor–dependent signaling pathway that generates prothrombotic TF, defining a link between inflammation and thrombosis with potential implications for antithrombotic therapy.

Authors

Christian Furlan-Freguia, Patrizia Marchese, András Gruber, Zaverio M. Ruggeri, Wolfram Ruf

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Figure 9

Bypassing activity of anti-PDI clone 34 in P2rx7–/– mice to induce TF-dependent thrombosis.

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Bypassing activity of anti-PDI clone 34 in P2rx7–/– mice to induce TF-de...
Clone 34 (50 μg/mouse) restored vascular occlusion in P2rx7–/– mice subjected to 8% FeCl3•6H2O carotid artery injury. The noninhibitory dose of anti-FXI 14E11 (65 ng/g) did not significantly reverse the effect of clone 34 injection. Combined treatment with anti-TF 21E10 (25 μg/g body weight) and anti-FXI 14E11 prevented the thrombosis-promoting effect of clone 34 in P2rx7–/– mice. Results are presented and differences evaluated as in Figure 5; controls are reproduced from Figure 5A for comparison. *P < 0.05; **P < 0.01.