Thromboxane A2 Potentiates Thrombin-Induced Proliferation of Coronary Artery Smooth Muscle Cells

Abstract

The activation of thrombin is the key event in clot formation after vascular injury. Thrombin itself, but also other clot-derived factors, such as thromboxane A₂ (TXA₂), are mitogenic for vascular smooth muscle cells. We have studied the possible interactions between thrombin and TXA₂ in stimulation of coronary artery smooth muscle cell (SMC) proliferation. Thrombin (1 U/ml) caused a significant proliferatory response in SMC. U 46619, a stable TXA₂ mimetic, had only a minor stimulating effect by its own but markedly potentiated the thrombin-induced mitogenesis. A possible mechanism for these potentiating effects is provided by the demonstration of a marked (6fold) but transient (maximum after 20 min) increase in the expression of TXA₂ receptor (TP receptor) mRNA in SMC by thrombin. Since a significant clot-related TXA₂ generation was detected for at least 2 hours, the up-regulation of TP receptors by thrombin may represent a mechanism that is relevant for the in vivo situation of SMC proliferation after vessel injury.