Portola Pharmaceuticals Inc, South San Francisco, CA, USA.
Blood. 2011 Nov 3;118(18):5000-10. doi: 10.1182/blood-2011-06-360743. Epub 2011 Aug 31.
Although current antiplatelet therapies provide potent antithrombotic effects, their efficacy is limited by a heightened risk of bleeding and failure to affect vascular remodeling after injury. New lines of research suggest that thrombosis and hemorrhage may be uncoupled at the interface of pathways controlling thrombosis and inflammation. Here, as one remarkable example, studies using a novel and highly selective pharmacologic inhibitor of the spleen tyrosine kinase Syk [PRT060318; 2-((1R,2S)-2-aminocyclohexylamino)-4-(m-tolylamino)pyrimidine-5-carboxamide] coupled with genetic experiments, demonstrate that Syk inhibition ameliorates both the acute and chronic responses to vascular injury without affecting hemostasis. Specifically, lack of Syk (murine radiation chimeras) attenuated shear-induced thrombus formation ex vivo, and PRT060318 strongly inhibited arterial thrombosis in vivo in multiple animal species while having minimal impact on bleeding. Furthermore, leukocyte-platelet-dependent responses to vascular injury, including inflammatory cell recruitment and neointima formation, were markedly inhibited by PRT060318. Thus, Syk controls acute and long-term responses to arterial vascular injury. The therapeutic potential of Syk may be exemplary of a new class of antiatherothrombotic agents that target the interface between thrombosis and inflammation.
尽管当前的抗血小板治疗提供了强大的抗血栓作用,但它们的疗效受到出血风险增加和损伤后血管重塑效果有限的限制。新的研究表明,血栓形成和出血可能在控制血栓形成和炎症的途径界面上脱偶联。在这里,作为一个显著的例子,使用新型和高度选择性的脾酪氨酸激酶 Syk 药理学抑制剂(PRT060318;2-((1R,2S)-2-氨基环己基氨基)-4-(m-甲苯基氨基)嘧啶-5-甲酰胺)结合遗传实验的研究表明,Syk 抑制改善了血管损伤的急性和慢性反应,而不影响止血。具体来说,缺乏 Syk(小鼠辐射嵌合体)减弱了体外剪切诱导的血栓形成,PRT060318 强烈抑制了多种动物体内的动脉血栓形成,而对出血的影响最小。此外,白细胞-血小板对血管损伤的反应,包括炎症细胞募集和新生内膜形成,被 PRT060318 显著抑制。因此,Syk 控制动脉血管损伤的急性和长期反应。Syk 的治疗潜力可能是一类针对血栓形成和炎症之间界面的新型抗动脉粥样硬化血栓形成药物的典范。
