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Studies of Benzothiophene Template as Potent Factor IXa (FIXa) Inhibitors in Thrombosis

机译:苯并噻吩模板作为血栓形成中的有效因子IXa(FIXa)抑制剂的研究

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FIXa is a serine protease enzyme involved in the intrinsic pathway of the coagulation cascade. The upstream intervention of the coagulation cascade in selectively inhibiting FIXa would leave hemostasis Intact via the extrinsic pathway, leading to an optimum combination of efficacy and safety with low incidence of bleeding. We have identified 2-amindinobenzothiophene template as a lead scaffold for FIXa inhibiton based on its homology with urokinase plasminogen activator (uPA). Subsequent SAR work oil the template revealed a number of highly potent FIXa inhibitors, though with moderate selectivity against FXa. X-ray Study with one of the analogues demonstrated active site binding interaction with the induced opening of the S1 beta pocket and a secondary binding at the S2-S4 sites, which is ill direct contrast with the previous finding.
机译:FIXa是一种丝氨酸蛋白酶,参与凝血级联的内在途径。凝血级联在选择性抑制FIXa的上游干预将通过外在途径保持止血完好无损,从而导致功效和安全性的最佳组合,且出血发生率低。我们已基于其与尿激酶纤溶酶原激活物(uPA)的同源性,将2-amindinobenzothiophene模板鉴定为FIXa抑制剂的先导支架。随后的SAR工作油使模板显示出许多高效的FIXa抑制剂,尽管对FXa具有中等选择性。用类似物之一进行的X射线研究表明,活性位点与S1 beta口袋的诱导开口发生了相互作用,并在S2-S4位点发生了二次结合,这与先前的发现没有直接的对比。

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