†Atherosclerosis Research Laboratory, ‡Small Molecule Discovery Platform, Molecular Therapeutics Program, §Experimental Hepathology, Center for Applied Medical Research (CIMA), and ∥Hematology Service, Clínica Universidad de Navarra, University of Navarra, Pamplona, 31008, Spain.
J Med Chem. 2015 Apr 9;58(7):2941-57. doi: 10.1021/jm501939z. Epub 2015 Feb 25.
Discovery of potent and safe therapeutics that improve upon currently available antifibrinolytics, e.g., tranexamic acid (TXA, 1) and aprotinin, has been challenging. Matrix metalloproteinases (MMPs) participate in thrombus dissolution. Then we designed a novel series of optimized MMP inhibitors that went through phenotypic screening consisting of thromboelastometry and mouse tail bleeding. Our optimized lead compound, CM-352 (2), inhibited fibrinolysis in human whole blood functional assays and was more effective than the current standard of care, 1, in the tail-bleeding model using a 30 000 times lower dose. Moreover, 2 reduced blood loss during liver hepatectomy, while 1 and aprotinin had no effect. Molecule 2 displayed optimal pharmacokinetic and safety profiles with no evidence of thrombosis or coagulation impairment. This novel mechanism of action, targeting MMP, defines a new class of antihemorrhagic agents without interfering with normal hemostatic function. Furthermore, 2 represents a preclinical candidate for the acute treatment of bleeding.
发现能够改善现有抗纤维蛋白溶解剂(如氨甲环酸(TXA,1)和抑肽酶)的有效且安全的治疗方法一直具有挑战性。基质金属蛋白酶(MMPs)参与血栓溶解。然后,我们设计了一系列经过表型筛选的新型优化 MMP 抑制剂,包括血栓弹性测定法和小鼠尾巴出血。我们优化的先导化合物 CM-352(2)在人全血功能测定中抑制纤维蛋白溶解,并且在使用 30000 倍低剂量的尾巴出血模型中比目前的标准治疗方法 1 更有效。此外,2 减少了肝切除术期间的失血,而 1 和抑肽酶没有效果。分子 2 表现出最佳的药代动力学和安全性特征,没有血栓形成或凝血功能障碍的证据。这种针对 MMP 的新型作用机制定义了一类新型的抗出血剂,而不会干扰正常的止血功能。此外,2 代表了用于急性出血治疗的临床前候选药物。
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