The serine protease thrombin plays several key roles in the clotting cascade within the hemostatic system, such as in fibrin formation and platelet activation. Thus, development of an inhibitor that binds to the enzyme's active site (a direct thrombin inhibitor) offers an approach for the treatment of thrombus-associated diseases. Previous structure–activity relationship studies originally based on the bradykinin breakdown product Arg-Pro-Pro- ...
![3-[(Z)-N'-hydroxycarbamimidoyl]benzoic acid Structure](https://image.chemsrc.com/caspic/089/199447-10-4.png)
