Dönnecke Daniel, Schweinitz Andrea, Stürzebecher Anne, Steinmetzer Peter, Schuster Maj, Stürzebecher Uta, Nicklisch Silke, Stürzebecher Jörg, Steinmetzer Torsten
Curacyte Discovery GmbH, Winzerlaer Str. 2, D-07745 Jena, Germany.
Bioorg Med Chem Lett. 2007 Jun 15;17(12):3322-9. doi: 10.1016/j.bmcl.2007.03.105. Epub 2007 Apr 6.
Highly potent and selective substrate analogue factor Xa inhibitors were obtained by incorporation of non-basic or modestly basic P1 residues known from the development of thrombin inhibitors. The modification of the P2 and P3 amino acids strongly influenced the selectivity and provided potent dual factor Xa and thrombin inhibitors without affecting the fibrinolytic enzymes. Several inhibitors demonstrated excellent anticoagulant efficacy in standard clotting assays in human plasma.
通过引入凝血酶抑制剂开发过程中已知的非碱性或适度碱性的P1残基,获得了高效且选择性的底物类似物因子Xa抑制剂。P2和P3氨基酸的修饰强烈影响了选择性,并提供了高效的双因子Xa和凝血酶抑制剂,而不影响纤溶酶。几种抑制剂在人血浆的标准凝血试验中显示出优异的抗凝效果。
