Structure based drug design: development of potent and selective factor IXa (FIXa) inhibitors.
J. Med. Chem.2010 Feb 25;53(4):1473-82. doi:10.1021/jm901476x
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摘要
On the basis of our understanding on the binding interactions of the benzothiophene template within the FIXa active site by X-ray crystallography and molecular modeling studies, we developed our SAR strategy by targeting the 4-position of the template to access the S1 beta and S2-S4 sites. A number of highly selective and potent factor Xa (FXa) and FIXa inhibitors were identified by simple switch of functional groups with conformational changes toward the S2-S4 sites.
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