Title of article :
Prodrug-based design, synthesis, and biological evaluation of N-benzenesulfonylpiperidine derivatives as novel, orally active factor Xa inhibitors Original Research Article
Author/Authors :
Tsukasa Ishihara، نويسنده , , Norio Seki، نويسنده , , Fukushi Hirayama، نويسنده , , Masaya Orita، نويسنده , , Hiroyuki Koshio، نويسنده , , Yuta Taniuchi، نويسنده , , Yumiko Sakai-Moritani، نويسنده , , Yoshiyuki Iwatsuki، نويسنده , , Seiji Kaku، نويسنده , , Tomihisa Kawasaki، نويسنده , , Yuzo Matsumoto، نويسنده , , Shin-ichi Tsukamoto، نويسنده ,
Abstract :
We describe here our investigation of a new series of orally active fXa inhibitors based on a prodrug strategy. Solid-phase parallel synthesis identified a unique series of fXa inhibitors with a substituted benzenesulfonyl group as a novel S4 binding element. This series resulted in compound 39, which exhibited potent inhibitory activity against fXa (IC50 = 13 nM) and excellent selectivity over thrombin (>7000-fold). The masking of its highly hydrophilic groups led to the creation of related prodrug 28, which demonstrated an anticoagulant effect after oral dosing.
Keywords :
Prodrug , Docking study , Factor Xa , Anticoagulant
