作者
Jeffrey T Kohrt, Kevin J Filipski, Wayne L Cody, Christopher F Bigge, Frances La, Kathleen Welch, Tawny Dahring, John W Bryant, Daniele Leonard, Gary Bolton, Lakshmi Narasimhan, Erli Zhang, J Thomas Peterson, Staci Haarer, Vaishali Sahasrabudhe, Nancy Janiczek, Shrilakshmi Desiraju, Mostofa Hena, Charles Fiakpui, Neerja Saraswat, Raman Sharma, Shaoyi Sun, Samarendra N Maiti, Robert Leadley, Jeremy J Edmunds
发表日期
2006/7/1
期刊
Bioorganic & medicinal chemistry
卷号
14
期号
13
页码范围
4379-4392
出版商
Pergamon
简介
Herein, we report on the identification of three potent glycine and related amino acid-based series of FXa inhibitors containing a neutral P1 chlorophenyl pharmacophore. A X-ray crystal structure has shown that constrained glycine derivatives with optimized N-substitution can greatly increase hydrophobic interactions in the FXa active site. Also, the substitution of a pyridone ring for a phenylsulfone ring in the P4 sidechain resulted in an inhibitor with enhanced oral bioavailability.
学术搜索中的文章
JT Kohrt, KJ Filipski, WL Cody, CF Bigge, F La, K Welch… - Bioorganic & medicinal chemistry, 2006