| Literature DB >> 22471376 |
Wieslaw M Kazmierski1, Robert Hamatake, Maosheng Duan, Lois L Wright, Gary K Smith, Richard L Jarvest, Jing-Jing Ji, Joel P Cooper, Matthew D Tallant, Renae M Crosby, Katrina Creech, Amy Wang, Xianfeng Li, Suoming Zhang, Yong-Kang Zhang, Yang Liu, Charles Z Ding, Yasheen Zhou, Jacob J Plattner, Stephen J Baker, Wei Bu, Liang Liu.
Abstract
The macrocyclic urea 2, a byproduct in the synthesis of benzoxaborole 1, was identified to be a novel and potent HCV protease inhibitor. We further explored this motif by synthesizing additional urea-based inhibitors and by characterizing them in replicase HCV protease-resistant mutants assay. Several compounds, exemplified by 12, were found to be more potent in HCV replicon assays than leading second generation inhibitors such as danoprevir and TMC-435350. Additionally, following oral administration, inhibitor 12 was found in rat liver in significantly higher concentrations than those reported for both danoprevir and TMC-435350, suggesting that inhibitor 12 has the combination of anti-HCV and pharmacokinetic properties that warrants further development of this series.Entities:
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Year: 2012 PMID: 22471376 DOI: 10.1021/jm201278q
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446