| Literature DB >> 15943472 |
Clarence J Maring1, Vincent S Stoll, Chen Zhao, Minghua Sun, Allan C Krueger, Kent D Stewart, Darold L Madigan, Warren M Kati, Yibo Xu, Robert J Carrick, Debra A Montgomery, Anita Kempf-Grote, Kennan C Marsh, Akhteruzzaman Molla, Kevin R Steffy, Hing L Sham, W Graeme Laver, Yu-gui Gu, Dale J Kempf, William E Kohlbrenner.
Abstract
The structure-activity relationship (SAR) of a novel hydrophobic binding interaction within a subsite of the influenza neuraminidase (NA) active site was characterized and optimized for a series of trisubstituted pyrrolidine inhibitors modified at the 4-position. Previously, potent inhibitors have targeted this subsite with hydrophilic substituents such as amines and guanidines. Inhibitor-bound crystal structures revealed that hydrophobic substituents with sp(2) hybridization could achieve optimal interactions by virtue of a low-energy binding conformation and favorable pi-stacking interactions with the residue Glu119. From a lead methyl ester, investigation of five-membered heteroaromatic substituents at C-4 produced a 3-pyrazolyl analogue that improved activity by making a targeted hydrogen bond with Trp178. The SAR of substituted vinyl substituents at C-4 produced a Z-propenyl analogue with improved activity over the lead methyl ester. The C-1 ethyl ester prodrugs of the substituted C-4 vinyl analogues gave compounds with excellent oral bioavailability (F > 60%) when dosed in rat.Entities:
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Year: 2005 PMID: 15943472 DOI: 10.1021/jm049276y
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446