| Literature DB >> 12408711 |
Ingrid C Choong1, Willard Lew, Dennis Lee, Phuongly Pham, Matthew T Burdett, Joni W Lam, Christian Wiesmann, Tinh N Luong, Bruce Fahr, Warren L DeLano, Robert S McDowell, Darin A Allen, Daniel A Erlanson, Eric M Gordon, Tom O'Brien.
Abstract
The design, synthesis, and in vitro activities of a series of potent and selective small-molecule inhibitors of caspase-3 are described. From extended tethering, a salicylic acid fragment was identified as having binding affinity for the S(4) pocket of caspase-3. X-ray crystallography and molecular modeling of the initial tethering hit resulted in the synthesis of 4, which reversibly inhibited caspase-3 with a K(i) = 40 nM. Further optimization led to the identification of a series of potent and selective inhibitors with K(i) values in the 20-50 nM range. One of the most potent compounds in this series, 66b, inhibited caspase-3 with a K(i) = 20 nM and selectivity of 8-500-fold for caspase-3 vs a panel of seven caspases (1, 2, and 4-8). A high-resolution X-ray cocrystal structure of 4 and 66b supports the predicted binding modes of our compounds with caspase-3.Entities:
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Year: 2002 PMID: 12408711 DOI: 10.1021/jm020230j
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446