| Literature DB >> 15115390 |
Joseph W Becker1, Jennifer Rotonda, Stephen M Soisson, Renee Aspiotis, Christopher Bayly, Sébastien Francoeur, Michel Gallant, Marga Garcia-Calvo, Andre Giroux, Erich Grimm, Yongxin Han, Dan McKay, Donald W Nicholson, Erin Peterson, Johanne Renaud, Sophie Roy, Nancy Thornberry, Robert Zamboni.
Abstract
Caspases are cysteine proteases that specifically cleave Asp-Xxx bonds. They are key agents in inflammation and apoptosis and are attractive targets for therapy against inflammation, neurodegeneration, ischemia, and cancer. Many caspase structures are known, but most involve either peptide or protein inhibitors, unattractive candidates for drug development. We present seven crystal structures of inhibited caspase-3 that illustrate several approaches to reducing the peptidyl characteristics of the inhibitors while maintaining their potency and selectivity. The inhibitors reduce the peptidyl nature of inhibitors while preserving binding potency by (1). exploiting a hydrophobic binding site C-terminal to the cleavage site, (2). replacing the negatively charged aspartyl residue at P4 with neutral groups, and (3). using a peptidomimetic 5,6,7-tricyclic system or a pyrazinone at P2-P3. In addition, we have found that two nicotinic acid aldehydes induce a significant conformational change in the S2 and S3 subsites of caspase-3, revealing an unexpected binding mode. These results advance the search for caspase-directed drugs by revealing how unacceptable molecular features can be removed without loss of potency.Entities:
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Year: 2004 PMID: 15115390 DOI: 10.1021/jm0305523
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446