| Literature DB >> 9599239 |
G J Pacofsky1, K Lackey, K J Alligood, J Berman, P S Charifson, R M Crosby, G F Dorsey, P L Feldman, T M Gilmer, C W Hummel, S R Jordan, C Mohr, L M Shewchuk, D D Sternbach, M Rodriguez.
Abstract
The design, synthesis, and evaluation of dipeptide analogues as ligands for the pp60c-src SH2 domain are described. The critical binding interactions between Ac-Tyr-Glu-N(n-C5H11)2 (2) and the protein are established and form the basis for our structure-based drug design efforts. The effects of changes in both the C-terminal (11-27) and N-terminal (51-69) portions of the dipeptide are explored. Analogues with reduced overall charge (92-95) are also investigated. We demonstrate the feasibility of pairing structurally diverse subunits in a modest dipeptide framework with the goal of increasing the druglike attributes without sacrificing binding affinity.Entities:
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Year: 1998 PMID: 9599239 DOI: 10.1021/jm970853a
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446