Nonpeptidal P-2 ligands for HIV protease inhibitors: Structure-based design, synthesis, and biological evaluation
Design and synthesis of nonpeptidal bis-tetrahydrofuran ligands based upon the X-ray crystal structure of the HIV-1 protease-inhibitor complex 1 led to replacement of two amide bonds and a 10 pi-aromatic system of Ro 31-8959 class of HIV protease inhibitors. Detailed structure-activity studies have now established that the position of ring oxygens, ring size, and stereochemistry are all crucial to potency. Of particular interest, compound 49 with (3S,3aS,6aS)-bis-Thf is the most potent inhibitor (IC50 value 1.8 +/- 0.2 nM; CIC95 value 46 +/- 4 nM) in this series. The X-ray structure of protein-inhibitor complex 49 has provided insight into the ligand-binding site interactions. As it turned out, both oxygens in the bis-Thf ligands are involved in hydrogen-bonding interactions with Asp 29 and Asp 30 NH present in the S-2 subsite of HIV-1 protease. Stereoselective routes have been developed to obtain these novel ligands in optically pure form.
- Publisher
- AMER CHEMICAL SOC
- Issue Date
- 1996-08
- Language
- English
- Article Type
- Article
- Keywords
PROTEINASE-INHIBITORS; CYCLIC SULFOLANES; CRYSTAL-STRUCTURE; RATIONAL DESIGN; POTENT; TARGET; AIDS; P-2-LIGANDS; L-735,524; REAGENTS
- Citation
JOURNAL OF MEDICINAL CHEMISTRY, v.39, no.17, pp.3278 - 3290
- ISSN
- 0022-2623
- Appears in Collection
- CH-Journal Papers(저널논문)
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