Evaluation of substituted benzamides as P2 ligands for symmetry-based inhibitors of HIV protease

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• 作者：Kempf ; Dale J. ; Flentge ; Charles A. ; Wideburg ; Norman E. ; Saldivar ; Ayda ; Vasavanonda ; Sudthida ; et. al.
• 刊名：Bioorganic and Medicinal Chemistry Letters
• 出版年：1995
• 出版时间：November 16, 1995
• 年：1995
• 卷：5
• 期：22
• 页码：2725-2728
• 全文大小：227 K

文摘

Substituted benzamides were evaluated as P2 ligands for symmetry-based HIV protease inhibitors. In contrast to previous reports, 2-methyl substitution provided only a modest potency increase in combination with hydrogen bonding groups at the 3-position. Furthermore, hydrogen bonding functionality at the 4-position was well tolerated and independent of substitution at the 3-position.