Through a series of synthetic model peptides, we have examined the structural requirements of the P₂ and P₃ residues in statine-based HIV protease (PR) inhibitors. Results agree with the general observations that, the more bulky the P₃ aromatic hydrophobic side chain, the more potent is the inhibitor. At P₂, an isopropyl side chain is critical in maintaining potency. Three-dimensional modeling demonstrates that the steric bulk of a leucyl residue or the unfavorable energy transfer, from water to enzyme, for a basic amino acid residue at P₂ markedly compromises activity. A naphthylalaninyl-valyl P₃-P₂ substituted analogue inhibits PR with an IC₅₀ value of 6 nM, and was also effective as an antiviral agent.