1992
DOI: 10.1111/j.1399-3011.1992.tb00302.x
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HIV protease (HIV PR) inhibitor structure‐activity‐selectivity, and active site molecular modeling of high affinity Leu [CH(OH)CH2]Val modified viral and nonviral substrate analogs

Abstract: This report details the structure‐activity relationships of the HIV gag substrate analog Val‐Ser‐Gln‐Asn‐LeuΨ[CH(OH)CH2]Val‐Ile‐Val (U‐85548E), an inhibitor exhibiting subnanomolar affinity towards HIV type‐1 aspartic proteinase (HIV‐1 PR). Our data show that the P1‐P′2 tripeptidyl sequence provides the minimal chemical determinant for HIV‐1 PR binding. We describe the structure‐activity properties of LeuiΨ[CH(OH)CH2]Val substitution in other peptidyl ligands of nonviral substrate origin (e.g., angiotensinogen… Show more

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Cited by 10 publications
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