Hydroxyethylamine analogues of the p17/p24 substrate cleavage site are tight-binding inhibitors of HIV protease.

Daniel H. Rich,Jeremy Green,Mihaly V. Toth,Garland R. Marshall,Stephen B. H. Kent

Hydroxyethylamine analogues of the p17/p24 substrate cleavage site are tight-binding inhibitors of HIV protease.

1990

Daniel H. Rich
Jeremy Green
Mihaly V. Toth
Garland R. Marshall
Stephen B. H. Kent

We report the synthesis of hydroxyethylamine dipeptidyl isosteres that were designed to mimic the tetrahedral intermediate for hydrolysis of Tyr-Pro, one of the partial substrate sequences cleaved by HIV protease

Keywords:

Protease
Biochemistry
Substrate (chemistry)
Hydrolysis
Cleavage (embryo)
Tetrahedral carbonyl addition compound
Enzyme inhibitor
Peptide
Chemistry
Chemical synthesis
Stereochemistry

Correction
Source
Cite
Save
Machine Reading By IdeaReader

References

142

Citations