A rational approach in the search for potent inhibitors against HIV proteinase
Autor: | Theresa Gygi, William M. Shannon, Bonnie J. Bowdon, Kathy A. Keith, Kwan Y. Hui, Mei-Huei T. Lai, Joseph V. Manetta |
---|---|
Rok vydání: | 1991 |
Předmět: |
medicine.medical_treatment
Molecular Sequence Data Chick Embryo Biology Biochemistry Virus Gene Expression Regulation Enzymologic law.invention Transition state analog law Renin Genetics medicine Escherichia coli Animals Humans Protease Inhibitors Amino Acid Sequence Molecular Biology Histidine Cells Cultured chemistry.chemical_classification Oligopeptide Protease Gene Expression Regulation Bacterial HIV Protease Inhibitors Virology In vitro Recombinant Proteins Rats Enzyme chemistry Genes Bacterial Recombinant DNA Peptides Biotechnology |
Zdroj: | FASEB journal : official publication of the Federation of American Societies for Experimental Biology. 5(11) |
ISSN: | 0892-6638 |
Popis: | Synthetic peptides described as dog renin inhibitors were found to effectively inhibit the aspartyl protease of human immunodeficiency virus (HIV). The selection of oligopeptides for the HIV protease inhibition study was based on 1) the current strategy of inhibiting aspartyl proteases with transition state analogs, and 2) our previous observations regarding optimal structural differentiation at the P2 position among human, dog, and rat renin inhibitors. In an in vitro assay system consisting of recombinant HIV protease and a synthetic decapeptide substrate (at pH 5.5), results show that HIV protease was unaffected by statine-containing analogs carrying histidine at the P2 position whereas analogs containing valine at the same position yielded anti-protease IC50 values ranging from 50 to 500 nM. As anticipated, some analogs were also shown to inhibit processing of recombinant polyprotein substrate by HIV protease in vitro. The anti-viral activity of three inhibitors was studied in HIV-infected CEM and MT-2 cells. Results showed that one compound, Ac-Naphthylalanyl-Pro-Phe-Val-Statine-Leu-Phe-NH2 (antiprotease IC50 value = 0.4 microM), protected the infected cells effectively with IC50 values (0.73 microM for CEM cells and 0.88 microM for MT-2 cells). This antiviral effect is comparable to those obtained with AZT and ddC in parallel studies of MT-2 cells. |
Databáze: | OpenAIRE |
Externí odkaz: |