Ultra-potent P1 modified arylsulfonamide HIV protease inhibitors: The discovery of GW0385

Ultra-potent P1 modified arylsulfonamide HIV protease inhibitors: The discovery of GW0385

A novel series of P1 modified HIV protease inhibitors was synthesized and evaluated for in vitro antiviral activity against wild-type virus and protease inhibitor-resistant viruses. Optimization of the P1 moiety resulted in compounds with femtomolar enzyme activities and cellular antiviral activitie...

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Veröffentlicht in:Bioorganic & medicinal chemistry letters 2006-04, Vol.16 (7), p.1788-1794
Hauptverfasser: Miller, John F., Andrews, C. Webster, Brieger, Michael, Furfine, Eric S., Hale, Michael R., Hanlon, Mary H., Hazen, Richard J., Kaldor, Istvan, McLean, Ed W., Reynolds, David, Sammond, Douglas M., Spaltenstein, Andrew, Tung, Roger, Turner, Elizabeth M., Xu, Robert X., Sherrill, Ronald G.
Format: Artikel
Sprache:eng
Schlagworte:
Antibiotics. Antiinfectious agents. Antiparasitic agents
Antiretroviral
Antiviral
Antiviral agents
Arylsulfonamide
Biological and medical sciences
Brecanavir
Drug resistance
GW0385
HIV protease
HIV Protease Inhibitors - chemistry
HIV Protease Inhibitors - pharmacology
Human immunodeficiency virus
Medical sciences
Molecular Structure
Pharmacology. Drug treatments
Sulfonamides - chemistry
Sulfonamides - pharmacology
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Zusammenfassung:A novel series of P1 modified HIV protease inhibitors was synthesized and evaluated for in vitro antiviral activity against wild-type virus and protease inhibitor-resistant viruses. Optimization of the P1 moiety resulted in compounds with femtomolar enzyme activities and cellular antiviral activities in the low nanomolar range culminating in the identification of clinical candidate GW0385. A novel series of P1 modified HIV protease inhibitors was synthesized and evaluated for in vitro antiviral activity against wild-type virus and protease inhibitor-resistant viruses. Optimization of the P1 moiety resulted in compounds with femtomolar enzyme activities and cellular antiviral activities in the low nanomolar range culminating in the identification of clinical candidate GW0385.
ISSN:0960-894X
1464-3405
DOI:10.1016/j.bmcl.2006.01.035