Structure-based discovery of tipranavir disodium (PNU-140690E): A potent, orally bioavailable, nonpeptidic HIV protease inhibitor

Efforts to develop therapeutically relevant HIV protease inhibitors as medicinal agents in confronting the AIDS crisis have been aided by the wealth of fundamental information acquired during related drug discovery campaigns against other aspartyl proteases. This knowledge base was brought to full f...

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Bibliographic Details
Published inBIOPOLYM Vol. 51; no. 1; pp. 51 - 58
Main Authors Thaisrivongs, Suvit, Strohbach, Joseph W.
Format Journal Article
LanguageEnglish
Published New York John Wiley & Sons, Inc 1999
Subjects
Administration, Oral
AIDS
AIDS/HIV
Anti-HIV Agents - chemistry
Anti-HIV Agents - pharmacokinetics
Anti-HIV Agents - therapeutic use
Antibiotics
aspartyl protease
Biological Availability
Biosynthesis
Cell culture
Drug Design
drug discovery
HIV
HIV Infections - drug therapy
HIV Protease Inhibitors - chemistry
HIV Protease Inhibitors - pharmacokinetics
HIV Protease Inhibitors - therapeutic use
Human immunodeficiency virus
Humans
Models, Molecular
Molecular structure
Pharmacokinetics
PNU-140690E
protease inhibitors
Pyridines - chemistry
Pyridines - pharmacokinetics
Pyridines - therapeutic use
Pyrones - chemistry
Pyrones - pharmacokinetics
Pyrones - therapeutic use
Sodium compounds
Structure-Activity Relationship
Tipranavir disodium
Viruses
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Summary:Efforts to develop therapeutically relevant HIV protease inhibitors as medicinal agents in confronting the AIDS crisis have been aided by the wealth of fundamental information acquired during related drug discovery campaigns against other aspartyl proteases. This knowledge base was brought to full force with the broad screening identification of small, nonpeptidic, inhibitory molecules as templates for chemical elaboration. Significantly, the ability to collect crystallographic data on the inhibitor–enzyme complexes in a rapid fashion afforded the opportunity for a structure‐based approach to drug discovery. Iterative cycles of synthesis, biological testing, and structural information gathering followed by prudent design modifications afforded compounds suitable for clinical evaluation. Displaying high enzymatic inhibition (Ki = 8 pM), potent in vitro antiviral cell culture activity (IC90 = 100 nM), and a useful pharmacokinetic profile, PNU‐140690E (Tipranavir disodium) has entered into clinical studies. Promising results from these early trials supported further evaluation of this compound in HIV‐infected individuals. PNU‐140690E is currently under extensive clinical study. © 1999 John Wiley & Sons, Inc. Biopoly 51: 51–58, 1999
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ISSN:0006-3525
1097-0282
DOI:10.1002/(SICI)1097-0282(1999)51:1<51::AID-BIP6>3.0.CO;2-U