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Efficient Synthesis of HIV-1 Protease Inhibitors

Summary
Researchers at Purdue University have developed a new series of hexahydrofuropyran-derived HIV-1 protease inhibitors for treatment of HIV infection and AIDS. These inhibitors are novel and remarkably potent, similar to Darunavir, an FDA approved inhibitor also developed at Purdue. They also show excellent activity against multiple PI-resistant variants, superior to other FDA approved inhibitors.
Technology Benefits
High antiviral potencyEffective against wide range of variants
Technology Application
Medical/HealthcarePharmaceuticalsHIV/AIDS TreatmentDrug Development
Detailed Technology Description
Arun GhoshGhosh GroupPurdue Chemistry
Countries
United States
Application No.
9,024,038
*Abstract

*Background
HIV-1 protease inhibitors are critical components of highly active antiretroviral therapy (HAART). The HAART treatment regimens significantly reduced HIV/AIDS-related mortality. However, the rapid emergence of drug-resistant HIV-1 strains and the appearance of cross-resistance are severely limiting long-term treatment options.
*IP Issue Date
May 5, 2015
*IP Type
Cont-in-Part
*Stage of Development
Proof of Concept
*Web Links
Purdue Office of Technology CommercializationPurdueInnovation and EntrepreneurshipArun GhoshGhosh GroupPurdue Chemistry
Country/Region
USA

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