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Disubstituted BIS-THF moieties as new P2 ligands in nonpeptidal HIV-1 protease inhibitors

by Konrad Hohlfeld, Cyrille Tomassi, Jörg Kurt Wegner, Bart Kesteleyn, Bruno Linclau
ACS Medicinal Chemistry Letters ()

Abstract

A series of darunavir analogues featuring a substituted bis-THF ring as P2 ligand have been synthesized and evaluated. High affinity protease inhibitors (PIs) with an interesting activity on wild-type HIV and a panel of multi-PI resistant HIV-1 mutants containing clinically observed, primary mutations were identified using a cell-based assay. A number of PIs have been synthesized that show equivalent and greater activity for HIV-1 mutant strains as compared to wild-type HIV-1. The activity on the purified enzyme was confirmed for a selection of analogues

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