Discovery of BI 224436, a Noncatalytic Site Integrase Inhibitor (NCINI) of HIV-1

Lee Fader,Eric Malenfant,Mathieu Parisien,Rebekah Carson,François Bilodeau,Serge Landry,Marc Pesant,Christian Brochu,Sébastien Morin,Catherine Chabot,Ted Halmos,Yves Bousquet,Murray D. Bailey,Stephen H. Kawai,René Coulombe,Steven R. LaPlante,Araz Jakalian,Punit Bhardwaj,Dominik Wernic,Patricia Schroeder,Ma’an Amad,Paul J. Edwards,Michel Garneau,Jianmin Duan,Michael G. Cordingley,Richard C. Bethell,Stephen W. Mason,Michael Bös,Pierre R. Bonneau,Marc-André Poupart,Anne-Marie Faucher,Bruno Simoneau,Craig Fenwick,Christiane Yoakim,Youla S. Tsantrizos

Discovery of BI 224436, a Noncatalytic Site Integrase Inhibitor (NCINI) of HIV-1

2014

An assay recapitulating the 3′ processing activity of HIV-1 integrase (IN) was used to screen the Boehringer Ingelheim compound collection. Hit-to-lead and lead optimization beginning with compound 1 established the importance of the C3 and C4 substituent to antiviral potency against viruses with different aa124/aa125 variants of IN. The importance of the C7 position on the serum shifted potency was established. Introduction of a quinoline substituent at the C4 position provided a balance of potency and metabolic stability. Combination of these findings ultimately led to the discovery of compound 26 (BI 224436), the first NCINI to advance into a phase Ia clinical trial.

Keywords:

Biology
Integrase inhibitor
Pharmacology
Potency
Integrase
Allosteric regulation
Quinoline
Substituent
Combinatorial chemistry
metabolic stability
human immunodeficiency virus

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