Synthesis and optimization of a novel series of HCV NS3 protease inhibitors: 4-Arylproline analogs

François Bilodeau,Murray D. Bailey,Punit Bhardwaj,Josée Bordeleau,Pat Forgione,Michel Garneau,Elise Ghiro,Vida Gorys,Ted Halmos,Eric Jolicoeur,Mélissa Leblanc,Christopher T. Lemke,Julie Naud,Jeff O’Meara,Peter W. White,Montse Llinas-Brunet

Synthesis and optimization of a novel series of HCV NS3 protease inhibitors: 4-Arylproline analogs

2013

François Bilodeau
Murray D. Bailey
Punit Bhardwaj
Josée Bordeleau
Pat Forgione
Michel Garneau
Elise Ghiro
Vida Gorys
Ted Halmos
Eric Jolicoeur
Mélissa Leblanc
Christopher T. Lemke
Julie Naud
Jeff O’Meara
Peter W. White
Montse Llinas-Brunet

Abstract In this report we describe the synthesis and evaluation of diverse 4-arylproline analogs as HCV NS3 protease inhibitors. Introduction of this novel P2 moiety opened up new SAR and, in combination with a synthetic approach providing a versatile handle, allowed for efficient exploitation of this novel series of NS3 protease inhibitors. Multiple structural modifications of the aryl group at the 4-proline, guided by structural analysis, led to the identification of analogs which were very potent in both enzymatic and cell based assays. The impact of this systematic SAR on different drug properties is reported.

Keywords:

Protease
Enzyme
Aryl
Moiety
Organic chemistry
NS3
Biochemistry
Chemistry
cell based assays
Drug
hcv ns3 protease

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