Molecular Modeling Based Approach to Potent P2−P4 Macrocyclic Inhibitors of Hepatitis C NS3/4A Protease

Nigel J. Liverton,M. Katharine Holloway,John A. McCauley,Michael T. Rudd,John W. Butcher,Steven S. Carroll,Jillian DiMuzio,Christine Fandozzi,Kevin F. Gilbert,Shi-Shan Mao,Charles J. McIntyre,Kevin T. Nguyen,Joseph J. Romano,Mark Stahlhut,Bang-Lin Wan,David B. Olsen,Joseph P. Vacca

Molecular Modeling Based Approach to Potent P2−P4 Macrocyclic Inhibitors of Hepatitis C NS3/4A Protease

2008

Nigel J. Liverton
M. Katharine Holloway
John A. McCauley
Michael T. Rudd
John W. Butcher
Steven S. Carroll
Jillian DiMuzio
Christine Fandozzi
Kevin F. Gilbert
Shi-Shan Mao
Charles J. McIntyre
Kevin T. Nguyen
Joseph J. Romano
Mark Stahlhut
Bang-Lin Wan
David B. Olsen
Joseph P. Vacca

Molecular modeling of inhibitor bound full length HCV NS3/4A protease structures proved to be a valuable tool in the design of a new series of potent NS3 protease inhibitors. Optimization of initial compounds provided 25a. The in vitro activity and selectivity as well as the rat pharmacokinetic profile of 25a compare favorably with the data for other NS3/4A protease inhibitors currently in clinical development for the treatment of HCV.

Keywords:

Protease
Hepatitis C
NS3
In vitro
Chemistry
Molecular biology
Molecular model
Pharmacokinetics
Biochemistry
ns3 4a protease

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