Key steps in the structure-based optimization of the hepatitis C virus NS3/4A protease inhibitor SCH503034

Vincent Madison,Andrew Prongay,Zhuyan Guo,Nanhua Yao,John Pichardo,Thierry O. Fischmann,Corey O. Strickland,Jr J Myers,Patricia C. Weber,Brian M. Beyer,Richard N. Ingram,Zhi Hong,Winifred W. Prosise,Lata Ramanathan,S. Shane Taremi,Taisa Yarosh-Tomaine,Rumin Zhang,Mary M. Senior,Rong-Sheng Yang,Bruce A. Malcolm,Ashok Arasappan,Frank Bennett,Stephane L. Bogen,K. Chen,Edwin Jao,Yalei Liu,Raymond G. Lovey,Anil K. Saksena,Srikanth Venkatraman,Viyyoor M. Girijavallabhan,F. Njoroge

Key steps in the structure-based optimization of the hepatitis C virus NS3/4A protease inhibitor SCH503034

2008

The structures of both native and S139A holo-HCV NS3/4A protease domain were solved to high resolution. Subsequently, structures were determined for a series of ketoamide inhibitors in complex with the protease. The changes in the inhibitor potency were correlated with changes in the buried surface area upon binding the inhibitor to the active site. The largest contributions to the binding energy arise from the hydrophobic interactions of the P1 and P2 groups as they bind to the S1 and S2 pockets. This correlation of the changes in potency with increased buried surface area contributed directly to the design of a potent tripeptide inhibitor of the HCV NS3/4A protease, which is currently in clinical trials.

Keywords:

NS2-3 protease
Protease
Physics
Hepatitis C virus
Potency
Tripeptide
Kunitz STI protease inhibitor
NS3
Biochemistry
Molecular biology
Active site
Hydrophobic effect

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