Discovery of MK-1220: A Macrocyclic Inhibitor of Hepatitis C Virus NS3/4A Protease with Improved Preclinical Plasma Exposure

Michael T Rudd; John A McCauley; John W Butcher; Joseph J Romano; Charles J McIntyre; Kevin T Nguyen; Kevin F Gilbert; Kimberly J Bush; M Katharine Holloway; John Swestock; Bang-Lin Wan; Steven S Carroll; Jillian M DiMuzio; Donald J Graham; Steven W Ludmerer; Mark W Stahlhut; Christine M Fandozzi; Nicole Trainor; David B Olsen; Joseph P Vacca; Nigel J Liverton

doi:10.1021/ml1002426

Discovery of MK-1220: A Macrocyclic Inhibitor of Hepatitis C Virus NS3/4A Protease with Improved Preclinical Plasma Exposure

ACS Med Chem Lett. 2011 Jan 12;2(3):207-12. doi: 10.1021/ml1002426. eCollection 2011 Mar 10.

Authors

Michael T Rudd¹, John A McCauley¹, John W Butcher¹, Joseph J Romano¹, Charles J McIntyre¹, Kevin T Nguyen¹, Kevin F Gilbert¹, Kimberly J Bush¹, M Katharine Holloway¹, John Swestock¹, Bang-Lin Wan¹, Steven S Carroll¹, Jillian M DiMuzio¹, Donald J Graham¹, Steven W Ludmerer¹, Mark W Stahlhut¹, Christine M Fandozzi¹, Nicole Trainor¹, David B Olsen¹, Joseph P Vacca¹, Nigel J Liverton¹

Affiliation

¹ Departments of Medicinal Chemistry, Molecular Systems, Antiviral Research, and Drug Metabolism, Merck Research Laboratories , West Point, Pennsylvania 19486, United States.

Abstract

The discovery of MK-1220 is reported along with the development of a series of HCV NS3/4A protease inhibitors containing a P2 to P4 macrocyclic constraint with improved preclinical pharmacokinetics. Optimization of the P2 heterocycle substitution pattern as well as the P3 amino acid led to compounds with greatly improved plasma exposure following oral dosing in both rats and dogs while maintaining excellent enzyme potency and cellular activity. These studies led to the identification of MK-1220.

Keywords: HCV; Hepatitis C; NS3/4A; macrocycle; ring-closing metathesis.