Synthesis and SAR of geminal substitutions at the C5′ carbosugar position of pyrimidine-derived HCV inhibitors

Vishal Verma,Randall R. Rossman,Frank Bennett,Lei Chen,Stephen Gavalas,Vinay Girijavallabhan,Yuhua Huang,Seong Heon Kim,Aneta Kosinski,Patrick Pinto,Razia Rizvi,Bandarpalle B. Shankar,Ling Tong,Francisco Velazquez,Srikanth Venkatraman,Joseph A. Kozlowski,Malcolm Maccoss,Cecil D. Kwong,Namita Bansal,Hollis S. Kezar,Robert C. Reynolds,Joseph A. Maddry,Subramaniam Ananthan,John A. Secrist,Cheng Li,Robert Chase,Stephanie Curry,Hsueh-Cheng Huang,Xiao Tong,F. George Njoroge,Ashok Arasappan

Synthesis and SAR of geminal substitutions at the C5′ carbosugar position of pyrimidine-derived HCV inhibitors

2012

Abstract The installation of geminal substitution at the C5′ position of the carbosugar in our pyrimidine-derived hepatitis C inhibitor series is reported. SAR studies around the C5′ position led to the installation of the dimethyl group as the optimal functionality. An improved route was subsequently designed to access these substitutions. Expanded SAR at the C2 amino position led to the utilization of C2 ethers. These compounds exhibited good potency, high selectivity, and excellent plasma exposure and bioavailability in rodent as well as in higher species.

Keywords:

Pyrimidine
Hepatitis C virus
Organic chemistry
Potency
Geminal
Bioavailability
Biochemistry
Chemistry
Stereochemistry
high selectivity
plasma exposure

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