Discovery and preclinical evaluation of potent, orally bioavailable, metabolically stable cyclopropylindolobenzazepine acylsulfonamides as thumb site 1 inhibitors of the hepatitis c virus NS5B RNA-dependent, RNA polymerase

Piyasena Hewawasam,Yong Tu,Min Gao,Umesh Hanumegowda,Jay O. Knipe,Julie A. Lemm,Dawn D. Parker,Karen Rigat,Susan B. Roberts,Nicholas A. Meanwell,John F. Kadow

Discovery and preclinical evaluation of potent, orally bioavailable, metabolically stable cyclopropylindolobenzazepine acylsulfonamides as thumb site 1 inhibitors of the hepatitis c virus NS5B RNA-dependent, RNA polymerase

2016

Piyasena Hewawasam
Yong Tu
Min Gao
Umesh Hanumegowda
Jay O. Knipe
Julie A. Lemm
Dawn D. Parker
Karen Rigat
Susan B. Roberts
Nicholas A. Meanwell
John F. Kadow

Abstract Herein, we describe the synthesis, antiviral structure–activity relationships (SAR), metabolic stability, and pharmacokinetic (PK) properties for a series of cyclopropylindolobenzazepine acylsulfonamide HCV NS5B polymerase inhibitors. Optimization of SAR, metabolic stability and PK led to the identification of compound 19 which was advanced into pre-IND enabling toxicology studies.

Keywords:

Hepatitis C virus
NS5B
Biochemistry
Polymerase
RNA-dependent RNA polymerase
Chemistry
Structure–activity relationship
Pharmacology
Bioavailability
Hepacivirus
Pharmacokinetics
ns5b polymerase

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