Inhibition of Hepatitis C Virus Replication by GS-6620, a Potent C-Nucleoside Monophosphate Prodrug

被引:30
作者
Feng, Joy Y. [1 ]
Cheng, Guofeng [1 ]
Perry, Jason [1 ]
Barauskas, Ona [1 ]
Xu, Yili [1 ]
Fenaux, Martijn [1 ]
Eng, Stacey [1 ]
Tirunagari, Neeraj [1 ]
Peng, Betty [1 ]
Yu, Mei [1 ]
Tian, Yang [1 ]
Lee, Yu-Jen [1 ]
Stepan, George [1 ]
Lagpacan, Leanna L. [1 ]
Jin, Debi [1 ]
Hung, Magdeleine [1 ]
Ku, Karin S. [1 ]
Han, Bin [1 ]
Kitrinos, Kathryn [1 ]
Perron, Michel [1 ]
Birkus, Gabriel [1 ]
Wong, Kelly A. [1 ]
Zhong, Weidong [1 ]
Kim, Choung U. [1 ]
Carey, Anne [1 ]
Cho, Aesop [1 ]
Ray, Adrian S. [1 ]
机构
[1] Gilead Sci Inc, Foster City, CA 94404 USA
关键词
MITOCHONDRIAL TOXICITY; CHIMERIC REPLICONS; POLYMERASE; EFFICACY; THERAPY; ANALOG;
D O I
10.1128/AAC.02351-13
中图分类号
Q93 [微生物学];
学科分类号
071005 ; 100705 ;
摘要
As a class, nucleotide inhibitors (NIs) of the hepatitis C virus (HCV) nonstructural protein 5B (NS5B) RNA-dependent RNA polymerase offer advantages over other direct-acting antivirals, including properties, such as pangenotype activity, a high barrier to resistance, and reduced potential for drug-drug interactions. We studied the in vitro pharmacology of a novel C-nucleoside adenosine analog monophosphate prodrug, GS-6620. It was found to be a potent and selective HCV inhibitor against HCV replicons of genotypes 1 to 6 and against an infectious genotype 2a virus (50% effective concentration [EC50], 0.048 to 0.68 mu M). GS-6620 showed limited activities against other viruses, maintaining only some of its activity against the closely related bovine viral diarrhea virus (EC50, 1.5 mu M). The active 5'-triphosphate metabolite of GS-6620 is a chain terminator of viral RNA synthesis and a competitive inhibitor of NS5B-catalyzed ATP incorporation, with K-i/K-m values of 0.23 and 0.18 for HCV NS5B genotypes 1b and 2a, respectively. With its unique dual substitutions of 1'-CN and 2'-C-Me on the ribose ring, the active triphosphate metabolite was found to have enhanced selectivity for the HCV NS5B polymerase over host RNA polymerases. GS-6620 demonstrated a high barrier to resistance in vitro. Prolonged passaging resulted in the selection of the S282T mutation in NS5B that was found to be resistant in both cellular and enzymatic assays (>30-fold). Consistent with its in vitro profile, GS-6620 exhibited the potential for potent anti-HCV activity in a proof-of-concept clinical trial, but its utility was limited by the requirement of high dose levels and pharmacokinetic and pharmacodynamic variability.
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收藏
页码:1930 / 1942
页数:13
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