1. Academic Validation
  2. The novel nucleoside analog R1479 (4'-azidocytidine) is a potent inhibitor of NS5B-dependent RNA synthesis and hepatitis C virus replication in cell culture

The novel nucleoside analog R1479 (4'-azidocytidine) is a potent inhibitor of NS5B-dependent RNA synthesis and hepatitis C virus replication in cell culture

  • J Biol Chem. 2006 Feb 17;281(7):3793-9. doi: 10.1074/jbc.M510195200.
Klaus Klumpp 1 Vincent Lévêque Sophie Le Pogam Han Ma Wen-Rong Jiang Hyunsoon Kang Caroline Granycome Margaret Singer Carl Laxton Julie Qi Hang Keshab Sarma David B Smith Dieter Heindl Chris J Hobbs John H Merrett Julian Symons Nick Cammack Joseph A Martin Rene Devos Isabel Nájera
Affiliations

Affiliation

  • 1 Roche Palo Alto LLC, CA 94304, USA. klaus.klumpp@roche.com
Abstract

Hepatitis C virus (HCV) polymerase activity is essential for HCV replication. Targeted screening of nucleoside analogs identified R1479 (4'-azidocytidine) as a specific inhibitor of HCV replication in the HCV subgenomic replicon system (IC(50) = 1.28 microM) with similar potency compared with 2'-C-methylcytidine (IC(50) = 1.13 microM). R1479 showed no effect on cell viability or proliferation of HCV replicon or Huh-7 cells at concentrations up to 2 mM. HCV replicon RNA could be fully cleared from replicon cells after prolonged incubation with R1479. The corresponding 5'-triphosphate derivative (R1479-TP) is a potent inhibitor of native HCV replicase isolated from replicon cells and of recombinant HCV polymerase (NS5B)-mediated RNA synthesis activity. R1479-TP inhibited RNA synthesis as a CTP-competitive inhibitor with a K(i) of 40 nM. On an HCV RNA-derived template substrate (complementary internal ribosome entry site), R1479-TP showed similar potency of NS5B inhibition compared with 3'-dCTP. R1479-TP was incorporated into nascent RNA by HCV polymerase and reduced further elongation with similar efficiency compared with 3'-dCTP under the reaction conditions. The S282T point mutation in the coding sequence of NS5B confers resistance to inhibition by 2'-C-MeATP and Other 2'-methyl-nucleotides. In contrast, the S282T mutation did not confer cross-resistance to R1479.

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