1. Academic Validation
  2. Effects of resistance-associated variants in genotype 2 hepatitis C virus on viral replication and susceptibility to antihepatitis C virus drugs

Effects of resistance-associated variants in genotype 2 hepatitis C virus on viral replication and susceptibility to antihepatitis C virus drugs

  • Hepatol Res. 2019 Nov;49(11):1275-1285. doi: 10.1111/hepr.13401.
Goki Suda 1 Megumi Kimura 1 Taku Shigesawa 1 Kazuharu Suzuki 1 Akihisa Nakamura 1 Masatsugu Ohara 1 Naoki Kawagishi 1 Masato Nakai 1 Takuya Sho 1 Osamu Maehara 1 Tomoe Shimazaki 1 Kenichi Morikawa 1 Mitsuteru Natsuizaka 1 Koji Ogawa 1 Naoya Sakamoto 1
Affiliations

Affiliation

  • 1 Department of Gastroenterology and Hepatology, Hokkaido University, Sapporo, Japan.
Abstract

Aims: Development of direct-acting antivirals (DAAs) has made antihepatitis C virus (HCV) treatment highly safe and effective. However, the emergence of resistant-associated variants (RAVs) after failure of DAA therapy affects retreatment outcomes. In particular, genotype 1 HCV with P32 deletion has been reported to be highly resistant to all approved non-structural protein (NS)5A inhibitors. However, analysis of RAVs in genotype 2 HCV has been limited. Accordingly, in this study, we evaluated the roles of genotype 2 HCV variants in Antiviral drug efficacy.

Methods: We utilized HCV-2b/2a (JFH-1) chimeric virus (genotype 2a), which replicates more robustly than JFH-1. We constructed various genotype 2a JFH-1-based HCV Cell Culture systems with NS3 (D168E), NS5A (F28S, F28S/M31I, P32 deletion, and Y93H), and NS5B (S282 T) RAVs and analyzed the replication ability and sensitivity to various anti-HCV reagents.

Results: Genotype 2a-based HCV with NS5A-P32 deletion could not replicate even in long-term cultures. Genotype 2a-based HCV with NS5A-F28S/M31I showed significantly higher replication ability than the wild-type strain, and replication could not be suppressed, even with high concentrations of NS5A inhibitors, including pibrentasvir and velpatasvir (<1000-10 000 fold-resistance compared with the wild-type strain). However, genotype 2a-based HCV with NA5A-F28S/M31I was sensitive to HCV Protease Inhibitor, NS5B inhibitor, interferon-α, and ribavirin. Genotype 2a-based HCV with NS5B-S282 T was resistant to sofosbuvir, but was highly sensitive to ribavirin compared with the control.

Conclusions: When undertaking retreatment for genotype 2a HCV-infected patients who fail to respond to DAAs, the optimized retreatment should be chosen according to the sensitivity of the emerging RAVs to anti-HCV drugs.

Keywords

NS5A F28S/M31I; NS5B S282 T; genotype 2; hepatitis C virus; resistant-associated variant.

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