Viruses (Nov 2021)

Drug Resistance Profile and Clinical Features for Hepatitis C Patients Experiencing DAA Failure in Taiwan

  • Chun-Ming Hong,
  • You-Yu Lin,
  • Chun-Jen Liu,
  • Ya-Yun Lai,
  • Shiou-Hwei Yeh,
  • Hung-Chih Yang,
  • Jia-Horng Kao,
  • Shih-Jer Hsu,
  • Yi-Hsiang Huang,
  • Sheng-Shun Yang,
  • Hsing-Tao Kuo,
  • Pin-Nan Cheng,
  • Ming-Lung Yu,
  • Pei-Jer Chen

DOI
https://doi.org/10.3390/v13112294
Journal volume & issue
Vol. 13, no. 11
p. 2294

Abstract

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About 4% of the population in Taiwan are seropositive for anti-HCV Ab and 70% with HCV RNA. To address this high chronic hepatitis C disease load, Taiwan National Health Insurance started reimbursing genotype-specific DAAs in 2017 and pangenotype DAAs in mid-2018. With a 97% SVR12 rate, there were still 2–3% of patients that failed to clear HCV. To understand the causes of DAA failure in Taiwan, we conducted a multi-center, clinical, and virologic study. A total of 147 DAA-failure patients were recruited, and we searched HCV NS3/4A, NS5A and NS5B for known resistance-associated substitutions (RASs) by population sequencing, and conducted whole genome sequencing (WGS) for those without known RASs. A total of 107 patients received genotype-specific DAAs while 40 had pangenotype DAAs. Clinically, the important cause of failure is poor adherence. Virologically, common RASs in genotype-specific DAAs were NS5A-L31, NS5A-Y93, and NS5B-C316, while common RASs in pangenotype DAAs were NS5A-L31, NS5A-A/Q/R30, and NS5A-Y93. Additionally, new amino acid changes were found by WGS. Finally, we identified 12 cases with inconsistent baseline and post-treatment HCV genotypes, which is suggestive of re-infection rather than treatment failure. Our study described the drug resistance profile for DAA failure in Taiwan, showing differences from other countries.

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