Virology Journal (Dec 2024)

Mechanisms underlying the compromised clinical efficacy of interferon in clearing HBV

  • Zhuoyan Lei,
  • Luye Wang,
  • Hanlin Gao,
  • Shubian Guo,
  • Xinjian Kang,
  • Jiajun Yuan,
  • Ziying Lv,
  • Yuxin Jiang,
  • Jinping Yi,
  • Zhi Chen,
  • Gang Wang

DOI
https://doi.org/10.1186/s12985-024-02589-3
Journal volume & issue
Vol. 21, no. 1
pp. 1 – 13

Abstract

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Abstract Hepatitis B virus (HBV) is a hepatotropic DNA virus that can cause acute or chronic hepatitis, representing a significant global health concern. By 2019, approximately 296 million individuals were chronically infected with HBV, with 1.5 million new cases annually and 820,000 deaths due to HBV-related cirrhosis and liver cancer. Current treatments for chronic hepatitis B include nucleotide analogs (NAs) and interferons (IFNs), particularly IFN-α. NAs, such as entecavir and tenofovir, inhibit viral reverse transcription, while IFN-α exerts antiviral effects by directly suppressing viral replication, modulating viral genome epigenetics, degrading cccDNA, and activating immune responses. Despite its potential, IFN-α shows limited clinical efficacy, partly due to HBV’s interference with the IFN signaling pathway. HBV encodes proteins like HBc, Pol, HBsAg, and HBx that disrupt IFN-α function. For example, HBV Pol inhibits STAT1 phosphorylation, HBsAg suppresses STAT3 phosphorylation, and HBx interferes with IFN-α efficacy through multiple mechanisms. Additionally, HBV downregulates key genes in the IFN signaling pathway, further diminishing IFN-α’s antiviral effects. Understanding these interactions is crucial for improving IFN-α-based therapies. Future research may focus on overcoming HBV resistance by targeting viral proteins or optimizing IFN-α delivery. In summary, HBV’s ability to resist IFN-α limits its therapeutic effectiveness, highlighting the need for new strategies to enhance treatment outcomes.

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