Retreatment with HBV siRNA Results in Additional Reduction in HBV Antigenemia and Immune Stimulation in the AAV-HBV Mouse Model

Viruses. 2024 Feb 23;16(3):347. doi: 10.3390/v16030347.

Abstract

Background and aims: Treatment with siRNAs that target HBV has demonstrated robust declines in HBV antigens. This effect is also observed in the AAV-HBV mouse model, which was used to investigate if two cycles of GalNAc-HBV-siRNA treatment could induce deeper declines in HBsAg levels or prevent rebound, and to provide insights into the liver immune microenvironment.

Methods: C57Bl/6 mice were transduced with one of two different titers of AAV-HBV for 28 days, resulting in stable levels of HBsAg of about 103 or 105 IU/mL. Mice were treated for 12 weeks (four doses q3wk) per cycle with 3 mg/kg of siRNA-targeting HBV or an irrelevant sequence either once (single treatment) or twice (retreatment) with an 8-week treatment pause in between. Blood was collected to evaluate viral parameters. Nine weeks after the last treatment, liver samples were collected to perform phenotyping, bulk RNA-sequencing, and immunohistochemistry.

Results: Independent of HBsAg baseline levels, treatment with HBV-siRNA induced a rapid decline in HBsAg levels, which then plateaued before gradually rebounding 12 weeks after treatment stopped. A second cycle of HBV-siRNA treatment induced a further decline in HBsAg levels in serum and the liver, reaching undetectable levels and preventing rebound when baseline levels were 103 IU/mL. This was accompanied with a significant increase in inflammatory macrophages in the liver and significant upregulation of regulatory T-cells and T-cells expressing immune checkpoint receptors.

Conclusions: Retreatment induced an additional decline in HBsAg levels, reaching undetectable levels when baseline HBsAg levels were 3log10 or less. This correlated with T-cell activation and upregulation of Trem2.

Keywords: T-cell exhaustion; Trem2; hepatitis surface antigen; liver; sequencing.

MeSH terms

  • Animals
  • Antiviral Agents / therapeutic use
  • DNA, Viral
  • Hepatitis B Surface Antigens*
  • Hepatitis B virus* / genetics
  • Liver
  • Membrane Glycoproteins
  • Mice
  • RNA, Small Interfering / genetics
  • Receptors, Immunologic
  • Retreatment

Substances

  • Hepatitis B Surface Antigens
  • RNA, Small Interfering
  • DNA, Viral
  • Antiviral Agents
  • Trem2 protein, mouse
  • Membrane Glycoproteins
  • Receptors, Immunologic

Grants and funding

This research received no external funding.