PD-1 signaling is essential for the early accumulation of HBV-specific CD8+ T cells during HBV infection

  1. Xiaoqing Zeng
  2. Wen Pan
  3. Ziwei Li
  4. Zhaoli Liu
  5. Hongming Huang
  6. Xuecheng Yang
  7. Kathrin Sutter
  8. Mengji Lu
  9. Ulf Dittmer
  10. Gennadiy Zelinskyy
  11. Xin Zheng
  12. Dongliang Yang
  13. Patrick T.F. Kennedy
  14. Yanqin Du
  15. Jia Liu
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Abstract

Background & Aims

Programmed cell death Protein 1(PD-1) is one of the key inhibitory receptors that regulates CD8 T cell exhaustion during chronic viral infection. However, the role of PD-1 in modulating effector T cell differentiation and function during early phase of hepatitis B virus (HBV) infection remains poorly defined.

Methods

Using adoptive transfer of wild-type or PD-1 KO HBV-specific TCR transgenic (C93-TCRtg) CD8⁺ T cells, flow cytometry, and transcriptome sequencing, we systematically profiled early PD-1 dynamics in splenic and intrahepatic T cells and evaluated how PD-1 deficiency shapes anti-HBV T cell responses in acute self-resolving (AR) and chronic (CH) HBV mouse models.

Results

Acute HBV infection induced sustained PD-1 upregulation on intrahepatic/splenic CD8⁺ T cells, which predominantly exhibited an effector phenotype. PD-1⁺ cells displayed enhanced proliferation, cytotoxicity, and effector cytokine production compared to PD-1⁻ counterparts. Adoptive transfer of PD-1 KO C93-TCRtg CD8⁺ T cells resulted in significantly impaired early expansion in both spleen and liver during acute infection, accompanied by reduced granzyme B expression while maintaining IFN-γ, TNF-α, or IL-2 production. Transcriptomic analysis revealed that PD-1 deficiency was associated with the upregulation of apoptosis gene signatures. In chronic HBV infection, PD-1 KO cells failed to expand long-term and exhibited exacerbated exhaustion evidenced by a loss of IFN-γ production.

Conclusions

PD-1 is essential for the early expansion and survival of HBV-specific CD8⁺ T cells during acute infection and does not suppress their effector cytokine function. Its absence impairs proliferation and promotes exhaustion of HBV-specific CD8⁺ T cell in chronic infections.

Impact and implications

Our study redefines PD-1’s role in acute HBV infection. Rather than merely constraining effector function, PD-1 is essential for the early expansion and survival of HBV-specific CD8 + T cells, acting as a safeguard against activation-induced apoptosis. The context-dependent functions position PD-1 as a critical rheostat calibrating the magnitude and quality of the antiviral CD8 + T cell response, with significant implications for immunotherapeutic strategies targeting this pathway in hepatitis B.

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  1. Version published to 10.1101/2025.09.17.676789 on bioRxiv