AAV-HBV mouse model replicates the intrahepatic immune landscape of chronic HBV patients at single-cell level

被引:0
作者
Conceicao-Neto, Nadia [1 ]
Pierson, Wim [1 ]
Han, Qinglin [2 ]
Yao, Zhiyuan [3 ]
Wu, Qun [2 ]
Dockx, Koen [4 ]
Aerts, Liese [1 ]
De Maeyer, Dries [5 ]
Beyens, Matthias [5 ]
Van den Berge, Koen [6 ]
Li, Chris [3 ]
Kukolj, George [3 ,8 ]
Zhu, Ren [2 ]
Krishna, Vinod [7 ]
Podlaha, Ondrej [3 ]
Najera, Isabel [3 ]
Van Gulck, Ellen [1 ]
机构
[1] Johnson & Johnson Innovat Med, ID Discovery, Infect Dis Therapeut Area, Beerse, Belgium
[2] Johnson & Johnson Innovat Med, ID Discovery, Infect Dis Therapeut Area, Shanghai, Peoples R China
[3] Johnson & Johnson Innovat Med, ID Discovery, Infect Dis Therapeut Area, Brisbane, CA USA
[4] Charles River Labs, Beerse, Belgium
[5] Johnson & Johnson Innovat Med, Discovery Therapeut & Mol Pharmacol, Beerse, Belgium
[6] Johnson & Johnson Innovat Med, Stat & Decis Sci, Beerse, Belgium
[7] Johnson & Johnson Innovat Med, ID Discovery, Infect Dis Therapeut Area, Spring House, PA USA
[8] McGill Univ, Dept Microbiol & Immunol, Montreal, PQ, Canada
来源
FRONTIERS IN IMMUNOLOGY | 2025年 / 16卷
关键词
hepatitis B virus; single-cell transcriptome; AAV-HBV-infected mouse model; T cell exhaustion; chronic HBV; HEPATITIS-B-VIRUS; CD8(+) T-CELLS; PROGRAMMED DEATH-1; EXPRESSION; DYSFUNCTION; EXHAUSTION; INFECTION; RESPONSES; BLOCKADE;
D O I
10.3389/fimmu.2025.1421712
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Introduction Unresolved hepatitis B virus (HBV) infection leads to a progressive state of HBV-specific immune dysfunctionality that characterizes chronic infection. The immune-competent adeno associated virus (AAV)-HBV mouse model is commonly used preclinically, though a comprehensive characterization of the liver immune microenvironment and its translatability to human infection is still lacking. We investigated the intrahepatic immune profile of the AAV-HBV mouse model at a single-cell level and compared with data from CHB patients in immune tolerant (IT) and immune active (IA) clinical stages.Methods Immune exhaustion was profiled through an iterative subclustering approach for cell-typing analyses of single-cell RNA-sequencing data in CHB donors and compared to the AAV-HBV mouse model 4-weeks and 24-weeks post-transduction to assess its translatability. This was confirmed using an exhaustion flow cytometry panel at 4 and 42-weeks post-transduction.Results Using single-cell RNA-sequencing, CD8 pre-exhausted T-cells with self-renewing capacity (TCF7+), and terminally exhausted CD8 T-cells (TCF7-) were detected in the AAV-HBV model. These terminally exhausted CD8 T-cells (expressing Pdcd1, Tox, Lag3, Tigit) were significantly enriched versus control mice and independently identified through flow cytometry. Importantly, comparison to CHB human data showed a similar exhausted CD8 T-cell population in IT and IA donors, but not in uninfected individuals.Discussion Long term high titer AAV-HBV mouse liver transduction led to T-cell exhaustion, as evidenced by expression of conventional immune checkpoint markers at mRNA and protein levels. In both IT and IA donors, a similar CD8 exhausted T-cell population was identified, with increased frequency observed in IA donors. These data support the use of the AAV-HBV mouse model to study classical T-cell exhaustion in HBV infection and the effect of immune-based therapeutic interventions.
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