Intrahepatic CD161hiCD8+T Cell Recruitment Has a Pathogenetic Potential in Chronic HBV Infection

IF 3.1 4区 医学 Q3 IMMUNOLOGY Immunity, Inflammation and Disease Pub Date : 2025-01-12 DOI:10.1002/iid3.70118
Jianfei Li, Qian Liu, Wanlu Duan, Zhi Duan, Futing Liu, Mengqi Ruan, Qiyin Zong, Hao Zhang, Qiang Zhou, Qin Wang
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Abstract

Backgrounds and Aims

CD8+T cells are crucially associated with the fight against hepatitis B virus (HBV) infection. CD161 has been shown to express remarkably on HCV-specific CD8+T cells. However, the accurate function of CD161+CD8+T cells in HBV immunity or pathogenesis remains undetermined.

Methods

Blood samples were collected from 25 chronic hepatitis B (CHB) patients. Peripheral blood levels of CD161+CD8+T cells and their correlation with serum ALT levels were analyzed in CHB patients. To analyze the in vivo CD161+CD8+T cell's number, function, and intrahepatic recruitment characteristics, HBV replication mouse models were established. The expression of CD161 on HBV-specific CD8+T cells was also detected by analyzing CD161+CD8+T cell functions during infection.

Results

Patients with CHB infection had a markedly lower peripheral blood frequency of CD161+CD8+T cells than did healthy controls and negatively correlated with serum ALT level. Furthermore, compared to the control mice, the frequency of CD161+CD8+T cells was significantly decreased in the blood of acute and chronic HBV-replicating mice. Moreover, CHB-replicating mice had significantly increased hepatic levels of CD161+CD8+T cells, which was not observed in the acute group of mice. Additionally, the CD161+CD8+T cells were categorized into CD161hi and CD161intCD8+T cells and it was revealed that in the liver of CHB-replicating mice the primary recruited cells were CD161hiCD8+T. Intrahepatic CD161hiCD8+T cells demonstrated increased CXCR6 expression, enhanced production of cytokine IL-17 and TNF-ɑ, and reduced IFN-γ secretion. Accordingly, the CXCL16 mRNA expression in the liver tissue of CHB-replication mice was markedly higher than in acute HBV-replicating and control mice. The study also revealed that HBV-specific CD8+T cells were mainly CD161-CD8+T cells.

Conclusion

During HBV infection, the intrahepatic recruitment of CD161+CD8+T cells was mainly CD161hiCD8+T cell subpopulation, which has a weak antiviral response, but increased pro-inflammatory effect, suggesting that CD161 may serve as a potential marker of liver-damaging T cells.

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肝内CD161hiCD8+T细胞募集在慢性HBV感染中具有致病潜力。
背景和目的:CD8+T 细胞与抗击乙型肝炎病毒(HBV)感染密切相关。CD161 已被证明在 HCV 特异性 CD8+T 细胞上显著表达。然而,CD161+CD8+T 细胞在 HBV 免疫或发病机制中的确切功能仍未确定:方法:采集了 25 名慢性乙型肝炎(CHB)患者的血样。方法:采集 25 名慢性乙型肝炎(CHB)患者的血样,分析其外周血 CD161+CD8+T 细胞水平及其与血清 ALT 水平的相关性。为了分析体内 CD161+CD8+T 细胞的数量、功能和肝内募集特征,建立了 HBV 复制小鼠模型。通过分析 CD161+CD8+T 细胞在感染过程中的功能,还检测了 CD161 在 HBV 特异性 CD8+T 细胞上的表达:结果:CHB 感染患者外周血 CD161+CD8+T 细胞的频率明显低于健康对照组,且与血清 ALT 水平呈负相关。此外,与对照组小鼠相比,急性和慢性 HBV 复制小鼠血液中 CD161+CD8+T 细胞的频率明显降低。此外,慢性 HBV 复制小鼠肝脏中的 CD161+CD8+T 细胞水平明显升高,而急性组小鼠未观察到这一现象。此外,CD161+CD8+T细胞被分为CD161hi和CD161intCD8+T细胞,结果显示,在CHB复制小鼠的肝脏中,主要被招募的细胞是CD161hiCD8+T细胞。肝内 CD161hiCD8+T 细胞的 CXCR6 表达增加,细胞因子 IL-17 和 TNF-ɑ 的产生增强,IFN-γ 的分泌减少。因此,CHB 复制小鼠肝组织中的 CXCL16 mRNA 表达明显高于急性 HBV 复制小鼠和对照组小鼠。研究还发现,HBV 特异性 CD8+T 细胞主要是 CD161-CD8+T 细胞:结论:在HBV感染期间,肝内招募的CD161+CD8+T细胞主要是CD161hiCD8+T细胞亚群,其抗病毒反应较弱,但促炎作用增强,提示CD161可作为肝损伤T细胞的潜在标志物。
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来源期刊
Immunity, Inflammation and Disease
Immunity, Inflammation and Disease Medicine-Immunology and Allergy
CiteScore
3.60
自引率
0.00%
发文量
146
审稿时长
8 weeks
期刊介绍: Immunity, Inflammation and Disease is a peer-reviewed, open access, interdisciplinary journal providing rapid publication of research across the broad field of immunology. Immunity, Inflammation and Disease gives rapid consideration to papers in all areas of clinical and basic research. The journal is indexed in Medline and the Science Citation Index Expanded (part of Web of Science), among others. It welcomes original work that enhances the understanding of immunology in areas including: • cellular and molecular immunology • clinical immunology • allergy • immunochemistry • immunogenetics • immune signalling • immune development • imaging • mathematical modelling • autoimmunity • transplantation immunology • cancer immunology
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