C-C趋化因子受体7型(CCR7)调节肝脏CD8+ T细胞的稳态和对急性肝损伤的反应。

IF 12.9 1区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY
Hepatology Pub Date : 2024-11-01 Epub Date: 2024-01-17 DOI:10.1097/HEP.0000000000000757
Patricia Niemietz, Moritz Peiseler, Marlene Kohlhepp, Paul Horn, Kylie Matchett, Yuting Wang, Leon Haas, Tianjiao Zhang, Alix Bruneau, Adrien Guillot, Hilmar Berger, Anke Liepelt, Klaudia Warzecha, Catharina Demske, Diana Möckel, Twan Lammers, Neil Henderson, Felix Heymann, Frank Tacke
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引用次数: 0

摘要

背景目的:急性肝衰竭(ALF)是一种罕见但危及生命的疾病,药物性肝损伤(DILI),尤其是对乙酰氨基酚(APAP)毒性,是导致ALF的主要原因。先天性免疫机制进一步延续了肝损伤,而适应性免疫系统在 DILI 相关 ALF 中的作用尚不清楚:我们分析了两个独立的 ALF 患者队列的肝组织,发现肝 T 细胞浸润是人类 ALF 的一个显著特征。CD8+ T细胞的特征是向坏死区域分带和活化的基因表达特征。在 APAP 诱导的小鼠肝损伤中,体视显微镜显示 CD8+ T 细胞在坏死区域呈带状分布,而不是 CD4+ T 细胞。基因表达分析显示,肝脏中的C-C趋化因子受体7(CCR7)及其配体CCL21上调,肝脏CD8+T细胞的表型广泛活化。在两种 ALF 小鼠模型中,Ccr7-/-小鼠的早期肝损伤明显加重。在功能上,CCR7不参与CD8+ T细胞的招募,但可能通过淋巴管的排出调节其活化谱。Ccr7-/- CD8+ T细胞的特点是活化、效应和衰竭特征表达升高。收养性转移显示,CCR7缺陷的CD8+ T细胞优先归巢到肝脏,CD8+ T细胞的耗竭减轻了小鼠的肝损伤:我们的研究表明,适应性免疫系统参与了人类和小鼠的 ALF。结论:我们的研究表明,适应性免疫系统参与了人类和小鼠的 ALF。我们发现 CCR7-CCL21 轴是一个重要的调节途径,可提供下游保护,防止 T 细胞介导的肝损伤。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
C-C chemokine receptor type 7 (CCR7) regulates hepatic CD8 + T cell homeostasis and response to acute liver injury.

Background and aims: Acute liver failure (ALF) is a rare but life-threatening condition, and DILI, particularly acetaminophen toxicity, is the leading cause of ALF. Innate immune mechanisms further perpetuate liver injury, while the role of the adaptive immune system in DILI-related ALF is unclear.

Approach and results: We analyzed liver tissue from 2 independent patient cohorts with ALF and identified hepatic T cell infiltration as a prominent feature in human ALF. CD8 + T cells were characterized by zonation toward necrotic regions and an activated gene expression signature. In murine acetaminophen-induced liver injury, intravital microscopy revealed zonation of CD8 + but not CD4 + T cells at necrotic areas. Gene expression analysis exposed upregulated C-C chemokine receptor 7 (CCR7) and its ligand CCL21 in the liver as well as a broadly activated phenotype of hepatic CD8 + T cells. In 2 mouse models of ALF, Ccr7-/- mice had significantly aggravated early-phase liver damage. Functionally, CCR7 was not involved in the recruitment of CD8 + T cells, but regulated their activation profile potentially through egress to lymphatics. Ccr7-/- CD8 + T cells were characterized by elevated expression of activation, effector, and exhaustion profiles. Adoptive transfer revealed preferential homing of CCR7-deficient CD8 + T cells to the liver, and depletion of CD8 + T cells attenuated liver damage in mice.

Conclusions: Our study demonstrates the involvement of the adaptive immune system in ALF in humans and mice. We identify the CCR7-CCL21 axis as an important regulatory pathway, providing downstream protection against T cell-mediated liver injury.

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来源期刊
Hepatology
Hepatology 医学-胃肠肝病学
CiteScore
27.50
自引率
3.70%
发文量
609
审稿时长
1 months
期刊介绍: HEPATOLOGY is recognized as the leading publication in the field of liver disease. It features original, peer-reviewed articles covering various aspects of liver structure, function, and disease. The journal's distinguished Editorial Board carefully selects the best articles each month, focusing on topics including immunology, chronic hepatitis, viral hepatitis, cirrhosis, genetic and metabolic liver diseases, liver cancer, and drug metabolism.
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