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Literature DB >> 30661248

Lymphocyte Antigen 6 Complex, Locus C⁺ Monocytes and Kupffer Cells Orchestrate Liver Immune Responses Against Hepatitis B Virus in Mice.

Li-Ling Wu¹, Wei-Hao Peng^2,3, Hui-Lin Wu⁴, Shi-Chuen Miaw⁵, Shiou-Hwei Yeh⁶, Hung-Chih Yang⁶, Pei-Hsuan Liao¹, Jing-Shan Lin¹, Yan-Rong Chen¹, Yen-Tien Hong¹, Hurng-Yi Wang^1,7, Pei-Jer Chen^1,4,6,8,9, Ding-Shinn Chen^1,4,8,9.

Abstract

To understand the mechanism(s) of age-dependent outcomes of hepatitis B virus (HBV) infection in humans, we previously established an age-related HBV mouse model in which 6-week-old (N6W) C3H/HeN mice exhibited virus tolerance whereas 12-week-old (N12W) counterparts presented virus clearance. By investigating the hepatic myeloid cell dynamics in mice of these two ages, we aim to identify factors associated with HBV clearance. C3H/HeN mice were transfected with an HBV plasmid by hydrodynamic injection. Serum HBV markers were monitored weekly. Hepatic leucocyte populations and their cytokine/chemokine productions were examined at baseline, day 3 (D3), day 7 (D7), and day 14 after injection. C-C chemokine receptor type 2 (CCR2) antagonist and clodronate (CLD) were respectively administered to N12W and N6W mice to study the roles of lymphocyte antigen 6 complex, locus C (Ly6C)+ monocytes and Kupffer cells (KCs) in viral clearance. N12W mice had a significantly higher number of TNF-α-secreting Ly6C+ monocytes and fewer IL-10-secreting KCs at D3 in the liver than their younger N6W counterparts after HBV transfection. In addition, the elevated number of interferon-γ+ TNF-α+ CD8+ T cells at D7 was only seen in the older cohort. The enhanced Ly6C+ monocyte induction in N12W mice resulted from elevated C-C motif chemokine ligand 2 (CCL2) secretion by hepatocytes. CCR2 antagonist administration hampered Ly6C+ monocyte recruitment and degree of KC reduction and delayed HBV clearance in N12W animals. Depletion of KCs by CLD liposomes enhanced Ly6C+ monocyte recruitment and accelerated HBV clearance in N6W mice. Conclusions: Ly6C+ monocytes and KCs may, respectively, represent the resistance and tolerance arms of host defenses. These two cell types play an essential role in determining HBV clearance/tolerance. Manipulation of these cells is a promising avenue for immunotherapy of HBV-related liver diseases.

Entities: Chemical Disease Gene Mutation Species

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Year: 2019 PMID： 30661248 DOI： 10.1002/hep.30510

Source DB: PubMed Journal: Hepatology ISSN： 0270-9139 Impact factor: 17.425

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Cited

14 in total

1. Stem Cell-Derived Viral Ag-Specific T Lymphocytes Suppress HBV Replication in Mice.

Authors: Xiaofang Xiong; Fengyang Lei; Mohammad Haque; Jianxun Song
Journal: J Vis Exp Date: 2019-09-25 Impact factor: 1.355

2. TLR5 activation in hepatocytes alleviates the functional suppression of intrahepatic CD8⁺ T cells.

Authors: Hu Yan; Maohua Zhong; Jingyi Yang; Jiabao Guo; Jie Yu; Yi Yang; Zhiyong Ma; Bali Zhao; Yue Zhang; Junzhong Wang; Chunchen Wu; Ulf Dittmer; Dongliang Yang; Mengji Lu; Ejuan Zhang; Huimin Yan
Journal: Immunology Date: 2020-10-12 Impact factor: 7.397

3. Human amniotic mesenchymal stromal cells alleviate acute liver injury by inhibiting the pro-inflammatory response of liver resident macrophage through autophagy.

Authors: Dongxu Hua; Zheng Ju; Xiaojie Gan; Qi Wang; Chenghuan Luo; Jian Gu; Yue Yu
Journal: Ann Transl Med Date: 2019-08

Review 4. Pathogenetic Mechanisms of T Cell Dysfunction in Chronic HBV Infection and Related Therapeutic Approaches.

Authors: Paola Fisicaro; Valeria Barili; Marzia Rossi; Ilaria Montali; Andrea Vecchi; Greta Acerbi; Diletta Laccabue; Alessandra Zecca; Amalia Penna; Gabriele Missale; Carlo Ferrari; Carolina Boni
Journal: Front Immunol Date: 2020-05-12 Impact factor: 7.561

5. Acidic Microenvironment Aggravates the Severity of Hepatic Ischemia/Reperfusion Injury by Modulating M1-Polarization Through Regulating PPAR-γ Signal.

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Journal: Front Immunol Date: 2021-06-21 Impact factor: 7.561

6. HBV X protein-based therapeutic vaccine accelerates viral antigen clearance by mobilizing monocyte infiltration into the liver in HBV carrier mice.

Authors: Jau-Hau Horng; Wei-Hsiang Lin; Chang-Ru Wu; You-Yu Lin; Li-Ling Wu; Ding-Shinn Chen; Pei-Jer Chen
Journal: J Biomed Sci Date: 2020-05-28 Impact factor: 8.410

7. Stem Cell-Derived Viral Antigen-Specific T Cells Suppress HBV Replication through Production of IFN-γ and TNF-⍺.

Authors: Mohammad Haque; Fengyang Lei; Xiaofang Xiong; Yijie Ren; Anil Kumar; Jugal Kishore Das; Xingcong Ren; Deyu Fang; Paul de Figueiredo; Jin-Ming Yang; Jianxun Song
Journal: iScience Date: 2020-07-01

Review 8. HBV-Induced Immune Imbalance in the Development of HCC.

Authors: Yongyan Chen; Zhigang Tian
Journal: Front Immunol Date: 2019-08-27 Impact factor: 7.561

9. Hepatitis B Core Antigen Impairs the Polarization While Promoting the Production of Inflammatory Cytokines of M2 Macrophages via the TLR2 Pathway.

Authors: Hongyu Yi; Ye Zhang; Xiaofei Yang; Mengyuan Li; Haifeng Hu; Jie Xiong; Ning Wang; Jingyi Jin; Yusi Zhang; Yun Song; Xian Wang; Lihua Chen; Jianqi Lian
Journal: Front Immunol Date: 2020-03-27 Impact factor: 7.561

10. Ultrastructural and diffusion tensor imaging studies reveal axon abnormalities in Pompe disease mice.

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Journal: Sci Rep Date: 2020-11-19 Impact factor: 4.379