Cytokines and Chemokines in HBV Infection

Zhong, Shihong; Zhang, Tianling; Tang, Libo; Li, Yongyin

doi:10.3389/fmolb.2021.805625

Cited by 32 publications

(39 citation statements)

References 177 publications

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“…These findings implied that chronic HBV infection resulted in the host’s immune disorder and dysregulation by upregulating immune checkpoint molecules, including TIM-3, PD-1, CTLA-4, and LAG-3 on T cells, that induced T-cell dysfunction in chronic HBV infection. In addition, our results showed that serum cytokines (IL-2, IL-4, and TNF-a) had a low trend in chronic ASCs with HBeAg-negative in comparison with HC, which were partially consistent with previous reports ( Ayada et al, 2006 ; Wang X. et al, 2018 ; Zhong et al, 2021 ). These cytokines play a critical role in regulating CD4/CD8 + T cell proliferation and differentiation and the production of various specific antibodies to control persistent HBV infection ( Buschow and Jansen, 2021 ; Mak et al, 2021 ; Zhong et al, 2021 ).…”

Section: Discussionsupporting

confidence: 92%

“…In addition, our results showed that serum cytokines (IL-2, IL-4, and TNF-a) had a low trend in chronic ASCs with HBeAg-negative in comparison with HC, which were partially consistent with previous reports ( Ayada et al, 2006 ; Wang X. et al, 2018 ; Zhong et al, 2021 ). These cytokines play a critical role in regulating CD4/CD8 + T cell proliferation and differentiation and the production of various specific antibodies to control persistent HBV infection ( Buschow and Jansen, 2021 ; Mak et al, 2021 ; Zhong et al, 2021 ).…”

Section: Discussionsupporting

confidence: 92%

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Immune Checkpoint Molecules Expressed on CD4+ T Cell Subsets in Chronic Asymptomatic Hepatitis B Virus Carriers With Hepatitis B e Antigen-Negative

Cui

Yan

Liu³

et al. 2022

Front. Microbiol.

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BackgroundChronic hepatitis B virus (HBV) infection remains a major public health problem worldwide. Immune checkpoint molecules expressed on CD4+ T cells play critical roles in chronic HBV infection. However, their roles in chronic asymptomatic HBV carriers (ASCs) with hepatitis B e antigen (HBeAg)-negative remain unclear. In this study, we explored the role of immune checkpoint molecules expressed on CD4+ T cell subsets in chronic ASCs with HBeAg-negative.MethodsHuman peripheral blood mononuclear cells (PBMCs) from the ASCs with HBeAg-negative and healthy controls (HC) were isolated, and immune checkpoint molecules expressed on CD4+ T cell subsets and serum cytokines were detected by flow cytometry. Moreover, the mRNA expressions of immune checkpoint molecules were analyzed by a real-time quantitative PCR assay.ResultsIn comparison with HC, CD4+ T cells highly expressed LAG-3, TIM-3, and PD-1 in PBMCs from chronic ASCs with HBeAg-negative. Interestingly, the expressions of TIM-3 and PD-1 on circulating follicular helper T (Tfh) cells in ASCs were significantly high. Moreover, high expressions of LAG-3, TIM-3, and PD-1 were different among Treg, Th1, Th2, and Th17 cells. In addition, the expressions of TIM-3 and CTLA-4 mRNA in PBMCs from ASCs were significantly elevated. However, the frequency of CTLA-4+CD4+ T cell subsets in PBMCs from ASCs was not different from HC. The levels of six cytokines in serum from ASCs were not clearly different from HC.ConclusionImmune checkpoint molecules highly expressed on CD4+ T cell subsets indicated an important role in chronic ASCs with HBeAg-negative, which provided potential therapeutic targets in the pathogenesis of chronic HBV infection.

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Section: Discussionsupporting

confidence: 92%

Section: Discussionsupporting

confidence: 92%

Immune Checkpoint Molecules Expressed on CD4+ T Cell Subsets in Chronic Asymptomatic Hepatitis B Virus Carriers With Hepatitis B e Antigen-Negative

Cui

Yan

Liu³

et al. 2022

Front. Microbiol.

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“…Similarly, IL-6 inhibits HBV transcription by epigenetic mechanisms, in addition to performing a broad range of pro-and anti-inflammatory signaling (36). This pro-inflammatory cytokine pattern is similar to that resulted after the viral infection or TLR-9 stimulation, suggesting a crosstalk between that innate and adaptive immunity influencing the antigen specific immune response (34,67). Clearly, further research involving more relevant animal models is needed to understand the true benefit of a particular Tcell activation pattern.…”

Section: Discussionmentioning

confidence: 92%

“…Clearly, further research involving more relevant animal models is needed to understand the true benefit of a particular Tcell activation pattern. This will ultimately depend on the fine balance between the capacity of the complex cytokine-mediated pathways to boost anti-HBV immunity on one hand, and to potentially cause liver inflammation, on the other (34). An important finding emerging from this study is the equivalence of the S and S/preS1 antigens produced in mammalian cells in terms of activating an efficient WT HBVneutralizing humoral immune response and the evident superiority of the latter immunogen to prevent infection with the G145R vaccine-escape mutant.…”

Section: Discussionmentioning

confidence: 99%

“…The clustered heatmap resulting from this analysis indicates a broad spectrum of HBV-reactive T cells generated by immunization with the S and S/preS1 antigens (Figure 6). The complexity of this immune response is illustrated by the presence of pro-(TNF-a, IL-1b, IL-6, IL-17A) and anti-inflammatory cytokines (IL-10) (34), some of them with known antiviral activity against HBV (IL-1b, IL-6, IL-17A) (35)(36)(37). Importantly, both immunogens induced secretion of IFN-g, the well-accepted marker of Th cell activation, above the levels found in controls; however, this was not the predominant cytokine (Figure 6).…”

Section: Expression and Characterization Of The Novel S/pres1 Antigen...mentioning

confidence: 99%

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Efficient cellular and humoral immune response and production of virus-neutralizing antibodies by the Hepatitis B Virus S/preS116-42 antigen

et al. 2022

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Despite the availability of improved antiviral therapies, infection with Hepatitis B virus (HBV) remains a3 significant health issue, as a curable treatment is yet to be discovered. Current HBV vaccines relaying on the efficient expression of the small (S) envelope protein in yeast and the implementation of mass vaccination programs have clearly contributed to containment of the disease. However, the lack of an efficient immune response in up to 10% of vaccinated adults, the controversies regarding the seroprotection persistence in vaccine responders and the emergence of vaccine escape virus mutations urge for the development of better HBV immunogens. Due to the critical role played by the preS1 domain of the large (L) envelope protein in HBV infection and its ability to trigger virus neutralizing antibodies, including this protein in novel vaccine formulations has been considered a promising strategy to overcome the limitations of S only-based vaccines. In this work we aimed to combine relevant L and S epitopes in chimeric antigens, by inserting preS1 sequences within the external antigenic loop of S, followed by production in mammalian cells and detailed analysis of their antigenic and immunogenic properties. Of the newly designed antigens, the S/preS116–42 protein assembled in subviral particles (SVP) showed the highest expression and secretion levels, therefore, it was selected for further studies in vivo. Analysis of the immune response induced in mice vaccinated with S/preS116–42- and S-SVPs, respectively, demonstrated enhanced immunogenicity of the former and its ability to activate both humoral and cellular immune responses. This combined activation resulted in production of neutralizing antibodies against both wild-type and vaccine-escape HBV variants. Our results validate the design of chimeric HBV antigens and promote the novel S/preS1 protein as a potential vaccine candidate for administration in poor-responders to current HBV vaccines.

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Alpha‐kinase 1 (ALPK1) agonist DF‐006 demonstrates potent efficacy in mouse and primary human hepatocyte (PHH) models of hepatitis B

Fan

Liu

et al. 2022

Hepatology

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Background and Aims: In the treatment of chronic hepatitis B (CHB) infection, stimulation of innate immunity may lead to hepatitis B virus (HBV) cure. Alpha‐kinase 1 (ALPK1) is a pattern recognition receptor (PRR) that activates the NF‐κB pathway and stimulates innate immunity. Here we characterized the preclinical anti‐HBV efficacy of DF‐006, an orally active agonist of ALPK1 currently in clinical development for CHB. Approach and Results: In adeno‐associated virus (AAV)‐HBV mouse models and primary human hepatocytes (PHHs) infected with HBV, we evaluated the antiviral efficacy of DF‐006. In the mouse models, DF‐006 rapidly reduced serum HBV DNA, hepatitis B surface antigen, and hepatitis B e antigen levels using doses as low as 0.08 μg/kg, 1 μg/kg, and 5 μg/kg, respectively. DF‐006 in combination with the HBV nucleoside reverse transcriptase inhibitor, entecavir, further reduced HBV DNA. Antiviral efficacy in mice was associated with an increase in immune cell infiltration and decrease of hepatitis B core antigen, encapsidated pregenomic RNA, and covalently closed circular DNA in liver. At subnanomolar concentrations, DF‐006 also showed anti‐HBV efficacy in PHH with significant reductions of HBV DNA. Following dosing with DF‐006, there was upregulation of NF‐κB‐targeted genes that are involved in innate immunity. Conclusion: DF‐006 was efficacious in mouse and PHH models of HBV without any indications of overt toxicity. In mice, DF‐006 localized primarily to the liver where it potently activated innate immunity. The transcriptional response in mouse liver provides insights into mechanisms that mediate anti‐HBV efficacy by DF‐006.

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Cytokines and Chemokines in HBV Infection

Cited by 32 publications

References 177 publications

Immune Checkpoint Molecules Expressed on CD4+ T Cell Subsets in Chronic Asymptomatic Hepatitis B Virus Carriers With Hepatitis B e Antigen-Negative

Immune Checkpoint Molecules Expressed on CD4+ T Cell Subsets in Chronic Asymptomatic Hepatitis B Virus Carriers With Hepatitis B e Antigen-Negative

Efficient cellular and humoral immune response and production of virus-neutralizing antibodies by the Hepatitis B Virus S/preS116-42 antigen

Alpha‐kinase 1 (ALPK1) agonist DF‐006 demonstrates potent efficacy in mouse and primary human hepatocyte (PHH) models of hepatitis B

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