Phenotypic and functional differences of HBV core-specific versus HBV polymerase-specific CD8+ T cells in chronically HBV-infected patients with low viral load

Schuch, Anita; Alizei, Elahe Salimi; Heim, Kathrin; Wieland, Dominik; Kiraithe, Michael Muthamia; Kemming, Janine; Llewellyn-Lacey, Sian; Soğukpınar, Özlem; Ni, Yi; Urban, Stephan; Zimmermann, Peter Jan; Nassal, Michael; Emmerich, Florian; Price, David A.; Bengsch, Bertram; Luxenburger, Hendrik; Neumann‐Haefelin, Christoph; Hofmann, Maike; Thimme, Robert

doi:10.1136/gutjnl-2018-316641

Cited by 122 publications

(138 citation statements)

References 34 publications

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“…Interestingly, it has been published in various pre-clinical studies that an intermediate dose of Ad5based vaccines is typically associated with better quality of T-cells (higher polyfunctionality, strongest proliferative capacity and lower expression of exhaustion markers) compared with higher doses. [26][27][28] Unfortunately, we could not perform additional immune assays such as recently reported in the field (e.g., tetramer analysis, ex vivo ELISPOT, phenotypic analysis 25,[29][30][31] in order to better characterize the detected cells due to limited sample quantities. Such analyses will need to be conducted in future clinical trials.…”

Section: Discussionmentioning

confidence: 99%

“…In particular, inducing POL-educated T-cells would be important as POL-specific CD8 + T cells appear to be more severely exhausted during CHB than Core ones. 31 POL is a very large antigen, notoriously difficult to purify and engineer in genetically stable vectors for vaccine development. To our knowledge, only one other vaccine beside TG1050, i.e.…”

Section: Discussionmentioning

confidence: 99%

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Safety and immunogenicity of the therapeutic vaccine TG1050 in chronic hepatitis B patients: a phase 1b placebo-controlled trial

Zoulim

Fournier

Habersetzer³

et al. 2019

Human Vaccines & Immunotherapeutics

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Treatment of chronic hepatitis B (CHB) typically requires lifelong administration of drugs. Cohort and preclinical studies have established the link between a functional T-cell-mounted immunity and resolution of infection. TG1050 is an adenovirus 5-based vaccine that expresses HBV polymerase and domains of core and surface antigen and has shown immunogenicity and antiviral effects in mice. We performed a phase 1 clinical trial to assess safety and explore immunogenicity and early efficacy of TG1050 in CHB patients. This randomized, double blind, placebo-controlled study included two sequential phases: one single dose cohort (SD, n = 12) and one multiple (3) doses cohort (MD, n = 36). Patients, virally suppressed under nucleoside(d)tide analog NUC therapy, were randomized 1:1:1 across 3 dose levels (DL) and assigned to receive 10 9 , 10 10 , 10 11 virus particles (vp) of TG1050 and then randomized within each DL to placebo (3:1 and 9:3 vaccines/placebo in each DL, respectively, for the SD and MD cohorts). Cellular (ELISPOT) and antibody responses (anti-Adenovirus), as well as evolution of circulating HBsAg and HBcrAg, were monitored. All doses were well tolerated in both cohorts, without severe adverse event. TG1050 was capable to induce IFN-γ producing T-cells targeting 1 to 3 encoded antigens, in particular at the 10 10 vp dose. Overall, minor decreases of HBsAg were observed while a number of vaccinees reached unquantifiable HBcrAg by end of the study. In CHB patients under NUC, TG1050 exhibited a good safety profile and was capable to induce HBV-specific cellular immune response. These data support further clinical evaluation, especially in combination studies.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Safety and immunogenicity of the therapeutic vaccine TG1050 in chronic hepatitis B patients: a phase 1b placebo-controlled trial

Zoulim

Fournier

Habersetzer³

et al. 2019

Human Vaccines & Immunotherapeutics

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“…The two manuscripts, Schuch et al 1 and Hoogeveen et al ,2 in Gut tackle this knowledge gap and undertake a direct and detailed ex vivo analysis of the phenotypic and functional features of CD8 T cells targeting epitopes located in different HBV proteins in patients with acute self-limited hepatitis B and in patients with eAg-negative chronic hepatitis B (CHB).…”

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confidence: 99%

HBV antiviral immunity: not all CD8 T cells are born equal

Bertoletti

Kennedy

2019

Gut

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“…HBcAg, acting as an important stimulus in a host of stages of HBV life cycle, possesses the strong immunogenicity. It is said that HBcAg-specific CD8 + T cells of CHB patients may not totally exhausted, therefore can help eliminate HBV infection (29,30). Besides, Cooper et al found the core protein of HBV could upregulate the activation of NF-κB and promote inflammatory cytokine release in THP-1 macrophages in vitro.…”

Section: Discussionmentioning

confidence: 99%

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

Zhang

Yang

et al. 2020

Front. Immunol.

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Although several evidences suggesting the vital roles that innate immunity plays in the persistence and elimination of chronic hepatitis B virus (CHB) infection, the exact mechanism is still complicated. Here, we successfully polarized monocytes derived from healthy human peripheral blood mononuclear cells (PBMCs) into M1/M2 macrophages and detected the effects of hepatitis B core antigen (HBcAg) on the polarization and function of macrophages via the Toll-like receptor (TLR) 2 signaling pathway. The results showed that HBcAg had a negligible impact on M1 polarization, while it effectively impaired M2 polarization and promoted the production of pro-inflammatory cytokines such as IL-6 and TNF-α. Additionally, HBcAg treatment increased TLR2 expression on M2 macrophages and TLR2 blockade abolished the effects of HBcAg on the impaired phenotype and pro-inflammatory cytokine productions of M2 macrophages. Signaling pathway analysis revealed that the nuclear factor κB (NF-κB) pathway, the downstream of TLR2, was upregulated upon HBcAg treatment in both M1 and M2 macrophages. Furthermore, a CD8 + T-macrophage coculture system implied that compared with PBS stimulation, HBcAg-stimulated M2 macrophages regained their ability to activate CD8 + T cells with higher secretion of IFN-γ. Finally, we found impaired expression of M2-related molecules and increased levels of pro-inflammation cytokines in M2 macrophages from CHB patients upon HBcAg stimulation. In conclusion, these results imply a favorable role of HBcAg in the establishment of a pro-inflammatory microenvironment by macrophages, which may suggest a potential therapeutic strategy of HBcAg-induced macrophage activation in CHB infection.

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Phenotypic and functional differences of HBV core-specific versus HBV polymerase-specific CD8+ T cells in chronically HBV-infected patients with low viral load

Cited by 122 publications

References 34 publications

Safety and immunogenicity of the therapeutic vaccine TG1050 in chronic hepatitis B patients: a phase 1b placebo-controlled trial

Safety and immunogenicity of the therapeutic vaccine TG1050 in chronic hepatitis B patients: a phase 1b placebo-controlled trial

HBV antiviral immunity: not all CD8 T cells are born equal

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

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