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A unique B cell epitope-based particulate vaccine shows effective suppression of hepatitis B surface antigen in mice
Tian-Ying Zhang1,2, Xue-Ran Guo1,2, Yang-Tao Wu1,2, Xiao-Zhen Kang1,2, Qing-Bing Zheng1,2, Ruo-Yao Qi1,2, Bin-Bing Chen1,2, Ying Lan1,2, Min Wei1,2, Shao-Juan Wang1,2, Hua-Long Xiong1,2, Jia-Li Cao1,2, Bao-Hui Zhang1,2, Xiao-Yang Qiao1,2, Xiao-Fen Huang1,2, Ying-Bin Wang1,2, Mu-Jin Fang1,2, Ya-Li Zhang1,2, Tong Cheng1,2, Yi-Xin Chen1,2, Qin-Jian Zhao1,2, Shao-Wei Li1,2, Sheng-Xiang Ge1,2, Pei-Jer Chen3, Jun Zhang1,2, Quan Yuan1,2, Ning-shao Xia1,2
Author affiliations
State Key Laboratory of Molecular Vaccinology and Molecular Diagnostics, School of Public Health & School of Life Science, Xiamen University, Xiamen, China
National Institute of Diagnostics and Vaccine Development in Infectious Diseases, School of Public Health & School of Life Science, Xiamen University, Xiamen, China
Hepatitis Research Center, National Taiwan University Hospital, Taipei, Taiwan
Correspondence to Professor Jun Zhang; [email protected], Dr Quan Yuan; [email protected] and Professor Ning-shao Xia; [email protected]
Abstract
Objective This study aimed to develop a novel therapeutic vaccine based on a unique B cell epitope and investigate its therapeutic potential against chronic hepatitis B (CHB) in animal models.
Methods A series of peptides and carrier proteins were evaluated in HBV-tolerant mice to obtain an optimised therapeutic molecule. The immunogenicity, therapeutic efficacy and mechanism of the candidate were investigated systematically.
Results Among the HBsAg-aa119-125-containing peptides evaluated in this study, HBsAg-aa113-135 (SEQ13) exhibited the most striking therapeutic effects. A novel immunoenhanced virus-like particle carrier (CR-T3) derived from the roundleaf bat HBV core antigen (RBHBcAg) was created and used to display SEQ13, forming candidate molecule CR-T3-SEQ13. Multiple copies of SEQ13 displayed on the surface of this particulate antigen promote the induction of a potent anti-HBs antibody response in mice, rabbits and cynomolgus monkeys. Sera and purified polyclonal IgG from the immunised animals neutralised HBV infection in vitro and mediated efficient HBV/hepatitis B virus surface antigen (HBsAg) clearance in the mice. CR-T3-SEQ13-based vaccination induced long-term suppression of HBsAg and HBV DNA in HBV transgenic mice and eradicated the virus completely in hydrodynamic-based HBV carrier mice. The suppressive effects on HBsAg were strongly correlated with the anti-HBs level after vaccination, suggesting that the main mechanism of CR-T3-SEQ13 vaccination therapy was the induction of a SEQ13-specific antibody response that mediated HBV/HBsAg clearance.
Conclusions The novel particulate protein CR-T3-SEQ13 suppressed HBsAg effectively through induction of a humoural immune response in HBV-tolerant mice. This B cell epitope-based therapeutic vaccine may provide a novel immunotherapeutic agent against chronic HBV infection in humans.
https://creativecommons.org/licenses/by-nc/4.0/
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http://dx.doi.org/10.1136/gutjnl-2018-317725
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Significance of this study
What is already known on this subject?
Achievement of hepatitis B virus surface antigen (HBsAg) loss is an ideal endpoint of chronic hepatitis B (CHB) treatment, and it is rarely achieved by current approved anti-HBV drugs.
High load of HBsAg directly inhibit both adaptive and innate immune functions and ultimately leads to specific tolerance that prevents the host from eradicating HBV infection. A long-term suppression of HBsAg hopefully allows for restoration of anti-HBs B cell response and HBV specific T cell function.
Most HBV therapeutic vaccines based on the native HBsAg and HBcAg could induce specific T cells in HBV carrier mice, even in patients with CHB, but there was no significant effective antibody response that mediates viral clearance, thus exhibited limited inhibitory effect on HBsAg levels.
The antibodies recognise the sA epitope (HBsAg-aa119-125) and exhibit more remarkable and prolonged HBsAg suppression effects than antibodies binding to other epitopes as we described previously.
Significance of this study
What are the new findings?
Among the HBsAg-aa119-125-containing peptides evaluated in this study, HBsAg-aa113-135 (SEQ13) exhibited the most striking therapeutic effects. A novel immuno-enhanced virus-like particle carrier (CR-T3) derived from the roundleaf bat HBV core antigen (RBHBcAg) was created and used to display SEQ13, forming the novel particulate protein CR-T3-SEQ13.
Multiple copies of SEQ13 displayed on the surface of this particulate antigen promote the induction of a potent antibody response in mice, rabbits and cynomolgus monkeys, and dominant antibodies recognise HBsAg-aa119-125, which exhibit broad spectrum of activity to mediate HBsAg clearance in vivo and neutralise HBV infection in vitro.
CR-T3-SEQ13-based vaccination showed a long-term suppression of HBsAg and HBV DNA in HBV transgenic mice and eradicated the virus completely in hydrodynamic-based HBV carrier mice by induction of a SEQ13-specific antibody response that mediated HBV/HBsAg clearance.
How might it impact on clinical practice in the foreseeable future?
CR-T3-SEQ13 is a superior candidate based on a unique B cell eiptope for developing therapeutic vaccine against HBV, which will be tested in the clinic alone or in combination with current available anti-HBV drugs to treat patients with CHB, and aims to increase the HBsAg loss rate.
If successful, CR-T3-SEQ13-based immunotherapy will provide a novel anti-HBV strategy to achieve long-term inhibition of the HBsAg levels and improve the clinical management of CHB. |
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发表于 2020-1-8 17:42