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Dual-targeting nanoparticle vaccine elicits a therapeutic antibody response against chronic hepatitis B.


ABSTRACT: Chronic hepatitis B is caused by prolonged infection with the hepatitis B virus (HBV), which can substantially increase the risk of developing liver disease. Despite the development of preventive vaccines against HBV, a therapeutic vaccine inducing an effective antibody response still remains elusive. The preS1 domain of the large HBV surface protein is the major viral attachment site on hepatocytes and thus offers a therapeutic target; however, its poor immunogenicity limits clinical translation. Here, we design a ferritin nanoparticle vaccine that can deliver preS1 to specific myeloid cells, including SIGNR1+ dendritic cells (which activate T follicular helper cells) and lymphatic sinus-associated SIGNR1+ macrophages (which can activate B cells). This nanoparticle vaccine induces a high-level and persistent anti-preS1 response that results in efficient viral clearance and partial serological conversion in a chronic HBV mouse model, offering a promising translatable vaccination strategy for the functional cure of chronic hepatitis B.

SUBMITTER: Wang W 

PROVIDER: S-EPMC7223715 | biostudies-literature | 2020 May

REPOSITORIES: biostudies-literature

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Dual-targeting nanoparticle vaccine elicits a therapeutic antibody response against chronic hepatitis B.

Wang Wenjun W   Zhou Xiaoxiao X   Bian Yingjie Y   Wang Shan S   Chai Qian Q   Guo Zhenqian Z   Wang Zhenni Z   Zhu Ping P   Peng Hua H   Yan Xiyun X   Li Wenhui W   Fu Yang-Xin YX   Zhu Mingzhao M  

Nature nanotechnology 20200302 5


Chronic hepatitis B is caused by prolonged infection with the hepatitis B virus (HBV), which can substantially increase the risk of developing liver disease. Despite the development of preventive vaccines against HBV, a therapeutic vaccine inducing an effective antibody response still remains elusive. The preS1 domain of the large HBV surface protein is the major viral attachment site on hepatocytes and thus offers a therapeutic target; however, its poor immunogenicity limits clinical translatio  ...[more]

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