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[乙肝疫苗——历史、成就、挑战与展望]

[Hepatitis B vaccines-history, achievements, challenges, and perspectives].

作者信息

Gerlich Wolfram H

机构信息

Institut für Medizinische Virologie, Nationales Referenzzentrum für Hepatitis-B-Viren und Hepatitis-D-Viren, Justus-Liebig-Universität Gießen, Schubertstr. 81, 35392, Gießen, Deutschland.

出版信息

Bundesgesundheitsblatt Gesundheitsforschung Gesundheitsschutz. 2022 Feb;65(2):170-182. doi: 10.1007/s00103-021-03484-w. Epub 2022 Jan 11.

Abstract

The first experimental vaccinations against hepatitis B virus (HBV) were performed in 1970, even before the nature of the administered "Australia antigen" was known. Soon, it was realized that this antigen was the envelope protein (HBV surface antigen, HBsAg), and it was purified from HBV-containing human plasma. Later, it was produced in genetically engineered yeast cells. The excellent efficacy of the HBsAg vaccine was confirmed in numerous studies, particularly in newborns from HBV-infected mothers who almost always become chronic HBV carriers without vaccination. But the vaccine is also highly effective in older children and adults and has been applied worldwide since 1984, leading to a circa tenfold decrease of HBV infections in the vaccinated.Still, there are several challenges with hepatitis B vaccination. In newborns from mothers with very high virus load, the vaccine may fail. Recipients who are immunocompromised, older, smokers, or obese may not produce protective antibodies. Early studies suggested that the vaccine with HBsAg subtype adw2 also protected against infections by other subtypes, but recent observations show that the protection is weaker against heterologous subtypes. Occasionally, escape mutations may develop.Most current HB vaccines are based on the knowledge of 40 years ago and could be significantly improved. Inclusion of the currently neglected preS domains in the HBV envelope would add the most important protective T‑ and B‑cell epitopes to the vaccines. Expression of the HBsAg in mammalian cell cultures would enhance the folding of neutralizing HBsAg epitopes. Use of the regionally prevalent HBsAg subtypes would increase the protection. Optimal adjuvants and epitope carriers may enhance the immunogenicity to the level necessary for immune therapy of chronic hepatitis B.

摘要

1970年开展了首批针对乙型肝炎病毒(HBV)的实验性疫苗接种,甚至在所施用的“澳大利亚抗原”的性质尚不清楚之前就已进行。很快,人们意识到这种抗原就是包膜蛋白(HBV表面抗原,HBsAg),并从含HBV的人血浆中进行了纯化。后来,它在基因工程酵母细胞中生产。HBsAg疫苗的卓越疗效在众多研究中得到证实,尤其是在来自HBV感染母亲的新生儿中,这些新生儿如果不接种疫苗几乎总会成为慢性HBV携带者。但该疫苗在大龄儿童和成人中也非常有效,自1984年以来已在全球应用,使接种人群中的HBV感染率大约下降了十倍。

尽管如此,乙型肝炎疫苗接种仍存在若干挑战。对于来自病毒载量非常高的母亲的新生儿,疫苗可能无效。免疫功能低下、年龄较大、吸烟或肥胖的接种者可能无法产生保护性抗体。早期研究表明,含有HBsAg adw2亚型的疫苗也能预防其他亚型的感染,但最近的观察结果显示,针对异源亚型的保护作用较弱。偶尔,可能会出现逃逸突变。

当前大多数乙肝疫苗是基于40年前的知识,还有很大的改进空间。在HBV包膜中纳入目前被忽视的前S结构域将为疫苗增添最重要的保护性T细胞和B细胞表位。在哺乳动物细胞培养物中表达HBsAg将增强中和性HBsAg表位的折叠。使用地区流行的HBsAg亚型将增强保护作用。最佳佐剂和表位载体可能会将免疫原性提高到慢性乙型肝炎免疫治疗所需的水平。

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