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疫苗工程:在由T细胞和B细胞表位组成的化学限定模型中增强与肝炎相关的合成肽疫苗的免疫原性。

Vaccine engineering: enhancement of immunogenicity of synthetic peptide vaccines related to hepatitis in chemically defined models consisting of T- and B-cell epitopes.

作者信息

Tam J P, Lu Y A

机构信息

Rockefeller University, New York, NY 10021.

出版信息

Proc Natl Acad Sci U S A. 1989 Dec;86(23):9084-8. doi: 10.1073/pnas.86.23.9084.

DOI:10.1073/pnas.86.23.9084
PMID:2480595
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC298438/
Abstract

We report the development of two models for synthetic hepatitis B vaccines. The models were based on the multiple antigen peptide (MAP) system and contained the relevant B- and T-cell epitopes without any macromolecular carrier. Two peptides, representing the a determinant of the S region (S protein) of hepatitis B surface antigen, a dominant serotype of hepatitis B virus infection found in humans, and residues 12-26 of the pre-S(2) region of the middle protein were incorporated as either monoepitope or diepitope MAP models. Immunizations of outbred rabbits with the monoepitope MAP that contains the pre-S(2) antigen resulted in high-titered antibody response to the middle protein, but the other monoepitope, containing only the a-determinant peptide antigen, resulted in poor immune responses to either the peptide antigens or to the S protein. The diepitope MAPs containing both the a and the pre-S(2) determinants produced high-titer antibodies reactive to the a-synthetic peptide and the S protein, as well as to the middle proteins. Thus, our results show that the diepitope MAP models eliminate the need for a protein carrier and that the pre-S(2) peptide determinant serves as a T-helper cell epitope that enhances the immune response of the S region and overcomes the poor immunogenicity encountered with a single epitope of the S region.

摘要

我们报告了两种合成乙型肝炎疫苗模型的研发情况。这些模型基于多抗原肽(MAP)系统,包含相关的B细胞和T细胞表位,且不含任何大分子载体。两种肽被整合为单表位或双表位MAP模型,其中一种代表乙肝表面抗原S区(S蛋白)的α决定簇,这是在人类中发现的乙肝病毒感染的一种主要血清型,另一种是中蛋白前S(2)区的12 - 26位残基。用含有前S(2)抗原的单表位MAP对远交系兔子进行免疫,可产生针对中蛋白的高滴度抗体反应,但另一种仅含α决定簇肽抗原的单表位,对肽抗原或S蛋白的免疫反应较差。同时含有α和前S(2)决定簇的双表位MAP产生了对α合成肽、S蛋白以及中蛋白有反应的高滴度抗体。因此,我们的结果表明,双表位MAP模型无需蛋白质载体,且前S(2)肽决定簇可作为T辅助细胞表位,增强S区的免疫反应,并克服了S区单一表位所遇到的免疫原性差的问题。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9bd6/298438/565342855733/pnas00290-0045-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9bd6/298438/565342855733/pnas00290-0045-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9bd6/298438/565342855733/pnas00290-0045-a.jpg

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