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全合成糖肽缀合物疫苗的合理设计策略。

A strategy for rational design of fully synthetic glycopeptide conjugate vaccines.

作者信息

Chong P, Chan N, Kandil A, Tripet B, James O, Yang Y P, Shi S P, Klein M

机构信息

Research Centre, Pasteur Merieux Connaught Canada, North York, Ontario.

出版信息

Infect Immun. 1997 Dec;65(12):4918-25. doi: 10.1128/iai.65.12.4918-4925.1997.

Abstract

The present study describes a strategy to rationally design fully synthetic glycopeptide conjugate vaccines. Glycopeptide immunogens were constructed by coupling synthetic oligosaccharides comprising repeating units of synthetic 3-beta-D-ribose-(1-1)-D-ribitol-5-phosphate (sPRP) to synthetic peptides containing potent T-helper cell determinants and B-cell epitopes of the Haemophilus influenzae type b (Hib) outer membrane proteins (OMPs) P1, P2, and P6. Rabbit immunogenicity studies revealed that some of these fully synthetic glycoconjugates were capable of eliciting high titers of both anti-PRP and anti-OMP immunoglobulin G antibodies. In addition, we systematically investigated the factors which could influence their immunogenicity. We observed that the magnitude of the anti-PRP antibody response markedly depended on the relative spatial orientation of sPRP and T-cell epitopes, the anti-PRP antibody response was enhanced when a multiple antigenic peptide was used as a carrier, the anti-PRP antibody response was optimal for three PRP repeating units, and lipidation of peptide-PRP conjugates had a minimal effect on the magnitude of the anti-PRP antibody response. The results of this study clearly demonstrate that coupling a carbohydrate hapten to a peptide can provide T-cell help and convert it into a T-cell-dependent antigen. The antisera raised against these conjugates were also found to be protective against Hib infection in the infant rat model of bacteremia.

摘要

本研究描述了一种合理设计全合成糖肽共轭疫苗的策略。糖肽免疫原是通过将包含合成3-β-D-核糖-(1-1)-D-核糖醇-5-磷酸(sPRP)重复单元的合成寡糖与含有b型流感嗜血杆菌(Hib)外膜蛋白(OMP)P1、P2和P6的有效T辅助细胞决定簇和B细胞表位的合成肽偶联而构建的。兔免疫原性研究表明,其中一些全合成糖缀合物能够引发高滴度的抗PRP和抗OMP免疫球蛋白G抗体。此外,我们系统地研究了可能影响其免疫原性的因素。我们观察到,抗PRP抗体反应的强度明显取决于sPRP和T细胞表位的相对空间取向,当使用多抗原肽作为载体时,抗PRP抗体反应增强,抗PRP抗体反应在三个PRP重复单元时最佳,肽-PRP缀合物的脂化对抗PRP抗体反应的强度影响最小。本研究结果清楚地表明,将碳水化合物半抗原与肽偶联可以提供T细胞辅助并将其转化为T细胞依赖性抗原。在婴儿大鼠菌血症模型中,针对这些缀合物产生的抗血清也被发现对Hib感染具有保护作用。

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