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用包含特定B细胞和T细胞表位的多抗原肽进行免疫:产生针对B群脑膜炎奈瑟菌的杀菌抗体。

Immunization with a multiple antigen peptide containing defined B- and T-cell epitopes: production of bactericidal antibodies against group B Neisseria meningitidis.

作者信息

Christodoulides M, Heckels J E

机构信息

University of Southampton, Southampton General Hospital, UK.

出版信息

Microbiology (Reading). 1994 Nov;140 ( Pt 11):2951-60. doi: 10.1099/13500872-140-11-2951.

DOI:10.1099/13500872-140-11-2951
PMID:7529096
Abstract

Previous analysis of the class 1 outer-membrane (OM) protein of Neisseria meningitidis has identified discrete epitopes to be potential targets for immune attack. The conformation of these epitopes is important for inducing antibodies which can react with the native protein and promote complement-mediated lysis of the meningococcus. The multiple antigen peptide (MAP) system, which consists of an oligomeric branching lysine core to which are attached dendritic arms of defined peptide antigens, confers some conformational stability and also allows for the preparation of immunogens containing both B-cell and T helper (Th)-cell epitopes. In this study, MAPs were synthesized to contain (i) the subtype P1.16b meningococcal class 1 protein B-cell epitope (B-MAP), and (ii) the P1.16b epitope in tandem with a defined Th-cell epitope, chosen from tetanus toxin (BT-MAP). The B-MAP was nonimmunogenic in animals. In contrast, incorporation of the Th-cell epitope into BT-MAP induced a strong humoral response towards the class 1 protein B-cell epitope. Antisera from immunized mice and rabbits reacted in ELISA with synthetic peptides containing the B-cell epitope, and also cross-reacted with meningococcal OMs from strains of subtype P1.16b and P1.16a. Murine and rabbit antisera showed similar reactivity and epitope specificity, but did not react with denatured class 1 protein in Western blotting, indicating the predominance of antibodies directed towards conformational epitopes. The antisera from rabbits immunized with BT-MAP promoted complement-mediated bactericidal killing not only of the homologous meningococcal subtype P1.16b strain but also of subtype P1.16a.

摘要

先前对脑膜炎奈瑟菌1类外膜(OM)蛋白的分析已确定离散表位是免疫攻击的潜在靶点。这些表位的构象对于诱导能与天然蛋白反应并促进补体介导的脑膜炎球菌裂解的抗体很重要。多抗原肽(MAP)系统由一个寡聚分支赖氨酸核心组成,特定肽抗原的树突状臂连接在该核心上,它赋予了一定的构象稳定性,还能制备包含B细胞和T辅助(Th)细胞表位的免疫原。在本研究中,合成的MAP包含:(i)P1.16b亚型脑膜炎球菌1类蛋白B细胞表位(B-MAP),以及(ii)与从破伤风毒素中选取的特定Th细胞表位串联的P1.16b表位(BT-MAP)。B-MAP在动物中无免疫原性。相比之下,将Th细胞表位掺入BT-MAP可诱导针对1类蛋白B细胞表位的强烈体液反应。免疫小鼠和兔子的抗血清在ELISA中与含B细胞表位的合成肽发生反应,还与P1.16b和P1.16a亚型菌株的脑膜炎球菌外膜发生交叉反应。小鼠和兔子的抗血清表现出相似的反应性和表位特异性,但在蛋白质免疫印迹中不与变性的1类蛋白反应,表明针对构象表位的抗体占主导。用BT-MAP免疫兔子产生的抗血清不仅能促进补体介导的对同源脑膜炎球菌P1.16b亚型菌株的杀菌作用,还能促进对P1.16a亚型菌株的杀菌作用。

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