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利用同时多肽合成组装的重叠肽鉴定脑膜炎球菌1类外膜蛋白中出现的T细胞表位。

Identification of T cell epitopes occurring in a meningococcal class 1 outer membrane protein using overlapping peptides assembled with simultaneous multiple peptide synthesis.

作者信息

Wiertz E J, van Gaans-van den Brink J A, Gausepohl H, Prochnicka-Chalufour A, Hoogerhout P, Poolman J T

机构信息

National Institute of Public Health and Environmental Protection, Bilthoven, The Netherlands.

出版信息

J Exp Med. 1992 Jul 1;176(1):79-88. doi: 10.1084/jem.176.1.79.

Abstract

The meningococcal class 1 outer membrane protein (OMP) plays an important role in the development of protective immunity against meningococcal infection, and is therefore considered to be a promising candidate antigen (Ag) for a meningococcal vaccine. The induction of an effective antibody response entirely depends upon T helper cells. To identify T cell epitopes of the OMP, we prepared 45 overlapping synthetic peptides representing the entire sequence of the class 1 protein of reference strain H44/76. Fully automated simultaneous multiple peptide synthesis (SMPS) was used to assemble the 45 twenty mer which overlapped by 12 amino acid residues on a 12 mumol scale. The peptides were tested for recognition by peripheral blood mononuclear cells (PBMC) obtained from 34 volunteers. Surprisingly, all synthetic peptides induced proliferative responses of PBMC isolated from one or more human histocompatibility leukocyte antigen (HLA)-typed immune adults. With PBMC from seven nonimmune donors, no proliferative response was observed. Immunodominant regions were found, recognized by PBMC from many volunteers, irrespective of their HLA type. Most of the immunodominant T cell epitopes are located outside the variable regions and, thus, will be conserved among different meningococcal (and gonococcal) strains. Furthermore, the overlapping peptides could be used to identify the epitopes recognized by OMP-specific T cell clones with known HLA restriction. It is interesting that the epitopes defined with the clones occur in highly conserved areas, shared by all neisserial porin proteins. In summary, this analysis of the T cell response to the meningococcal class 1 OMP constitutes a complete study of reactivity to a foreign protein, and illustrates some important features of Ag recognition by T cells. Our data demonstrate unexpected diversity in the T cell recognition of the OMP, and imply that the T cell repertoire against foreign Ag may be greater than previously assumed. This observation is supported by recent data on the interaction of peptide and major histocompatibility complex (MHC) class II, the latter being much less selective than MHC class I. Finally, a comparative analysis pointed out the limitations of algorithms predicting T cell determinants, and the importance of the empirical methodology provided by SMPS.

摘要

脑膜炎球菌1类外膜蛋白(OMP)在针对脑膜炎球菌感染的保护性免疫的发展中起重要作用,因此被认为是脑膜炎球菌疫苗的一个有前景的候选抗原(Ag)。有效的抗体反应的诱导完全依赖于T辅助细胞。为了鉴定OMP的T细胞表位,我们制备了45个重叠的合成肽,代表参考菌株H44/76的1类蛋白的整个序列。使用全自动同步多肽合成(SMPS)以12微摩尔规模组装45个二十肽,它们彼此重叠12个氨基酸残基。用从34名志愿者获得的外周血单核细胞(PBMC)测试这些肽的识别情况。令人惊讶的是,所有合成肽均诱导了从一名或多名进行了人类组织相容性白细胞抗原(HLA)分型的免疫成年人中分离出的PBMC的增殖反应。对于来自7名非免疫供体的PBMC,未观察到增殖反应。发现了免疫显性区域,许多志愿者的PBMC均可识别,而不论其HLA类型如何。大多数免疫显性T细胞表位位于可变区之外,因此在不同的脑膜炎球菌(和淋球菌)菌株之间是保守的。此外,重叠肽可用于鉴定具有已知HLA限制性的OMP特异性T细胞克隆所识别的表位。有趣的是,用这些克隆定义的表位出现在所有奈瑟氏菌孔蛋白共有的高度保守区域中。总之,对脑膜炎球菌1类OMP的T细胞反应的这一分析构成了对外源蛋白反应性的完整研究,并阐明了T细胞识别Ag的一些重要特征。我们的数据表明,T细胞对OMP的识别具有意想不到的多样性,这意味着针对外源Ag的T细胞库可能比以前设想的要大。最近关于肽与主要组织相容性复合体(MHC)II类相互作用的数据支持了这一观察结果,后者的选择性远低于MHC I类。最后,一项比较分析指出了预测T细胞决定簇的算法的局限性,以及SMPS提供的经验方法的重要性。

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