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脑膜炎奈瑟菌1类外膜蛋白的T细胞识别。用选定的合成肽鉴定T细胞表位并确定HLA限制元件。

T cell recognition of Neisseria meningitidis class 1 outer membrane proteins. Identification of T cell epitopes with selected synthetic peptides and determination of HLA restriction elements.

作者信息

Wiertz E J, van Gaans-van den Brink J A, Schreuder G M, Termijtelen A 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 Immunol. 1991 Sep 15;147(6):2012-8.

PMID:1716291
Abstract

No vaccine is yet available against serogroup B meningococci, which are a common cause of bacterial meningitis. Some outer membrane proteins (OMP), LPS, and capsular polysaccharides have been identified as protective Ag. The amino acid sequence of the protective B cell epitopes present within the class 1 OMP has been described recently. Synthetic peptides containing OMP B cell epitopes as well as capsular polysaccharides or LPS protective B cell epitopes have to be presented to the immune system in association with T cell epitopes to achieve an optimal Ir. The use of homologous, i.e., meningococcal, T cell epitopes has many advantages. We therefore investigated recognition sites for human T cells within the meningococcal class 1 OMP. We have synthesized 16 class 1 OMP-derived peptides encompassing predicted T cell epitopes. Peptides corresponding to both surface loops and trans-membrane regions (some of which occur as amphipathic beta-sheets) of the class 1 OMP were found to be recognized by T cells. In addition, 10 of 11 peptides containing predicted amphipathic alpha-helices and four of five peptides containing T cell epitope motifs according to Rothbard and Taylor (Rothbard, J. B., and W. R. Taylor. 1988. EMBO J 7:93) were recognized by lymphocytes from one or more volunteers. Some of the T and B cell epitopes were shown to map to identical regions of the protein. At least six of the peptides that were found to contain T cell epitopes show homology to constant regions of the meningococcal class 3 OMP and the gonococcal porins PIA and PIB. Peptide-specific T cell lines and T cell clones were established to investigate peptide recognition in more detail. The use of a panel of HLA-typed APC revealed clear HLA-DR restriction patterns. It seems possible now to develop a (semi-) synthetic meningococcal vaccine with a limited number of constant T cell epitopes that cover all HLA-DR locus products.

摘要

目前尚无针对B群脑膜炎球菌的疫苗,而该菌是细菌性脑膜炎的常见病因。一些外膜蛋白(OMP)、脂多糖(LPS)和荚膜多糖已被确定为保护性抗原。最近已描述了1类OMP中存在的保护性B细胞表位的氨基酸序列。含有OMP B细胞表位以及荚膜多糖或LPS保护性B细胞表位的合成肽必须与T细胞表位一起呈递给免疫系统,以实现最佳的免疫应答(Ir)。使用同源的,即脑膜炎球菌的T细胞表位有许多优点。因此,我们研究了脑膜炎球菌1类OMP中人类T细胞的识别位点。我们合成了16种源自1类OMP的肽,这些肽包含预测的T细胞表位。发现与1类OMP的表面环和跨膜区域(其中一些以两亲性β-折叠形式出现)相对应的肽能被T细胞识别。此外,11种含有预测的两亲性α-螺旋的肽中的10种以及5种含有根据Rothbard和Taylor(Rothbard,J.B.,和W.R.Taylor.1988.EMBO J 7:93)的T细胞表位基序的肽中的4种被来自一名或多名志愿者的淋巴细胞识别。一些T细胞和B细胞表位被证明位于蛋白质的相同区域。发现至少六种含有T细胞表位的肽与脑膜炎球菌3类OMP以及淋球菌孔蛋白PIA和PIB的恒定区具有同源性。建立了肽特异性T细胞系和T细胞克隆以更详细地研究肽识别。使用一组HLA分型的抗原呈递细胞(APC)揭示了明确的HLA-DR限制模式。现在似乎有可能开发一种含有有限数量恒定T细胞表位的(半)合成脑膜炎球菌疫苗,这些表位可覆盖所有HLA-DR位点产物。

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