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插入的T细胞决定簇侧翼载体蛋白的氨基酸对T细胞刺激的影响。

Influence of amino acids of a carrier protein flanking an inserted T cell determinant on T cell stimulation.

作者信息

Janssen R, Wauben M, van der Zee R, de Gast M, Tommassen J

机构信息

Department of Molecular Cell Biology, Utrecht University, The Netherlands.

出版信息

Int Immunol. 1994 Aug;6(8):1187-93. doi: 10.1093/intimm/6.8.1187.

Abstract

CD4+ helper T cells recognize antigen in association with MHC class II molecules. To investigate the role of the context of a minimal T cell epitope on presentation and recognition in association with MHC class II molecules, an epitope of the 65 kDa heat shock protein of Mycobacterium tuberculosis was inserted at four different sites in the outer membrane protein PhoE of Escherichia coli. Only some of the constructs could stimulate the epitope-specific T cell clone A2b in vitro. One non-stimulatory construct could be made stimulatory by denaturation, suggesting that the protein conformation prevents correct presentation of the epitope. Other non-stimulatory constructs did not become stimulatory with denaturation. One of these constructs could be made stimulatory by substitution of either one of the two amino acids directly preceding the minimal epitope in the recombinant protein. In synthetic peptides the presence of these upstream residues did not interfere with T cell recognition, suggesting that these residues influence processing of the recombinant protein. Flanking amino acids also influenced induction of a T cell response against the inserted epitope in vivo. These results demonstrate that insertion of minimal T cell epitopes in carrier proteins for the design of vaccines might fail because of the inhibiting effects of flanking residues.

摘要

CD4 +辅助性T细胞识别与MHC II类分子相关的抗原。为了研究最小T细胞表位的背景在与MHC II类分子相关的呈递和识别中的作用,将结核分枝杆菌65 kDa热休克蛋白的一个表位插入大肠杆菌外膜蛋白PhoE的四个不同位点。只有一些构建体能在体外刺激表位特异性T细胞克隆A2b。一种无刺激作用的构建体经变性后可变为有刺激作用,这表明蛋白质构象会阻止表位的正确呈递。其他无刺激作用的构建体经变性后并未变得有刺激作用。其中一种构建体通过替换重组蛋白中最小表位之前的两个氨基酸中的任何一个可变为有刺激作用。在合成肽中,这些上游残基的存在并不干扰T细胞识别,这表明这些残基会影响重组蛋白的加工。侧翼氨基酸也会影响体内针对插入表位的T细胞应答的诱导。这些结果表明,由于侧翼残基的抑制作用,在载体蛋白中插入最小T细胞表位用于疫苗设计可能会失败。

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