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肽-Ia结合水平上的抗原竞争

Antigenic competition at the level of peptide-Ia binding.

作者信息

Babbitt B P, Matsueda G, Haber E, Unanue E R, Allen P M

出版信息

Proc Natl Acad Sci U S A. 1986 Jun;83(12):4509-13. doi: 10.1073/pnas.83.12.4509.

Abstract

We examined the direct binding of a hen egg white lysozyme peptide, HEL(46-61), to membrane I-Ak (protein encoded in the A locus of the I region) molecules in the presence of detergent. A number of synthetic peptide derivatives, which did not stimulate our T-cell reactive hybridomas, competed for the binding of HEL(46-61) to I-Ak and also inhibited the functional presentation of HEL(46-61). Inhibitors included a peptide lacking a tyrosine at position 53 and a peptide corresponding to the autologous lysozyme peptide. Presentation was examined with cells or with supported planar phospholipid membranes bearing only I-Ak and HEL(46-61). Other peptides that did not compete for the binding did not inhibit functional presentation. We concluded that the binding of an immunogenic peptide to I-A is critical for presentation, that the I-A molecule does not discriminate between autologous and foreign related determinants but does recognize structurally different peptides. Our evidence suggests that our immunogenic peptide bears noncontiguous amino acids critical for contact I-A binding interspersed with amino acids critical for interaction with T cells.

摘要

我们研究了在去污剂存在的情况下,鸡卵清溶菌酶肽HEL(46 - 61)与膜I - Ak(I区A位点编码的蛋白质)分子的直接结合。许多不刺激我们的T细胞反应性杂交瘤的合成肽衍生物,竞争HEL(46 - 61)与I - Ak的结合,并且还抑制HEL(46 - 61)的功能性呈递。抑制剂包括在53位缺乏酪氨酸的肽和与自身溶菌酶肽对应的肽。使用细胞或仅带有I - Ak和HEL(46 - 61)的支持平面磷脂膜来检测呈递情况。其他不竞争结合的肽不抑制功能性呈递。我们得出结论,免疫原性肽与I - A的结合对于呈递至关重要,I - A分子不区分自身和外来相关决定簇,但确实识别结构不同的肽。我们的证据表明,我们的免疫原性肽带有对与I - A结合至关重要的不连续氨基酸,这些氨基酸与对与T细胞相互作用至关重要的氨基酸相间分布。

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