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首页> 外文期刊>The journal of immunology >Impact of Orthologous Melan-A Peptide Immunizations on the Anti-Self Melan-A/HLA-A2 T Cell Cross-Reactivity
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Impact of Orthologous Melan-A Peptide Immunizations on the Anti-Self Melan-A/HLA-A2 T Cell Cross-Reactivity

机译:同源Melan-A肽免疫对抗自我Melan-A / HLA-A2 T细胞交叉反应的影响

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In HLA-A2 individuals, the CD8 T cell response against the differentiation Ag Melan-A is mainly directed toward the peptide Melan-A26–35. The murine Melan-A24–33 sequence encodes a peptide that is identical with the human Melan-A26–35 decamer, except for a Thr-to-Ile substitution at the penultimate position. Here, we show that the murine Melan-A24–33 is naturally processed and presented by HLA-A2 molecules. Based on these findings, we compared the CD8 T cell response to human and murine Melan-A peptide by immunizing HLA-A2 transgenic mice. Even though the magnitude of the CTL response elicited by the murine Melan-A peptide was lower than the one elicited by the human Melan-A peptide, both populations of CTL recognized the corresponding immunizing peptide with the same functional avidity. Interestingly, CTL specific for the murine Melan-A peptide were completely cross-reactive against the orthologous human peptide, whereas anti-human Melan-A CTL recognized the murine Melan-A peptide with lower avidity. Structurally, this discrepancy could be explained by the fact that Ile32 of murine Melan-A24–33 created a larger TCR contact area than Thr34 of human Melan-A26–35. These data indicate that, even if immunizations with orthologous peptides can induce strong specific T cell responses, the quality of this response against syngeneic targets might be suboptimal due to the structure of the peptide-TCR contact surface.
机译:在HLA-A2个体中,针对分化的Ag Melan-A的CD8 T细胞反应主要针对Melan-A26-35肽。鼠Melan-A24-33序列编码的肽段与人类Melan-A26-35 decamer序列相同,除了倒数第二位的Thr-Ile取代。在这里,我们证明了小鼠Melan-A24-33是由HLA-A2分子自然加工并呈递的。基于这些发现,我们通过免疫HLA-A2转基因小鼠比较了CD8 T细胞对人和鼠Melan-A肽的反应。即使鼠Melan-A肽引起的CTL反应的强度低于人Melan-A肽引起的CTL响应,两个CTL群体均识别具有相同功能亲和力的相应免疫肽。有趣的是,对鼠Melan-A肽特异的CTL与直系同源人肽完全交叉反应,而抗人Melan-A CTL识别鼠亲Melan-A肽的亲和力较低。从结构上讲,这种差异可以通过以下事实来解释:鼠Melan-A24-33的Ile32产生的TCR接触面积大于人Melan-A26-35的Thr34。这些数据表明,即使用直系同源肽免疫可以诱导强烈的特异性T细胞应答,由于肽-TCR接触表面的结构,针对同源靶标的这种应答的质量可能不是最佳的。

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