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Synthesis and Biological Evaluation of Hapten-Clicked Analogues of The Antigenic Peptide Melan-A/MART-126(27L)-35

机译:抗原肽黑光-A / MART-126(27L)-35的半抗体点击模数的合成与生物学评价

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摘要

A click-chemistry-based approach was implemented to prepare peptidomimetics designed in silico and made from aromatic azides and a propargylated GIGI-mimicking platform derived from the altered Melan-A/MART-126(27L)-35 antigenic peptide ELAGIGILTV. The CuI-catalyzed Huisgen cycloaddition was carried out on solid support to generate rapidly a first series of peptidomimetics, which were evaluated for their capacity to dock at the interface between the major histocompatibility complex class-I (MHC-I) human leucocyte antigen (HLA)-A2 and T-cell receptors (TCRs). Despite being a weak HLA-A2 ligand, one of these 11 first synthetic com- pounds bearing a p-nitrobenzyl-triazole side chain was recognized by the receptor proteins of Melan-A/MART-1-specific T-cells. After modification of the N and C termini of this agonist, which was intended to enhance HLA-A2 binding, one of the resulting seven additional compounds triggered significant T-cell responses. Thus, these results highlight the capacity of naturally circulating human TCRs that are specific for the native Melan-A/MART-126-35 peptide to cross-react with peptidomimetics bearing organic motifs structurally different from the native central amino acids.
机译:实施了基于点击化学的方法以制备在硅中设计的肽模拟物,并由芳族叠氮化物和衍生自改变的Melan-A / MART-126(27L)-35抗原肽ElagiGILTV制成的芳族叠氮化物和普氏锭型模拟平台。在固体载体上进行Cui催化的Huisgen环加成,以快速产生第一系列肽模拟物,这是在主要组织相容性复合体 - I(MHC-1)人体白细胞抗原(HLA)之间的界面处对界面进行停靠的能力(HLA )-A2和T细胞受体(TCRS)。尽管是弱HLA-A2配体,但是这11个载有P-硝基苄基 - 三唑侧链的第11个第一合成浓度之一被Melan-A / MART-1特异性T细胞的受体蛋白识别。在改变该激动剂的N和C Termini之后,该激动剂旨在增强HLA-A2结合,得到的七种另外的化合物之一触发了显着的T细胞反应。因此,这些结果突出了对本地Melan-A / MART-126-35肽特异性的天然循环的人TCR的能力与轴承与天然中央氨基酸结构不同的有机基序的肽模拟物交叉反应。

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