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首页> 外文期刊>Journal of Computer-Aided Molecular Design >Modeling the interactions of a peptide-major histocompatibility class I ligand with its receptors. II. Cross-reaction between a monoclonal antibody and two alpha beta T cell receptors
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Modeling the interactions of a peptide-major histocompatibility class I ligand with its receptors. II. Cross-reaction between a monoclonal antibody and two alpha beta T cell receptors

机译:用受体模拟肽 - 主要组织相容性I类配体的相互作用。 II。 单克隆抗体与两种αβT细胞受体之间的交叉反应

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摘要

The recombinant antibody, pSAN13.4.1, has a unique T cell like specificity; it binds an Influenza Hemagglutinin octapeptide (Ha(255-262)) in an MHC (H-2K(k))-restricted manner, and a detailed comparison of the fine specificity of pSAN13.4.1 with the fine specificity of two Ha(255-262)-specific, H-2K(k)-restricted T cell hybridomas has supported this contention. A three-dimensional model of pSAN13.4.1 has been derived by homology modeling techniques. Subsequently, the structure of the pSAN13.4.1 antibody in complex with the antigenic Ha-K-k ligand was derived after a flexible and automated docking of the MHC-peptide pair into the Fab combining site. Interestingly, the most energetically favored binding mode shows numerous analogies to the recently determined recognition of class I MHC-peptide complexes by alpha beta T cell receptors (TCRs). The pSAN13.4.1 also binds diagonally across the MHC binding groove but is more deeply anchored to the peptide-MHC (pep/MHC) ligand than TCRs, notably through numerous interactions of its heavy chain. The present model accounts well for the experimentally determined binding affinity of a set of 144 single amino acid substituted Ha analogues and the observed shared specificity between the pSAN antibody and two different T cell receptors for the Ha-K-k antigenic ligand. Analogies and differences between Fab and TCR recognition are explained by dissecting the binding role of each chain of the immune receptors as well as the contribution of all peptide amino acids. [References: 34]
机译:重组抗体PSAN13.4.1具有独特的T细胞,如特异性;它以MHC(H-2K(k))限制的方式与流感血凝素八肽(HA(255-262))结合,并详细比较PSAN13.4.1的细细性,具有两只公顷的细细性(255 -262) - 特异性,H-2K(k)-Restricted T细胞杂交瘤支持这一争论。 PSAN13.4.1的三维模型是通过同源建模技术推导的。随后,在将MHC-肽对的柔性和自动对接到Fab组合部位的柔性和自动对接之后,衍生碱基与抗原HA-K-K-K配体的蛋白质的结构。有趣的是,最有利于最有利的结合模式表明了αβTT细胞受体(TCR)最近确定了最近确定的I类MHC肽复合物的类比。 PSAN13.4.1还在MHC结合槽上对角线粘合,但比TCRS更深入地锚固到肽-MHC(PEP / MHC)配体,特别是通过其重链的许多相互作用。本模型综述良好的一组144个单氨基酸取代的HA类似物的实验确定的结合亲和力和PSAN抗体与HA-K-K抗原配体的两种不同T细胞受体之间的观察到的共同特异性。通过对所有免疫受体的每个链的结合作用以及所有肽氨基酸的贡献来解释Fab和TCR识别之间的类比和差异。 [参考:34]

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