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一种主要组织相容性复合体肽限制性抗体和T细胞受体分子通过不同的结合模式识别其靶标:人白细胞抗原(HLA)-A1-MAGE-A1与FAB-HYB3复合物的晶体结构。

A major histocompatibility complex-peptide-restricted antibody and t cell receptor molecules recognize their target by distinct binding modes: crystal structure of human leukocyte antigen (HLA)-A1-MAGE-A1 in complex with FAB-HYB3.

作者信息

Hülsmeyer Martin, Chames Patrick, Hillig Roman C, Stanfield Robyn L, Held Gerhard, Coulie Pierre G, Alings Claudia, Wille Gabriele, Saenger Wolfram, Uchanska-Ziegler Barbara, Hoogenboom Hennie R, Ziegler Andreas

机构信息

Institut für Chemie/Kristallographie, Freie Universität Berlin, 14195 Berlin, Germany, Cellectis, 93235 Romainville, France.

出版信息

J Biol Chem. 2005 Jan 28;280(4):2972-80. doi: 10.1074/jbc.M411323200. Epub 2004 Nov 10.

DOI:10.1074/jbc.M411323200
PMID:15537658
Abstract

Antibodies with T cell receptor-like specificity possess a considerable diagnostic and therapeutic potential, but the structural basis of the interaction between an antibody and an histocompatibility antigen has so far not been determined. We present here the crystal structure (at 2.15 A resolution) of the recombinant, affinity-matured human antibody fragment Fab-Hyb3 bound to the tumor-associated human leukocyte antigen (HLA)/peptide complex HLA-A1.MAGE-A1. Fab-Hyb3 employs a diagonal docking mode resembling that of T cell receptors. However, other than these natural ligands, the antibody uses only four of its six complementarity-determining regions for direct interactions with the target. It recognizes the C-terminal half of the MAGE-A1 peptide, the HLA-A1 alpha1-helix, and N-terminal residues of the alpha2-helix, accompanied by a large tilting angle between the two types of molecules within the complex. Interestingly, only a single hydrogen bond between a peptide side chain and Fab-Hyb3 contributes to the interaction, but large buried surface areas with pronounced shape complementarity assure high affinity and specificity for MAGE-A1. The HLA-A1.MAGE-A1.antibody structure is discussed in comparison with those of natural ligands recognizing HLA.peptide complexes.

摘要

具有类似T细胞受体特异性的抗体具有相当大的诊断和治疗潜力,但迄今为止,抗体与组织相容性抗原之间相互作用的结构基础尚未确定。我们在此展示了重组的、亲和力成熟的人抗体片段Fab-Hyb3与肿瘤相关人白细胞抗原(HLA)/肽复合物HLA-A1.MAGE-A1结合的晶体结构(分辨率为2.15埃)。Fab-Hyb3采用类似于T细胞受体的对角对接模式。然而,除了这些天然配体之外,该抗体仅使用其六个互补决定区中的四个与靶标进行直接相互作用。它识别MAGE-A1肽的C端一半、HLA-A1α1螺旋以及α2螺旋的N端残基,复合物中两种分子之间存在较大的倾斜角。有趣的是,肽侧链与Fab-Hyb3之间仅一个氢键有助于这种相互作用,但具有明显形状互补性的大掩埋表面积确保了对MAGE-A1的高亲和力和特异性。与识别HLA-肽复合物的天然配体的结构相比,对HLA-A1.MAGE-A1-抗体结构进行了讨论。

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