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铍特异性 TCR 的诱变表明抗原识别具有不寻常的结合拓扑结构。

Mutagenesis of beryllium-specific TCRs suggests an unusual binding topology for antigen recognition.

机构信息

Department of Medicine, University of Colorado Denver, Aurora, CO 80045, USA.

出版信息

J Immunol. 2011 Oct 1;187(7):3694-703. doi: 10.4049/jimmunol.1101872. Epub 2011 Aug 26.

Abstract

Unconventional Ags, such as metals, stimulate T cells in a very specific manner. To delineate the binding landscape for metal-specific T cell recognition, alanine screens were performed on a set of Be-specific TCRs derived from the lung of a chronic beryllium disease patient. These TCRs are HLA-DP2-restricted and express nearly identical TCR Vβ5.1 chains coupled with different TCR α-chains. Site-specific mutagenesis of all amino acids comprising the CDRs of the TCRA and TCRB genes showed a dominant role for Vβ5.1 residues in Be recognition, with little contribution from the TCR α-chain. Solvent-exposed residues along the α-helices of the HLA-DP2 α- and β-chains were also mutated to alanine. Two β-chain residues, located near the proposed Be binding site of HLA-DP2, played a dominant role in T cell recognition with no contribution from the HLA-DP2 α-chain. These findings suggest that Be-specific T cells recognize Ag using an unconventional binding topology, with the majority of interactions contributed by TCR Vβ5.1 residues and the HLA-DP2 β1-chain. Thus, unusual docking topologies are not exclusively used by autoreactive T cells, but also for the recognition of unconventional metal Ags, such as Be.

摘要

非常规抗原,如金属,以非常特定的方式刺激 T 细胞。为了描绘金属特异性 T 细胞识别的结合景观,对一组源自慢性铍病患者肺部的 Be 特异性 TCR 进行了丙氨酸筛选。这些 TCR 受 HLA-DP2 限制,表达几乎相同的 TCR Vβ5.1 链,并与不同的 TCRα 链结合。对 TCRα和 TCRB 基因的 CDR 中所有氨基酸进行的定点突变显示,Vβ5.1 残基在 Be 识别中起主导作用,而 TCRα 链的贡献很小。HLA-DP2α和β链的α螺旋上的溶剂暴露残基也被突变为丙氨酸。位于 HLA-DP2 拟议 Be 结合位点附近的两个β链残基在 T 细胞识别中起主导作用,而 HLA-DP2α 链没有贡献。这些发现表明,Be 特异性 T 细胞使用非常规的结合拓扑结构来识别 Ag,其中大多数相互作用由 TCR Vβ5.1 残基和 HLA-DP2β1 链贡献。因此,不寻常的对接拓扑结构不仅被自身反应性 T 细胞使用,而且还被非常规金属 Ag(如 Be)的识别所使用。

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