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基于结构的主要犬过敏原 Can f 1 的 IgE 表位预测。

Structure-based prediction of the IgE epitopes of the major dog allergen Can f 1.

机构信息

Department of Applied Life Sciences, Graduate School of Life and Environmental Sciences, Osaka Prefecture University, Sakai, Osaka, Japan.

Department of Food and Nutrition, Senri Kinran University, Suita, Osaka, Japan.

出版信息

FEBS J. 2022 Mar;289(6):1668-1679. doi: 10.1111/febs.16252. Epub 2021 Nov 7.

DOI:10.1111/febs.16252
PMID:34699686
Abstract

Allergy to dogs has become increasingly prominent worldwide. Seven dog allergens have been identified, including Canis familiaris allergen 1-7 (Can f 1-7). Although Can f 1 is a major dog allergen sensitized to 50-75% of dog-allergic subjects, its IgE epitopes have not been identified. The structural analysis of an allergen is important to identify conformational epitopes. In this study, we generated a recombinant Can f 1 protein and determined its crystal structure using X-ray crystallography. Can f 1 had a typical lipocalin fold, which is composed of an eight-stranded β-barrel and α-helix, and has high similarity to Can f 2, Can f 4, and Can f 6 in overall structure. However, the localizations of surface charges on these proteins were quite different. Based on sequence alignment and tertiary structure, we predicted five critical residues (His86, Glu98, Arg111, Glu138, and Arg152) for the IgE epitopes. The relevance of these residues to IgE reactivity was assessed by generating Can f 1 mutants with these residues substituted for alanine. Although the effects of the mutation on IgE binding depended on the sera of dog-allergic patients, H86A and R152A mutants showed reduced IgE reactivity compared with wild-type Can f 1. These results suggest that Can f 1 residues His86 and Arg152 are candidates for the IgE conformational epitope.

摘要

对狗的过敏反应在全球范围内变得越来越突出。已经确定了七种狗过敏原,包括犬过敏原 1-7(Can f 1-7)。虽然 Can f 1 是一种主要的狗过敏原,可使 50-75%的狗过敏患者致敏,但尚未鉴定其 IgE 表位。过敏原的结构分析对于鉴定构象表位很重要。在这项研究中,我们生成了重组 Can f 1 蛋白,并使用 X 射线晶体学确定了其晶体结构。Can f 1 具有典型的亲脂素折叠,由八链β-桶和α-螺旋组成,与 Can f 2、Can f 4 和 Can f 6 在整体结构上具有高度相似性。然而,这些蛋白质表面电荷的定位差异很大。基于序列比对和三级结构,我们预测了五个关键残基(His86、Glu98、Arg111、Glu138 和 Arg152)用于 IgE 表位。通过用这些残基取代丙氨酸生成 Can f 1 突变体来评估这些残基对 IgE 反应性的相关性。尽管突变对 IgE 结合的影响取决于狗过敏患者的血清,但与野生型 Can f 1 相比,H86A 和 R152A 突变体显示出降低的 IgE 反应性。这些结果表明,Can f 1 残基 His86 和 Arg152 是 IgE 构象表位的候选者。

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引用本文的文献

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Structural and ligand binding analysis of the pet allergens Can f 1 and Fel d 7.
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