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完整和消化的 Ara h 1 的 IgE 表位:在人类和大鼠中的比较研究。

IgE epitopes of intact and digested Ara h 1: a comparative study in humans and rats.

机构信息

National Food Institute, Division of Toxicology and Risk Assessment, Technical University of Denmark, Mørkhøj Bygade 19, Søborg, Denmark.

出版信息

Mol Immunol. 2012 Jul;51(3-4):337-46. doi: 10.1016/j.molimm.2012.04.002. Epub 2012 May 1.

Abstract

BACKGROUND

Allergen epitope characterization provides valuable information useful for the understanding of proteins as food allergens. It is believed that IgE epitopes in general are conformational, nevertheless, for food allergens known to sensitize through the gastrointestinal tract linear epitopes have been suggested to be of great importance.

OBJECTIVE

The aim of this study was to identify IgE specific epitopes of intact and digested Ara h 1, and to compare epitope patterns between humans and rats.

METHODS

Sera from five peanut allergic patients and five Brown Norway rats were used to identify intact and digested Ara h 1-specific IgE epitopes by competitive immunoscreening of a phage-displayed random hepta-mer peptide library using polyclonal IgE from the individual sera. The resulting peptide sequences were mapped on the surface of a three-dimensional structure of the Ara h 1 molecule to mimic epitopes using a computer-based algorithm.

RESULTS

Patients as well as rats were shown to have individual IgE epitope patterns. All epitope mimics were conformational and found to cluster into three different areas of the Ara h 1 molecule. Five epitope motifs were identified by patient IgE, which by far accounted for most of the eluted peptide sequences. Epitope patterns were rather similar for both intact and digested Ara h 1 as well as for humans and rats.

CONCLUSIONS

Individual patient specific epitope patterns have been identified for the major allergen Ara h 1. IgE binding epitopes have been suggested as biomarkers for persistency and severity of food allergy, wherefore recognition of particular epitope patterns or motifs could be a valuable tool for prevention, diagnosis, and treatment of food allergy.

摘要

背景

变应原表位特征提供了有价值的信息,有助于理解蛋白质作为食物过敏原。人们认为 IgE 表位通常是构象的,然而,对于已知通过胃肠道致敏的食物过敏原,线性表位被认为非常重要。

目的

本研究旨在鉴定完整和消化的 Ara h 1 的 IgE 特异性表位,并比较人类和大鼠之间的表位模式。

方法

使用来自 5 名花生过敏患者和 5 只 Brown Norway 大鼠的血清,通过使用个体血清中的多克隆 IgE 对噬菌体展示的随机七肽文库进行竞争性免疫筛选,鉴定完整和消化的 Ara h 1 特异性 IgE 表位。将所得的肽序列映射到 Ara h 1 分子的三维结构表面上,使用基于计算机的算法模拟表位。

结果

显示患者和大鼠都具有个体 IgE 表位模式。所有表位模拟物均为构象性的,并且发现聚集在 Ara h 1 分子的三个不同区域。通过患者 IgE 鉴定了 5 个表位基序,迄今为止,这些基序占洗脱肽序列的大部分。完整和消化的 Ara h 1 以及人类和大鼠的表位模式非常相似。

结论

已经确定了主要过敏原 Ara h 1 的个体患者特异性表位模式。IgE 结合表位被认为是食物过敏持续性和严重程度的生物标志物,因此识别特定的表位模式或基序可能是预防、诊断和治疗食物过敏的有价值的工具。

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