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首页> 外文期刊>The Journal of Allergy and Clinical Immunology >An experimental and modeling-based approach to locate IgE epitopes of plant profilin allergens.
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An experimental and modeling-based approach to locate IgE epitopes of plant profilin allergens.

机译:一种基于实验和基于模型的方法来定位植物profilin过敏原的IgE表位。

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摘要

BACKGROUND: Plant profilins are actin-binding proteins that form a well-known panallergen family responsible for cross-sensitization between plant foods and pollens. Melon profilin, Cuc m 2, is the major allergen of this fruit. OBJECTIVE: We sought to map IgE epitopes on the 3-dimensional structure of Cuc m 2. METHODS: IgE binding to synthetic peptides spanning the full Cuc m 2 amino acid sequence was assayed by using a serum pool and individual sera from 10 patients with melon allergy with significant specific IgE levels to this allergen. Three-dimensional modeling and potential epitope location were based on analysis of both solvent exposure and electrostatic properties of the Cuc m 2 surface. RESULTS: Residues included in synthetic peptides that exerted the strongest IgE-binding capacity defined 2 major epitopes (E1, consisting of residues 66-75 and 81-93, and E2, consisting of residues 95-99 and 122-131) that partially overlapped with the actin-binding site of Cuc m 2. Two additional epitopes (E3, including residues 2-10, and E4, including residues 35-45) that should show weaker putative antigen-antibody associations and shared most residues with synthetic peptides with low IgE-binding capacity were predicted on theoretical grounds. CONCLUSIONS: Strong and weak IgE epitopes have been uncovered in melon profilin, Cuc m 2. CLINICAL IMPLICATIONS: The different types of IgE epitopes located in the 3-dimensional structure of melon profilin can constitute the molecular basis to explain the sensitization and cross-reactivity exhibited by this panallergen family.
机译:背景:植物纤维蛋白原是肌动蛋白结合蛋白,形成众所周知的泛过敏原家族,负责植物性食物和花粉之间的交叉致敏作用。甜瓜脯氨酸蛋白(Cuc m 2)是这种水果的主要过敏原。目的:我们试图将IgE抗原决定簇定位在Cuc m 2的3维结构上。方法:通过使用血清库和来自10例哈密瓜患者的单独血清来测定IgE与跨越整个Cuc m 2氨基酸序列的合成肽的结合对这种过敏原具有明显的特定IgE水平的过敏。三维建模和潜在的抗原决定簇位置是基于对Cuc m 2表面的溶剂暴露和静电性质的分析。结果:具有最强IgE结合能力的合成肽中包含的残基定义了部分重叠的2个主要表位(E1,由残基66-75和81-93组成,E2,由残基95-99和122-131组成) Cuc m 2的肌动蛋白结合位点。另外两个抗原决定簇(E3,包括2-10残基,E4,包括35-45残基),应该显示较弱的推定抗原-抗体结合力,并且大多数残基与合成肽低IgE结合能力是在理论基础上预测的。结论:瓜蛋白2,Cuc m 2中已发现强和弱的IgE表位。临床意义:位于瓜蛋白3维结构中的不同类型的IgE表位可构成解释敏化和交叉反应性的分子基础。该panallergen系列展出的产品。

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