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Tertiary structure of peanut allergen ara h 1

机译:花生过敏原ara h 1的三级结构

摘要

Ara h 1, a major peanut allergen, has been isolated and shown to contain 23 linear IgE-binding epitopes, 6-10 residues in length. Analysis of wild-type and mutant peptides with single amino acids substitutions showed that amino acids residing in the middle of the epitope were more critical for IgE binding; that polar charged residues occurred more frequently within the epitope while apolar residues were more important for IgE binding; and that a single amino acid substitution in an epitope resulted in a loss of ability to bind IgE. In addition, a homology-based molecular model of the Ara h 1 protein representing residues 171-586 was made and allowed visualization of epitopes 10-22. The majority of these epitopes appear clustered and many of the critical amino acids involved in binding are evenly distributed on the surface. The information from the mutational analysis and the molecular model will aid in the design of immunotherapies.
机译:已分离出主要花生过敏原Ara h 1,并显示其包含23个线性IgE结合表位,长度为6-10个残基。对具有单个氨基酸取代的野生型和突变型肽的分析表明,位于表位中间的氨基酸对于IgE结合更为关键。极性带电荷的残基在表位内的发生频率更高,而非极性残基对IgE的结合更重要;并且表位中的单个氨基酸取代导致结合IgE的能力丧失。另外,制备了代表残基171-586的Ara h 1蛋白的基于同源性的分子模型,并允许可视化表位10-22。这些表位中的大多数似乎是簇状的,并且参与结合的许多关键氨基酸均匀地分布在表面上。来自突变分析和分子模型的信息将有助于免疫疗法的设计。

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