首页> 美国卫生研究院文献>Biochemical Journal >Mutational epitope analysis of Pru av 1 and Api g 1 the major allergens of cherry (Prunus avium) and celery (Apium graveolens): correlating IgE reactivity with three-dimensional structure.
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Mutational epitope analysis of Pru av 1 and Api g 1 the major allergens of cherry (Prunus avium) and celery (Apium graveolens): correlating IgE reactivity with three-dimensional structure.

机译:樱桃(Prunus avium)和芹菜(Apium graveolens)的主要过敏原Pru av 1和Api g 1的突变表位分析:将IgE反应性与三维结构相关联。

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摘要

Birch pollinosis is often accompanied by adverse reactions to food due to pollen-allergen specific IgE cross-reacting with homologous food allergens. The tertiary structure of Pru av 1, the major cherry (Prunus avium) allergen, for example, is nearly identical with Bet v 1, the major birch (Betula verrucosa) pollen allergen. In order to define cross-reactive IgE epitopes, we generated and analysed mutants of Pru av 1 and Api g 1.0101, the major celery (Apium graveolens) allergen, by immunoblotting, EAST (enzyme allergosorbent test), CD and NMR spectroscopy. The mutation of Glu45 to Trp45 in the P-loop region, a known IgE epitope of Bet v 1, significantly reduced IgE binding to Pru av 1 in a subgroup of cherry-allergic patients. The backbone conformation of Pru av 1 wild-type is conserved in the three-dimensional structure of Pru av 1 Trp45, demonstrating that the side chain of Glu45 is involved in a cross-reactive IgE epitope. Accordingly, for a subgroup of celery-allergic patients, IgE binding to the homologous celery allergen Api g 1.0101 was enhanced by the mutation of Lys44 to Glu. The almost complete loss of IgE reactivity to the Pru av 1 Pro112 mutant is due to disruption of its tertiary structure. Neither the mutation Ala112 nor deletion of the C-terminal residues 155-159 influenced IgE binding to Pru av 1. In conclusion, the structure of the P-loop partially explains the cross-reactivity pattern, and modulation of IgE-binding by site-directed mutagenesis is a promising approach to develop hypo-allergenic variants for patient-tailored specific immunotherapy.
机译:桦木花粉症通常伴随食物不良反应,这是由于花粉-变应原特异性IgE与同源食物变应原发生交叉反应。例如,主要樱桃(Prunus avium)过敏原Pru av 1的三级结构与主要桦树(Betula verrucosa)花粉过敏原Bet v 1的三级结构几乎相同。为了定义交叉反应性IgE表位,我们通过免疫印迹,EAST(酶敏吸附试验),CD和NMR光谱法生成并分析了主要芹菜(Apium graveolens)过敏原Pru av 1和Api g 1.0101的突变体。在樱桃过敏患者亚组中,Bet v 1的已知IgE表位P环区域中Glu45突变为Trp45,显着降低了IgE与Pru av 1结合的IgE结合力。 Pru av 1 Trp45的三维结构中保守了Pru av 1野生型的骨架构象,表明Glu45的侧链参与了交叉反应性IgE表位。因此,对于一族芹菜过敏患者,通过将Lys44突变为Glu增强了与同源芹菜过敏原Api g 1.0101结合的IgE。 IgE对Pru av 1 Pro112突变体的反应性几乎完全丧失是由于其三级结构的破坏。突变Ala112或C末端残基155-159的缺失都不会影响IgE与Pru av 1的结合。总而言之,P环的结构部分解释了交叉反应性模式以及位点对IgE结合的调节。定向诱变是开发针对患者量身定制的特异性免疫疗法的低变应原性变体的有前途的方法。

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