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鉴定和生化特性分析来自土曲霉的新真菌过敏原 Asp t 36。

Identification and biochemical characterization of Asp t 36, a new fungal allergen from Aspergillus terreus.

机构信息

Division of Plant Biology, Bose Institute (Main Campus), Kolkata, India.

CSIR-Institute of Genomics and Integrative Biology, New Delhi, India.

出版信息

J Biol Chem. 2020 Dec 18;295(51):17852-17864. doi: 10.1074/jbc.RA120.015801.

Abstract

Aspergillus terreus is an allergenic fungus, in addition to causing infections in both humans and plants. However, the allergens in this fungus are still unknown, limiting the development of diagnostic and therapeutic strategies. We used a proteomic approach to search for allergens, identifying 16 allergens based on two-dimensional immunoblotting with A. terreus susceptible patient sera. We further characterized triose-phosphate isomerase (Asp t 36), one of the dominant IgE (IgE)-reactive proteins. The gene was cloned and expressed in Escherichia coli. Phylogenetic analysis showed Asp t 36 to be highly conserved with close similarity to the triose-phosphate isomerase protein sequence from Dermatophagoides farinae, an allergenic dust mite. We identified four immunodominant epitopes using synthetic peptides, and mapped them on a homology-based model of the tertiary structure of Asp t 36. Among these, two were found to create a continuous surface patch on the 3D structure, rendering it an IgE-binding hotspot. Biophysical analysis indicated that Asp t 36 shows similar secondary structure content and temperature sensitivity with other reported triose-phosphate isomerase allergens. In vivo studies using a murine model displayed that the recombinant Asp t 36 was able to stimulate airway inflammation, as demonstrated by an influx of eosinophils, goblet cell hyperplasia, elevated serum Igs, and induction of Th2 cytokines. Collectively, our results reveal the immunogenic property of Asp t 36, a major allergen from A. terreus, and define a new fungal allergen more broadly. This allergen could serve as a potent candidate for investigating component resolved diagnosis and immunotherapy.

摘要

土曲霉是一种致敏真菌,除了引起人类和植物感染外。然而,这种真菌的过敏原仍然未知,这限制了诊断和治疗策略的发展。我们使用蛋白质组学方法来寻找过敏原,根据与土曲霉易感患者血清的二维免疫印迹,鉴定出 16 种过敏原。我们进一步表征了三磷酸甘油异构酶(Asp t 36),这是一种主要的 IgE(IgE)反应蛋白之一。该基因在大肠杆菌中被克隆和表达。系统发育分析表明,Asp t 36 与尘螨过敏原——屋尘螨的三磷酸甘油异构酶蛋白序列高度保守,具有密切的相似性。我们使用合成肽鉴定了四个免疫显性表位,并将其映射到 Asp t 36 的基于同源性的三级结构模型上。其中,有两个被发现构成了 3D 结构上的连续表面斑块,使其成为 IgE 结合的热点。生物物理分析表明,Asp t 36 显示出与其他报道的三磷酸甘油异构酶过敏原相似的二级结构含量和温度敏感性。使用小鼠模型的体内研究表明,重组 Asp t 36 能够刺激气道炎症,表现为嗜酸性粒细胞流入、杯状细胞增生、血清 Ig 升高和 Th2 细胞因子的诱导。总之,我们的结果揭示了土曲霉主要过敏原 Asp t 36 的免疫原性,并定义了一种更广泛的新型真菌过敏原。该过敏原可作为研究成分解析诊断和免疫治疗的有力候选物。

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