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首页> 外文期刊>RSC Advances >Hypoallergenic acid-sensitive modification preserves major mugwort allergen fold and delivers full repertoire of MHC class II-binding peptides during endolysosomal degradation
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Hypoallergenic acid-sensitive modification preserves major mugwort allergen fold and delivers full repertoire of MHC class II-binding peptides during endolysosomal degradation

机译:在底溶解剂降解期间,低过敏性酸敏感改性保留了主要的Mugwort过敏原折叠,并在底溶解剂降解期间提供全曲目的MHC类II结合肽

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Modified allergens are a safer and more efficient alternative to natural allergens for specific immunotherapy. As the modification of an allergen can diminish its immunogenicity due to the alteration of T-cell epitopes, in this paper we study the effects of a reversible chemical modification of Art v 1, the main allergen of mugwort pollen, on its allergenicity and immunogenicity. Modification of Art v 1 by cis -aconitylation into a polyanionic derivative (CAA) did not result in any significant structural alteration. However, IgE-binding epitopes on CAA were blocked, resulting in a reduced IgE-binding and basophil activation. Both proteins induced proliferation of CD3 ~(+) CD4 ~(+) T-cells in mugwort-allergic patients, but only unmodified allergens increased IL-4, IL-5 and IL-10 production. Rabbit and mouse anti-CAA antibodies exhibited cross-reactivity with native allergens and blocked human IgE-binding to Art v 1. Degradation of CAA by lysosomal fraction enzymes resulted in a similar set of peptides, harboring MHC class II-binding peptides, as unmodified proteins. Thus, cis -aconitylation modified Art v 1 had a significantly reduced allergenicity, whereas its immunogenicity was completely preserved. Acid-environment-responsive modification, which releases a full repertoire of native allergen epitopes within a particular site, can be considered a smart drug delivery system, which is able to deliver a therapeutically-effective dose in a controlled manner, and minimizes adverse side effects.
机译:改性过敏原是对特定免疫疗法的天然过敏原的更安全和更有效的替代品。由于过敏原的修饰可以通过T细胞表位的改变来减少其免疫原性,因此在本文中,我们研究了艺术V 1,Mugwort Pollen的主要过敏原的可逆化学改性,对其过敏性和免疫原性的影响。通过CIS-Aconitylation将ART V 1改性为多阴离子衍生物(CAA)并未导致任何显着的结构改变。然而,CAA上的IgE结合表位被封闭,导致IgE结合和嗜碱性激活降低。蛋白质诱导了Mugwort-过敏患者的CD3〜(+)CD4〜(+)T细胞增殖,但只有未修饰的过敏原增加IL-4,IL-5和IL-10生产。兔和小鼠抗CAA抗体表现出与天然过敏原的交叉反应性,并阻止人IgE结合到ART V 1.通过溶酶体级分酶降解CAA,导致类似的一组肽,含有MHC II类结合肽,如未修改蛋白质。因此,CIS-Aconitylation改性的技术V 1具有显着降低的过敏性,而其免疫原性完全保存。酸环响应的修饰,释放特定部位内的本地过敏原表位的完全反弹,可被认为是一种智能药物输送系统,其能够以受控的方式递送治疗性有效剂量,并最大限度地减少不良副作用。

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