首页> 外文期刊>International Journal of Molecular Sciences >Modulating Shrimp Tropomyosin-Mediated Allergy: Hypoallergen DNA Vaccines Induce Regulatory T Cells to Reduce Hypersensitivity in Mouse Model
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Modulating Shrimp Tropomyosin-Mediated Allergy: Hypoallergen DNA Vaccines Induce Regulatory T Cells to Reduce Hypersensitivity in Mouse Model

机译:调节虾Tropomyosin介导的过敏:低变应原DNA疫苗诱导调节性T细胞减少小鼠模型中的超敏反应。

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Shellfish allergy is one of the most common food allergies, with tropomyosin as the major cross-reactive allergen. However, no allergen-specific immunotherapy is clinically available. Recently, we designed two shrimp hypoallergens MEM49 and MED171. This study aimed to examine and compare the efficacy of the MEM49- and MED171-based DNA vaccines (pMEM49 and pMED171) in modulating shrimp allergy in a murine model of shrimp tropomyosin sensitivity. Intradermal immunization of BALB/c mice with pMEM49 or pMED171 effectively down-modulated allergic symptoms, tropomyosin-specific IgE levels, intestinal Th2 cytokines expression, and inflammatory cell infiltration. Both pMEM49 and pMED171 increased the frequency of regulatory T cells, but to a greater extent by pMED171 with upregulation of gut-homing molecules integrin-α4β7. The functionality of the pMED171-induced Treg cells was further illustrated by anti-CD25-mediated depletion of Treg cells and the adoptive transfer of CD4 + CD25 + Foxp3 + Treg cells. Collectively, the data demonstrate that intradermal administration of pMED171 leads to the priming, activation, and migration of dermal dendritic cells which subsequently induce Treg cells, both locally and systemically, to downregulate the allergic responses to tropomyosin. This study is the first to demonstrate the potency of hypoallergen-encoding DNA vaccines as a therapeutic strategy for human shellfish allergy via the vigorous induction of functional Treg cells.
机译:贝类过敏是最常见的食物过敏之一,原肌球蛋白是主要的交叉反应性过敏原。但是,临床上尚无过敏原特异性免疫疗法。最近,我们设计了两种虾低过敏原MEM49和MED171。这项研究旨在检查和比较基于MEM49和MED171的DNA疫苗(pMEM49和pMED171)在对虾原肌球蛋白敏感性小鼠模型中调节虾过敏的功效。用pMEM49或pMED171对BALB / c小鼠进行皮内免疫可有效下调过敏症状,原肌球蛋白特异性IgE水平,肠道Th2细胞因子表达和炎性细胞浸润。 pMEM49和pMED171均增加了调节性T细胞的频率,但更大程度上是pMED171上调了肠归巢分子整联蛋白-α4β7的表达。通过抗CD25介导的Treg细胞耗竭和CD4 + CD25 + Foxp3 + Treg细胞的过继转移,进一步说明了pMED171诱导的Treg细胞的功能。总体而言,数据表明皮内注射pMED171导致真皮树突状细胞的引发,激活和迁移,继而局部和全身诱导Treg细胞,从而下调对原肌球蛋白的过敏反应。这项研究首次证明了编码低变应原的DNA疫苗通过强烈诱导功能性Treg细胞诱导作为人类贝类过敏的治疗策略的潜力。

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