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梯牧草花粉主要过敏原Phl p 5a的低免疫球蛋白E结合突变体的产生。

Generation of a low immunoglobulin E-binding mutant of the timothy grass pollen major allergen Phl p 5a.

作者信息

Wald M, Kahlert H, Weber B, Jankovic M, Keller W, Cromwell O, Nandy A, Fiebig H

机构信息

Allergopharma J. Ganzer KG, Research & Development, Reinbek, Germany.

出版信息

Clin Exp Allergy. 2007 Mar;37(3):441-50. doi: 10.1111/j.1365-2222.2007.02669.x.

Abstract

BACKGROUND

Immunotherapy of grass pollen allergy is currently based on the administration of pollen extracts containing natural allergens. Specifically designed recombinant allergens with reduced IgE reactivity could be used in safer and more efficacious future therapy concepts.

OBJECTIVES

This study aimed to generate hypoallergenic variants of the timothy grass major allergen Phl p 5a as candidates for allergen-specific immunotherapy.

METHODS

Three deletion mutants were produced in Escherichia coli and subsequently purified. The overall IgE-binding capacity of the mutants was compared with the recombinant wild-type allergen by membrane blot and IgE-inhibition assays. The capacity for effector cell activation was determined in basophil activation assays. T cell proliferation assays with allergen-specific T cell lines were performed to confirm the retention of T cell reactivity. Structural properties were characterized by circular dichroism analysis and homogeneity by native isoelectric focusing. The deletion sites were mapped on homology models comprising the N- and C-terminal halves of Phl p 5a, respectively.

RESULTS

The double-deletion mutant rPhl p 5a Delta(94-113, 175-198) showed strongly diminished IgE binding in membrane blot and IgE-inhibition assays. Both deletions affect predominantly alpha-helical regions located in the N- and C-terminal halves of Phl p 5a, respectively. Whereas deletion of Delta175-198 alone was sufficient to cause a large reduction of the IgE reactivity in a subgroup of allergic sera, only the combination of both deletions was highly effective for all the sera tested. rPhl p 5a Delta(94-113, 175-198) consistently showed at least an 11.5-fold reduced capacity to activate basophils compared with the recombinant wild-type molecule, and the T cell proliferation assays demonstrated retention of T cell reactivity.

CONCLUSION

The mutant rPhl p 5a Delta(94-113, 175-198) fulfils the basic requirements for a hypoallergenic molecule suitable for a future immunotherapy of grass pollen allergy; it offers substantially reduced IgE binding and maintained T cell reactivity.

摘要

背景

目前,草花粉过敏的免疫疗法是基于给予含有天然过敏原的花粉提取物。具有降低的IgE反应性的专门设计的重组过敏原可用于更安全、更有效的未来治疗方案。

目的

本研究旨在生成梯牧草主要过敏原Phl p 5a的低变应原性变体,作为变应原特异性免疫疗法的候选物。

方法

在大肠杆菌中产生了三个缺失突变体,随后进行纯化。通过膜印迹和IgE抑制试验,将突变体的总体IgE结合能力与重组野生型过敏原进行比较。在嗜碱性粒细胞活化试验中测定效应细胞活化能力。用变应原特异性T细胞系进行T细胞增殖试验,以确认T细胞反应性的保留。通过圆二色性分析表征结构特性,通过天然等电聚焦表征均一性。缺失位点分别定位在包含Phl p 5a N端和C端一半的同源模型上。

结果

双缺失突变体rPhl p 5a Δ(94 - 113, 175 - 198)在膜印迹和IgE抑制试验中显示IgE结合显著减少。两个缺失分别主要影响位于Phl p 5a N端和C端一半的α螺旋区域。虽然单独缺失Δ175 - 198足以导致一部分过敏血清中IgE反应性大幅降低,但只有两个缺失的组合对所有测试血清都非常有效。与重组野生型分子相比,rPhl p 5a Δ(94 - 113, 175 - 198)始终显示激活嗜碱性粒细胞的能力至少降低了11.5倍,并且T细胞增殖试验证明保留了T细胞反应性。

结论

突变体rPhl p 5a Δ(94 - 113, 175 - 198)满足了适合未来草花粉过敏免疫疗法的低变应原性分子的基本要求;它提供了显著降低的IgE结合并保持了T细胞反应性。

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