桦树花粉和榛子过敏患者来源的 IL-10 调节树突状细胞促进 Treg 介导的过敏原特异性和交叉反应性耐受。

IL-10-modulated dendritic cells from birch pollen- and hazelnut-allergic patients facilitate Treg-mediated allergen-specific and cross-reactive tolerance.

机构信息

Department of Dermatology, Division for Experimental and Translational Research, University Medical Center of the Johannes Gutenberg-University, Mainz, Germany.

Department of Internal Medicine, University Hospital Erlangen, University Erlangen-Nürnberg, Erlangen, Germany.

出版信息

Allergy. 2024 Oct;79(10):2826-2839. doi: 10.1111/all.16255. Epub 2024 Jul 28.

DOI:10.1111/all.16255

PMID:39073174

Abstract

BACKGROUND

Approximately 70% of individuals allergic to birch pollen (Bet v 1.01 [Bet]) develop a secondary food allergy (e.g., hazelnut: Cor a 1.04 [Cor]), due to allergen cross-reactivity. However, standard immunotherapy for type I allergies often does not improve the food allergy sufficiently. We analyzed the allergen-specific and cross-reactive suppressive capacity of primary human regulatory T cells (Treg) induced by autologous IL-10-modulated dendritic cells (IL-10 DC) in vitro and in vivo.

METHODS

CD4 T cells of patients with birch pollen and associated hazelnut allergies were differentiated into Bet-specific or non-specific induced Treg (iTreg). After Bet- or Cor-specific restimulation the phenotype, proliferation, and suppressive capacity of iTreg subsets were analyzed. iTreg function was further investigated in humanized mouse models of airway and intestinal allergy, generated by engraftment of peripheral blood mononuclear cells from allergic donors into immunodeficient animals.

RESULTS

After IL-10 DC priming and allergen-specific restimulation (Bet or Cor), non-specific control iTreg remained anergic, whereas Bet-specific iTreg proliferated extensively and exhibited a regulatory phenotype (enhanced expression of CTLA-4, PD-1, TNFR2, IL-10). Accordingly, activated Bet-specific iTreg displayed a high capacity to suppress Bet- and Cor-induced responder Th2 cell responses in vitro, indicating induction of both allergen-specific (birch) and cross-reactive tolerance (hazelnut). In vivo, the beneficial effect of Bet-specific iTreg was verified in humanized mouse models of allergic airway and intestinal inflammation, resulting in reduced allergen-induced clinical symptoms, and immune responses.

CONCLUSION

Human IL-10 DC-induced iTreg facilitate allergen-specific and cross-reactive tolerance. Therefore, they are potential candidates for regulatory cell therapy in allergic and autoimmune diseases.

摘要

背景

大约 70%的桦树花粉过敏个体（Bet v 1.01 [Bet]）会因过敏原交叉反应而发展为继发性食物过敏（例如榛子：Cor a 1.04 [Cor]）。然而，针对 I 型过敏的标准免疫疗法通常无法充分改善食物过敏。我们分析了自体白细胞介素 10 调节树突状细胞（IL-10-DC）体外和体内诱导的原代人调节性 T 细胞（Treg）的过敏原特异性和交叉反应性抑制能力。

方法

桦树花粉和相关榛子过敏患者的 CD4 T 细胞分化为特异性 Bet 或非特异性诱导 Treg（iTreg）。在特异性 Bet 或 Cor 再刺激后，分析 iTreg 亚群的表型、增殖和抑制能力。进一步通过移植过敏供体的外周血单核细胞到免疫缺陷动物中，建立气道和肠道过敏的人源化小鼠模型，研究 iTreg 的功能。

结果

在 IL-10-DC 启动和特异性抗原再刺激（Bet 或 Cor）后，非特异性对照 iTreg 仍处于无反应状态，而特异性 Bet iTreg 则广泛增殖并表现出调节表型（增强 CTLA-4、PD-1、TNFR2、IL-10 的表达）。因此，激活的特异性 Bet iTreg 在体外显示出抑制 Bet 和 Cor 诱导的应答 Th2 细胞反应的高能力，表明诱导了特异性（桦树）和交叉反应性（榛子）耐受。在体内，在过敏气道和肠道炎症的人源化小鼠模型中验证了特异性 Bet iTreg 的有益作用，导致减少了过敏原诱导的临床症状和免疫反应。