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特异性效应性 Th2 细胞对变应原的识别使人类的调节性 T 细胞反应能够依赖于 IL-2 的激活。

Allergen recognition by specific effector Th2 cells enables IL-2-dependent activation of regulatory T-cell responses in humans.

机构信息

Icahn School of Medicine at Mount Sinai, Jaffe Food Allergy Institute, New York, New York, USA.

Icahn School of Medicine at Mount Sinai, Precision Immunology Institute, New York, New York, USA.

出版信息

Allergy. 2023 Mar;78(3):697-713. doi: 10.1111/all.15512. Epub 2022 Sep 20.

Abstract

Type 2 allergen-specific T cells are essential for the induction and maintenance of allergies to foods, and Tregs specific for these allergens are assumed to be involved in their resolution. However, it has not been convincingly demonstrated whether allergen-specific Treg responses are responsible for the generation of oral tolerance in humans. We observed that sustained food allergen exposure in the form of oral immunotherapy resulted in increased frequency of Tregs only in individuals with lasting clinical tolerance. We sought to identify regulatory components of the CD4 T-cell response to food allergens by studying their functional activation over time in vitro and in vivo. Two subsets of Tregs expressing CD137 or CD25/OX40 were identified with a delayed kinetics of activation compared with clonally enriched pathogenic effector Th2 cells. Treg activation was dependent on IL-2 derived from effector T cells. In vivo exposure to peanut in the form of an oral food challenge of allergic subjects induced a delayed and persistent activation of Tregs after initiation of the allergen-specific Th2 response. The novel finding of our work is that a sustained wave of Treg activation is induced by the release of IL-2 from Th2 effector cells, with the implication that therapeutic administration of IL-2 could improve current OIT approaches.

摘要

2 型过敏原特异性 T 细胞对于诱导和维持食物过敏至关重要,而针对这些过敏原的 Tregs 被认为参与了其缓解。然而,尚未令人信服地证明过敏原特异性 Treg 反应是否负责人类口服耐受的产生。我们观察到,持续的食物过敏原暴露形式的口服免疫治疗仅在具有持久临床耐受的个体中导致 Tregs 频率增加。我们试图通过研究体外和体内随时间推移对食物过敏原的 CD4 T 细胞反应的调节成分来识别它们。与克隆富集的致病性效应 Th2 细胞相比,鉴定出表达 CD137 或 CD25/OX40 的两个 Treg 亚群,其激活的动力学延迟。Treg 激活依赖于效应 T 细胞衍生的 IL-2。以过敏受试者口服食物挑战的形式对花生进行体内暴露,在启动过敏原特异性 Th2 反应后,诱导 Treg 的延迟和持续激活。我们工作的新发现是,IL-2 从 Th2 效应细胞释放诱导了持续的 Treg 激活波,这意味着 IL-2 的治疗性给药可能会改善当前的 OIT 方法。

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