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The effect of regulatory T cells on tolerance to airborne allergens and allergen immunotherapy

机译:调节性T细胞对空气传播过敏原和过敏原免疫疗法耐受的影响

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摘要

Forkhead box P3-positive regulatory T (Treg) cells are essential mediators of tolerance against self-antigens and harmless exogenous antigens. Treg cell deficiencies result in multiple autoimmune and allergic syndromes in neonates. How Treg cells affect conventional allergies against aeroantigens, which are restricted to a few specific proteins released from inhaled particles, remains controversial. The hallmarks of antigen-Specific loss of tolerance are allergen-specific T(H)2 cells and IgE. However, difficulties in identifying the rare allergen-specific Treg cells have obscured the cellular basis of tolerance to aeroallergens, which is also a major obstacle for the rational design of novel and more efficient allergen-specific immunotherapies. Recent technological progress allowing characterization of allergen-specific effectors and Treg cells with minimal in vitro manipulation revealed their detailed contribution to tolerance. The data identified inhaled particles as immunodominant Treg cell targets in healthy and allergic subjects. Conversely, the supposed immunodominant major allergens being rapidly released from inhaled particles apparently do not actively induce tolerance but are ignored by the immune system. Here, the partially contradictory data on various allergen-specific T-cell types in healthy subjects, allergic patients, and patients undergoing allergen-specific immunotherapy are discussed and integrated into one model, postulating Treg cell-dependent and Treg cell-independent checkpoints of tolerance and allergy development.
机译:叉头框P3-正向调节性T(Treg)细胞是对自身抗原和无害的外源性抗原的耐受性至关重要介质。 Treg细胞的缺陷导致在新生儿多种自身免疫疾病和过敏性综合征。 Treg细胞如何影响对aeroantigens,这仅限于从吸入颗粒释放一些特定的蛋白质过敏的传统,仍存在争议。公差的抗原特异性损失的特点是变应原特异性T(H)2个细胞和IgE。然而,在变应原鉴定特定的稀土困难Treg细胞已遮蔽耐受性过敏原的细胞基础,这也是新颖的和更有效的变应原免疫疗法的特定的合理设计的重要障碍。最近的技术进步使过敏原特异性效应和调节性T细胞的特性,在体外操作最小透露他们的宽容详细的贡献。数据确定吸入颗粒在健康和过敏症对象的免疫Treg细胞目标。相反,应该免疫的主要过敏原正迅速从吸入颗粒释放显然不主动诱导耐受,但免疫系统会被忽略。在此,在健康受试者中,过敏性患者和经历变应原 - 特异性免疫疗法的患者的各种变应原特异性T细胞类型的部分矛盾的数据进行了讨论和集成到一个模型中,postulating公差的调节性T细胞依赖性和T reg细胞无关的检查点和过敏的发展。

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