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过敏中 T 滤泡辅助细胞的异质性、亚群和可塑性。

Heterogeneity, subsets, and plasticity of T follicular helper cells in allergy.

机构信息

Department of Medicine, Schroeder Allergy and Immunology Research Institute, McMaster Immunology Research Centre, McMaster University, Hamilton, Ontario, Canada.

Department of Medicine, Schroeder Allergy and Immunology Research Institute, McMaster Immunology Research Centre, McMaster University, Hamilton, Ontario, Canada.

出版信息

J Allergy Clin Immunol. 2022 Nov;150(5):990-998. doi: 10.1016/j.jaci.2022.08.023. Epub 2022 Sep 6.

DOI:10.1016/j.jaci.2022.08.023
PMID:36070826
Abstract

Antibody responses are critical for protection against pathogens. However, diseases such as allergic rhinitis or food allergy result from aberrant production of IgE antibodies against otherwise innocuous environmental antigens. The production of allergen-specific IgE requires interaction between B cells and CD4 T cells, and a granular understanding of these interactions is required to develop novel therapies for allergic disease. CD4 T cells are exceptionally heterogeneous in their transcriptional, epigenetic, and proteomic profiles, which poses significant challenges when attempting to define subsets relevant to the study of allergy among a continuum of cells. Defining subsets such as the T follicular helper (T) cell cluster provides a shorthand to understand the functions of CD4 T cells in antibody production and supports mechanistic experimentation for hypothesis-driven discovery. With a focus on allergic disease, this Rostrum article broadly discusses heterogeneity among CD4 T cells and provides a rationale for subdividing T cells into both functional and cytokine-skewed subsets. Further, it highlights the plasticity demonstrated by T cells during the primary response and after recall, and it explores the possibility of harnessing this plasticity to reprogram immunity for therapeutic benefit in allergic disease.

摘要

抗体反应对于抵御病原体至关重要。然而,过敏性鼻炎或食物过敏等疾病是由于对原本无害的环境抗原产生异常的 IgE 抗体而导致的。过敏原特异性 IgE 的产生需要 B 细胞和 CD4 T 细胞之间的相互作用,为了开发治疗过敏性疾病的新疗法,需要对这些相互作用有深入的了解。CD4 T 细胞在转录、表观遗传和蛋白质组学特征上具有极高的异质性,这给试图在细胞连续体中定义与过敏研究相关的亚群带来了重大挑战。定义 T 滤泡辅助 (Tfh) 细胞簇等亚群为理解 CD4 T 细胞在抗体产生中的功能提供了一种简写方式,并支持基于假设的发现进行机制实验。本文重点讨论了 CD4 T 细胞的异质性,并为将 T 细胞细分为功能和细胞因子偏向亚群提供了理论依据。此外,本文还强调了 T 细胞在初次应答和回忆期间表现出的可塑性,并探讨了利用这种可塑性为过敏性疾病的治疗益处重新编程免疫的可能性。

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