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通过液质联用技术对人 CD3 CD56 T 细胞进行深度表型特征分析。

Deep phenotypical characterization of human CD3 CD56 T cells by mass cytometry.

机构信息

Institute for Medical Microbiology and Hospital Hygiene, University of Marburg, Marburg, Germany.

German Rheumatism Research Center Berlin (DRFZ), Leibniz Institute, Berlin, Germany.

出版信息

Eur J Immunol. 2021 Mar;51(3):672-681. doi: 10.1002/eji.202048941. Epub 2020 Dec 15.

DOI:10.1002/eji.202048941
PMID:33231295
Abstract

CD56 T cells are a group of pro-inflammatory CD3 lymphocytes with characteristics of natural killer cells, being involved in antimicrobial immune defense. Here, we performed deep phenotypic profiling of CD3 CD56 cells in peripheral blood of normal human donors and individuals sensitized to birch-pollen or/and house dust mite by high-dimensional mass cytometry combined with manual and computational data analysis. A co-regulation between major conventional T-cell subsets and their respective CD3 CD56 cell counterparts appeared restricted to CD8 , MAIT, and TCRγδ T-cell compartments. Interestingly, we find a co-regulation of several CD3 CD56 cell subsets in allergic but not in healthy individuals. Moreover, using FlowSOM, we distinguished a variety of CD56 T-cell phenotypes demonstrating a hitherto underestimated heterogeneity among these cells. The novel CD3 CD56 subset description comprises phenotypes superimposed with naive, memory, type 1, 2, and 17 differentiation stages, in part represented by a phenotypical continuum. Frequencies of two out of 19 CD3 CD56 FlowSOM clusters were significantly diminished in allergic individuals, demonstrating less frequent presence of cells with cytolytic, presumably protective, capacity in these donors consistent with defective expansion or their recruitment to the affected tissue. Our results contribute to defining specific cell populations to be targeted during therapy for allergic conditions.

摘要

CD56 T 细胞是一群具有自然杀伤细胞特征的促炎 CD3 淋巴细胞,参与抗微生物免疫防御。在这里,我们通过高维质谱流式细胞术结合手动和计算数据分析,对正常人类供体和对桦树花粉和/或屋尘螨过敏的个体外周血中的 CD3 CD56 细胞进行了深度表型分析。主要常规 T 细胞亚群与其各自的 CD3 CD56 细胞对应物之间的共同调节似乎仅限于 CD8、MAIT 和 TCRγδ T 细胞区室。有趣的是,我们发现过敏个体中存在几种 CD3 CD56 细胞亚群的共同调节,但在健康个体中不存在。此外,使用 FlowSOM,我们区分了多种 CD56 T 细胞表型,这些细胞表现出迄今为止被低估的异质性。新的 CD3 CD56 亚群描述包括与幼稚、记忆、1 型、2 型和 17 型分化阶段叠加的表型,部分由表型连续体表示。在过敏个体中,19 个 CD3 CD56 FlowSOM 簇中的两个簇的频率显著降低,表明这些供体中具有细胞毒性、可能具有保护作用的细胞存在频率较低,与它们的扩增缺陷或向受影响组织的募集一致。我们的研究结果有助于确定过敏治疗中靶向的特定细胞群体。

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