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三模态单细胞分析揭示了一种新型儿科 CD8αα T 细胞亚群,并广泛揭示了 T 细胞区室中与年龄相关的分子重编程。

Trimodal single-cell profiling reveals a novel pediatric CD8αα T cell subset and broad age-related molecular reprogramming across the T cell compartment.

机构信息

Allen Institute for Immunology, Seattle, WA, USA.

Department of Genome Sciences, University of Washington School of Medicine, Seattle, WA, USA.

出版信息

Nat Immunol. 2023 Nov;24(11):1947-1959. doi: 10.1038/s41590-023-01641-8. Epub 2023 Oct 16.

DOI:10.1038/s41590-023-01641-8
PMID:37845489
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10602854/
Abstract

Age-associated changes in the T cell compartment are well described. However, limitations of current single-modal or bimodal single-cell assays, including flow cytometry, RNA-seq (RNA sequencing) and CITE-seq (cellular indexing of transcriptomes and epitopes by sequencing), have restricted our ability to deconvolve more complex cellular and molecular changes. Here, we profile >300,000 single T cells from healthy children (aged 11-13 years) and older adults (aged 55-65 years) by using the trimodal assay TEA-seq (single-cell analysis of mRNA transcripts, surface protein epitopes and chromatin accessibility), which revealed that molecular programming of T cell subsets shifts toward a more activated basal state with age. Naive CD4 T cells, considered relatively resistant to aging, exhibited pronounced transcriptional and epigenetic reprogramming. Moreover, we discovered a novel CD8αα T cell subset lost with age that is epigenetically poised for rapid effector responses and has distinct inhibitory, costimulatory and tissue-homing properties. Together, these data reveal new insights into age-associated changes in the T cell compartment that may contribute to differential immune responses.

摘要

年龄相关的 T 细胞群变化已有充分描述。然而,目前的单模态或双模态单细胞检测方法(包括流式细胞术、RNA 测序和 CITE-seq)的局限性限制了我们对更复杂的细胞和分子变化进行剖析的能力。在这里,我们通过使用三模态检测方法 TEA-seq(单细胞分析 mRNA 转录物、表面蛋白表位和染色质可及性)对来自健康儿童(11-13 岁)和老年人(55-65 岁)的超过 300,000 个单个 T 细胞进行了分析,结果表明 T 细胞亚群的分子编程随着年龄的增长向更活跃的基础状态转移。被认为相对不易衰老的幼稚 CD4 T 细胞表现出明显的转录和表观遗传重编程。此外,我们发现了一种随着年龄增长而丢失的新型 CD8αα T 细胞亚群,该亚群在表观遗传上为快速效应反应做好了准备,并且具有独特的抑制、共刺激和组织归巢特性。总之,这些数据揭示了 T 细胞群与年龄相关变化的新见解,这些变化可能导致免疫反应的差异。

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