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Integrating single-cell RNA and T cell/B cell receptor sequencing with mass cytometry reveals dynamic trajectories of human peripheral immune cells from birth to old age

质量细胞仪 免疫系统 生物 核糖核酸 细胞 流式细胞术 单细胞分析 细胞生物学 受体 外围设备 免疫学 遗传学 基因 医学 表型 内科学
作者
Yufei Wang,Ronghong Li,Renyang Tong,Taiwei Chen,Mingze Sun,Lingjie Luo,Zheng Li,Yifan Chen,Yichao Zhao,Chensheng Zhang,Wei Lin,Wei Lin,Haoyan Chen,Kun Qian,Alex F. Chen,Junling Liu,Lei Chen,Bin Li,Feng Wang,Li Wang
出处
期刊:Nature Immunology [Nature Portfolio]
卷期号:26 (2): 308-322 被引量:84
标识
DOI:10.1038/s41590-024-02059-6
摘要

A comprehensive understanding of the evolution of the immune landscape in humans across the entire lifespan at single-cell transcriptional and protein levels, during development, maturation and senescence is currently lacking. We recruited a total of 220 healthy volunteers from the Shanghai Pudong Cohort (NCT05206643), spanning 13 age groups from 0 to over 90 years, and profiled their peripheral immune cells through single-cell RNA-sequencing coupled with single T cell and B cell receptor sequencing, high-throughput mass cytometry, bulk RNA-sequencing and flow cytometry validation experiments. We revealed that T cells were the most strongly affected by age and experienced the most intensive rewiring in cell–cell interactions during specific age. Different T cell subsets displayed different aging patterns in both transcriptomes and immune repertoires; examples included GNLY+CD8+ effector memory T cells, which exhibited the highest clonal expansion among all T cell subsets and displayed distinct functional signatures in children and the elderly; and CD8+ MAIT cells, which reached their peaks of relative abundance, clonal diversity and antibacterial capability in adolescents and then gradually tapered off. Interestingly, we identified and experimentally verified a previously unrecognized ‘cytotoxic’ B cell subset that was enriched in children. Finally, an immune age prediction model was developed based on lifecycle-wide single-cell data that can evaluate the immune status of healthy individuals and identify those with disturbed immune functions. Our work provides both valuable insights and resources for further understanding the aging of the immune system across the whole human lifespan. In this Resource, authors profile peripheral immune cells from a total of 220 healthy volunteers from birth to over 90 years. This revealed that T cells were most affected by aging with divergent aging patterns in different subsets and identified a population of cytotoxic B cells that were enriched in children.
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