Protein & Cell (Aug 2020)

A human circulating immune cell landscape in aging and COVID-19

  • Yingfeng Zheng,
  • Xiuxing Liu,
  • Wenqing Le,
  • Lihui Xie,
  • He Li,
  • Wen Wen,
  • Si Wang,
  • Shuai Ma,
  • Zhaohao Huang,
  • Jinguo Ye,
  • Wen Shi,
  • Yanxia Ye,
  • Zunpeng Liu,
  • Moshi Song,
  • Weiqi Zhang,
  • Jing-Dong J. Han,
  • Juan Carlos Izpisua Belmonte,
  • Chuanle Xiao,
  • Jing Qu,
  • Hongyang Wang,
  • Guang-Hui Liu,
  • Wenru Su

DOI
https://doi.org/10.1007/s13238-020-00762-2
Journal volume & issue
Vol. 11, no. 10
pp. 740 – 770

Abstract

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Abstract Age-associated changes in immune cells have been linked to an increased risk for infection. However, a global and detailed characterization of the changes that human circulating immune cells undergo with age is lacking. Here, we combined scRNA-seq, mass cytometry and scATAC-seq to compare immune cell types in peripheral blood collected from young and old subjects and patients with COVID-19. We found that the immune cell landscape was reprogrammed with age and was characterized by T cell polarization from naive and memory cells to effector, cytotoxic, exhausted and regulatory cells, along with increased late natural killer cells, age-associated B cells, inflammatory monocytes and age-associated dendritic cells. In addition, the expression of genes, which were implicated in coronavirus susceptibility, was upregulated in a cell subtype-specific manner with age. Notably, COVID-19 promoted age-induced immune cell polarization and gene expression related to inflammation and cellular senescence. Therefore, these findings suggest that a dysregulated immune system and increased gene expression associated with SARS-CoV-2 susceptibility may at least partially account for COVID-19 vulnerability in the elderly.

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