A wave of Foxp3+ regulatory T cell accumulation in the neonatal liver plays unique roles in maintaining self-tolerance

  • Mingyang Li
  • , Weijia Zhao
  • , Yifan Wang
  • , Lixue Jin
  • , Gaowen Jin
  • , Xiuyuan Sun
  • , Wei Wang
  • , Ke Wang
  • , Xi Xu
  • , Jie Hao
  • , Rong Jin
  • , Wenxian Fu
  • , Ying Sun
  • , Yingjun Chang
  • , Xiaojun Huang
  • , Xuyu Zhou
  • , Hounan Wu
  • , Kunshan Zhang
  • , Qing Ge

Research output: Contribution to journalArticlepeer-review

31 Scopus citations

Abstract

Newborn animals require tightly regulated local and systemic immune environments to govern the development and maturation of multiple organs/tissues even though the immune system itself is far from mature during the neonatal period. Regulatory T cells (Tregs) are essential for maintaining immune tolerance/homeostasis and modulating inflammatory responses. The features of Tregs in the neonatal liver under steady-state conditions are not well understood. The present study aimed to investigate the phenotype, functions, and significance of neonatal Tregs in the liver. We found a wave of thymus-derived Treg influx into the liver during 1–2 weeks of age. Depletion of these Tregs between days 7 and 11 after birth rapidly resulted in Th1-type liver inflammation and metabolic disorder. More Tregs in the neonatal liver than in the spleen underwent MHC II-dependent activation and proliferation, and the liver Tregs acquired stronger suppressive functions. The transcriptomic profile of these neonatal liver Tregs showed elevated expression of PPARγ and T-bet and features of Tregs that utilize lipid metabolic machinery and are capable of regulating Th1 responses. The accumulation of Tregs with unique features in the neonatal liver is critical to ensure self-tolerance and liver maturation.

Original languageEnglish
Pages (from-to)507-518
Number of pages12
JournalCellular and Molecular Immunology
Volume17
Issue number5
DOIs
StatePublished - 1 May 2020
Externally publishedYes

Keywords

  • Foxp3
  • Neonatal period
  • Th1-type inflammation
  • Treg cells
  • liver

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