Neonatal liver niches program T cell tolerance

  1. Eva-Lena Stange
  2. Trong-Hieu Nguyen
  3. Dustyn Mendoza
  4. Aiara Lobo Gomes
  5. Marlene Sophia Kohlhepp
  6. Jonas Pes
  7. Shahed Al Bounny
  8. Julian Brueck
  9. Yunus Cetiner
  10. Urs Moerbe
  11. Milas Ugur
  12. Cristina Kalbermatter
  13. Jarrett Lopez-Scarim
  14. Aline Dupont
  15. Susan A. V. Jennings
  16. Julia Heckmann
  17. Aaron Silva-Sanchez
  18. Solveig Runge
  19. Christoph Kuppe
  20. Oliver Pabst
  21. Thomas Clavel
  22. Dorothee Viemann
  23. Stephan P. Rosshart
  24. Vuk Cerovic
  25. Stephanie C. Ganal-Vonarburg
  26. Adrien Guillot
  27. Eva Billerbeck
  28. Mathias W. Hornef
  29. Natalia Torow
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Abstract

After birth, the immune system must learn to tolerate a rapidly changing milieu of commensals and self while remaining ready for pathogens. Here we characterize the neonatal liver as a central hub in this process: In postnatal week 1–2, the liver hosts a developmentally encoded, microbiota-independent expansion of regulatory T cells (Tregs) that coexists with microbiota-tuned conventional wave of activated CD4⁺ T cells (Tconvs). Mechanistically, the Treg expansion is governed by MHCII-mediated antigen presentation by CCR7+ cDC1s, which establish tolerogenic DC:T cell clusters in the liver parenchyma, allowing for local expansion and control via PD-L1 checkpoints that selectively increase Tregs without unleashing Tconvs. Importantly, this transient, neonatal program predisposes hepatotropic viral infections to progress toward chronic disease but also protects the adult liver from steatotic disease. These data position the neonatal liver as a unique site of early life T-cell education with timing-sensitive implications for early-life interventions.

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