Frontiers in Immunology (Sep 2022)

Transcriptional programming of immunoregulatory responses in human Langerhans cells

  • James Davies,
  • Sofia Sirvent,
  • Andres F. Vallejo,
  • Kalum Clayton,
  • Gemma Douilhet,
  • Patrick S. Keeler,
  • Jonathan West,
  • Jonathan West,
  • Michael Ardern-Jones,
  • Ben D. MacArthur,
  • Harinder Singh,
  • Marta E. Polak,
  • Marta E. Polak

DOI
https://doi.org/10.3389/fimmu.2022.892254
Journal volume & issue
Vol. 13

Abstract

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Human epidermal Langerhans cells (LCs) maintain immune homeostasis in the skin. To examine transcriptional programming of human primary LCs during homeostasis, we performed scRNA-seq analysis of LCs before and after migration from the epidermis, coupled with functional assessment of their regulatory T cell priming capabilities. The analysis revealed that steady-state LCs exist in a continuum of maturation states and upregulate antigen presentation genes along with an immunoregulatory module including the genes IDO1, LGALS1, LAMTOR1, IL4I, upon their migration. The migration-induced transition in genomic state is accompanied by the ability of LCs to more efficiently prime regulatory T cell responses in co-culture assays. Computational analyses of the scRNAseq datasets using SCENIC and Partial Information Decomposition in Context identified a set of migration-induced transcription factors including IRF4, KLF6 and RelB as key nodes within a immunoregulatory gene regulatory network. These findings support a model in which efficient priming of immunoregulatory responses by LCs is dependent on coordinated upregulation of a migration-coupled maturation program with a immunoregulation-promoting genomic module.

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