Single cell transcriptomics of regulatory T cells reveals trajectories of tissue adaptation

Author:

Miragaia Ricardo JORCID,Gomes TomásORCID,Chomka Agnieszka,Jardine Laura,Riedel Angela,Hegazy Ahmed N.,Lindeman Ida,Emerton Guy,Krausgruber Thomas,Shields Jacqueline,Haniffa Muzlifah,Powrie Fiona,Teichmann Sarah A.ORCID

Abstract

SummaryNon-lymphoid tissues (NLTs) harbour a pool of adaptive immune cells, the development and phenotype of which remains largely unexplored. Here, we used single-cell RNA-seq to characterise CD4+ regulatory (Treg) and memory (Tmem) T cells in mouse skin and colon, the respective draining lymph nodes and spleen. From this data, we modelled a continuous lymphoid-to-NLT trajectory for Treg, and reconstructed the mechanisms of cell migration and NLT adaption. This revealed a shared transcriptional programme of NLT priming in both skin and colon-associated lymph nodes, followed by tissue-specific adaptation. Predicted migration kinetics were validated using a melanoma-induction model, emphasizing the relevance of key regulators and receptors, including Batf, Rora, Ccr8, Samsn1. Finally, we profiled human blood and NLT Treg and Tmem cells, identifying cross-mammalian conserved tissue signatures. In summary, we have identified molecular signals mediating NLT Treg recruitment and tissue adaptation through the combined use of computational prediction and in vivo validation.

Publisher

Cold Spring Harbor Laboratory

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