Abstract
The impact of the microenvironment on innate lymphoid cell (ILC)-mediated immunity in humans remains largely unknown. Here we used full-length Smart-seq2 single-cell RNA-sequencing to unravel tissue-specific transcriptional profiles and heterogeneity of CD127+ ILCs across four human tissues. Correlation analysis identified gene modules characterizing the migratory properties of tonsil and blood ILCs, and signatures of tissue-residency, activation and modified metabolism in colon and lung ILCs. Trajectory analysis revealed potential differentiation pathways from circulating and tissue-resident naïve ILCs to a spectrum of mature ILC subsets. In the lung we identified both CRTH2+ and CRTH2- ILC2 with lung-specific signatures, which could be recapitulated by alarmin-exposure of circulating ILC2. Finally, we describe unique TCR-V(D)J-rearrangement patterns of blood ILC1-like cells, revealing a subset of potentially immature ILCs with TCR-δ rearrangement. Our study provides a useful resource for in-depth understanding of ILC-mediated immunity in humans, with implications for disease.
Original language | English |
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Pages (from-to) | 554–568 |
Number of pages | 15 |
Journal | Cell Research |
Volume | 31 |
Issue number | 5 |
Early online date | 2021 Jan 8 |
DOIs | |
Publication status | Published - 2021 May 1 |
Subject classification (UKÄ)
- Bioinformatics and Computational Biology
- Immunology
- Immunology in the Medical Area (including Cell and Immunotherapy)
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National Bioinformatics Infrastructure Sweden
Ahrén, D. (Manager), Ringnér, M. (Manager), Levander, F. (Manager), Manoharan, L. (Manager), Oskolkov, N. (Manager), Vasquez, L. J. A. (Manager), Pyl, P. T. (Manager), Agarwal, P. (Manager), Li, Y. (Manager), Volpe, M. (Manager) & Kozjek, K. (Manager)
Department of BiologyInfrastructure