Single-cell analysis of signalling and transcriptional responses to type I interferons

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Abstract

Type I interferons (IFNs) play crucial roles in antiviral defence, autoinflammation and cancer immunity. The human genome encodes 17 different type I IFNs that all signal through the same receptor. Non-redundant functions have been reported for some type I IFNs. However, whether different type I IFNs induce different responses remains largely unknown. We stimulated human peripheral blood mononuclear cells (PBMCs) with recombinant type I IFNs to address this question in multiple types of primary cells. We analysed signalling responses by mass cytometry and changes in gene expression by bulk and single-cell RNA sequencing. We found cell-type specific changes in the phosphorylation of STAT transcription factors and in the gene sets induced and repressed upon type I IFN exposure. We further report that the magnitude of these responses varied between different type I IFNs, whilst qualitatively different responses to type I IFN subtypes were not apparent. Taken together, we provide a rich resource mapping signalling responses and IFN-regulated genes in immune cells.

Highlights

  • Mass cytometry and scRNAseq analysis of human PBMCs stimulated with type I IFNs

  • Cell type-specific phosphorylation of STAT proteins and induction of ISGs

  • Different type I IFNs induce qualitatively similar responses that vary in magnitude

  • Identification of ten core ISGs, up-regulated by all cell types in response to all type I IFNs

In brief

Rigbyet al.provide a single-cell map of signalling and transcriptomic responses to type I IFNs inex vivostimulated human PBMCs. Different cell types responded in unique ways but differences between different type I IFNs were only quantitative. These rich datasets are available via an easy-to-use interactive interface (<ext-link xmlns:xlink="http://www.w3.org/1999/xlink" ext-link-type="uri" xlink:href="https://rehwinkellab.shinyapps.io/ifnresource/">https://rehwinkellab.shinyapps.io/ifnresource/</ext-link>).

Graphical abstract

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