Single-Cell Transcriptomics Identifies the Adaptation of Scart1+ Vγ6+ T Cells to Skin Residency as Activated Effector Cells

Tan, Likai; Sandrock, Inga; Odak, Ivan; Aizenbud, Yuval; Wilharm, Anneke; Barros‐Martins, Joana; Tabib, Yaara; Borchers, Alina; Amado, Tiago; Gangoda, Lahiru; Herold, Marco J.; Schmidt-Supprian, Marc; Kisielow, Jan; Silva‐Santos, Bruno; Koenecke, Christian; Hovav, Avi‐Hai; Krebs, Christian; Prinz, Immo; Ravens, Sarina

doi:10.1016/j.celrep.2019.05.064

Cited by 84 publications

(105 citation statements)

References 93 publications

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“…In mouse skin, a self-renewing population of dermal γδ T cells was identified as the major source of IL-17 in steady state (Gray et al, 2011;Sumaria et al, 2011). These IL-17-producing γδ T cells (γδ17 cells) in the dermis are chronically activated by local signals and fairly tissue-resident (Laidlaw et al, 2019;Tan et al, 2019). In human skin, the contribution of γδ17 cells and other innate lymphocytes to steady state IL-17 production is currently less clear (Brüggen et al, 2016).…”

Section: Il-17 Immunitymentioning

confidence: 99%

Interleukin-17 cytokines: Effectors and targets in psoriasis—A breakthrough in understanding and treatment

Prinz

Sandrock

Mrowietz³

2019

Journal of Experimental Medicine

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The IL-17 cytokine family comprising IL-17A to IL-17F and receptor subunits IL-17RA to IL-17RE represents a genetically ancient intercellular network regulating local tissue homeostasis. Its pivotal role in antifungal defense and its central position in the pathogenesis of inflammatory diseases including psoriasis were discovered only relatively late in the early 2000s. Since the connection of dysregulated IL-17 and psoriasis pathogenesis turned out to be particularly evident, a number of monoclonal antibodies targeting IL-17 pathways have been approved and are used as first line treatment of moderate-to-severe plaque psoriasis and psoriatic arthritis, and further agents are currently in clinical development.

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Section: Il-17 Immunitymentioning

confidence: 99%

Interleukin-17 cytokines: Effectors and targets in psoriasis—A breakthrough in understanding and treatment

Prinz

Sandrock

Mrowietz³

2019

Journal of Experimental Medicine

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“…GM_A included genes such as LEF1 and TCF7 that are key regulators of naïve T cells 22,23 as well as known regulatory TFs of murine immature γδ T cells (e.g. SOX4) 13,24 (Fig. 2a).…”

Section: Scrna-seq Reveals High Heterogeneity Among Human γδ T Cellsmentioning

confidence: 99%

“…The module GM_G indicated acute T cell activation in c2 and c7. Of note, the type-3 immunity gene module GM_D, characterized by gene signatures connected to interleukin-17 (IL-17) producing T cells 13,[26][27][28] , was exclusively enriched within c8, which contained neonatal as well as adult γδ T cells ( Fig. 2 and Supplementary Fig.…”

Section: Scrna-seq Reveals High Heterogeneity Among Human γδ T Cellsmentioning

confidence: 99%

“…In mice, distinct waves of effector γδ T cells with restricted TCR diversity develop sequentially in the fetal thymus 11 . In particular, IL-17-producing effector γδ T (γδT17) cells are exclusively generated before birth and persist throughout the entire life as self-renewing, tissue-resident T cells in a diverse range of tissues 12,13 . There are parallels in humans, as Vγ9Vδ2 + T cells with restricted TCR diversity are preferentially generated before birth, expand postnatally and persist into adulthood [14][15][16][17] .…”

Section: Introductionmentioning

confidence: 99%

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A fetal wave of human type-3 γδ T cells with restricted TCR diversity persists into adulthood

Tan

Fichtner

Bubke

et al. 2020

Preprint

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Accumulating evidence suggests that the human embryonic thymus produces distinct waves of innate effector γδ T cells. However, it is unclear whether this process comprises a dedicated subset of IL-17-producing γδ T (γδT17) cells, like reported in mice. Here we present a novel protocol for high-throughput paired γδ TCR-sequencing, which in combination with single-cell RNA-sequencing revealed a high heterogeneity of effector γδ T cell clusters. While immature γδ T cell clusters displayed mixed and diverse TCR, effector cell types in neonatal and adult blood segregated according to γδTCR usage. In adult samples, mature Vδ1+ T cells segregated into exhausted PD-1hi and active PD-1low clusters. Among Vγ9Vδ2+ T cell subsets, we identified distinct PLZF-positive effector γδ T cell clusters with innate type-1 and type-3 T cell signatures that were already detectable in a public dataset of early embryonic thymus organogenesis. Together, this suggests that functionally distinct waves of human innate effector γδ T cells including CCR6+ γδT17 cells develop in the early fetal thymus and persist into adulthood.

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“…to as type 3 (or type 17) immune cells, producing the prototypical cytokines IL-17 and IL-22 and including Th17 CD4 + T cells, gdT17 cells, group 3 innate lymphoid cells (ILC3s) and NKT17 cells 6,[11][12][13][14] . Moreover, the Littman group included Tmem176a/b in the restricted group of 11 genes whose expression is directly dependent on RORγt in Th17 cells 15 .…”

Section: /36mentioning

confidence: 99%

Dendritic cells require TMEM176A/B ion channels for optimal MHC II antigen presentation to naive CD4⁺ T cells

Lancien

Bienvenu

Gueno

et al. 2019

Preprint

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Intracellular ion fluxes emerge as critical actors of immunoregulation but still remain poorly explored. Here we investigated the role of the redundant cation channels TMEM176A and TMEM176B (TMEM176A/B) in RORgt + cells and conventional dendritic cells (cDCs) using germline and conditional double knock-out (DKO) mice. While Tmem176a/b appeared surprisingly dispensable for the protective function of Th17 and group 3 innate lymphoid cells (ILC3s) in the intestinal mucosa, we found that they were required in cDCs for optimal antigen processing and presentation to CD4 + T cells. Using a real-time imaging method, we show that TMEM176A/B accumulate in dynamic post-Golgi vesicles preferentially linked to the late endolysosomal system and strongly colocalize with HLA-DM. Together, our results suggest that TMEM176A/B ion channels play a direct role in the MHC II compartment (MIIC) of DCs for the fine regulation of antigen presentation and naive CD4 + T cell priming.Lancien et al. 3/36

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Single-Cell Transcriptomics Identifies the Adaptation of Scart1+ Vγ6+ T Cells to Skin Residency as Activated Effector Cells

Cited by 84 publications

References 93 publications

Interleukin-17 cytokines: Effectors and targets in psoriasis—A breakthrough in understanding and treatment

Interleukin-17 cytokines: Effectors and targets in psoriasis—A breakthrough in understanding and treatment

A fetal wave of human type-3 γδ T cells with restricted TCR diversity persists into adulthood

Dendritic cells require TMEM176A/B ion channels for optimal MHC II antigen presentation to naive CD4⁺ T cells

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Single-Cell Transcriptomics Identifies the Adaptation of Scart1+ Vγ6+ T Cells to Skin Residency as Activated Effector Cells

Cited by 84 publications

References 93 publications

Interleukin-17 cytokines: Effectors and targets in psoriasis—A breakthrough in understanding and treatment

Interleukin-17 cytokines: Effectors and targets in psoriasis—A breakthrough in understanding and treatment

A fetal wave of human type-3 γδ T cells with restricted TCR diversity persists into adulthood

Dendritic cells require TMEM176A/B ion channels for optimal MHC II antigen presentation to naive CD4+ T cells

Contact Info

Product

Resources

About

Dendritic cells require TMEM176A/B ion channels for optimal MHC II antigen presentation to naive CD4⁺ T cells