Maturing human CD127+ CCR7+ PDL1+ dendritic cells express AIRE in the absence of tissue restricted antigens

Joannah R. Fergusson; Michael D. Morgan; Melanie Bruchard; Leonie Huitema; Balthasar A. Heesters; Vincent van Unen; Jan Piet van Hamburg; Nicole N. van der Wel; Daisy Picavet; Frits Koning; Sander W. Tas; Mark S. Anderson; John C. Marioni; Georg A. Holländer; Hergen Spits

doi:10.3389/fimmu.2018.02902

Maturing human CD127+ CCR7+ PDL1+ dendritic cells express AIRE in the absence of tissue restricted antigens

Joannah R. Fergusson^* (Corresponding Author), Michael D. Morgan, Melanie Bruchard, Leonie Huitema, Balthasar A. Heesters, Vincent van Unen, Jan Piet van Hamburg, Nicole N. van der Wel, Daisy Picavet, Frits Koning, Sander W. Tas, Mark S. Anderson, John C. Marioni, Georg A. Holländer, Hergen Spits

^*Corresponding author for this work

Medical Sciences

Research output: Contribution to journal › Article › peer-review

33 Citations (Scopus)

Abstract

Expression of the Autoimmune regulator (AIRE) outside of the thymus has long been suggested in both humans and mice, but the cellular source in humans has remained undefined. Here we identify AIRE expression in human tonsils and extensively analyzed these “extrathymic AIRE expressing cells” (eTACs) using combinations of flow cytometry, CyTOF and single cell RNA-sequencing. We identified AIRE+ cells as dendritic cells (DCs) with a mature and migratory phenotype including high levels of antigen presenting molecules and costimulatory molecules, and specific expression of CD127, CCR7, and PDL1. These cells also possessed the ability to stimulate and re-stimulate T cells and displayed reduced responses to toll-like receptor (TLR) agonists compared to conventional DCs. While expression of AIRE was enriched within CCR7+CD127+ DCs, single-cell RNA sequencing revealed expression of AIRE to be transient, rather than stable, and associated with the differentiation to a mature phenotype. The role of AIRE in central tolerance induction within the thymus is well-established, however our study shows that AIRE expression within the periphery is not associated with an enriched expression of tissue-restricted antigens (TRAs). This unexpected finding, suggestive of wider functions of AIRE, may provide an explanation for the non-autoimmune symptoms of APECED patients who lack functional AIRE.

Original language	English
Article number	2902
Number of pages	17
Journal	Frontiers in Immunology
Volume	10
Issue number	JAN
DOIs	https://doi.org/10.3389/fimmu.2018.02902
Publication status	Published - 14 Jan 2019

Bibliographical note

Funding Information:
JF and HS were funded by project ERC-2013-ADG number 341038. MB was funded by EMBO ALTF 786-2013. BH was supported by the Netherlands Organization for Scientific Research (NWO) Veni program (91618032). LH, JpvH, and ST were supported by a grant from the Dutch Arthritis Foundation (2013_2_37). MM was supported by Wellcome Trust (grant105045/Z/14/Z). JM was supported by core funding from the European Molecular Biology Laboratory and from Cancer Research UK (award number 17197).

Publisher Copyright:
© 2007 - 2019 Frontiers Media S.A. All Rights Reserved.

Data Availability Statement

CODE AVAILABILITY
All code used to analyse bulk and single-cell RNA-sequencing
data, and used to generate figure panels are available at https://
github.com/MikeDMorgan/Human_eTAC2018.
DATA AVAILABILITY
Single cell gene expression data are available through
ArrayExpress under accession E-MTAB-7381, and bulk
RNA-sequencing gene expression data are available through
accession E-MTAB-7383.

Keywords

AIRE
Dendritic cells
Maturation
PDL1
Tissue restricted antigen

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10.3389/fimmu.2018.02902

Cite this

Fergusson, J. R., Morgan, M. D., Bruchard, M., Huitema, L., Heesters, B. A., van Unen, V., van Hamburg, J. P., van der Wel, N. N., Picavet, D., Koning, F., Tas, S. W., Anderson, M. S., Marioni, J. C., Holländer, G. A., & Spits, H. (2019). Maturing human CD127+ CCR7+ PDL1+ dendritic cells express AIRE in the absence of tissue restricted antigens. Frontiers in Immunology, 10(JAN), Article 2902. https://doi.org/10.3389/fimmu.2018.02902

Fergusson, JR, Morgan, MD, Bruchard, M, Huitema, L, Heesters, BA, van Unen, V, van Hamburg, JP, van der Wel, NN, Picavet, D, Koning, F, Tas, SW, Anderson, MS, Marioni, JC, Holländer, GA & Spits, H 2019, 'Maturing human CD127+ CCR7+ PDL1+ dendritic cells express AIRE in the absence of tissue restricted antigens', Frontiers in Immunology, vol. 10, no. JAN, 2902. https://doi.org/10.3389/fimmu.2018.02902

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title = "Maturing human CD127+ CCR7+ PDL1+ dendritic cells express AIRE in the absence of tissue restricted antigens",

abstract = "Expression of the Autoimmune regulator (AIRE) outside of the thymus has long been suggested in both humans and mice, but the cellular source in humans has remained undefined. Here we identify AIRE expression in human tonsils and extensively analyzed these “extrathymic AIRE expressing cells” (eTACs) using combinations of flow cytometry, CyTOF and single cell RNA-sequencing. We identified AIRE+ cells as dendritic cells (DCs) with a mature and migratory phenotype including high levels of antigen presenting molecules and costimulatory molecules, and specific expression of CD127, CCR7, and PDL1. These cells also possessed the ability to stimulate and re-stimulate T cells and displayed reduced responses to toll-like receptor (TLR) agonists compared to conventional DCs. While expression of AIRE was enriched within CCR7+CD127+ DCs, single-cell RNA sequencing revealed expression of AIRE to be transient, rather than stable, and associated with the differentiation to a mature phenotype. The role of AIRE in central tolerance induction within the thymus is well-established, however our study shows that AIRE expression within the periphery is not associated with an enriched expression of tissue-restricted antigens (TRAs). This unexpected finding, suggestive of wider functions of AIRE, may provide an explanation for the non-autoimmune symptoms of APECED patients who lack functional AIRE.",

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author = "Fergusson, {Joannah R.} and Morgan, {Michael D.} and Melanie Bruchard and Leonie Huitema and Heesters, {Balthasar A.} and {van Unen}, Vincent and {van Hamburg}, {Jan Piet} and {van der Wel}, {Nicole N.} and Daisy Picavet and Frits Koning and Tas, {Sander W.} and Anderson, {Mark S.} and Marioni, {John C.} and Holl{\"a}nder, {Georg A.} and Hergen Spits",

note = "Funding Information: JF and HS were funded by project ERC-2013-ADG number 341038. MB was funded by EMBO ALTF 786-2013. BH was supported by the Netherlands Organization for Scientific Research (NWO) Veni program (91618032). LH, JpvH, and ST were supported by a grant from the Dutch Arthritis Foundation (2013_2_37). MM was supported by Wellcome Trust (grant105045/Z/14/Z). JM was supported by core funding from the European Molecular Biology Laboratory and from Cancer Research UK (award number 17197). Publisher Copyright: {\textcopyright} 2007 - 2019 Frontiers Media S.A. All Rights Reserved.",

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AU - Fergusson, Joannah R.

AU - Morgan, Michael D.

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AU - Huitema, Leonie

AU - Heesters, Balthasar A.

AU - van Unen, Vincent

AU - van Hamburg, Jan Piet

AU - van der Wel, Nicole N.

AU - Picavet, Daisy

AU - Koning, Frits

AU - Tas, Sander W.

AU - Anderson, Mark S.

AU - Marioni, John C.

AU - Holländer, Georg A.

AU - Spits, Hergen

N1 - Funding Information: JF and HS were funded by project ERC-2013-ADG number 341038. MB was funded by EMBO ALTF 786-2013. BH was supported by the Netherlands Organization for Scientific Research (NWO) Veni program (91618032). LH, JpvH, and ST were supported by a grant from the Dutch Arthritis Foundation (2013_2_37). MM was supported by Wellcome Trust (grant105045/Z/14/Z). JM was supported by core funding from the European Molecular Biology Laboratory and from Cancer Research UK (award number 17197). Publisher Copyright: © 2007 - 2019 Frontiers Media S.A. All Rights Reserved.

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N2 - Expression of the Autoimmune regulator (AIRE) outside of the thymus has long been suggested in both humans and mice, but the cellular source in humans has remained undefined. Here we identify AIRE expression in human tonsils and extensively analyzed these “extrathymic AIRE expressing cells” (eTACs) using combinations of flow cytometry, CyTOF and single cell RNA-sequencing. We identified AIRE+ cells as dendritic cells (DCs) with a mature and migratory phenotype including high levels of antigen presenting molecules and costimulatory molecules, and specific expression of CD127, CCR7, and PDL1. These cells also possessed the ability to stimulate and re-stimulate T cells and displayed reduced responses to toll-like receptor (TLR) agonists compared to conventional DCs. While expression of AIRE was enriched within CCR7+CD127+ DCs, single-cell RNA sequencing revealed expression of AIRE to be transient, rather than stable, and associated with the differentiation to a mature phenotype. The role of AIRE in central tolerance induction within the thymus is well-established, however our study shows that AIRE expression within the periphery is not associated with an enriched expression of tissue-restricted antigens (TRAs). This unexpected finding, suggestive of wider functions of AIRE, may provide an explanation for the non-autoimmune symptoms of APECED patients who lack functional AIRE.

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Maturing human CD127+ CCR7+ PDL1+ dendritic cells express AIRE in the absence of tissue restricted antigens

Abstract

Bibliographical note

Data Availability Statement

Keywords

Access to Document

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