IL-6 dysregulation originates in dendritic cells and mediates graft-versus-host disease via classical signaling

Andrew N. Wilkinson; Karshing Chang; Rachel D. Kuns; Andrea S. Henden; Simone A. Minnie; Kathleen S. Ensbey; Andrew D. Clouston; Ping Zhang; Motoko Koyama; Juan Hidalgo; Stefan Rose-John; Antiopi Varelias; Slavica Vuckovic; Kate H. Gartlan; Geoffrey R. Hill

doi:10.1182/blood.2019000396

IL-6 dysregulation originates in dendritic cells and mediates graft-versus-host disease via classical signaling

Andrew N. Wilkinson, Karshing Chang, Rachel D. Kuns, Andrea S. Henden, Simone A. Minnie, Kathleen S. Ensbey, Andrew D. Clouston, Ping Zhang, Motoko Koyama, Juan Hidalgo, Stefan Rose-John, Antiopi Varelias, Slavica Vuckovic, Kate H. Gartlan, Geoffrey R. Hill^*

^*Autor corresponent d’aquest treball

Producció científica: Contribució a revista › Article › Recerca › Avaluat per experts

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Graft-versus-host disease (GVHD) after allogeneic stem cell transplantation (alloSCT) is characterized by interleukin-6 (IL-6) dysregulation. IL-6 can mediate effects via various pathways, including classical, trans, and cluster signaling. Given the recent availability of agents that differentially inhibit these discrete signaling cascades, understanding the source and signaling and cellular targets of this cytokine is paramount to inform the design of clinical studies. Here we demonstrate that IL-6 secretion from recipient dendritic cells (DCs) initiates the systemic dysregulation of this cytokine. Inhibition of DC-driven classical signaling after targeted IL-6 receptor (IL-6R) deletion in T cells eliminated pathogenic donor Th17/Th22 cell differentiation and resulted in long-term survival. After engraftment, donor DCs assume the same role, maintaining classical IL-6 signaling–dependent GVHD responses. Surprisingly, cluster signaling was not active after transplantation, whereas inhibition of trans signaling with soluble gp130Fc promoted severe, chronic cutaneous GVHD. The latter was a result of exaggerated polyfunctional Th22-cell expansion that was reversed by IL-22 deletion or IL-6R inhibition. Importantly, inhibition of IL-6 classical signaling did not impair the graft-versus-leukemia effect. Together, these data highlight IL-6 classical signaling and downstream Th17/Th22 differentiation as important therapeutic targets after alloSCT.

Idioma original	Anglès nord-americà
Pàgines (de-a)	2092-2106
Nombre de pàgines	15
Revista	Blood
Volum	134
Número	23
DOIs	https://doi.org/10.1182/blood.2019000396
Estat de la publicació	Publicada - 5 de des. 2019

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10.1182/blood.2019000396

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Wilkinson, A. N., Chang, K., Kuns, R. D., Henden, A. S., Minnie, S. A., Ensbey, K. S., Clouston, A. D., Zhang, P., Koyama, M., Hidalgo, J., Rose-John, S., Varelias, A., Vuckovic, S., Gartlan, K. H., & Hill, G. R. (2019). IL-6 dysregulation originates in dendritic cells and mediates graft-versus-host disease via classical signaling. Blood, 134(23), 2092-2106. https://doi.org/10.1182/blood.2019000396

@article{b81523b383de4f12abb01ad2f9ca3fec,

title = "IL-6 dysregulation originates in dendritic cells and mediates graft-versus-host disease via classical signaling",

abstract = "Graft-versus-host disease (GVHD) after allogeneic stem cell transplantation (alloSCT) is characterized by interleukin-6 (IL-6) dysregulation. IL-6 can mediate effects via various pathways, including classical, trans, and cluster signaling. Given the recent availability of agents that differentially inhibit these discrete signaling cascades, understanding the source and signaling and cellular targets of this cytokine is paramount to inform the design of clinical studies. Here we demonstrate that IL-6 secretion from recipient dendritic cells (DCs) initiates the systemic dysregulation of this cytokine. Inhibition of DC-driven classical signaling after targeted IL-6 receptor (IL-6R) deletion in T cells eliminated pathogenic donor Th17/Th22 cell differentiation and resulted in long-term survival. After engraftment, donor DCs assume the same role, maintaining classical IL-6 signaling–dependent GVHD responses. Surprisingly, cluster signaling was not active after transplantation, whereas inhibition of trans signaling with soluble gp130Fc promoted severe, chronic cutaneous GVHD. The latter was a result of exaggerated polyfunctional Th22-cell expansion that was reversed by IL-22 deletion or IL-6R inhibition. Importantly, inhibition of IL-6 classical signaling did not impair the graft-versus-leukemia effect. Together, these data highlight IL-6 classical signaling and downstream Th17/Th22 differentiation as important therapeutic targets after alloSCT.",

author = "Wilkinson, {Andrew N.} and Karshing Chang and Kuns, {Rachel D.} and Henden, {Andrea S.} and Minnie, {Simone A.} and Ensbey, {Kathleen S.} and Clouston, {Andrew D.} and Ping Zhang and Motoko Koyama and Juan Hidalgo and Stefan Rose-John and Antiopi Varelias and Slavica Vuckovic and Gartlan, {Kate H.} and Hill, {Geoffrey R.}",

note = "Funding Information: The authors acknowledge the assistance of the QIMR Berghofer Flow Cytometry & Imaging Facility, Paula Hall, Michael Rist, and Grace Chojnowski as well as illustrations by Madeleine Flynn. The visual abstract is a modification of an illustration from Hill and Ferrara.72 This work was supported by research grants from the National Health and Medical Research Council and the Ministry of Economy and Competitiveness and European Regional Development Fund SAF2014-56546-R and RTI2018-101105-B-I00. G.R.H. is an Andy Hill CARE Distinguished Researcher. The work of S.R.-J. was funded by grants from the Deutsche Forschungsgemeinschaft (Bonn, Germany; SFB877 project A1) and by the Cluster of Excellence Inflammation at Interfaces. Publisher Copyright: {\textcopyright} 2019 by The American Society of Hematology Copyright: Copyright 2019 Elsevier B.V., All rights reserved.",

year = "2019",

month = dec,

day = "5",

doi = "10.1182/blood.2019000396",

language = "Ingl{\'e}s estadounidense",

volume = "134",

pages = "2092--2106",

journal = "Blood",

issn = "0006-4971",

number = "23",

}

Wilkinson, AN, Chang, K, Kuns, RD, Henden, AS, Minnie, SA, Ensbey, KS, Clouston, AD, Zhang, P, Koyama, M, Hidalgo, J, Rose-John, S, Varelias, A, Vuckovic, S, Gartlan, KH & Hill, GR 2019, 'IL-6 dysregulation originates in dendritic cells and mediates graft-versus-host disease via classical signaling', Blood, vol. 134, núm. 23, pàg. 2092-2106. https://doi.org/10.1182/blood.2019000396

TY - JOUR

T1 - IL-6 dysregulation originates in dendritic cells and mediates graft-versus-host disease via classical signaling

AU - Wilkinson, Andrew N.

AU - Chang, Karshing

AU - Kuns, Rachel D.

AU - Henden, Andrea S.

AU - Minnie, Simone A.

AU - Ensbey, Kathleen S.

AU - Clouston, Andrew D.

AU - Zhang, Ping

AU - Koyama, Motoko

AU - Hidalgo, Juan

AU - Rose-John, Stefan

AU - Varelias, Antiopi

AU - Vuckovic, Slavica

AU - Gartlan, Kate H.

AU - Hill, Geoffrey R.

N1 - Funding Information: The authors acknowledge the assistance of the QIMR Berghofer Flow Cytometry & Imaging Facility, Paula Hall, Michael Rist, and Grace Chojnowski as well as illustrations by Madeleine Flynn. The visual abstract is a modification of an illustration from Hill and Ferrara.72 This work was supported by research grants from the National Health and Medical Research Council and the Ministry of Economy and Competitiveness and European Regional Development Fund SAF2014-56546-R and RTI2018-101105-B-I00. G.R.H. is an Andy Hill CARE Distinguished Researcher. The work of S.R.-J. was funded by grants from the Deutsche Forschungsgemeinschaft (Bonn, Germany; SFB877 project A1) and by the Cluster of Excellence Inflammation at Interfaces. Publisher Copyright: © 2019 by The American Society of Hematology Copyright: Copyright 2019 Elsevier B.V., All rights reserved.

PY - 2019/12/5

Y1 - 2019/12/5

N2 - Graft-versus-host disease (GVHD) after allogeneic stem cell transplantation (alloSCT) is characterized by interleukin-6 (IL-6) dysregulation. IL-6 can mediate effects via various pathways, including classical, trans, and cluster signaling. Given the recent availability of agents that differentially inhibit these discrete signaling cascades, understanding the source and signaling and cellular targets of this cytokine is paramount to inform the design of clinical studies. Here we demonstrate that IL-6 secretion from recipient dendritic cells (DCs) initiates the systemic dysregulation of this cytokine. Inhibition of DC-driven classical signaling after targeted IL-6 receptor (IL-6R) deletion in T cells eliminated pathogenic donor Th17/Th22 cell differentiation and resulted in long-term survival. After engraftment, donor DCs assume the same role, maintaining classical IL-6 signaling–dependent GVHD responses. Surprisingly, cluster signaling was not active after transplantation, whereas inhibition of trans signaling with soluble gp130Fc promoted severe, chronic cutaneous GVHD. The latter was a result of exaggerated polyfunctional Th22-cell expansion that was reversed by IL-22 deletion or IL-6R inhibition. Importantly, inhibition of IL-6 classical signaling did not impair the graft-versus-leukemia effect. Together, these data highlight IL-6 classical signaling and downstream Th17/Th22 differentiation as important therapeutic targets after alloSCT.

AB - Graft-versus-host disease (GVHD) after allogeneic stem cell transplantation (alloSCT) is characterized by interleukin-6 (IL-6) dysregulation. IL-6 can mediate effects via various pathways, including classical, trans, and cluster signaling. Given the recent availability of agents that differentially inhibit these discrete signaling cascades, understanding the source and signaling and cellular targets of this cytokine is paramount to inform the design of clinical studies. Here we demonstrate that IL-6 secretion from recipient dendritic cells (DCs) initiates the systemic dysregulation of this cytokine. Inhibition of DC-driven classical signaling after targeted IL-6 receptor (IL-6R) deletion in T cells eliminated pathogenic donor Th17/Th22 cell differentiation and resulted in long-term survival. After engraftment, donor DCs assume the same role, maintaining classical IL-6 signaling–dependent GVHD responses. Surprisingly, cluster signaling was not active after transplantation, whereas inhibition of trans signaling with soluble gp130Fc promoted severe, chronic cutaneous GVHD. The latter was a result of exaggerated polyfunctional Th22-cell expansion that was reversed by IL-22 deletion or IL-6R inhibition. Importantly, inhibition of IL-6 classical signaling did not impair the graft-versus-leukemia effect. Together, these data highlight IL-6 classical signaling and downstream Th17/Th22 differentiation as important therapeutic targets after alloSCT.

UR - http://www.scopus.com/inward/record.url?scp=85076194283&partnerID=8YFLogxK

U2 - 10.1182/blood.2019000396

DO - 10.1182/blood.2019000396

M3 - Artículo

C2 - 31578204

AN - SCOPUS:85076194283

SN - 0006-4971

VL - 134

SP - 2092

EP - 2106

JO - Blood

JF - Blood

IS - 23

ER -

IL-6 dysregulation originates in dendritic cells and mediates graft-versus-host disease via classical signaling

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