IL-34 is a Treg-specific cytokine and mediates transplant tolerance
Séverine Bézie, … , Ignacio Anegon, Carole Guillonneau
Séverine Bézie, … , Ignacio Anegon, Carole Guillonneau
Published September 21, 2015
Citation Information: J Clin Invest. 2015;125(10):3952-3964. https://doi.org/10.1172/JCI81227.
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Research Article

IL-34 is a Treg-specific cytokine and mediates transplant tolerance

Abstract

Cytokines and metabolic pathway–controlling enzymes regulate immune responses and have potential as powerful tools to mediate immune tolerance. Blockade of the interaction between CD40 and CD40L induces long-term cardiac allograft survival in rats through a CD8+CD45RClo Treg potentiation. Here, we have shown that the cytokine IL-34, the immunoregulatory properties of which have not been previously studied in transplantation or T cell biology, is expressed by rodent CD8+CD45RClo Tregs and human FOXP3+CD45RCloCD8+ and CD4+ Tregs. IL-34 was involved in the suppressive function of both CD8+ and CD4+ Tregs and markedly inhibited alloreactive immune responses. Additionally, in a rat cardiac allograft model, IL-34 potently induced transplant tolerance that was associated with a total inhibition of alloantibody production. Treatment of rats with IL-34 promoted allograft tolerance that was mediated by induction of CD8+ and CD4+ Tregs. Moreover, these Tregs were capable of serial tolerance induction through modulation of macrophages that migrate early to the graft. Finally, we demonstrated that human macrophages cultured in the presence of IL-34 greatly expanded CD8+ and CD4+ FOXP3+ Tregs, with a superior suppressive potential of antidonor immune responses compared with non–IL-34–expanded Tregs. In conclusion, we reveal that IL-34 serves as a suppressive Treg–specific cytokine and as a tolerogenic cytokine that efficiently inhibits alloreactive immune responses and mediates transplant tolerance.

Authors

Séverine Bézie, Elodie Picarda, Jason Ossart, Laurent Tesson, Claire Usal, Karine Renaudin, Ignacio Anegon, Carole Guillonneau

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Figure 4

Il34 gene transfer prolongs allograft survival alone and in combination with a suboptimal dose of rapamycin.

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Il34 gene transfer prolongs allograft survival alone and in combination...
(A) Recipients given i.v. 1012 vg/rat AAV–IL-34 or noncoding AAV or no treatment were grafted 30 days later with no additional treatment or in combination with a suboptimal dose of rapamycin (10 days, starting on day 0). Graft survival was evaluated by palpation through the abdominal wall. Log-rank test, *P < 0.05, **P < 0.01, ***P < 0.001, ****P < 0.0001. (B) Representative image of the anatomopathological analysis of graft from AAV–IL-34 plus rapamycin–treated, day-120 long-term surviving recipients. Original magnification, ×100. (C) IgG alloantibody production was evaluated in naive and treated long-term recipients more than 120 days after transplantation. Graph represents MFI ± SEM. Two-way ANOVA with Bonferroni’s post test, *P < 0.05, ***P < 0.001, ****P < 0.0001 for noncoding AAV–IL-34 versus noncoding AAV.