IL-34 deficiency impairs FOXP3<sup>+</sup> Treg function in a model of autoimmune colitis and decreases immune tolerance homeostasis.

Freuchet, Antoine; Salama, Apolline; Bézie, Séverine; Tesson, Laurent; Rémy, Séverine; Humeau, Romain; Règue, Hadrien; Sérazin, Céline; Flippe, Léa; Peterson, Pärt; Vimond, Nadège; Usal, Claire; Ménoret, Séverine; Heslan, Jean-Marie; Duteille, Franck; Blanchard, Frédéric; Giral, Magali; Colonna, Marco; Anegon, Ignacio; Guillonneau, Carole

IL-34 deficiency impairs FOXP3⁺ Treg function in a model of autoimmune colitis and decreases immune tolerance homeostasis.

Freuchet, Antoine; Salama, Apolline; Bézie, Séverine; Tesson, Laurent; Rémy, Séverine; Humeau, Romain; Règue, Hadrien; Sérazin, Céline; Flippe, Léa; Peterson, Pärt; Vimond, Nadège; Usal, Claire; Ménoret, Séverine; Heslan, Jean-Marie; Duteille, Franck; Blanchard, Frédéric; Giral, Magali; Colonna, Marco; Anegon, Ignacio; Guillonneau, Carole.

Affiliation

Freuchet A; Nantes Université, CHU Nantes, CNRS, INSERM, Center for Research in Transplantation and Translational Immunology, UMR 1064, ITUN5, Nantes, F-44000, France.
Salama A; Nantes Université, CHU Nantes, CNRS, INSERM, Center for Research in Transplantation and Translational Immunology, UMR 1064, ITUN5, Nantes, F-44000, France.
Bézie S; Nantes Université, CHU Nantes, CNRS, INSERM, Center for Research in Transplantation and Translational Immunology, UMR 1064, ITUN5, Nantes, F-44000, France.
Tesson L; Nantes Université, CHU Nantes, CNRS, INSERM, Center for Research in Transplantation and Translational Immunology, UMR 1064, ITUN5, Nantes, F-44000, France.
Rémy S; Nantes Université, CHU Nantes, CNRS, INSERM, Center for Research in Transplantation and Translational Immunology, UMR 1064, ITUN5, Nantes, F-44000, France.
Humeau R; Nantes Université, CHU Nantes, CNRS, INSERM, Center for Research in Transplantation and Translational Immunology, UMR 1064, ITUN5, Nantes, F-44000, France.
Règue H; Nantes Université, CHU Nantes, CNRS, INSERM, Center for Research in Transplantation and Translational Immunology, UMR 1064, ITUN5, Nantes, F-44000, France.
Sérazin C; Nantes Université, CHU Nantes, CNRS, INSERM, Center for Research in Transplantation and Translational Immunology, UMR 1064, ITUN5, Nantes, F-44000, France.
Flippe L; Nantes Université, CHU Nantes, CNRS, INSERM, Center for Research in Transplantation and Translational Immunology, UMR 1064, ITUN5, Nantes, F-44000, France.
Peterson P; Institute of Biomedicine and Translational Medicine, University of Tartu, Tartu, Estonia.
Vimond N; Nantes Université, CHU Nantes, CNRS, INSERM, Center for Research in Transplantation and Translational Immunology, UMR 1064, ITUN5, Nantes, F-44000, France.
Usal C; Nantes Université, CHU Nantes, CNRS, INSERM, Center for Research in Transplantation and Translational Immunology, UMR 1064, ITUN5, Nantes, F-44000, France.
Ménoret S; Nantes Université, CHU Nantes, CNRS, INSERM, Center for Research in Transplantation and Translational Immunology, UMR 1064, ITUN5, Nantes, F-44000, France.
Heslan JM; CHU Nantes, Inserm, CNRS, SFR Santé, Inserm UMS 016, CNRS UMS 3556, Nantes Université, Nantes, France.
Duteille F; Nantes Université, CHU Nantes, CNRS, INSERM, Center for Research in Transplantation and Translational Immunology, UMR 1064, ITUN5, Nantes, F-44000, France.
Blanchard F; Chirurgie Plastique Reconstructrice et Esthétique, CHU Nantes, Nantes, France.
Giral M; INSERM UMR1238, Bone Sarcoma and remodeling of calcified tissues, Nantes University, Nantes, France.
Colonna M; Nantes Université, CHU Nantes, CNRS, INSERM, Center for Research in Transplantation and Translational Immunology, UMR 1064, ITUN5, Nantes, F-44000, France.
Anegon I; Department of Pathology and Immunology, Washington University School of Medicine, St. Louis, Missouri, USA.
Guillonneau C; Nantes Université, CHU Nantes, CNRS, INSERM, Center for Research in Transplantation and Translational Immunology, UMR 1064, ITUN5, Nantes, F-44000, France.

Clin Transl Med ; 12(8): e988, 2022 08.

Article in En | MEDLINE | ID: mdl-36030499

ABSTRACT

ABSTRACT

BACKGROUND:

Immune homeostasis requires fully functional Tregs with a stable phenotype to control autoimmunity. Although IL-34 is a cytokine first described as mainly involved in monocyte cell survival and differentiation, we recently described its expression by CD8+ Tregs in a rat model of transplantation tolerance and by activated FOXP3+ CD4+ and CD8+ Tregs in human healthy individuals. However, its role in autoimmunity and potential in human diseases remains to be determined.

METHODS:

We generated Il34-/- rats and using both Il34-/- rats and mice, we investigated their phenotype under inflammatory conditions. Using Il34-/- rats, we further analyzed the impact of the absence of expression of IL-34 for CD4+ Tregs suppressive function. We investigated the potential of IL-34 in human disease to prevent xenogeneic GVHD and human skin allograft rejection in immune humanized immunodeficient NSG mice. Finally, taking advantage of a biocollection, we investigated the correlation between presence of IL-34 in the serum and kidney transplant rejection.

RESULTS:

Here we report that the absence of expression of IL-34 in Il34-/- rats and mice leads to an unstable immune phenotype, with production of multiple auto-antibodies, exacerbated under inflammatory conditions with increased susceptibility to DSS- and TNBS-colitis in Il34-/- animals. Moreover, we revealed the striking inability of Il34-/- CD4+ Tregs to protect Il2rg-/- rats from a wasting disease induced by transfer of pathogenic cells, in contrast to Il34+/+ CD4+ Tregs. We also showed that IL-34 treatment delayed EAE in mice as well as GVHD and human skin allograft rejection in immune humanized immunodeficient NSG mice. Finally, we show that presence of IL-34 in the serum is associated with a longer rejection-free period in kidney transplanted patients.

CONCLUSION:

Altogether, our data emphasize on the crucial necessity of IL-34 for immune homeostasis and for CD4+ Tregs suppressive function. Our data also shows the therapeutic potential of IL-34 in human transplantation and auto-immunity. HIGHLIGHTS -Absence of expression of IL-34 in Il34-/- rats and mice leads to an unstable immune phenotype, with a production of multiple auto-antibodies and exacerbated immune pathology under inflammatory conditions. -Il34-/- CD4+ Tregs are unable to protect Il2rg-/- rats from colitis induced by transfer of pathogenic cells. -IL-34 treatment delayed EAE in mice, as well as acute GVHD and human skin allograft rejection in immune-humanized immunodeficient NSG mice.

Subject(s)

Colitis; Graft vs Host Disease; Interleukins; T-Lymphocytes, Regulatory; Animals; Colitis/immunology; Forkhead Transcription Factors; Graft vs Host Disease/immunology; Homeostasis; Humans; Immune Tolerance; Interleukins/deficiency; Interleukins/genetics; Mice; Rats; T-Lymphocytes, Regulatory/immunology

Key words

CRISPR/Cas9; Foxp3; IL-34; Treg; autoimmunity; immunotherapy; knockout; rat; tolerance

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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Interleukins / T-Lymphocytes, Regulatory / Colitis / Graft vs Host Disease Type of study: Prognostic_studies Limits: Animals / Humans Language: En Journal: Clin Transl Med Year: 2022 Document type: Article Affiliation country: France

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