Interleukin‐35 in immune‐related diseases: protection or destruction

Zhang, Junfeng; Zhang, Yunsheng; Wang, Qingpeng; Li, Chunlei; Deng, Hongxin; Si, Chuanping; Xiong, Huabao

doi:10.1111/imm.13044

Cited by 69 publications

(48 citation statements)

References 91 publications

(189 reference statements)

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“…To the best of our knowledge, this was the first study on the direct regulatory role of IL-35 to CD14 + monocytes in Kawasaki disease. We showed an elevation of plasma IL- 35 Recent studies have revealed abnormal expression of IL-35 in inflammatory autoimmune diseases, and suggested the critical regulatory role in the onset and development of these diseases [21,22]. Decreased expression of peripheral IL-35 was reported in patients with systemic lupus erythematosus [23], multiple sclerosis [24], primary Sjogren's syndrome [25], and psoriasis vulgaris [26].…”

Section: Discussionmentioning

confidence: 69%

Increased Interleukin-35 suppresses peripheral CD14+ monocytes function in patients with Kawasaki disease

Xing

Tian

2020

BMC Immunol

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Background: Interleukin-35 (IL-35) is a newly identified IL-12 cytokine family member, which regulates the activity of immune cells in infectious diseases and autoimmune disorders. However, the regulatory function of IL-35 in Kawasaki disease is not well elucidated. Methods: Thirty-three patients with Kawasaki disease and seventeen healthy controls were studied. Peripheral IL-35 concentration was measured by enzyme linked immunosorbent assay. CD14 + monocytes were purified, and mRNA expression of IL-35 receptor (IL-12Rβ2 and gp130) was semi-quantified by real-time polymerase chain reaction. CD14 + monocytes were stimulated with recombinant IL-35. The modulatory role of IL-35 treated CD14 + monocytes to naïve CD4 + T cell activation was investigated by flow cytometry. The influence of IL-35 to cytotoxicity of CD14 + monocytes was assessed by measuring target cell death, cytokine and granzyme secretion.Results: Plasma IL-35 concentration was elevated in patients with Kawasaki disease. There was no significant differences of either IL-12Rβ2 or gp130 mRNA expression in CD14 + monocytes between Kawasaki disease patients and controls. IL-35 suppressed CD14 + monocytes induced naïve CD4 + T cell activation in Kawasaki disease, and this process required direct cell-to-cell contact. IL-35 also inhibited tumor necrosis factor-α and granzyme B secretion by CD14 + monocytes from patients with Kawasaki disease, however, only granzyme B was responsible for the cytotoxicity of CD14 + monocytes.Conclusions: IL-35 played an important immunosuppressive role to CD14 + monocytes function in Kawasaki disease.

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Section: Discussionmentioning

confidence: 69%

Increased Interleukin-35 suppresses peripheral CD14+ monocytes function in patients with Kawasaki disease

Xing

Tian

2020

BMC Immunol

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“…Indeed, we were able to show that PF-BaE5 and PF-BaE7-primed DCs promoted the polarization of CD4 + T cells towards a regulatory phenotype (CD4 + FoxP3 + IL-10 + ) with an increased expression of the gene encoding Ebi3. Ebi3 is a subunit of the heterodimeric cytokine IL-35, a potent immunosuppressive cytokine secreted by Tregs and B regulatory cells with a strong ability to inhibit T cell differentiation and effector functions [ 76 ]. IL-35-induced Treg cells (iTr35) produce more IL-35 [ 77 ] and type 1 Treg cells (Tr1) use IL-35 to suppress the immune response [ 78 ].…”

Section: Discussionmentioning

confidence: 99%

In Vitro Characterization of Gut Microbiota-Derived Commensal Strains: Selection of Parabacteroides distasonis Strains Alleviating TNBS-Induced Colitis in Mice

Cuffaro

Assohoun

Boutillier

et al. 2020

Cells

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Alterations in the gut microbiota composition and diversity seem to play a role in the development of chronic diseases, including inflammatory bowel disease (IBD), leading to gut barrier disruption and induction of proinflammatory immune responses. This opens the door for the use of novel health-promoting bacteria. We selected five Parabacteroides distasonis strains isolated from human adult and neonates gut microbiota. We evaluated in vitro their immunomodulation capacities and their ability to reinforce the gut barrier and characterized in vivo their protective effects in an acute murine model of colitis. The in vitro beneficial activities were highly strain dependent: two strains exhibited a potent anti-inflammatory potential and restored the gut barrier while a third strain reinstated the epithelial barrier. While their survival to in vitro gastric conditions was variable, the levels of P. distasonis DNA were higher in the stools of bacteria-treated animals. The strains that were positively scored in vitro displayed a strong ability to rescue mice from colitis. We further showed that two strains primed dendritic cells to induce regulatory T lymphocytes from naïve CD4+ T cells. This study provides better insights on the functionality of commensal bacteria and crucial clues to design live biotherapeutics able to target inflammatory chronic diseases such as IBD.

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“…66,72 Although IFNγ has proinflammatory consequences it has also been described as having pro-tolerogenic actions, through the production of molecules such as IDO, iNOs and FGL2. 66,72 Although IFNγ has proinflammatory consequences it has also been described as having pro-tolerogenic actions, through the production of molecules such as IDO, iNOs and FGL2.…”

Section: Treg Cells 62 Fgl2 Expression Was Then Reported In Mouse Cd8ααmentioning

confidence: 99%

“…IL-35 has been previously described as expressed by CD4 + Tregs 71 but it has also been described as expressed and playing a suppressive role for tumor-associated CD8 + Tregs. 66,72 Although IFNγ has proinflammatory consequences it has also been described as having pro-tolerogenic actions, through the production of molecules such as IDO, iNOs and FGL2. 68 IFNγ has been described as produced by several CD8 + Treg types 3,4,65,[73][74][75][76][77] although the function of IFNγ in CD8 + FOXP3 + cells has not been specifically analyzed.…”

Section: Treg Cells 62 Fgl2 Expression Was Then Reported In Mouse Cd8ααmentioning

confidence: 99%

Future prospects for CD8⁺ regulatory T cells in immune tolerance

Flippe

Bézie

Anegón

et al. 2019

Immunological Reviews

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CD8+ Tregs have been long described and significant progresses have been made about their phenotype, their functional mechanisms, and their suppressive ability compared to conventional CD4+ Tregs. They are now at the dawn of their clinical use. In this review, we will summarize their phenotypic characteristics, their mechanisms of action, the similarities, differences and synergies between CD8+ and CD4+ Tregs, and we will discuss the biology, development and induction of CD8+ Tregs, their manufacturing for clinical use, considering open questions/uncertainties and future technically accessible improvements notably through genetic modifications.

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Interleukin‐35 in immune‐related diseases: protection or destruction

Cited by 69 publications

References 91 publications

Increased Interleukin-35 suppresses peripheral CD14+ monocytes function in patients with Kawasaki disease

Increased Interleukin-35 suppresses peripheral CD14+ monocytes function in patients with Kawasaki disease

In Vitro Characterization of Gut Microbiota-Derived Commensal Strains: Selection of Parabacteroides distasonis Strains Alleviating TNBS-Induced Colitis in Mice

Future prospects for CD8⁺ regulatory T cells in immune tolerance

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Interleukin‐35 in immune‐related diseases: protection or destruction

Cited by 69 publications

References 91 publications

Increased Interleukin-35 suppresses peripheral CD14+ monocytes function in patients with Kawasaki disease

Increased Interleukin-35 suppresses peripheral CD14+ monocytes function in patients with Kawasaki disease

In Vitro Characterization of Gut Microbiota-Derived Commensal Strains: Selection of Parabacteroides distasonis Strains Alleviating TNBS-Induced Colitis in Mice

Future prospects for CD8+ regulatory T cells in immune tolerance

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Future prospects for CD8⁺ regulatory T cells in immune tolerance