Macrophage migration inhibitory factor regulates innate γδ T‐cell responses<i>via</i>IL‐17 expression

Kim, Hee Kyung; Garcia, Alvaro Baeza; Siu, Edwin; Tilstam, Pathricia V.; Das, Rita; Roberts, Scott; Leng, Lin; Bucala, Richard

doi:10.1096/fj.201802433r

Cited by 10 publications

(7 citation statements)

References 62 publications

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“…also reported that MIF neutralizing antibodies inhibited the proliferation of mouse splenocytes induced by the toxic-shock syndrome toxin 1 (TSST1) and protected mice from TSST1-induced shock 31 . However, apparently contradictory observations have just been reported 32 . Kim et al .…”

Section: Discussionmentioning

confidence: 99%

Macrophage migration inhibitory factor regulates TLR4 expression and modulates TCR/CD3-mediated activation in CD4+ T lymphocytes

Alibashe-Ahmed

Roger

Serre‐Beinier

et al. 2019

Sci Rep

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Toll-like receptor 4 (TLR4) is involved in CD4+ T lymphocyte-mediated pathologies. Here, we demonstrate that CD4+ T lymphocytes express functional TLR4 that contributes to their activation, proliferation and cytokine secretion. In addition, we demonstrate that TLR4-induced responses are mediated by macrophage migration inhibitory factor (MIF), a pro-inflammatory cytokine. We also demonstrate that MIF regulates suboptimal TCR/CD3-mediated activation of T lymphocytes. On one hand, MIF prevents excessive TCR/CD3-mediated activation of CD4+ T lymphocytes under suboptimal stimulation conditions and, on the other hand, MIF enables activated CD4+ T lymphocytes to sense their microenvironment and adapt their effector response through TLR4. Therefore, MIF appears to be a major regulator of the activation of CD4+ T lymphocytes and the intensity of their effector response. TLR4-mediated activation is thus an important process for T cell-mediated immunity.

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Section: Discussionmentioning

confidence: 99%

Macrophage migration inhibitory factor regulates TLR4 expression and modulates TCR/CD3-mediated activation in CD4+ T lymphocytes

Alibashe-Ahmed

Roger

Serre‐Beinier

et al. 2019

Sci Rep

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“…Although there are no reports of MIF driving gd T cell effector functions in the context of tumorigenesis, MIF has been shown to regulate gd T cell expression of IL-17 following stimulation with IL-1b and IL-23 in a mouse model of Gram-positive toxic shock syndrome (162). Interestingly, addition of recombinant MIF to lymph node-derived cells directly increases IL-17 production further supporting an amplification role for MIF in the regulation of gd T17 cell-expressed IL-17 (163).…”

Section: Gamma Delta T Cells (Gd T)mentioning

confidence: 99%

MIF-Dependent Control of Tumor Immunity

Noe

Mitchell

2020

Front. Immunol.

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Initially identified as a T lymphocyte-elicited inhibitor of macrophage motility, macrophage migration inhibitory factor (MIF) has since been found to be expressed by nearly every immune cell type examined and overexpressed in most solid and hematogenous malignant cancers. It is localized to both extracellular and intracellular compartments and physically interacts with more than a dozen different cell surface and intracellular proteins. Although classically associated with and characterized as a mediator of pro-inflammatory innate immune responses, more recent studies demonstrate that, in malignant disease settings, MIF contributes to anti-inflammatory, immune evasive, and immune tolerant phenotypes in both innate and adaptive immune cell types. This review will summarize the studies describing MIF in tumor-specific innate and adaptive immune responses and attempt to reconcile these various pleiotropic functions in normal physiology.

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“…AM is the majority part of alveolar and the macrophage is classical organ damage restorer. The activated macrophage is the main source of IL-17 [20]. Plasticity is the characteristics of macrophages.…”

Section: Discussionmentioning

confidence: 99%

IL-17 mediated macrophage polarization increased inflammatory damage in SWI-ALI models

Zhao

Zhang

et al. 2020

Preprint

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BackgroundSeawater inhalation induced acute lung injury (SWI-ALI) is the common accident in daily naval training. To investigate the mechanism of SWI-ALI will help to improve the treatment effect. Alveolar macrophages (AM) is the majority of alveolar, also paly the key role in SWI-ALI repair. IL-17 also paly the key role in the innate immunity process.MethodIn this study, we used seawater induced the ALI in mouse model. And the lungs and serum were exacted at D1, D3, D7 and D14. The AM polarization were tested by flow cytometry. The IL-17 concentration were tested by ELISA. Then the IL-17 function were confirmed by in vitro test. The mouse alveolar epithelial cell and mouse AM were co-cultured. The test compared the wound healing effect of MAE with and without IL-17.ResultThe AM switch into M1 and IL-17A increased were found after seawater dosing. And the IL-17a supplement attenuated wound healing of alveolar epithelial cells through improve the polarization of AM were confirmed in vitro model.ConclusionThe high IL-I7 micro-environment will increased the inflammatory damage through induced macrophage polarization in acute lung injury. The IL-17 antagonists have the potential to increase clinical effect in SWI-ALI treatment.

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Macrophage migration inhibitory factor regulates innate γδ T‐cell responsesviaIL‐17 expression

Cited by 10 publications

References 62 publications

Macrophage migration inhibitory factor regulates TLR4 expression and modulates TCR/CD3-mediated activation in CD4+ T lymphocytes

Macrophage migration inhibitory factor regulates TLR4 expression and modulates TCR/CD3-mediated activation in CD4+ T lymphocytes

MIF-Dependent Control of Tumor Immunity

IL-17 mediated macrophage polarization increased inflammatory damage in SWI-ALI models

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