CD11c depletion severely disrupts Th2 induction and development in vivo

Phythian‐Adams, Alexander; Cook, Peter C.; Lundie, Rachel J.; Jones, Lucy; Smith, Katherine A.; Barr, Tom A.; Hochweller, Kristin; Anderton, Stephen M.; Hämmerling, Günter J.; Maizels, Rick M.; MacDonald, Andrew S.

doi:10.1084/jem.20100734

Cited by 241 publications

(279 citation statements)

References 30 publications

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“…In contrast, we have established that DCs pulsed with SEA are capable inducers of Th2 responses both in vitro and in vivo, despite failing to upregulate traditional markers of activation (5). Although it has been debated recently whether DCs are needed to prime Th2 responses (4), we have definitively shown that Th2 priming to schistosomes is dependent on CD11c + DCs (25).…”

Section: Il-4 Up-regulates DC Expression Of Multiple Markers Of Altermentioning

confidence: 73%

See 1 more Smart Citation

Alternatively activated dendritic cells regulate CD4⁺T-cell polarization in vitro and in vivo

Cook

Jones

Jenkins

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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129

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Interleukin-4 is a cytokine widely known for its role in CD4 + T cell polarization and its ability to alternatively activate macrophage populations. In contrast, the impact of IL-4 on the activation and function of dendritic cells (DCs) is poorly understood. We report here that DCs respond to IL-4 both in vitro and in vivo by expression of multiple alternative activation markers with a different expression pattern to that of macrophages. We further demonstrate a central role for DC IL-4Rα expression in the optimal induction of IFNγ responses in vivo in both Th1 and Th2 settings, through a feedback loop in which IL-4 promotes DC secretion of IL-12. Finally, we reveal a central role for RELMα during T-cell priming, establishing that its expression by DCs is critical for optimal IL-10 and IL-13 promotion in vitro and in vivo. Together, these data highlight the significant impact that IL-4 and RELMα can have on DC activation and function in the context of either bacterial or helminth pathogens.antigen presenting cells | T lymphocytes | innate immunity | adaptive immunity

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Section: Il-4 Up-regulates DC Expression Of Multiple Markers Of Altermentioning

confidence: 73%

“…C57BL/6, BALB/c, Retnla −/− , IL-10eGFPxDOG, KN2 (C57BL/6), Il4ra −/− , and OTII mice (20,23,25,29,30) were maintained under specific pathogen-free conditions at the University of Edinburgh. Experiments were conducted under a Project License granted by the Home Office (United Kingdom) in accordance with local guidelines.…”

Section: Methodsmentioning

confidence: 99%

Alternatively activated dendritic cells regulate CD4⁺T-cell polarization in vitro and in vivo

Cook

Jones

Jenkins

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

129

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“…CD45.1 + C57BL/6 mice (59) were provided by S. M. Anderton, University of Edinburgh. CD11C-DOG mice (28) were provided by A. S. MacDonald, University of Edinburgh. Mice were bred under specific pathogen-free conditions at the University of Edinburgh.…”

Section: Methodsmentioning

confidence: 99%

Differential Ly-6C expression identifies the recruited macrophage phenotype, which orchestrates the regression of murine liver fibrosis

Ramachandran

Pellicoro

Vernon

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

798

947

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Although macrophages are widely recognized to have a profibrotic role in inflammation, we have used a highly tractable CCl 4 -induced model of reversible hepatic fibrosis to identify and characterize the macrophage phenotype responsible for tissue remodeling: the hitherto elusive restorative macrophage. This CD11B hi F4/80 int Ly-6C lo macrophage subset was most abundant in livers during maximal fibrosis resolution and represented the principle matrix metalloproteinase (MMP) -expressing subset. Depletion of this population in CD11B promoter-diphtheria toxin receptor (CD11B-DTR) transgenic mice caused a failure of scar remodeling. Adoptive transfer and in situ labeling experiments showed that these restorative macrophages derive from recruited Ly-6C hi monocytes, a common origin with profibrotic Ly-6C hi macrophages, indicative of a phenotypic switch in vivo conferring proresolution properties. Microarray profiling of the Ly-6C lo subset, compared with Ly-6C hi macrophages, showed a phenotype outside the M1/M2 classification, with increased expression of MMPs, growth factors, and phagocytosis-related genes, including Mmp9, Mmp12, insulin-like growth factor 1 (Igf1), and Glycoprotein (transmembrane) nmb (Gpnmb). Confocal microscopy confirmed the postphagocytic nature of restorative macrophages. Furthermore, the restorative macrophage phenotype was recapitulated in vitro by the phagocytosis of cellular debris with associated activation of the ERK signaling cascade. Critically, induced phagocytic behavior in vivo, through administration of liposomes, increased restorative macrophage number and accelerated fibrosis resolution, offering a therapeutic strategy to this orphan pathological process.

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“…Interestingly, some studies suggest that ILC, 129-131 basophils, [132][133][134] and eosinophils 135,136 can express major histocompatibility complex class II and directly prime Th2 responses, notably upon N. brasiliensis 131 and T. muris 132 infections, with each cell type having been shown to migrate to the mesenteric lymph nodes during infection. 85,87,137,138 However, given that protective immunity is abolished in mice where all 139,140 or specific subsets 104-106,108,109 of dendritic cells have been depleted, it is perhaps more likely that these other innate cells contribute to local tissue immunity by promoting dendritic cell activation, or by further enhancing the cytokine response of mature T cells that have migrated to the infected tissue. 53 Moreover, dendritic cells are responsive not only to cytokines produced by other innate cells, but also to epithelium-derived cytokines, including TSLP, 54,[141][142][143] IL-25, 144 and IL-33, 52,145 thus potentially bypassing ILC2 and granulocytes entirely.…”

Section: Inductionmentioning

confidence: 99%

Immunity to gastrointestinal nematode infections

2018

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CD11c depletion severely disrupts Th2 induction and development in vivo

Cited by 241 publications

References 30 publications

Alternatively activated dendritic cells regulate CD4⁺T-cell polarization in vitro and in vivo

Alternatively activated dendritic cells regulate CD4⁺T-cell polarization in vitro and in vivo

Differential Ly-6C expression identifies the recruited macrophage phenotype, which orchestrates the regression of murine liver fibrosis

Immunity to gastrointestinal nematode infections

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CD11c depletion severely disrupts Th2 induction and development in vivo

Cited by 241 publications

References 30 publications

Alternatively activated dendritic cells regulate CD4+T-cell polarization in vitro and in vivo

Alternatively activated dendritic cells regulate CD4+T-cell polarization in vitro and in vivo

Differential Ly-6C expression identifies the recruited macrophage phenotype, which orchestrates the regression of murine liver fibrosis

Immunity to gastrointestinal nematode infections

Contact Info

Product

Resources

About

Alternatively activated dendritic cells regulate CD4⁺T-cell polarization in vitro and in vivo

Alternatively activated dendritic cells regulate CD4⁺T-cell polarization in vitro and in vivo