A distinct subset of intestinal dendritic cells responds selectively to oral TLR7/8 stimulation

Yrlid, Ulf; Cerovic, Vuk; Milling, Simon; Jenkins, Christopher; Klavinskis, Linda; MacPherson, G. Gordon

doi:10.1002/eji.200636426

Cited by 45 publications

(60 citation statements)

References 31 publications

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“…The mechanism of R848 action is known to be through an indirect activity on plasmacytoid DCs. These cells then secrete high levels of type I IFN, which in turn acts on CD103 + DCs resulting in their activation and migration to the MLN (30,36). We hypothesize that the ability of sFliC to drive CD103 DC migration to the MLN is through the direct ligation of TLR5 on LP CD103 + DCs.…”

Section: Discussionmentioning

confidence: 99%

“…The selective migration of CD103 + DCs to the MLN after sFliC immunization occurred despite Ag being systemically administered. Although atypical for systemic adjuvants, this has been demonstrated after immunization with some subunit oral adjuvants such as R848 and Escherichia coli heat-labile enterotoxin (30,39). Additionally, the B subunit of heat-labile enterotoxin can induce cells with a regulatory phenotype after intranasal administration (40), although it is not clear if these are primed by CD103 + DCs.…”

Section: Discussionmentioning

confidence: 99%

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Systemic Flagellin Immunization Stimulates Mucosal CD103+ Dendritic Cells and Drives Foxp3+ Regulatory T Cell and IgA Responses in the Mesenteric Lymph Node

Flores‐Langarica

Marshall

Hitchcock

et al. 2012

The Journal of Immunology

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Mucosal immunity is poorly activated after systemic immunization with protein Ags. Nevertheless, induction of mucosal immunity in such a manner would be an attractive and simple way to overcome the intrinsic difficulties in delivering Ag to such sites. Flagellin from Salmonella enterica serovar Typhimurium (FliC) can impact markedly on host immunity, in part via its recognition by TLR5. In this study, we show that systemic immunization with soluble FliC (sFliC) drives distinct immune responses concurrently in the mesenteric lymph nodes (MLN) and the spleen after i.p. and s.c. immunization. In the MLN, but not the spleen, sFliC drives a TLR5-dependent recruitment of CD103+ dendritic cells (DCs), which correlates with a diminution in CD103+ DC numbers in the lamina propria. In the MLN, CD103+ DCs carry Ag and are the major primers of endogenous and transgenic T cell priming. A key consequence of these interactions with CD103+ DCs in the MLN is an increase in local regulatory T cell differentiation. In parallel, systemic sFliC immunization results in a pronounced switching of FliC-specific B cells to IgA in the MLN but not elsewhere. Loss of TLR5 has more impact on MLN than splenic Ab responses, reflected in an ablation of IgA, but not IgG, serum Ab titers. Therefore, systemic sFliC immunization targets CD103+ DCs and drives distinct mucosal T and B cell responses. This offers a potential “Trojan horse” approach to modulate mucosal immunity by systemically immunizing with sFliC.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Systemic Flagellin Immunization Stimulates Mucosal CD103+ Dendritic Cells and Drives Foxp3+ Regulatory T Cell and IgA Responses in the Mesenteric Lymph Node

Flores‐Langarica

Marshall

Hitchcock

et al. 2012

The Journal of Immunology

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“…Induction of DC migration by CT has been demonstrated by Shreedhar et al (23), who observed that fluorescent microsphereloaded DCs in the subepithelial dome relocated to T cell areas after feeding CT. MacPherson and colleagues have directly addressed the migration of DCs from the intestinal lamina propria by collecting lymph over time in cannulated rats (24 -26). They have shown that DC migration from the lamina propria to the MLN occurs constitutively and that this migration can be modulated by TLR agonists, in particular TLR4 and TLR7/8 agonists (24,25). However, they recently reported that another bacterial toxin with adjuvant activity (heat-labile enterotoxin from Escherichia coli) did not influence DC migration (26).…”

Section: Discussionmentioning

confidence: 99%

Gastrointestinal Dendritic Cells Promote Th2 Skewing via OX40L

Blázquez

Berin

2008

The Journal of Immunology

141

123

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Mice can be sensitized to food proteins by oral administration with the adjuvant cholera toxin (CT), such that they undergo anaphylaxis when rechallenged with the sensitizing allergen. In contrast, feeding of Ags alone leads to oral tolerance. Our aim was to define the mechanisms by which gastrointestinal dendritic cells (DCs) participate in the deviation of tolerance to allergic sensitization in the gut in response to CT. BALB/c mice were fed with CT or PBS. The impact of CT on DC subsets in the mesenteric lymph node (MLN) was assessed by flow cytometry. Ag presentation assays were performed with DCs isolated from the MLN of PBS- or CT-fed mice, using OVA-specific CD4+ T cells as responder cells. Gene expression in MLN DCs was determined by real-time PCR, and neutralizing Abs were used to test the function of OX40 ligand (OX40L) in Th2 skewing. Oral administration of CT induced an increase in the total CD11c+ population in the MLN. CT induced a selective increase in migration of the CD11c+CD11b−CD8α− DC subset and the maturation of all DC subsets. Maturation of DCs in vivo enhanced T cell proliferation and cytokine secretion. Oral CT induced up-regulation of Jagged-2 and OX40L by MLN DCs. Neutralizing anti-OX40L Abs completely abrogated the CT-induced Th2 cytokine response. We show that oral CT induces selective DC migration, maturation, and T cell priming activity in the MLN. Th2 skewing is mediated by OX40L, and we speculate that this molecule may be an important inducer of allergic sensitization to food allergens.

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“…121 Similarly, the MAP3 (mitogen-activated protein kinase kinase kinase) kinase TPL-2 was also shown to modulate immunity to H. polygyrus, as its deletion in dendritic cells resulted in enhanced resistance to infection that was attributed to its downstream influence on the homing of leukocytes. 122 Indeed, different dendritic cell subsets have divergent expression of certain cytokine and pattern-recognition receptors, [123][124][125][126] and might thus be inherently more or less prone to respond to specific pathogens and cytokines to begin with. These types of signals, in combination with cell-extrinsic cues from epithelial and innate immune cells, could determine which type of dendritic cell that gets activated upon parasite infection.…”

Section: Inductionmentioning

confidence: 99%