Antigen- and Cytokine-Driven Accumulation of Regulatory T Cells in Visceral Adipose Tissue of Lean Mice

Kolodin, Dmitriy; Panhuys, Nicholas J. Van; Li, Chaoran; Magnuson, Angela M.; Cipolletta, Daniela; Miller, Christine; Wagers, Amy J.; Germain, Ronald N.; Benoist, Christophe; Mathis, Diane

doi:10.1016/j.cmet.2015.03.005

Cited by 317 publications

(490 citation statements)

References 31 publications

(55 reference statements)

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“…[37][38][39][40][41] Although mechanisms controlling IL-33 pleiotropy are unclear, its activity is controlled by both the regulated availability of ST2-expressing cells, as well as the presence of proinflammatory cytokines. 57,58 Recipient conditioning prior to alloHCT causes a breach in the intestinal epithelium that allows commensal bacteria to trigger proinflammatory cytokine secretion by local macrophages and DCs.…”

Section: Discussionmentioning

confidence: 99%

“…32 Although IL-33 expands Tregs 38,39,41 and supports Treg stability, 37 when physiologic ratios of donor Tregs to non-Tregs were transferred into alloHCT recipients, endogenous or exogenous IL-33 stimulation of Tregs posttransplant was insufficient to prevent lethal GVHD. 32 The data depicted in Figures 1-3 BLOOD, 21 JULY 2016 x VOLUME 128, NUMBER 3…”

Section: Il-33 Responsiveness Is Critical For Treg-protective Capacitmentioning

confidence: 99%

“…[33][34][35][36] In addition to its potent type 1-and type 2-promoting capacity, a growing body of research supports a role for IL-33 in Treg immunobiology. [37][38][39][40][41][42] Our group and others have described a subset of Foxp3 In nonlymphoid compartments, ST2 1 Tregs are present at increased frequencies and would be well positioned to respond to IL-33 released from damaged tissue. 37,42 Despite these interesting observations, there are no definitive studies examining the impact of both donor and host IL-33-responsive Tregs after alloHCT.…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Peri-alloHCT IL-33 administration expands recipient T-regulatory cells that protect mice against acute GVHD

Matta

Reichenbach

Zhang

et al. 2016

Blood

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Section: Discussionmentioning

confidence: 99%

Section: Il-33 Responsiveness Is Critical For Treg-protective Capacitmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Peri-alloHCT IL-33 administration expands recipient T-regulatory cells that protect mice against acute GVHD

Matta

Reichenbach

Zhang

et al. 2016

Blood

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“…Cytokines-IL-2 foremost-are thought to be the main controllers of Treg proportions and numbers (15)(16)(17)(18)(19)(20)(21)(22), although the relative importance of these controllers varies with location and subphenotype [e.g., the alarmin IL-33 has a more profound role in tissue Tregs (21)(22)(23)]. Perhaps surprisingly, in light of this apparently tight control, there is a wide range of variation in Treg proportions, with several studies having observed up to fourfold variation in the blood of healthy humans (e.g., refs.…”

mentioning

confidence: 99%

Unstable FoxP3 ⁺ T regulatory cells in NZW mice

Dépis

Kwon

Mathis

et al. 2016

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

Self Cite

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Regulatory T (Treg) cells that express the transcription factor FoxP3 play a key role in self-tolerance and the control of inflammation. In mice and humans, there is a wide interindividual range in Treg frequency, but little is known about the underlying genetic or epigenetic mechanisms. We explored this issue in inbred strains of mice, with a special focus on the low proportion of Treg cells found in NZW mice. Mixed bone marrow chimera experiments showed this paucity to be intrinsic to NZW Treg cells, a dearth that could be tied to poor stability of the Treg pool and of FoxP3 expression. This instability was not a consequence of differential epigenetic marks, because Treg-specific CpG hypomethylation profiles at the Foxp3 locus were similar in all strains tested. It was also unrelated to the high expression of IFN signature genes in NZW, as shown by intercross to mice with an Ifnar1 knockout. NZW Tregs were less sensitive to limiting doses of trophic cytokines, IL-2 and -33, for population homeostasis and for maintenance of FoxP3 expression. Gene-expression profiles highlighted specific differences in the transcriptome of NZW Tregs compared with those of other strains, but no single defect could obviously account for the instability. Rather, NZW Tregs showed a general up-regulation of transcripts normally repressed in Treg cells, and we speculate that this network-level bias may account for NZW Treg instability.Treg homeostasis | FoxP3 stability | immunoregulation | inbred mice

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“…Adipose tissue inflammation involves activation of both innate and adaptive immune responses [1,2]. MHC class II-restricted signals from macrophages and dendritic cells contribute to T cell activation in response to obesogenic cues and contribute to metabolic dysfunction [3][4][5]. ATMs and dendritic cells can function as APCs and provide critical cues to generate proinflammatory signals that include activation of adipose tissue CD4 + T cells toward a Th1 and effector/memory phenotype [6][7][8].…”

Section: Introductionmentioning

confidence: 99%

CD40 promotes MHC class II expression on adipose tissue macrophages and regulates adipose tissue CD4+ T cells with obesity

Morris

Oatmen

Mergian

et al. 2015

Journal of Leukocyte Biology

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Obesity activates both innate and adaptive immune responses in adipose tissue, but the mechanisms critical for regulating these responses remain unknown. CD40/CD40L signaling provides bidirectional costimulatory signals between antigen-presenting cells and CD4 + T cells, and CD40L expression is increased in obese humans. Therefore, we examined the contribution of CD40 to the progression of obesity-induced inflammation in mice. CD40 was highly expressed on adipose tissue macrophages in mice, and CD40/CD40L signaling promoted the expression of antigen-presenting cell markers in adipose tissue macrophages. When fed a high fat diet, Cd40-deficient mice had reduced accumulation of con- ) in lean and obese fat was similar between wildtype and knockout mice. Adipose tissue macrophage content and inflammatory gene expression in fat did not differ between obese wild-type and knockout mice; however, major histocompatibility complex class II and CD86 expression on adipose tissue macrophages was reduced in visceral fat from knockout mice. Similar results were observed in chimeric mice with hematopoietic Cd40-deficiency. Nonetheless, neither whole body nor hematopoietic disruption of CD40 ameliorated obesityinduced insulin resistance in mice. In human adipose tissue, CD40 expression was positively correlated with CD80 and CD86 expression in obese patients with type 2 diabetes. These findings indicate that CD40 signaling in adipose tissue macrophages regulates major histocompatibility complex class II and CD86 expression to control the expansion of CD4 + T cells; however, this is largely dispensable for the development of obesity-induced inflammation and insulin resistance in mice.

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Antigen- and Cytokine-Driven Accumulation of Regulatory T Cells in Visceral Adipose Tissue of Lean Mice

Cited by 317 publications

References 31 publications

Peri-alloHCT IL-33 administration expands recipient T-regulatory cells that protect mice against acute GVHD

Peri-alloHCT IL-33 administration expands recipient T-regulatory cells that protect mice against acute GVHD

Unstable FoxP3 ⁺ T regulatory cells in NZW mice

CD40 promotes MHC class II expression on adipose tissue macrophages and regulates adipose tissue CD4+ T cells with obesity

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Antigen- and Cytokine-Driven Accumulation of Regulatory T Cells in Visceral Adipose Tissue of Lean Mice

Cited by 317 publications

References 31 publications

Peri-alloHCT IL-33 administration expands recipient T-regulatory cells that protect mice against acute GVHD

Peri-alloHCT IL-33 administration expands recipient T-regulatory cells that protect mice against acute GVHD

Unstable FoxP3 + T regulatory cells in NZW mice

CD40 promotes MHC class II expression on adipose tissue macrophages and regulates adipose tissue CD4+ T cells with obesity

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Unstable FoxP3 ⁺ T regulatory cells in NZW mice