2009
DOI: 10.1182/blood-2008-12-195354
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Indoleamine 2,3-dioxygenase controls conversion of Foxp3+ Tregs to TH17-like cells in tumor-draining lymph nodes

Abstract: IntroductionRegulatory T cells (Tregs) represent a critical barrier to immunotherapy of tumors. Established tumors suppress immune responses against their own antigens, and Tregs are emerging as a key mechanism contributing to this state of functional unresponsiveness. 1 In murine models, host Tregs become activated within days of tumor implantation. 2 Once activated, Tregs are difficult to eliminate and serve to potently and dominantly inhibit otherwise effective immune responses against the tumor. 3 We have … Show more

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Cited by 367 publications
(368 citation statements)
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“…It has been proposed that IL-17-mediated inflammation is tumor-promoting during the initial phase of tumor growth, whereas Th17 cells are anti-tumorigenic in established tumors (Wilke et al, 2011). The biological relevance of FoxP3 þ IL-17 þ converted Treg cells or Th17 matured CD4 þ cells is supported by studies with tumor models, where these cells can induce anti-tumor CD8 þ T-cell responses (Martin-Orozco et al, 2009;Sharma et al, 2009Sharma et al, , 2010. In the absence of CD200 signaling, we demonstrate that FoxP3 þ IL-17 þ are more frequent in skin-draining LNs.…”
Section: Cd200-cd200r Signaling In Tumorigenesismentioning
confidence: 99%
“…It has been proposed that IL-17-mediated inflammation is tumor-promoting during the initial phase of tumor growth, whereas Th17 cells are anti-tumorigenic in established tumors (Wilke et al, 2011). The biological relevance of FoxP3 þ IL-17 þ converted Treg cells or Th17 matured CD4 þ cells is supported by studies with tumor models, where these cells can induce anti-tumor CD8 þ T-cell responses (Martin-Orozco et al, 2009;Sharma et al, 2009Sharma et al, , 2010. In the absence of CD200 signaling, we demonstrate that FoxP3 þ IL-17 þ are more frequent in skin-draining LNs.…”
Section: Cd200-cd200r Signaling In Tumorigenesismentioning
confidence: 99%
“…58 Furthermore, treatment with adoptive T-cell transfer can result in synergistic anti-neoplastic effects owing to the increased immunogenicity of cancer cells. 59 Yet, for all these antitumor effects, there appears to be a balance between anti-and pro-tumor effects by both CD4 þ and CD8 þ T cells, [60][61][62] and regulatory T cells can migrate into the microenvironment and suppress antitumor responses in human ovarian carcinoma. 63 Considering the variable effects of this multitude of stromal cell and immune response interactions, the mechanism by which p53 deficiency in MSCs affects T-cell function in tumors warrants further exploration.…”
Section: Discussionmentioning
confidence: 99%
“…Engagement of several receptors, including CD80/CD86, or TLR9 59 , participates in active IDO induction. Amino acid withdrawal resulting from IDO enzymatic activity, stimulates the GCN2 kinase in PDC and then prevents IL-6 secretion by PDC 9 . Moreover, IDO exerts a regulatory function independently of its catabolic activity by participating in TGF-β-signaling pathway 60 .…”
Section: The Innate Immune Functions Of Plasmacytoid Dendritic Cellsmentioning
confidence: 99%
“…Finally, concerning amino acid metabolism, PDC are able to sense amino acid deficiency through their expression of GCN2 (general control nonderepressible 2) serine/threonine kinase. Indeed, the suppression of interleukin (IL)-6 production in PDC by indoleamine 2,3-dioxygenase (IDO) involves GCN2 kinase 9 (see section 2.3).…”
Section: Introductionmentioning
confidence: 99%