CD1d ligation on human monocytes directly signals rapid NF-κB activation and production of bioactive IL-12

Yue, Simon; Shaulov, Angela; Wang, Ruojie; Balk, Steven P.; Exley, Mark A.

doi:10.1073/pnas.0503366102

Cited by 88 publications

(105 citation statements)

References 38 publications

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“…CD62L + NKT cells may be CD1d dependent [38]. It is also notable that our results do not completely rule out the possibility that CD1d blocking antibody may also trigger CD1d, and thus in some way promote inflammatory responses in the gut, especially through CD1d ligation on monocytes, which could enhance inflammation via induction of IL-12 [39]. However, previously published data indicate that CD1d cross-linking on epithelial cells leads rather to the production of barrier-enhancing and immunoregulatory cytokines [40].…”

Section: Discussionmentioning

confidence: 75%

DX5⁺NKT cells induce the death of colitis‐associated cells: involvement of programmed death ligand‐1

et al. 2006

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+ NKT cells induced cell death of colon-infiltrating lymphocytes isolated from diseased mice. This effect was inhibited in the presence of either anti-CD1d or anti-programmed death ligand-1 (PD-L1) blocking antibodies. The specific potency of DX5 + NKT cells in regulating chronic colitis in two mouse models is demonstrated. In vitro testing suggests that DX5 + NKT cells activated by CD1d induce cell death of colitis-inducing lymphocytes, which is mediated through PD-L1. Therefore, DX5+ NKT cells could be important in the regulation of immune responses associated with chronic colitis.

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Section: Discussionmentioning

confidence: 75%

DX5⁺NKT cells induce the death of colitis‐associated cells: involvement of programmed death ligand‐1

et al. 2006

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“…Similar to other restriction molecules, CD1d plays additional biological functions, including cell signaling. In fact, several studies demonstrated that CD1d ligation produces activating signals within human monocytes and intestinal intraepithelial cells (60,64). We demonstrated that the CD1d engagement alone produced a tolerogenic signal and induced IL-10 release by immature DCs.…”

Section: Discussionmentioning

confidence: 82%

“…However, we cannot exclude that, in vivo, iNKT cells with a strongly biased cytokine profile preferentially induce either protolerogenic or proinflammatory DC maturation. For example, high levels of IFN-g and IL-12 released by adjuvant iNKT cells could synergize with the maturation signal transmitted by iNKT cells through cell-cell contact and favor proinflammatory DC maturation (60).…”

Section: Discussionmentioning

confidence: 99%

On/Off TLR Signaling Decides Proinflammatory or Tolerogenic Dendritic Cell Maturation upon CD1d-Mediated Interaction with Invariant NKT Cells

Conforti-Andreoni

Pietro

Usuelli

et al. 2010

The Journal of Immunology

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Invariant NKT (iNKT) cells play an effector/adjuvant function during antimicrobial and antitumoral immunity and a regulatory role to induce immune tolerance and prevent autoimmunity. iNKT cells that differentially modulate adaptive immunity do not bear a unique phenotype and/or specific cytokine secretion profile, thus opening questions on how a single T cell subset can exert opposite immunological tasks. In this study, we show that iNKT cells perform their dual roles through a single mechanism of action relying on the cognate interaction with myeloid dendritic cells (DCs) and leading to opposite effects depending on the presence of other maturation stimuli simultaneously acting on DCs. The contact of murine purified iNKT cells with immature autologous DCs directly triggers the tolerogenic maturation of DCs, rendering them able to induce regulatory T cell differentiation and prevent autoimmune diabetes in vivo. Conversely, the interaction of the same purified iNKT cells with DCs, in the presence of simultaneous TLR4 stimulation, significantly enhances proinflammatory DC maturation and IL-12 secretion. The different iNKT cell effects are mediated through distinct mechanisms and activation of different molecular pathways within the DC: CD1d signaling and activation of the ERK1/2 pathway for the tolerogenic action, and CD40–CD40L interaction and NF-κB activation for the adjuvant effect. Our data suggest that the DC decision to undergo proinflammatory or tolerogenic maturation results from the integration of different signals received at the time of iNKT cell contact and could have important therapeutic implications for exploiting iNKT cell adjuvant/regulatory properties in autoimmune diseases, infections, and cancer.

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“…Cd1d Ϫ/Ϫ C57BL/6 mice were previously reported to have an increased bacterial burden and joint inflammation after syringe infection with B. burgdorferi (30). However, T cells with more diverse TCRs also recognize CD1d; also, CD1d has been reported to have a signaling function that may be independent of T lymphocyte activity (33,34). In fact, in several experimental systems (35)(36)(37), analysis of Cd1d Ϫ/Ϫ and J␣18 Ϫ/Ϫ mice gave discordant results, suggesting either a role for CD1d-reactive T cells with more diverse TCRs or another function for CD1d besides antigen presentation.…”

Section: Discussionmentioning

confidence: 99%

NKT cells prevent chronic joint inflammation after infection withBorrelia burgdorferi

Tupin

Benhnia

Kinjo

et al. 2008

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

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Borrelia burgdorferi is the etiologic agent of Lyme disease, a multisystem inflammatory disorder that principally targets the skin, joints, heart, and nervous system. The role of T lymphocytes in the development of chronic inflammation resulting from B. burgdorferi infection has been controversial. We previously showed that natural killer T (NKT) cells with an invariant (i) TCR ␣ chain (iNKT cells) recognize glycolipids from B. burgdorferi, but did not establish an in vivo role for iNKT cells in Lyme disease pathogenesis. Here, we evaluate the importance of iNKT cells for host defense against these pathogenic spirochetes by using V␣14i NKT cell-deficient (J␣18 ؊/؊ ) BALB/c mice. On tick inoculation with B. burgdorferi, J␣18 ؊/؊ mice exhibited more severe and prolonged arthritis as well as a reduced ability to clear spirochetes from infected tissues. V␣14i NKT cell deficiency also resulted in increased production of antibodies directed against both B. burgdorferi protein antigens and borrelial diacylglycerols; the latter finding demonstrates that anti-glycolipid antibody production does not require cognate help from V␣14i NKT cells. V␣14i NKT cells in infected wild-type mice expressed surface activation markers and produced IFN␥ in vivo after infection, suggesting a participatory role for this unique population in cellular immunity. Our data are consistent with the hypothesis that the antigen-specific activation of V␣14i NKT cells is important for the prevention of persistent joint inflammation and spirochete clearance, and they counter the long-standing notion that humoral rather than cellular immunity is sufficient to facilitate Lyme disease resolution.cytokines ͉ glycolipids ͉ Lyme disease ͉ spirochetes

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CD1d ligation on human monocytes directly signals rapid NF-κB activation and production of bioactive IL-12

Cited by 88 publications

References 38 publications

DX5⁺NKT cells induce the death of colitis‐associated cells: involvement of programmed death ligand‐1

DX5⁺NKT cells induce the death of colitis‐associated cells: involvement of programmed death ligand‐1

On/Off TLR Signaling Decides Proinflammatory or Tolerogenic Dendritic Cell Maturation upon CD1d-Mediated Interaction with Invariant NKT Cells

NKT cells prevent chronic joint inflammation after infection withBorrelia burgdorferi

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CD1d ligation on human monocytes directly signals rapid NF-κB activation and production of bioactive IL-12

Cited by 88 publications

References 38 publications

DX5+NKT cells induce the death of colitis‐associated cells: involvement of programmed death ligand‐1

DX5+NKT cells induce the death of colitis‐associated cells: involvement of programmed death ligand‐1

On/Off TLR Signaling Decides Proinflammatory or Tolerogenic Dendritic Cell Maturation upon CD1d-Mediated Interaction with Invariant NKT Cells

NKT cells prevent chronic joint inflammation after infection withBorrelia burgdorferi

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DX5⁺NKT cells induce the death of colitis‐associated cells: involvement of programmed death ligand‐1

DX5⁺NKT cells induce the death of colitis‐associated cells: involvement of programmed death ligand‐1