Natural killer T-cell autoreactivity leads to a specialized activation state

Wang, Xiaohua; Chen, Xiuxu; Rodenkirch, Lance A.; Simonson, William; Wernimont, Sarah A.; Ndonye, Rachel M.; Veerapen, Natacha; Gibson, Darren; Howell, Amy R.; Besra, Gurdyal S.; Painter, Gavin F.; Huttenlocher, Anna; Gumperz, Jenny E.

doi:10.1182/blood-2008-05-157529

Cited by 38 publications

(64 citation statements)

References 51 publications

(72 reference statements)

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“…The lower-well cells were then harvested for use in the analyses described below. Because we have found that human NKT cells that are activated by recognition of auto-antigens mainly secrete GM-CSF and IL-13, whereas those that are stimulated by ␣-GalCer also secrete other cytokines (such as IFN-␥ and IL-4) that may influence monocyte differentiation [49], we compared NKT-instructed APCs in which the NKT cells were stimulated by untreated monocytes (i.e., presenting auto-antigen), with those that differentiated in response to NKT cells that were stimulated by ␣-GalCer pulsed monocytes.…”

Section: Resultsmentioning

confidence: 99%

“…We have previously found that NKT cells that are activated by recognition of auto-antigens secrete little or no IFN␥ or IL-4, whereas those that are activated by the potent agonist ␣-GalCer robustly produce these cytokines [43,49]. Since exposure to IFN-␥ has been associated with enhancing IL-12p70 production by myeloid DCs, we investigated whether the route of NKT cell activation influences the pattern of cytokine production by the resulting APCs.…”

Section: Cytokine Production By Nkt-instructed Apcsmentioning

confidence: 98%

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Human NKT cells promote monocyte differentiation into suppressive myeloid antigen-presenting cells

Hegde

Jankowska‐Gan

Roenneburg

et al. 2009

Journal of Leukocyte Biology

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NKT cells have been shown to promote peripheral tolerance in a number of model systems, yet the processes by which they exert their regulatory effects remain poorly understood. Here, we show that soluble factors secreted by human NKT cells instruct human peripheral blood monocytes to differentiate into myeloid APCs that have suppressive properties. NKT instructed monocytes acquired a cell surface phenotype resembling myeloid DCs. However, whereas control DCs that were generated by culturing monocytes with recombinant GM-CSF and IL-4 had a proinflammatory phenotype characterized by the production of IL-12 with little IL-10, NKT-instructed APCs showed the opposite cytokine production profile of high IL-10 with little or no IL-12. The control DCs efficiently stimulated peripheral blood T cell IFN-gamma secretion and proliferation, whereas NKT-instructed APCs silenced these T cell responses. Exposure to NKT cell factors had a dominant effect on the functional properties of the DCs, since DCs differentiated by recombinant GM-CSF and IL-4 in the presence of NKT cell factors inhibited T cell responses. To confirm their noninflammatory effects, NKT-instructed APCs were tested in an in vivo assay that depends on the activation of antigen-specific human T cells. Control DCs promoted substantial tissue inflammation; however, despite a marked neutrophilic infiltrate, there was little edema in the presence of NKT-instructed APCs, suggesting the inflammatory cascade was held in check. These results point to a novel pathway initiated by NKT cells that can contribute to the regulation of human antigen-specific Th1 responses.

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Section: Resultsmentioning

confidence: 99%

Section: Cytokine Production By Nkt-instructed Apcsmentioning

confidence: 98%

Human NKT cells promote monocyte differentiation into suppressive myeloid antigen-presenting cells

Hegde

Jankowska‐Gan

Roenneburg

et al. 2009

Journal of Leukocyte Biology

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“…These effects were observed with two different types of transfectants (THP-1 and C1R), excluding unique behavior associated with the nature of APCs. The differential influence on the type of released cytokines probably reflects the reported different signal strength required for secretion of GM-CSF versus IL-4 and IFN-γ (12). The presence of CD1e might influence the number and nature of CD1-antigen complexes, leading to a reduced TCR signal strength that might affect IFN-γ production more readily than that of GM-CSF.…”

Section: Discussionmentioning

confidence: 99%

“…CD1e might directly influence the number of CD1d-antigen complexes available over time, which has been shown to affect the type of cytokines released (12)(13)(14). To test this possibility, antigen-pulse experiments were performed to compare the time required for the generation of CD1d-antigen stimulatory complexes.…”

Section: Cd1e Effects On Exogenous Glycolipid Antigen Presentation Tomentioning

confidence: 99%

Fine tuning by human CD1e of lipid-specific immune responses

Facciotti

Cavallari

Angénieux

et al. 2011

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

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CD1e is a member of the CD1 family that participates in lipid antigen presentation without interacting with the T-cell receptor. It binds lipids in lysosomes and facilitates processing of complex glycolipids, thus promoting editing of lipid antigens. We find that CD1e may positively or negatively affect lipid presentation by CD1b, CD1c, and CD1d. This effect is caused by the capacity of CD1e to facilitate rapid formation of CD1-lipid complexes, as shown for CD1d, and also to accelerate their turnover. Similar results were obtained with antigen-presenting cells from CD1e transgenic mice in which lipid complexes are assembled more efficiently and show faster turnover than in WT antigen-presenting cells. These effects maximize and temporally narrow CD1-restricted responses, as shown by reactivity to Sphingomonas paucimobilis-derived lipid antigens. CD1e is therefore an important modulator of both group 1 and group 2 CD1-restricted responses influencing the lipid antigen availability as well as the generation and persistence of CD1-lipid complexes.CD1 restriction | lipid transfer proteins | natural killer T cells

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“…iNKT cells contain preformed IFN-g mRNA in their cytoplasm, which promotes immediate secretion of this cytokine on TCR stimulation at levels 200 times higher than conventional MHC-restricted CD4 þ T cells (Stetson et al 2003). This secretion of cytokines is controlled by the strength of TCR signal received during antigen recognition (Wang et al 2008), which depends on the number of CD1 complexes as well as their persistence on the surface of APCs. In addition, human NKT cells express granulysin (Gansert et al 2003) that participates in killing intracellular bacteria resident within target cells.…”

Section: Functions Of Cd1-restricted T Cells During Mycobacterial Infmentioning

confidence: 99%

Nonclassical T Cells and Their Antigens in Tuberculosis

Libero

Singhal

Lepore

et al. 2014

Cold Spring Harbor Perspectives in Medicine

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Correspondence: gennaro_delibero@immunol.a-star.edu.sg T cells that recognize nonpeptidic antigens, and thereby are identified as nonclassical, represent important yet poorly characterized effectors of the immune response. They are present in large numbers in circulating blood and tissues and are as abundant as T cells recognizing peptide antigens. Nonclassical T cells exert multiple functions including immunoregulation, tumor control, and protection against infections. They recognize complexes of nonpeptidic antigens such as lipid and glycolipid molecules, vitamin B 2 precursors, and phosphorylated metabolites of the mevalonate pathway. Each of these antigens is presented by antigen-presenting molecules other than major histocompatibility complex (MHC), including CD1, MHC class I-related molecule 1 (MR1), and butyrophilin 3A1 (BTN3A1) molecules. Here, we discuss how nonclassical T cells participate in the recognition of mycobacterial antigens and in the mycobacterial-specific immune response.T he recognition by T lymphocytes of antigenic complexes formed by antigens and antigen-presenting molecules is a hallmark of the adaptive immune system. Awide range of exogenous and endogenous antigenic molecules reflecting a variety of chemical structures have been identified and are represented by proteins, lipids, phosphorylated metabolites, or vitamin B 2 pathway metabolites. The role of classical T cells, which recognize peptidic antigens associated with MHC-encoded molecules, during Mycobacterium tuberculosis (MTB) infection is well documented and studied for a long time (Cooper 2009). On the contrary, nonclassical T cells recognizing nonpeptidic antigens associated with non-MHC antigen-presenting molecules have been described more recently. They have also been identified as important contributors to host defense against infections, although many aspects of their physiological role still remain to be discovered. Based on the restriction molecule, antigen specificity, and T-cell receptor (TCR) structure, non-MHC-restricted T cells can be grouped into three categories: lipid-and glycolipid-specific CD1-restricted T cells, mucosal-associated invariant T (MAIT) MR1-restricted cells, and TCR gd BTN3A1-restricted T cells. In this article, we review critical issues of the basic immunobiology of non-MHC-restricted T cells related to recognition of Editors:

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Natural killer T-cell autoreactivity leads to a specialized activation state

Cited by 38 publications

References 51 publications

Human NKT cells promote monocyte differentiation into suppressive myeloid antigen-presenting cells

Human NKT cells promote monocyte differentiation into suppressive myeloid antigen-presenting cells

Fine tuning by human CD1e of lipid-specific immune responses

Nonclassical T Cells and Their Antigens in Tuberculosis

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