Polyclonal type II natural killer T cells require PLZF and SAP for their development and contribute to CpG-mediated antitumor response

Zhao, Jie; Weng, Xiufang; Bagchi, Sreya; Wang, Chyung Ru

doi:10.1073/pnas.1323845111

Cited by 61 publications

(89 citation statements)

References 55 publications

(50 reference statements)

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“…21 However, recent studies using sulfatide-reactive type II NKT cell hybridoma XV19 and Ja18-deficient IL-4 reporter mice report recognition of b-GlcCer (12:0 and 24:1) by murine type II NKT cells. 24,26 In contrast to initial findings from Brennan et al, our data pointed to b-glucosylceramide as a ligand for type II as opposed to type I NKT cells. Recent studies have attributed Brennan's initial findings to a contaminating minor lipid species, consistent with endogenous a-linked glucosylceramide.…”

Section: Discussionmentioning

(Expert classified)

“…In addition to its well-documented role in type I NKT cells, PLZF was recently implicated in the differentiation of type II NKT cells as well. 26,57 Crosstalk between type I and II NKT cells is increasingly implicated in the regulation of immunity to pathogens, tumors, and autoimmunity. 5,7,50,58 The mechanism underlying the crosstalk between NKT subsets requires further study and may be more prominent with specific ligands.…”

Section: Discussionmentioning

confidence: 99%

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Type II NKT-TFH cells against Gaucher lipids regulate B-cell immunity and inflammation

Nair¹,

Boddupalli²,

Verma³

et al. 2015

Blood

116

130

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Key Points• A new subset of human and murine type II NKT-T FH cells against Gaucher lipids that regulate B-cell immunity.• A novel pathway for B-cell help providing a mechanism underlying chronic B-cell activation and gammopathy in metabolic lipid disorders.Chronic inflammation including B-cell activation is commonly observed in both inherited (Gaucher disease [GD]) and acquired disorders of lipid metabolism. However, the cellular mechanisms underlying B-cell activation in these settings remain to be elucidated. Here, we report that b-glucosylceramide 22:0 (bGL1-22) and glucosylsphingosine (LGL1), 2 major sphingolipids accumulated in GD, can be recognized by a distinct subset of CD1d-restricted human and murine type II natural killer T (NKT) cells. Human bGL1-22-and LGL1-reactive CD1d tetramer-positive T cells have a distinct T-cell receptor usage and genomic and cytokine profiles compared with the classical type I NKT cells. In contrast to type I NKT cells, bGL1-22-and LGL1-specific NKT cells constitutively express T-follicular helper (T FH ) phenotype. Injection of these lipids leads to an increase in respective lipidspecific type II NKT cells in vivo and downstream induction of germinal center B cells, hypergammaglobulinemia, and production of antilipid antibodies. Human bGL1-22-and LGL1-specific NKT cells can provide efficient cognate help to B cells in vitro. Frequency of LGL1-specific T cells in GD mouse models and patients correlates with disease activity and therapeutic response. Our studies identify a novel type II NKT-mediated pathway for glucosphingolipid-mediated dysregulation of humoral immunity and increased risk of B-cell malignancy observed in metabolic lipid disorders. (Blood. 2015;125(8):1256-1271

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Section: Discussionmentioning

(Expert classified)

Section: Discussionmentioning

confidence: 99%

Type II NKT-TFH cells against Gaucher lipids regulate B-cell immunity and inflammation

Nair¹,

Boddupalli²,

Verma³

et al. 2015

Blood

116

130

View full text Add to dashboard Cite

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“…Unlike both types of CD1d-restricted NKT cells, which are activated by b-linked glycosphingolipids, HJ1 T cells were not activated by sphingolipids. 22,[41][42][43] A recent study also suggests that mammalian a-linked glycosphingolipids can activate type I NKT cells. 44 Although ether-linked forms of pLPE and lysophaphatidic have been implicated in the selection of type I NKT cells, nothing is known about the selecting self-lipids for type II NKT cells and group 1 CD1-reactive T cells.…”

Section: Discussionmentioning

confidence: 98%

“…[18][19][20][21] Interestingly, a previous study showed that the immunosuppressive effect of type II NKT cells is reversed in the presence of CpG oligodeoxynucleotides (ODN), a TLR 9 agonist, leading to an increased ratio of IFNg to IL-13 production. 22 These data suggested that CD1d-restricted NKT cells could potentially be used in adoptive immunotherapy to treat tumors.…”

Section: Introductionmentioning

confidence: 96%

CD1b-autoreactive T cells recognize phospholipid antigens and contribute to antitumor immunity against a CD1b⁺T cell lymphoma

Bagchi

Wang

2016

OncoImmunology

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Adoptive immunotherapy for cancer treatment is an emerging field of study. Till now, several tumorderived, peptide-specific T cell responses have been harnessed for treating cancers. However, the contribution of lipid-specific T cells in tumor immunity has been understudied. CD1 molecules, which present self-and foreign lipid antigens to T cells, are divided into group 1 (CD1a, CD1b, and CD1c) and group 2 (CD1d). Although the role of CD1d-restricted natural killer T cells (NKT) in several tumor models has been well established, the contribution of group 1 CD1-restricted T cells in tumor immunity remains obscure due to the lack of group 1 CD1 expression in mice. In this study, we used a double transgenic mouse model expressing human group 1 CD1 molecules (hCD1Tg) and a CD1b-restricted, self-lipid reactive T cell receptor (HJ1Tg) to study the potential role of group 1 CD1-restricted autoreactive T cells in antitumor response. We found that HJ1 T cells recognized phospholipids and responded more potently to lipid extracted from tumor cells than the equivalent amount of lipids extracted from normal cells. Additionally, the autoreactivity of HJ1 T cells was enhanced upon treatment with various intracellular tolllike receptor (TLR) agonists, including CpG oligodeoxynucleotides (ODN), R848, and poly (I:C). Interestingly, the adoptive transfer of HJ1 T cells conferred protection against the CD1b-transfected murine T cell lymphoma (RMA-S/CD1b) and CpG ODN enhanced the antitumor effect. Thus, this study, for the first time, demonstrates the antitumor potential of CD1b-autoreactive T cells and their potential use in adoptive immunotherapy.

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“…While it has become clear that TLR signalling events upregulate presentation of endogenous lipids, which can then activate iNKT cells [17,18], the identity of such self-lipids capable of modulating iNKT cell auto-reactivity remains elusive (reviewed in [23]). In contrast to iNKT cells, due to limited reagents for type II NKT cell identification, the antigenic specificity of type II NKT cells is only just beginning to emerge; reactivity has been observed with sulfatide [24], lysophospholipids [25,26], and more recently with b-D-glucopyranosylceramide (b-GlcCer) and its deacylated product, glucosylsphingosine (LGL1), which are presented in Gaucher disease patients [27][28][29].…”

Section: Introductionmentioning

confidence: 99%

CD1d-dependent endogenous and exogenous lipid antigen presentation

McEwen-Smith

Salio

Cerundolo

2015

Current Opinion in Immunology

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Polyclonal type II natural killer T cells require PLZF and SAP for their development and contribute to CpG-mediated antitumor response

Cited by 61 publications

References 55 publications

Type II NKT-TFH cells against Gaucher lipids regulate B-cell immunity and inflammation

Type II NKT-TFH cells against Gaucher lipids regulate B-cell immunity and inflammation

CD1b-autoreactive T cells recognize phospholipid antigens and contribute to antitumor immunity against a CD1b⁺T cell lymphoma

CD1d-dependent endogenous and exogenous lipid antigen presentation

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Polyclonal type II natural killer T cells require PLZF and SAP for their development and contribute to CpG-mediated antitumor response

Cited by 61 publications

References 55 publications

Type II NKT-TFH cells against Gaucher lipids regulate B-cell immunity and inflammation

Type II NKT-TFH cells against Gaucher lipids regulate B-cell immunity and inflammation

CD1b-autoreactive T cells recognize phospholipid antigens and contribute to antitumor immunity against a CD1b+T cell lymphoma

CD1d-dependent endogenous and exogenous lipid antigen presentation

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CD1b-autoreactive T cells recognize phospholipid antigens and contribute to antitumor immunity against a CD1b⁺T cell lymphoma