Human Invariant NKT Cell Subsets Differentially Promote Differentiation, Antibody Production, and T Cell Stimulation by B Cells In Vitro

Zeng, Shijuan Grace; Ghnewa, Yasmeen G.; O’Reilly, Vincent; Lyons, Victoria; Atzberger, Ann; Hogan, Andrew E.; Exley, Mark A.; Doherty, Derek G.

doi:10.4049/jimmunol.1202223

Cited by 43 publications

(52 citation statements)

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“…This finding was later confirmed using fresh human iNKT cells [180]. In our own work, we investigated the effects of co-culturing expanded human CD4 + , CD8a + and CD4 À CD8a À iNKT cells with autologous peripheral B cells in vitro and found that all iNKT cell subsets induced IgM, IgA and IgG release by B cells by a mechanism that required CD1d but not added glycolipid, such as a-GC [181]. All iNKT cell subsets induced the expression of CD40, CD86 and HLA-DR by B cells, but iNKT cell-matured B cells were less able to drive proliferation of autologous and alloreactive conventional T cells than B cells cultured in the absence of iNKT cells.…”

Section: Other Unconventional T Cells Bridging Innate and Adaptive Immentioning

confidence: 79%

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Human Vγ9/Vδ2 T cells: Innate adaptors of the immune system

Tyler

Doherty

Moser

et al. 2015

Cellular Immunology

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a b s t r a c tUnconventional T cells are gaining center stage as important effector and regulatory cells that orchestrate innate and adaptive immune responses. Human Vc9/Vd2 T cells are amongst the best understood unconventional T cells, as they are easily accessible in peripheral blood, can readily be expanded and manipulated in vitro, respond to microbial infections in vivo and can be exploited for novel tumor immunotherapies. We here review findings that suggest that Vc9/Vd2 T cells, and possibly other unconventional human T cells, play an important role in bridging innate and adaptive immunity by promoting the activation and differentiation of various types of antigen-presenting cells (APCs) and even turning into APCs themselves, and thereby pave the way for antigen-specific effector responses and long-term immunological memory. Although the direct physiological relevance for most of these mechanisms still needs to be demonstrated in vivo, these findings may have implications for novel therapies, diagnostic tests and vaccines.Ó 2015 Published by Elsevier Inc. Introduction cd T cells represent a third lineage of lymphocytes expressingre-arranged antigen receptors that co-evolved with 'classical' B cells and ab T cells over 400 million years, arguing for a crucial and non-redundant contribution of each lymphocyte to effective immune responses, and hence the evolutionary survival of all jawed vertebrate species [1]. 30 years have passed since the accidental and unexpected cloning of the cd T cell receptor (TCR) and the subsequent realization that ab T cells and cd T cells are fundamentally different with respect to the types of antigens they recognize and the distinct effector functions triggered upon such recognition. However, the manifold contributions of cd T cells to homeostasis, inflammation, infection and tumor surveillance have historically been neglected and are only beginning to be integrated into comprehensive models of the immune system [1][2][3][4][5][6][7].1. Innate-like pattern recognition by human Vc9/Vd2 T cells Like other 'unconventional' T cells carrying an ab TCR such as mucosal-associated invariant T (MAIT) cells and natural killer T (NKT) cells, cd T cells are characterized by a markedly restrictedTCR usage that allows them to recognize self and non-self molecules in the absence of classical antigen presentation via MHC I or MHC II. Vc9/Vd2 + cd T cells represent the major cd T cell subset in human peripheral blood where they typically comprise 1-5% in healthy adults [8]. In many microbial infections, Vc9/Vd2 T cells increase locally and/or systemically [9,10] and can reach in excess of 50% of all peripheral T cells within a matter of days [11], revealing a fundamental role of this unconventional T cell population in acute disease and suggesting their exploitation for diagnostic and therapeutic purposes [12][13][14]. Vc9/Vd2 T cells uniformly respond to a class of low molecular weight molecules often referred to as 'phosphoantigens' that represent metabolites of the isoprenoid biosynthesis...

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Section: Other Unconventional T Cells Bridging Innate and Adaptive Immentioning

confidence: 79%

“…Additionally, CD4 + iNKT cells induced expansions of cells with phenotypes of regulatory B cells. Therefore, human iNKT cell subsets may differentially promote and regulate antibody production and T cell activation by B cells [181].…”

Section: Other Unconventional T Cells Bridging Innate and Adaptive Immentioning

confidence: 99%

Human Vγ9/Vδ2 T cells: Innate adaptors of the immune system

Tyler

Doherty

Moser

et al. 2015

Cellular Immunology

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“…13,14 iNKT cells are a small but critical T-cell population involved in the B-cell response to glycolipid antigens via CD1d, a major histocompatibility complex-like molecule. 14 iNKT cells promote B-cell proliferation, B memory responsiveness, plasma cell generation and antibody production.…”

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confidence: 99%

“…14 iNKT cells promote B-cell proliferation, B memory responsiveness, plasma cell generation and antibody production. 14,15 Their relative absence in common variable immunodeficiency may contribute to both B-cell defects and hypogammaglobulinemia. Recent studies suggest that iNKT can stimulate B-cell proliferation and antibody production through cell-cell contact, probably due to the expression of stimulatory glycolipid self-antigens on B cells.…”

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confidence: 99%

“…Recent studies suggest that iNKT can stimulate B-cell proliferation and antibody production through cell-cell contact, probably due to the expression of stimulatory glycolipid self-antigens on B cells. 14,15 Recently, iNKT cells were identified as necessary for the development of allo-anti-A formation in a murine mouse model. 16 Tazawa et al 16 were able to induce high-titer anti-A in wild-type mice after repeated injections with group A human red cells, whereas little or no anti-A was observed in nude mice, which are deficient in iNKT cells.…”

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ABO, alemtuzumab and allogeneic transplantation

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Bone Marrow Transplant

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Immunological Evaluation of Co‐Assembling a Lipidated Peptide Antigen and Lipophilic Adjuvants: Self‐Adjuvanting Anti‐Breast‐Cancer Vaccine Candidates

et al. 2020

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Co‐assembling vaccines composed of a lipidated HER2‐derived antigenic CH401 peptide and either a lipophilic adjuvant, Pam3CSK4, α‐GalCer, or lipid A 506, were evaluated as breast cancer vaccine candidates. This vaccine design was aimed to inherit both antigen multivalency and antigen‐specific immunostimulation properties, observed in reported self‐adjuvanting vaccine candidates, by using self‐assembly and adjuvant‐conjugated antigens. Under vaccination concentrations, respective lipophilic adjuvants underwent co‐assembly with lipidated CH401, which boosted the anti‐CH401 IgG and IgM production. In particular, α‐GalCer was responsible for the most significant immune activation. Therefore, the newly developed vaccine design enabled the optimization of adjuvants against the antigenic CH401 peptide in a simple preparatory manner. Overall, the co‐assembling vaccine design opens the door for efficient and practical self‐adjuvanting vaccine development.

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Human Invariant NKT Cell Subsets Differentially Promote Differentiation, Antibody Production, and T Cell Stimulation by B Cells In Vitro

Cited by 43 publications

References 58 publications

Human Vγ9/Vδ2 T cells: Innate adaptors of the immune system

Human Vγ9/Vδ2 T cells: Innate adaptors of the immune system

ABO, alemtuzumab and allogeneic transplantation

Immunological Evaluation of Co‐Assembling a Lipidated Peptide Antigen and Lipophilic Adjuvants: Self‐Adjuvanting Anti‐Breast‐Cancer Vaccine Candidates

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