Recognition of microbial glycolipids by Natural Killer T cells

T cells can recognize microbial antigens when presented by dedicated antigen-presenting molecules. While peptides are presented by classical members of the Major Histocompatibility (MHC) family (MHC I and II), lipids, glycolipids and lipopeptides can be presented by the non-classical MHC member CD1....

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Main Authors: Dirk Michael Zajonc, Enrico eGirardi
Format: Article
Language:English
Published: Frontiers Media S.A. 2015-08-01
Series:Frontiers in Immunology
Subjects:
tcr
Online Access:http://journal.frontiersin.org/Journal/10.3389/fimmu.2015.00400/full
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spelling doaj-17ca9817b55b4154bafe3d6621ced1a32020-11-24T23:26:24ZengFrontiers Media S.A.Frontiers in Immunology1664-32242015-08-01610.3389/fimmu.2015.00400155589Recognition of microbial glycolipids by Natural Killer T cellsDirk Michael Zajonc0Enrico eGirardi1La Jolla Institute for Allergy and ImmunologyLa Jolla Institute for Allergy and ImmunologyT cells can recognize microbial antigens when presented by dedicated antigen-presenting molecules. While peptides are presented by classical members of the Major Histocompatibility (MHC) family (MHC I and II), lipids, glycolipids and lipopeptides can be presented by the non-classical MHC member CD1. The best studied subset of lipid-reactive T cells are Type I Natural killer T (iNKT) cells that recognize a variety of different antigens when presented by the non-classical MHCI homolog CD1d. iNKT cells have been shown to be important for the protection against various microbial pathogens, including B. burgdorferi the causative agents of Lyme disease and S. pneumoniae, which causes pneumococcal meningitis and community-acquired pneumonia. Both pathogens carry microbial glycolipids that can trigger the T cell antigen receptor (TCR), leading to iNKT cell activation. iNKT cells have an evolutionary conserved TCR alpha chain, yet retain the ability to recognize structurally diverse glycolipids. They do so using a conserved recognition mode, in which the TCR enforces a conserved binding orientation on CD1d. TCR binding is accompanied by structural changes within the TCR binding site of CD1d, as well as the glycolipid antigen itself. In addition to direct recognition of microbial antigens, iNKT cells can also be activated by a combination of cytokines (IL-12/IL-18) and TCR stimulation. Many microbes carry TLR antigens and microbial infections can lead to TLR activation. The subsequent cytokine response in turn lower the threshold of TCR mediated iNKT cell activation, especially when weak microbial or even self-antigens are presented during the cause of the infection. In summary, iNKT cells can be directly activated through TCR triggering of strong antigens, while cytokines produced by the innate immune response may be necessary for TCR triggering and iNKT cell activation in the presence of weak antigens. Here we will review the molecular basis of iNKT cell recognition of glychttp://journal.frontiersin.org/Journal/10.3389/fimmu.2015.00400/fullGlycolipidstcrMicrobesNKT cellsantigen-presentationCD1d
collection DOAJ
language English
format Article
sources DOAJ
author Dirk Michael Zajonc
Enrico eGirardi
spellingShingle Dirk Michael Zajonc
Enrico eGirardi
Recognition of microbial glycolipids by Natural Killer T cells
Frontiers in Immunology
Glycolipids
tcr
Microbes
NKT cells
antigen-presentation
CD1d
author_facet Dirk Michael Zajonc
Enrico eGirardi
author_sort Dirk Michael Zajonc
title Recognition of microbial glycolipids by Natural Killer T cells
title_short Recognition of microbial glycolipids by Natural Killer T cells
title_full Recognition of microbial glycolipids by Natural Killer T cells
title_fullStr Recognition of microbial glycolipids by Natural Killer T cells
title_full_unstemmed Recognition of microbial glycolipids by Natural Killer T cells
title_sort recognition of microbial glycolipids by natural killer t cells
publisher Frontiers Media S.A.
series Frontiers in Immunology
issn 1664-3224
publishDate 2015-08-01
description T cells can recognize microbial antigens when presented by dedicated antigen-presenting molecules. While peptides are presented by classical members of the Major Histocompatibility (MHC) family (MHC I and II), lipids, glycolipids and lipopeptides can be presented by the non-classical MHC member CD1. The best studied subset of lipid-reactive T cells are Type I Natural killer T (iNKT) cells that recognize a variety of different antigens when presented by the non-classical MHCI homolog CD1d. iNKT cells have been shown to be important for the protection against various microbial pathogens, including B. burgdorferi the causative agents of Lyme disease and S. pneumoniae, which causes pneumococcal meningitis and community-acquired pneumonia. Both pathogens carry microbial glycolipids that can trigger the T cell antigen receptor (TCR), leading to iNKT cell activation. iNKT cells have an evolutionary conserved TCR alpha chain, yet retain the ability to recognize structurally diverse glycolipids. They do so using a conserved recognition mode, in which the TCR enforces a conserved binding orientation on CD1d. TCR binding is accompanied by structural changes within the TCR binding site of CD1d, as well as the glycolipid antigen itself. In addition to direct recognition of microbial antigens, iNKT cells can also be activated by a combination of cytokines (IL-12/IL-18) and TCR stimulation. Many microbes carry TLR antigens and microbial infections can lead to TLR activation. The subsequent cytokine response in turn lower the threshold of TCR mediated iNKT cell activation, especially when weak microbial or even self-antigens are presented during the cause of the infection. In summary, iNKT cells can be directly activated through TCR triggering of strong antigens, while cytokines produced by the innate immune response may be necessary for TCR triggering and iNKT cell activation in the presence of weak antigens. Here we will review the molecular basis of iNKT cell recognition of glyc
topic Glycolipids
tcr
Microbes
NKT cells
antigen-presentation
CD1d
url http://journal.frontiersin.org/Journal/10.3389/fimmu.2015.00400/full
work_keys_str_mv AT dirkmichaelzajonc recognitionofmicrobialglycolipidsbynaturalkillertcells
AT enricoegirardi recognitionofmicrobialglycolipidsbynaturalkillertcells
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