Blocking and Redistribution ("Capping") of Antigen Receptors on T and B Lymphocytes by Anti-Immunoglobulin Antibody

Roelants, Georges E.; Forni, Luciana; Pernis, Benvenuto

doi:10.1084/jem.137.4.1060

Cited by 87 publications

(39 citation statements)

References 33 publications

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“…The following peptides were all synthesized using 9-fluorenylmethoxycarbonyl chemistry and verified using mass spectrometry: SIY (SIYRYYGL) found from a combinatorial library to activate the 2C TCR in complex with H2-K b (22); OVA (SIINFEKL) derived from OVA; QL9 (QLSPFPFDL) modified from an endogenous murine peptide presented on H2-L d ; influenza hemagglutinin (HA) 3 (PKYVKQNTLKLAT); and A2 (VGSDWRFLRGYHQYA) derived from the human class I MHC allele HLA-A2. For use in direct treatment of T cells or in making soluble class II MHCs, the peptides were purified using reverse-phase HPLC; crude peptide was used for refolding into soluble class I MHCs.…”

Section: Materials and Peptidesmentioning

confidence: 99%

“…However, despite much work in this area, the specific molecular event that is detected by the T cell upon Ag-specific TCR engagement has been difficult to identify. In other immune cells such as B cells or mast cells in which the Ag recognized is a soluble particle, multivalent receptor engagement has been observed to be crucial for stimulation (1)(2)(3). Conversely, T cells are triggered by antigenic stimuli presented on the surface of another cell, and the specific interaction is accompanied by a multitude of non-Ag-specific interactions including: binding of adhesion molecules, engagement of costimulatory receptors, possible contributions of nonstimulatory MHC-peptide complexes, and MHC coreceptor binding.…”

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confidence: 99%

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CD8 T Cells, Like CD4 T Cells, Are Triggered by Multivalent Engagement of TCRs by MHC-Peptide Ligands but Not by Monovalent Engagement

Stone

Stern

2006

The Journal of Immunology

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T cell activation is initiated by recognition of antigenic peptide presented in complex with MHC molecules on the surface of APCs. The mechanism by which this recognition occurs is still unclear, and many models exist in the literature. CD4 T cells have been shown to respond to soluble oligomers of activating class II MHC-peptide complexes, but not to soluble monomers. In determining the reactivity of CD8 T cells to soluble activating class I MHC-peptide complexes, a complicating phenomenon had been observed whereby peptide from soluble complexes was loaded onto cell surface MHCs on the T cells and re-presented to other T cells, clouding the true valency requirement for activation. This study uses soluble allogeneic class I MHC-peptide monomers and oligomers to stimulate murine CD8 T cells without the possible complication of peptide re-presentation. The results show that MHC class I monomers bind to, but do not activate, CD8 T cells whether the cells are in solution or adhered to a surface. Monomeric MHC class I binding can antagonize the stimulation triggered by soluble oligomers, a phenomenon also observed for CD4 T cells. Dimeric engagement is necessary and sufficient to stimulate downstream activation processes including TCR down-regulation, Zap70 phosphorylation, and CD25 and CD69 up-regulation, even in T cells that do not express the MHC coreceptor CD8. Thus, the valency dependence of the response of CD8 T cells to soluble MHC-peptide reagents is the same as previously observed for CD4 T cells.

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Section: Materials and Peptidesmentioning

confidence: 99%

mentioning

confidence: 99%

CD8 T Cells, Like CD4 T Cells, Are Triggered by Multivalent Engagement of TCRs by MHC-Peptide Ligands but Not by Monovalent Engagement

Stone

Stern

2006

The Journal of Immunology

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“…Antigen binding to T cells has been measured indirectly by exposing cells in vitro to [12~I]-antigen of high specific activity with subsequent killing or "suicide" of the specific antigen-binding T lymphocytes (9). More recently, theta-positive, surface immunoglobulin-negative antigen-binding cells have been visualized directly after incubation of primed mouse spleen cells with relatively high concentrations of 125I-labeled antigen (10) and by the cytoadherence techniques (11).…”

Section: (From the Laboratory Of Clinical Investigation And The Labormentioning

confidence: 99%

Function of Macrophages in Antigen Recognition by Guinea Pig T Lymphocytes

Rosenthal

Shevach

1973

The Journal of Experimental Medicine

954

129

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Antigen activation of DNA synthesis in immune thymus-derived lymphocytes of guinea pigs requires the cooperation of macrophages and lymphocytes. We have investigated the role of histocompatibility determinants in this macrophage-lymphocyte interaction using cells from inbred strain 2 and 13 guinea pigs. The data demonstrate that efficient presentation of macrophage-associated antigen to the lymphocyte requires identity between macrophage and lymphocyte at some portion of the major histocompatibility complex. The failure of allogeneic macrophages to effectively initiate immune lymphocyte proliferation was not the result of the presence of an inhibitor of blastogenesis released in mixtures of allogeneic cells, peculiarities of the antigen or lymphoid cells employed, nor differing kinetics of activation by allogeneic macrophages. In addition, data were presented that demonstrated that alloantisera inhibit lymphocyte DNA synthesis by functional interference with macrophage-lymphocyte interaction.

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“…This concept arose largely from observations of antigen-induced capping of surface immunoglobulins on B cells (1,2) and multivalent antigen triggering of histamine release from mast cells (3). Whether multivalent engagement of T cell antigen receptors (TCR) is required to initiate T cell activation has been difficult to determine, primarily because the antigens are peptide-MHC complexes normally found as integral membrane proteins on the surfaces of other cells.…”

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confidence: 99%

Soluble peptide–MHC monomers cause activation of CD8⁺T cells through transfer of the peptide to T cell MHC molecules

Stone

Thompson

et al. 2002

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

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T cell receptor (TCR)-mediated activation of CD4 ؉ T cells is known to require multivalent engagement of the TCR by, for example, oligomeric peptide-MHC complexes. In contrast, for CD8 ؉ T cells, there is evidence for TCR-mediated activation by univalent engagement of the TCR. We have here compared oligomeric and monomeric L d and K b peptide-MHC complexes and free peptide as stimulators of CD8 ؉ T cells expressing the 2C TCR. We found that the monomers are indeed effective in activating naïve and effector CD8 ؉ T cells, but through an unexpected mechanism that involves transfer of peptide from soluble monomers to T cell endogenous MHC (K b ) molecules. The result is that T cells, acting as antigenpresenting cells, are able to activate other naïve T cells.CD8 ϩ T lymphocytes ͉ T cell receptor ͉ major histocompatibility complex ͉ antigen presentation ͉ lymphocyte activation A ntigen-driven activation of cells of the immune system generally involves multivalent antigen engagement that leads to clustering or ''crosslinking'' of cell-surface receptors. This concept arose largely from observations of antigen-induced capping of surface immunoglobulins on B cells (1, 2) and multivalent antigen triggering of histamine release from mast cells (3). Whether multivalent engagement of T cell antigen receptors (TCR) is required to initiate T cell activation has been difficult to determine, primarily because the antigens are peptide-MHC complexes normally found as integral membrane proteins on the surfaces of other cells. However, experiments using soluble recombinant MHC molecules lacking transmembrane domains and carrying defined synthetic peptides have shown clearly that peptide-MHC oligomers, but not monomers, can activate CD4 ϩ T cells (4-7). Thus, for CD4 ϩ T cells, multivalent engagement of TCR is sufficient to initiate cellular activation, whereas monovalent engagement is apparently nonproductive.For CD8 ϩ T cells, however, the issue remains unclear. Several studies have found that multivalent engagement is required to activate these cells (4, 8-10), but some evidence suggests the sufficiency of monovalent TCR engagement to trigger a cytolytic response, such as the requirement for such a small number of peptide-MHC complexes per target cell in cytolytic assays, to imply that a single complex can trigger the cytolytic response in CD8 T cells (11). Activation of CD8 ϩ T cells by soluble peptide-MHC monomers has been clearly observed in the presence of CD8 molecules (12, 13). It was suggested from that result that monovalent engagement of TCR can serve as the initiating event when it results in TCR association with CD8 (12). However, in another study, TCR-CD8 heterodimerization induced by peptide-MHC monomers was observed but was found not to activate the cells (9).In this study, we investigated the requirements for initiating signaling processes in naïve and activated CD8 ϩ T cells carrying the 2C TCR. The 2C TCR recognizes various peptide-MHC complexes, including (i) the potent allogenic activator Materials and Methods...

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Blocking and Redistribution ("Capping") of Antigen Receptors on T and B Lymphocytes by Anti-Immunoglobulin Antibody

Cited by 87 publications

References 33 publications

CD8 T Cells, Like CD4 T Cells, Are Triggered by Multivalent Engagement of TCRs by MHC-Peptide Ligands but Not by Monovalent Engagement

CD8 T Cells, Like CD4 T Cells, Are Triggered by Multivalent Engagement of TCRs by MHC-Peptide Ligands but Not by Monovalent Engagement

Function of Macrophages in Antigen Recognition by Guinea Pig T Lymphocytes

Soluble peptide–MHC monomers cause activation of CD8⁺T cells through transfer of the peptide to T cell MHC molecules

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Blocking and Redistribution ("Capping") of Antigen Receptors on T and B Lymphocytes by Anti-Immunoglobulin Antibody

Cited by 87 publications

References 33 publications

CD8 T Cells, Like CD4 T Cells, Are Triggered by Multivalent Engagement of TCRs by MHC-Peptide Ligands but Not by Monovalent Engagement

CD8 T Cells, Like CD4 T Cells, Are Triggered by Multivalent Engagement of TCRs by MHC-Peptide Ligands but Not by Monovalent Engagement

Function of Macrophages in Antigen Recognition by Guinea Pig T Lymphocytes

Soluble peptide–MHC monomers cause activation of CD8+T cells through transfer of the peptide to T cell MHC molecules

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Soluble peptide–MHC monomers cause activation of CD8⁺T cells through transfer of the peptide to T cell MHC molecules