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

Ge, Qing; Stone, Jon R.; Thompson, Michael T.; Cochran, Jennifer R.; Rushe, Mia; Eisen, Herman N.; Chen, Jianzhu; Stern, Lawrence J.

doi:10.1073/pnas.212515299

Cited by 70 publications

(66 citation statements)

References 40 publications

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“…Thus, CTL acquire covalent pepMHC complexes in a signallingdependent manner. This observation also rules out the possibility that fluorescent peptide transfer results from peptide dissociation followed by reassociation on the MHC molecules of the CTL, a process that was proposed to account for CTL activation by soluble pepMHC monomers [41,42]. Detectable acquisition of covalent pepMHC complexes and IFN-c production require higher levels of TCR engagement than does triggering of biotin capture or cytotoxicity…”

Section: Ctl Capture Covalent Pepmhc Complexesmentioning

confidence: 79%

T cell activation correlates with an increasedproportion of antigen among the materials acquiredfrom target cells

et al. 2005

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We have investigated the density of peptides required to elicit different biological responses in cytotoxic T lymphocytes (CTL), including trogocytosis (i.e., the phenomenon whereby the lymphocytes actively capture fragments of plasma membrane from those cells with which they establish an immune synapse). We have used two separate mouse models of CTL recognising defined peptides presented by MHC class I molecules. In both systems, triggering of cytotoxicity and capture of membrane components reached saturation with low densities of ligand. On the other hand, down-modulation of cell-surface levels of TCR, induction of IFN-c production and detection of peptide captured required much higher ligand densities. Interestingly, fratricide (i.e., killing between CTL sharing the same specificity), a mechanism proposed to account for CTL exhaustion, was detected only at antigen concentrations still well above that second threshold leading to full blown activation. Taken together, our results show that the different thresholds that govern the elicitation of different CTL functions correlate with different proportions of antigen among the target cell components being captured via trogocytosis.

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Section: Ctl Capture Covalent Pepmhc Complexesmentioning

confidence: 79%

T cell activation correlates with an increasedproportion of antigen among the materials acquiredfrom target cells

et al. 2005

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“…Cross-presentation is a major pathway by which DNA vaccines elicit T cell responses, but the inefficiency of cross-presentation can be a contributing factor to relatively weak T cell responses after DNA vaccination. In addition, recent studies have documented the cross-presentation of synthetic peptides from recombinant MHC-I tetramers used to activate T cells (22,23). Thus biochemical stability of the SCT is a requirement for improved DNA vaccination or MHC-I tetramer approaches.…”

mentioning

confidence: 99%

Human Major Histocompatibility Complex (MHC) Class I Molecules with Disulfide Traps Secure Disease-related Antigenic Peptides and Exclude Competitor Peptides

Truscott

Wang

Lybarger

et al. 2008

Journal of Biological Chemistry

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The ongoing discovery of disease-associated epitopes detected by CD8 T cells greatly facilitates peptide-based vaccine approaches and the construction of multimeric soluble recombinant proteins (e.g. tetramers) for isolation and enumeration of antigen-specific CD8 T cells. Related to these outcomes of epitope discovery is the recent demonstration that MHC class I/peptide complexes can be expressed as single chain trimers (SCTs) with peptide, ␤ 2 m and heavy chain connected by linkers to form a single polypeptide chain. Studies using clinically relevant mouse models of human disease have shown that SCTs expressed by DNA vaccination are potent stimulators of cytotoxic T lymphocytes. Their vaccine efficacy has been attributed to the fact that SCTs contain a preprocessed and preloaded peptide that is stably displayed on the cell surface. Although SCTs of HLA class I/peptide complexes have been previously reported, they have not been characterized for biochemical stability or susceptibility to exogenous peptide binding. Here we demonstrate that human SCTs remain almost exclusively intact when expressed in cells and can incorporate a disulfide trap that dramatically excludes the binding of exogenous peptides. The mechanistic and practical applications of these findings for vaccine development and T cell isolation/enumeration are discussed.

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“…This type of study in CD4 T cells showed that dimers and higher oligomers of cognate class II MHC-peptide complexes were able to stimulate many T cell markers such as TCR down-regulation (4), CD69 up-regulation (5), and CD25 up-regulation (6); conversely, monomeric MHC-peptide complexes were not able to induce such markers (7)(8)(9)(10). When similar studies have been undertaken treating CD8 T cells with soluble, recombinant class I MHC-peptide complexes, conflicting studies reported activation in response to oligomeric complexes (10 -15), to monomeric complexes (13)(14)(15), and even to free peptide (14,15). A partial explanation for this discrepancy may be "cross-presentation" of peptide by T cells, wherein peptide adventitiously released from soluble MHC monomers can be loaded onto T cell endogenous class I MHC molecules with resultant T-T presentation and activation (14,15).…”

mentioning

confidence: 99%

“…When similar studies have been undertaken treating CD8 T cells with soluble, recombinant class I MHC-peptide complexes, conflicting studies reported activation in response to oligomeric complexes (10 -15), to monomeric complexes (13)(14)(15), and even to free peptide (14,15). A partial explanation for this discrepancy may be "cross-presentation" of peptide by T cells, wherein peptide adventitiously released from soluble MHC monomers can be loaded onto T cell endogenous class I MHC molecules with resultant T-T presentation and activation (14,15). When T cells that do not express endogenous MHC are used, neither peptide nor class I MHC monomers caused down-regulation of TCR or up-regulation of activation markers (14,15).…”

mentioning

confidence: 99%

“…A partial explanation for this discrepancy may be "cross-presentation" of peptide by T cells, wherein peptide adventitiously released from soluble MHC monomers can be loaded onto T cell endogenous class I MHC molecules with resultant T-T presentation and activation (14,15). When T cells that do not express endogenous MHC are used, neither peptide nor class I MHC monomers caused down-regulation of TCR or up-regulation of activation markers (14,15).…”

mentioning

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

Cited by 70 publications

References 40 publications

T cell activation correlates with an increasedproportion of antigen among the materials acquiredfrom target cells

T cell activation correlates with an increasedproportion of antigen among the materials acquiredfrom target cells

Human Major Histocompatibility Complex (MHC) Class I Molecules with Disulfide Traps Secure Disease-related Antigenic Peptides and Exclude Competitor Peptides

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

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

Cited by 70 publications

References 40 publications

T cell activation correlates with an increasedproportion of antigen among the materials acquiredfrom target cells

T cell activation correlates with an increasedproportion of antigen among the materials acquiredfrom target cells

Human Major Histocompatibility Complex (MHC) Class I Molecules with Disulfide Traps Secure Disease-related Antigenic Peptides and Exclude Competitor Peptides

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

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