An Altered gp100 Peptide Ligand with Decreased Binding by TCR and CD8α Dissects T Cell Cytotoxicity from Production of Cytokines and Activation of NFAT

Schaft, Niels; Coccoris, Miriam; Drexhage, Joost; Knoop, C. J.; Vries, I. Jolanda M. de; Adema, Gosse J.; Debets, Reno

doi:10.3389/fimmu.2013.00270

Cited by 8 publications

(12 citation statements)

References 50 publications

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“…The use of TCR variants either lacking or containing an LCK-nonbinding mutant of CD28 IC domain demonstrated a hierarchy with respect to dependency on CD28 signaling, in particular LCK signaling for different T cell functions (CD107a , IFN-g , IL-2). This observed hierarchy is in line with an earlier report using a peptide-MHC ligand with compromised TCR binding (a partial agonist of the human gp100 280-288 peptide) (42). In fact, mobilization of CD107a generally requires limited T cell signaling and is presynthesized and ready to be mobilized, whereas production of cytokines requires de novo synthesis; in particular, IL-2 requires strong T cell signaling and NFAT activation.…”

Section: Discussionsupporting

confidence: 72%

TCRs Genetically Linked to CD28 and CD3ε Do Not Mispair with Endogenous TCR Chains and Mediate Enhanced T Cell Persistence and Anti-Melanoma Activity

Govers

Sebestyén

Roszik

et al. 2014

The Journal of Immunology

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Adoptive transfer of T cells that are gene engineered to express a defined TCR represents a feasible and promising therapy for patients with tumors. However, TCR gene therapy is hindered by the transient presence and effectiveness of transferred T cells, which are anticipated to be improved by adequate T cell costimulation. In this article, we report the identification and characterization of a novel two-chain TCR linked to CD28 and CD3ε (i.e., TCR:28ε). This modified TCR demonstrates enhanced binding of peptide–MHC and mediates enhanced T cell function following stimulation with peptide compared with wild-type TCR. Surface expression of TCR:28ε depends on the transmembrane domain of CD28, whereas T cell functions depend on the intracellular domains of both CD28 and CD3ε, with IL-2 production showing dependency on CD28:LCK binding. TCR:28ε, but not wild-type TCR, induces detectable immune synapses in primary human T cells, and such immune synapses show significantly enhanced accumulation of TCR transgenes and markers of early TCR signaling, such as phosphorylated LCK and ERK. Importantly, TCR:28ε does not show signs of off-target recognition, as evidenced by lack of TCR mispairing, as well as preserved specificity. Notably, when testing TCR:28ε in immune-competent mice, we observed a drastic increase in T cell survival, which was accompanied by regression of large melanomas with limited recurrence. Our data argue that TCR transgenes that contain CD28, and, thereby, may provide T cell costimulation in an immune-suppressive environment, represent candidate receptors to treat patients with tumors.

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Section: Discussionsupporting

confidence: 72%

TCRs Genetically Linked to CD28 and CD3ε Do Not Mispair with Endogenous TCR Chains and Mediate Enhanced T Cell Persistence and Anti-Melanoma Activity

Govers

Sebestyén

Roszik

et al. 2014

The Journal of Immunology

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“…Indeed, even conservative peptide substitutions can have unexpected consequences for T-cell recognition due to knock-on structural changes in the HLA-bound peptide. Our findings provide a molecular explanation for the sensitivity to substitutions at gp100 280–288 peptide residue Glu 3 ( 16 , 17 ) and represent the first example of the structural mechanisms underlying T-cell recognition of this important therapeutic target for melanoma.…”

Section: Introductionmentioning

confidence: 76%

“…The CD8 + T-cell responses directed against gp100 280–288 have been shown to be polyclonal in nature ( 16 , 17 ). Along with the two TCRs under investigation here, the sequences of a further two TCRs have been published, demonstrating diverse gene usage and different CDR3 loop sequences ( Table 1 ).…”

Section: Resultsmentioning

confidence: 99%

“…Among these, the heteroclitic version of gp100 280–288 (in which a valine replaces alanine at anchor position 9 to improve pHLA stability ( 14 )) enhanced the induction of melanoma-reactive cytotoxic T lymphocytes in vitro and has been successfully used in clinical trials ( 15 ). Another heteroclitic form of gp100 280–288 , in which peptide residue Glu 3 was substituted to Ala, abrogated recognition by a polyclonal population of gp100 280–288 -specific T-cells ( 16 , 17 ). Thus, a more complete understanding of the molecular mechanisms underlying gp100 280–288 targeting by specific TCRs is needed to direct the design of improved altered peptide ligands.…”

Section: Introductionmentioning

confidence: 99%

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A Molecular Switch Abrogates Glycoprotein 100 (gp100) T-cell Receptor (TCR) Targeting of a Human Melanoma Antigen

Bianchi¹,

Bulek

Fuller

et al. 2016

Journal of Biological Chemistry

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Human CD8+ cytotoxic T lymphocytes can mediate tumor regression in melanoma through the specific recognition of HLA-restricted peptides. Because of the relatively weak affinity of most anti-cancer T-cell receptors (TCRs), there is growing emphasis on immunizing melanoma patients with altered peptide ligands in order to induce strong anti-tumor immunity capable of breaking tolerance toward these self-antigens. However, previous studies have shown that these immunogenic designer peptides are not always effective. The melanocyte differentiation protein, glycoprotein 100 (gp100), encodes a naturally processed epitope that is an attractive target for melanoma immunotherapies, in particular peptide-based vaccines. Previous studies have shown that substitutions at peptide residue Glu3 have a broad negative impact on polyclonal T-cell responses. Here, we describe the first atomic structure of a natural cognate TCR in complex with this gp100 epitope and highlight the relatively high affinity of the interaction. Alanine scan mutagenesis performed across the gp100280–288 peptide showed that Glu3 was critically important for TCR binding. Unexpectedly, structural analysis demonstrated that the Glu3 → Ala substitution resulted in a molecular switch that was transmitted to adjacent residues, abrogating TCR binding and T-cell recognition. These findings help to clarify the mechanism of T-cell recognition of gp100 during melanoma responses and could direct the development of altered peptides for vaccination.

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“…Partial agonists are variant peptides which elicit a subset of the T cell functions generated by the wild type peptide [ 70 , 71 ]. Using a panel of gp100 substituted peptides, an altered peptide capable of inducing cytotoxic function but limited cytokine secretion from responding T cells was identified [ 72 ]. Consequently, APLs which alter the function of T cells may be useful in autoimmune disease settings or diseases dependent on a Th1/Th2 balance where silencing of selected T cell functions could be beneficial.…”

Section: Peptide Structurementioning

confidence: 99%

Peptide Dose and/or Structure in Vaccines as a Determinant of T Cell Responses

Leggatt

2014

Vaccines

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While T cells recognise the complex of peptide and major histocompatibility complex (MHC) at the cell surface, changes in the dose and/or structure of the peptide component can have profound effects on T cell activation and function. In addition, the repertoire of T cells capable of responding to any given peptide is variable, but broader than a single clone. Consequently, peptide parameters that affect the interaction between T cells and peptide/MHC have been shown to select particular T cell clones for expansion and this impacts on clearance of disease. T cells with high functional avidity are selected on low doses of peptide, while low avidity T cells are favoured in high peptide concentrations. Altering the structure of the peptide ligand can also influence the selection and function of peptide-specific T cell clones. In this review, we will explore the evidence that the choice of peptide dose or the structure of the peptide are critical parameters in an effective vaccine designed to activate T cells.

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An Altered gp100 Peptide Ligand with Decreased Binding by TCR and CD8α Dissects T Cell Cytotoxicity from Production of Cytokines and Activation of NFAT

Cited by 8 publications

References 50 publications

TCRs Genetically Linked to CD28 and CD3ε Do Not Mispair with Endogenous TCR Chains and Mediate Enhanced T Cell Persistence and Anti-Melanoma Activity

TCRs Genetically Linked to CD28 and CD3ε Do Not Mispair with Endogenous TCR Chains and Mediate Enhanced T Cell Persistence and Anti-Melanoma Activity

A Molecular Switch Abrogates Glycoprotein 100 (gp100) T-cell Receptor (TCR) Targeting of a Human Melanoma Antigen

Peptide Dose and/or Structure in Vaccines as a Determinant of T Cell Responses

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