Fine-Tuning of Optimal TCR Signaling in Tumor-Redirected CD8 T Cells by Distinct TCR Affinity-Mediated Mechanisms

Presotto, Danilo; Erdes, Efe; Duong, Minh Ngoc; Allard, Mathilde; Regamey, Pierre-Olivier; Quadroni, Manfredo; Doucey, Marie‐Agnès; Rufer, Nathalie; Hebeisen, Michael

doi:10.3389/fimmu.2017.01564

Cited by 44 publications

(45 citation statements)

References 64 publications

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“…Although SHP-1 mediates inhibitory signals ( 78 ), SHP-2 is considered a positive regulator of T cell activation ( 79 – 81 ) and may act by dephosphorylating inhibitory sites of positive regulators. Both phosphatases are involved in the formation of the TCR signalosome ( 82 ), and their phosphatase activities are regulated by phosphorylation/dephosphorylation as well as by oxidation/reduction reactions ( 83 – 85 ). Since PD-1 expression is induced only after activation and participates in TCR signaling microclusters upon binding to PD-L1 ( 63 ), it is reasonable to speculate that PD-1 molecules are clustered and stabilized by PD-L1 interactions around TCR molecules, serving as “switches” of positive signalosome conformations to negative ones.…”

Section: Mechanisms and Targets Of Pd-1 Signalingmentioning

confidence: 99%

Revisiting the PD-1 pathway

et al. 2020

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Programmed Death-1 (PD-1; CD279) is an inhibitory receptor induced in activated T cells. PD-1 engagement by its ligands, PD-L1 and PD-L2, maintains peripheral tolerance but also compromises anti-tumor immunity. Blocking antibodies against PD-1 or its ligands have revolutionized cancer immunotherapy. However, only a fraction of patients develop durable antitumor responses. Clinical outcomes have reached a plateau without substantial advances by combinatorial approaches. Thus, great interest has recently emerged to investigate, in depth, the mechanisms by which the PD-1 pathway transmits inhibitory signals with the goal to identify molecular targets for improvement of the therapeutic success. These efforts have revealed unpredictable dimensions of the pathway and uncovered novel mechanisms involved in PD-1 and PD-L1 regulation and function. Here, we provide an overview of the recent advances on the mechanistic aspects of the PD-1 pathway and discuss the implications of these new discoveries and the gaps that remain to be filled.

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Section: Mechanisms and Targets Of Pd-1 Signalingmentioning

confidence: 99%

Revisiting the PD-1 pathway

et al. 2020

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“…TCR affinity increased beyond the physiological range comes with the risk of creating novel molecules with unpredictable binding specificities to structurally related peptide sequences from different antigens, creating off-target toxicity [8,9]. Moreover, TCR variants were tested and the existence of a TCR affinity-related activation threshold was demonstrated both in vitro [14] and in vivo [15]. Here the authors of the two studies proposed that this threshold marked the limit between epitope recognition and autoimmunity.…”

Section: Isolating Tcrs From Vaccinated Patientsmentioning

confidence: 99%

Long-term surviving cancer patients as a source of therapeutic TCR

Inderberg

Wälchli

2020

Cancer Immunol Immunother

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We have established a platform for the isolation of tumour-specific TCR from T cells of patients who experienced clinical benefit from cancer vaccination. In this review we will present the rationale behind this strategy and discuss the advantages of working with "natural" wild type TCRs. Indeed, the general trend in the field has been to use various modifications to enhance the affinity of such therapeutic TCRs. This was done to obtain stronger T cell responses, often at the cost of safety. We further describe antigen targets and recent in vitro and in vivo results obtained to validate them. We finally discuss the use of MHC class II-restricted TCR in immunotherapy. Typically cellular anti-tumour immune responses have been attributed to CD8 T cells; however, we isolated mainly CD4 T cells. Importantly, these MHC class II-restricted TCRs have the potential to induce broad, long lasting immune responses that enable cancer control. The use of CD4 T cell-derived TCRs for adoptive immunotherapy has so far been limited and we will here discuss their therapeutic potential.

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“…Using the OT‐1 APL system, low‐affinity–primed memory cells produce more IL‐2 and fully differentiated memory cells that are CD45RB HI 68 . Using specific T cells with low and high affinity for the NY‐ESO‐1 TAA peptide complexed with HLA‐A2, the high‐affinity interactions resulted in transient signal activation leading to poor MAPK production and low proliferation ability 69 . Taken together, these data suggest that low‐affinity T cells have a separate, but necessary role in T‐cell function (summarized in Figure 2).…”

Section: Differences Between Low‐ and High‐affinity Tcr‐pmhc Interactmentioning

confidence: 99%

T‐cell receptor affinity in the age of cancer immunotherapy

Hoffmann

Slansky

2020

Molecular Carcinogenesis

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The strength of the interaction between T-cell receptors (TCRs) and their ligands, peptide/major histocompatibility complex complexes (pMHCs), is one of the most frequently discussed and investigated features of T cells in immuno-oncology today.Although there are many molecules on the surface of T cells that interact with ligands on other cells, the TCR/pMHC is the only receptor-ligand pair that offers antigen specificity and dictates the functional response of the T cell. The strength of the TCR/pMHC interaction, along with the environment in which this interaction takes place, is key to how the T cell will respond. The TCR repertoire of T cells that interact with tumor-associated antigens is vast, although typically of low affinity.Here, we focus on the low-affinity interactions between TCRs from CD8+ T cells and different models used in immuno-oncology.

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Fine-Tuning of Optimal TCR Signaling in Tumor-Redirected CD8 T Cells by Distinct TCR Affinity-Mediated Mechanisms

Cited by 44 publications

References 64 publications

Revisiting the PD-1 pathway

Revisiting the PD-1 pathway

Long-term surviving cancer patients as a source of therapeutic TCR

T‐cell receptor affinity in the age of cancer immunotherapy

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