Molecular Insights for Optimizing T Cell Receptor Specificity Against Cancer

Hebeisen, Michael; Oberle, Susanne; Presotto, Danilo; Speiser, Daniel E.; Zehn, Dietmar; Rufer, Nathalie

doi:10.3389/fimmu.2013.00154

Cited by 38 publications

(37 citation statements)

References 128 publications

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“…Experimentally generated high-affinity TCRs might be advantageous by boosting effector function and proliferation, thereby persisting longer and in larger numbers as compared with T cells with low-affinity TCRs, but they may also bear an increased risk of unwanted toxicities (3,4,(9)(10)(11)(12). Low-avidity T cells would gain value if their effector functions could be enhanced, as they are reported to be less susceptible to tolerization and may represent a lower toxicity risk (3,4,13,14).…”

Section: Introductionmentioning

confidence: 99%

“…Although there is consensus that durable antitumor responses require highly active T cells, it is not clear how this is best achieved. At least two major impediments have been identified that impinge upon achieving this prerequisite: inherent intermediate-to low-affinity T-cell receptors (TCR) of antitumor T cells that may not mount a successful tumor-specific response (3,4), and functional inactivation of T cells in the tumor milieu (5)(6)(7)(8).…”

Section: Introductionmentioning

confidence: 99%

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Chimeric PD-1:28 Receptor Upgrades Low-Avidity T cells and Restores Effector Function of Tumor-Infiltrating Lymphocytes for Adoptive Cell Therapy

et al. 2017

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Inherent intermediate-to low-affinity T-cell receptors (TCR) that develop during the natural course of immune responses may not allow sufficient activation for tumor elimination, making the majority of T cells suboptimal for adoptive T-cell therapy (ATT). TCR affinity enhancement has been implemented to provide stronger T-cell activity but carries the risk of creating undesired cross-reactivity leading to potential serious adverse effects in clinical application. We demonstrate here that engineering of low-avidity T cells recognizing a naturally processed and presented tumor-associated antigen with a chimeric PD-1:28 receptor increases effector function to levels seen with high-avidity T cells of identical specificity. Upgrading the function of low-avidity T cells without changing the TCR affinity will allow a large arsenal of low-avidity T cells previously thought to be therapeutically inefficient to be considered for ATT. PD-1:28 engineering reinstated Th1 function in tumor-infiltrating lymphocytes that had been functionally disabled in the human renal cell carcinoma environment without unleashing undesired Th2 cytokines or IL10. Involved mechanisms may be correlated to restoration of ERK and AKT signaling pathways. In mouse tumor models of ATT, PD-1:28 engineering enabled low-avidity T cells to proliferate stronger and prevented PD-L1 upregulation and Th2 polarization in the tumor milieu. Engineered T cells combined with checkpoint blockade secreted significantly more IFNg compared with T cells without PD-1:28, suggesting a beneficial combination with checkpoint blockade therapy or other therapeutic strategies. Altogether, the supportive effects of PD-1:28 engineering on T-cell function make it an attractive tool for ATT. Cancer Res; 77(13); 3577-90. Ó2017 AACR.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Chimeric PD-1:28 Receptor Upgrades Low-Avidity T cells and Restores Effector Function of Tumor-Infiltrating Lymphocytes for Adoptive Cell Therapy

et al. 2017

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“…The functional avidity of T cells is primarily controlled by the strength of TCR-pMHC interactions, a key parameter shown to impact on numerous aspects of T cell biology, including their thymic selection (21), activation and differentiation (22), autoimmune pathogenicity (23), and protection against infection and cancer (24). In fact, TCR-pMHC binding avidity may offer a key metric by which the quality of the T cell response can be directly evaluated, since it controls T cell activation, differentiation, and functional efficacy (25).…”

Section: Introductionmentioning

confidence: 99%

TCR-ligand dissociation rate is a robust and stable biomarker of CD8+ T cell potency

Allard¹,

Couturaud²,

Carretero-Iglesia³

et al. 2017

JCI Insight

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“…5B) were stable over time (data not shown). Theoretically, higher intensity tetramer staining could be associated to a higher expression at the surface level of the TCR and/or the co-receptor (CD4), and/or to a higher TCR avidity (35,36). We next measured the expression level of TCR and CD4 separately, in order to avoid competition of the staining antibodies.…”

Section: Characterization Of Two Distinct Mage-a3-specific Cd4 T-cellmentioning

confidence: 99%

Vaccination with LAG-3Ig (IMP321) and Peptides Induces Specific CD4 and CD8 T-Cell Responses in Metastatic Melanoma Patients—Report of a Phase I/IIa Clinical Trial

Legat

Hajjami

Baumgaertner

et al. 2016

Clinical Cancer Research

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Purpose: Cancer vaccines aim to generate and maintain antitumor immune responses. We designed a phase I/IIa clinical trial to test a vaccine formulation composed of Montanide ISA-51 (Incomplete Freund's Adjuvant), LAG-3Ig (IMP321, a non-Toll like Receptor agonist with adjuvant properties), and five synthetic peptides derived from tumor-associated antigens (four short 9/10-mers targeting CD8 T-cells, and one longer 15-mer targeting CD4 T-cells). Primary endpoints were safety and T-cell responses.Experimental Design: Sixteen metastatic melanoma patients received serial vaccinations. Up to nine injections were subcutaneously administered in three cycles, each with three vaccinations every 3 weeks, with 6 to 14 weeks interval between cycles. Blood samples were collected at baseline, 1-week after the third, sixth and ninth vaccination, and 6 months after the last vaccination.Circulating T-cells were monitored by tetramer staining directly ex vivo, and by combinatorial tetramer and cytokine staining on in vitro stimulated cells.Results: Side effects were mild to moderate, comparable to vaccines with Montanide alone. Specific CD8 T-cell responses to at least one peptide formulated in the vaccine preparation were found in 13 of 16 patients. However, two of the four short peptides of the vaccine formulation did not elicit CD8 T-cell responses. Specific CD4 T-cell responses were found in all 16 patients.Conclusions: We conclude that vaccination with IMP321 is a promising and safe strategy for inducing sustained immune responses, encouraging further development for cancer vaccines as components of combination therapies.

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Molecular Insights for Optimizing T Cell Receptor Specificity Against Cancer

Cited by 38 publications

References 128 publications

Chimeric PD-1:28 Receptor Upgrades Low-Avidity T cells and Restores Effector Function of Tumor-Infiltrating Lymphocytes for Adoptive Cell Therapy

Chimeric PD-1:28 Receptor Upgrades Low-Avidity T cells and Restores Effector Function of Tumor-Infiltrating Lymphocytes for Adoptive Cell Therapy

TCR-ligand dissociation rate is a robust and stable biomarker of CD8+ T cell potency

Vaccination with LAG-3Ig (IMP321) and Peptides Induces Specific CD4 and CD8 T-Cell Responses in Metastatic Melanoma Patients—Report of a Phase I/IIa Clinical Trial

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