Functional analysis of peripheral and intratumoral neoantigen-specific TCRs identified in a patient with melanoma

Bräunlein, Eva; Lupoli, Gaia; Füchsl, Franziska; Abualrous, Esam T.; Gosmann, Dario; Wietbrock, Lukas; Lange, Sebastian; Engleitner, Thomas; Lan, Hongbo; Audehm, Stefan; Effenberger, Manuel; Boxberg, Melanie; Steiger, Katja; Chang, Yinshui; Yu, Kai; Atay, Çiğdem; Bassermann, Florian; Weichert, Wilko; Busch, Dirk H.; Rad, Roland; Freund, Christian; Antes, Iris; Krackhardt, Angela M.

doi:10.1136/jitc-2021-002754

Cited by 10 publications

(31 citation statements)

References 36 publications

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“…Meanwhile, very high binding strength leads to deteriorated signaling, such as poor mitogen-activated protein kinase (MAPK) phosphorylation [151]. Isolating neoantigen-reactive MHC-class I-restricted TCR from CD8+ T cells from a malignant melanoma patient, we also detected a higher overall frequency of TCR of lower functional avidity in different patient tissues over the course of several years [152,153]. All these findings suggest a "goldilocks" window of optimal T cell activation for in vivo application [154,155].…”

Section: General Aspects Of the Tcr-peptide-mhc Interactionmentioning

confidence: 88%

“…No further precise criteria for the "best" TCR for ACT are established to date-if such a best receptor even exists, rather than different qualities necessary at different disease stages, antigen densities or under different TME conditions. The heterogeneity in functional avidity of different TCRs in the anti-tumor T cell pool from melanoma patients as mentioned above suggests, that a deeper understanding of favorable TCR qualities is necessary across different entities [150,152]. Understanding, which TCR clonotypes have the greatest impact on immediate tumor killing, but also long-term tumor control and memory formation, will be essential to choose the optimal combination of TCR for ACT improving patient survival.…”

Section: Application and Engineering Approaches For Tcr-t Cells In MMmentioning

confidence: 99%

“…The extremely patient-specific nature of most epitopes recognized on top of the TCR's HLArestriction claim for single-patient protocols promising high specificity and minimized toxicity. Despite the preclinical success and progressive identification of various neoantigenspecific TCR with anti-tumor effector functions [150,152,153,207], no results from clinical trials are available, so far. Currently, one single-arm first-in-human phase Ia/Ib trial is open and recruiting patients for investigating the efficacy of a single dose of neoantigen-specific TCRs with and without additional anti-PD1 treatment in locally advanced or metastasized solid tumors (NCT03970382).…”

Section: Application and Engineering Approaches For Tcr-t Cells In MMmentioning

confidence: 99%

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Adoptive Cellular Therapy for Multiple Myeloma Using CAR- and TCR-Transgenic T Cells: Response and Resistance

Füchsl

Krackhardt

2022

Cells

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Despite the substantial improvement of therapeutic approaches, multiple myeloma (MM) remains mostly incurable. However, immunotherapeutic and especially T cell-based approaches pioneered the therapeutic landscape for relapsed and refractory disease recently. Targeting B-cell maturation antigen (BCMA) on myeloma cells has been demonstrated to be highly effective not only by antibody-derived constructs but also by adoptive cellular therapies. Chimeric antigen receptor (CAR)-transgenic T cells lead to deep, albeit mostly not durable responses with manageable side-effects in intensively pretreated patients. The spectrum of adoptive T cell-transfer covers synthetic CARs with diverse specificities as well as currently less well-established T cell receptor (TCR)-based personalized strategies. In this review, we want to focus on treatment characteristics including efficacy and safety of CAR- and TCR-transgenic T cells in MM as well as the future potential these novel therapies may have. ACT with transgenic T cells has only entered clinical trials and various engineering strategies for optimization of T cell responses are necessary to overcome therapy resistance mechanisms. We want to outline the current success in engineering CAR- and TCR-T cells, but also discuss challenges including resistance mechanisms of MM for evading T cell therapy and point out possible novel strategies.

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Section: General Aspects Of the Tcr-peptide-mhc Interactionmentioning

confidence: 88%

Section: Application and Engineering Approaches For Tcr-t Cells In MMmentioning

confidence: 99%

Section: Application and Engineering Approaches For Tcr-t Cells In MMmentioning

confidence: 99%

See 1 more Smart Citation

Adoptive Cellular Therapy for Multiple Myeloma Using CAR- and TCR-Transgenic T Cells: Response and Resistance

Füchsl

Krackhardt

2022

Cells

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“…Disadvantage of the direct labelling approach is the need of highly trained personal with experience in good manufacturing practice (GMP), as well as cell handling at the treatment side. In addition, with respect to track endogenously stimulated T-cells, tumor-specific T-cells circulating in the peripheral blood may have low frequencies and migration of blood-derived labelled cells into the tumor is so far ill-defined [ 82 ].…”

Section: Imaging Of Ex Vivo Labelled T-cellsmentioning

confidence: 99%

Promise and challenges of clinical non-invasive T-cell tracking in the era of cancer immunotherapy

et al. 2022

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In the last decades, our understanding of the role of the immune system in cancer has significantly improved and led to the discovery of new immunotherapeutic targets and tools, which boosted the advances in cancer immunotherapy to fight a growing number of malignancies. Approved immunotherapeutic approaches are currently mainly based on immune checkpoint inhibitors, antibody-derived targeted therapies, or cell-based immunotherapies. In essence, these therapies induce or enhance the infiltration and function of tumor-reactive T cells within the tumors, ideally resulting in complete tumor eradication. While the clinical application of immunotherapies has shown great promise, these therapies are often accompanied either by a variety of side effects as well as partial or complete unresponsiveness of a number of patients. Since different stages of disease progression elicit different local and systemic immune responses, the ability to longitudinally interrogate the migration and expansion of immune cells, especially T cells, throughout the whole body might greatly facilitate disease characterization and understanding. Furthermore, it can serve as a tool to guide development as well as selection of appropriate treatment regiments. This review provides an overview about a variety of immune-imaging tools available to characterize and study T-cell responses induced by anti-cancer immunotherapy. Moreover, challenges are discussed that must be taken into account and overcome to use immune-imaging tools as predictive and surrogate markers to enhance assessment and successful application of immunotherapies.

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“…The authors further hypothesized that neoantigen-specific TILs from non-responders expressed low avidity or affinity TCRs, leading to unfavorable transcriptional programs. However, the expression levels of tumor antigens and tumor microenvironments may also strongly influence the T cell differentiation, leading to different observations [ 154 , 160 ]. As a result, the further investigation of this hypothesis is required.…”

Section: The Role Of Neoantigens In Immunotherapymentioning

confidence: 99%

Neoantigen-Reactive T Cells: The Driving Force behind Successful Melanoma Immunotherapy

Davis

Tarduno

2021

Cancers

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Patients with metastatic cutaneous melanoma have experienced significant clinical responses after checkpoint blockade immunotherapy or adoptive cell therapy. Neoantigens are mutated proteins that arise from tumor-specific mutations. It is hypothesized that the neoantigen recognition by T cells is the critical step for T-cell-mediated anti-tumor responses and subsequent tumor regressions. In addition to describing neoantigens, we review the sentinel and ongoing clinical trials that are helping to shape the current treatments for patients with cutaneous melanoma. We also present the existing evidence that establishes the correlations between neoantigen-reactive T cells and clinical responses in melanoma immunotherapy.

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Functional analysis of peripheral and intratumoral neoantigen-specific TCRs identified in a patient with melanoma

Cited by 10 publications

References 36 publications

Adoptive Cellular Therapy for Multiple Myeloma Using CAR- and TCR-Transgenic T Cells: Response and Resistance

Adoptive Cellular Therapy for Multiple Myeloma Using CAR- and TCR-Transgenic T Cells: Response and Resistance

Promise and challenges of clinical non-invasive T-cell tracking in the era of cancer immunotherapy

Neoantigen-Reactive T Cells: The Driving Force behind Successful Melanoma Immunotherapy

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