Engineered TCR-T Cell Immunotherapy in Anticancer Precision Medicine: Pros and Cons

Zhao, Qijie; Jiang, Yu; Xiang, Shixin; Kaboli, Parham Jabbarzadeh; Shen, Jing; Zhao, Yueshui; Wu, Xu; Du, Fukuan; Li, Mingxing; Cho, Chi Hin; Li, Jing; Wen, Qinglian; Liu, Tao; Yi, Tao; Xiao, Zhangang

doi:10.3389/fimmu.2021.658753

Cited by 75 publications

(60 citation statements)

References 104 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…It is a construct composed of a soluble affinity-enhanced HLA-A*02:01–restricted T-cell receptor specific for the glycoprotein 100 (gp100) peptide YLEPGPVTA which is fused to an anti-CD3 single-chain variable fragment [ 376 , 378 ]. Thus, ImmTACs like Tebentafusp, are able to target any protein presented as a peptide–HLA complex on the surface of the target-cell, including intracellular antigens [ 379 , 380 ]. The binding of ImmTAC molecules to their target-cell surface specific peptide–HLA complexes initiates the recruitment and activation of polyclonal T cells, mediated through CD3, which efficiently leads to the release of cytokines and other cytolytic mediators to the target cells [ 379 , 380 ].…”

Section: Current Challenges and Future Perspectives In Uveal Melanomamentioning

confidence: 99%

“…Thus, ImmTACs like Tebentafusp, are able to target any protein presented as a peptide–HLA complex on the surface of the target-cell, including intracellular antigens [ 379 , 380 ]. The binding of ImmTAC molecules to their target-cell surface specific peptide–HLA complexes initiates the recruitment and activation of polyclonal T cells, mediated through CD3, which efficiently leads to the release of cytokines and other cytolytic mediators to the target cells [ 379 , 380 ]. In a recent phase 3 clinical trial involving 378 previously untreated HLAA*02:01–positive metastatic UM patients, stratified based on lactate dehydrogenase (LDH) levels, treatment with Tebentafusp was associated with a higher PFS and a 1-year OS of 73%, while in the control group (single agent pembrolizumab, ipilimumab, or dacarbazine) the observed 1-year OS was only 59% [ 376 ].…”

Section: Current Challenges and Future Perspectives In Uveal Melanomamentioning

confidence: 99%

See 1 more Smart Citation

Prognostic Biomarkers in Uveal Melanoma: The Status Quo, Recent Advances and Future Directions

Lamas

Martel

Nahon-Estève

et al. 2021

Cancers

View full text Add to dashboard Cite

Uveal melanoma (UM) is the most common malignant intraocular tumour in the adult population. It is a rare cancer with an incidence of nearly five cases per million inhabitants per year, which develops from the uncontrolled proliferation of melanocytes in the choroid (≈90%), ciliary body (≈6%) or iris (≈4%). Patients initially present either with symptoms like blurred vision or photopsia, or without symptoms, with the tumour being detected in routine eye exams. Over the course of the disease, metastases, which are initially dormant, develop in nearly 50% of patients, preferentially in the liver. Despite decades of intensive research, the only approach proven to mildly control disease spread are early treatments directed to ablate liver metastases, such as surgical excision or chemoembolization. However, most patients have a limited life expectancy once metastases are detected, since there are limited therapeutic approaches for the metastatic disease, including immunotherapy, which unlike in cutaneous melanoma, has been mostly ineffective for UM patients. Therefore, in order to offer the best care possible to these patients, there is an urgent need to find robust models that can accurately predict the prognosis of UM, as well as therapeutic strategies that effectively block and/or limit the spread of the metastatic disease. Here, we initially summarized the current knowledge about UM by compiling the most relevant epidemiological, clinical, pathological and molecular data. Then, we revisited the most important prognostic factors currently used for the evaluation and follow-up of primary UM cases. Afterwards, we addressed emerging prognostic biomarkers in UM, by comprehensively reviewing gene signatures, immunohistochemistry-based markers and proteomic markers resulting from research studies conducted over the past three years. Finally, we discussed the current hurdles in the field and anticipated the future challenges and novel avenues of research in UM.

show abstract

Section: Current Challenges and Future Perspectives In Uveal Melanomamentioning

confidence: 99%

Section: Current Challenges and Future Perspectives In Uveal Melanomamentioning

confidence: 99%

Prognostic Biomarkers in Uveal Melanoma: The Status Quo, Recent Advances and Future Directions

Lamas

Martel

Nahon-Estève

et al. 2021

Cancers

View full text Add to dashboard Cite

show abstract

“…Severe toxicities have also been observed in transgenic TCR clinical trials, i.e., severe colitis in patients receiving anti-human CEA TCR [ 92 ] and severe mental changes, coma, and death in patients receiving anti-MAGE-A3 TCR (later found to be the result of cross-reactivity with MAGE-A12 in the brain) [ 92 ]. TCR T cells are currently under investigation against a number of antigens, including TAAs such as NY-ESO-1 (NCT0369137) and MAGE-C2 (NCT04729543), and TSAs, such as HPV E6 (NCT03578406) and KRAS G12V (NCT04146298) [ 93 ].…”

Section: T Cell-mediated Immunitymentioning

confidence: 99%

Implications of Antigen Selection on T Cell-Based Immunotherapy

Camp

Slansky

2021

Pharmaceuticals

View full text Add to dashboard Cite

Many immunotherapies rely on CD8+ effector T cells to recognize and kill cognate tumor cells. These T cell-based immunotherapies include adoptive cell therapy, such as CAR T cells or transgenic TCR T cells, and anti-cancer vaccines which expand endogenous T cell populations. Tumor mutation burden and the choice of antigen are among the most important aspects of T cell-based immunotherapies. Here, we highlight various classes of cancer antigens, including self, neojunction-derived, human endogenous retrovirus (HERV)-derived, and somatic nucleotide variant (SNV)-derived antigens, and consider their utility in T cell-based immunotherapies. We further discuss the respective anti-tumor/anti-self-properties that influence both the degree of immunotolerance and potential off-target effects associated with each antigen class.

show abstract

“…It is a heterodimer consisting of an α chain and a β chain, each of which contain a variable region and a constant region. TCRs must be matched with human leukocyte antigen (HLA) alleles before they recognize and bind to specific antigens presented by peptide-MHC (pMHC) to effectively eliminate or reduce tumor cells, which is significantly distinct from the mechanism of CAR-T cells ( Table 2 ) ( 47 ). Antigens within any subcellular compartment, once processed and presented by MHC molecules, can be recognized by TCR-T cells.…”

Section: Tcr-t: a Promising Alternative To Traditional Immunotherapiesmentioning

confidence: 99%

Genetically Modified T Cells for Esophageal Cancer Therapy: A Promising Clinical Application

et al. 2021

View full text Add to dashboard Cite

Esophageal cancer is an exceedingly aggressive and malignant cancer that imposes a substantial burden on patients and their families. It is usually treated with surgery, chemotherapy, radiotherapy, and molecular-targeted therapy. Immunotherapy is a novel treatment modality for esophageal cancer wherein genetically engineered adoptive cell therapy is utilized, which modifies immune cells to attack cancer cells. Using chimeric antigen receptor (CAR) or T cell receptor (TCR) modified T cells yielded demonstrably encouraging efficacy in patients. CAR-T cell therapy has shown robust clinical results for malignant hematological diseases, particularly in B cell-derived malignancies. Natural killer (NK) cells could serve as another reliable and safe CAR engineering platform, and CAR-NK cell therapy could be a more generalized approach for cancer immunotherapy because NK cells are histocompatibility-independent. TCR-T cells can detect a broad range of targeted antigens within subcellular compartments and hold great potential for use in cancer therapy. Numerous studies have been conducted to evaluate the efficacy and feasibility of CAR and TCR based adoptive cell therapies (ACT). A comprehensive understanding of genetically-modified T cell technologies can facilitate the clinical translation of these adoptive cell-based immunotherapies. Here, we systematically review the state-of-the-art knowledge on genetically-modified T-cell therapy and provide a summary of preclinical and clinical trials of CAR and TCR-transgenic ACT.

show abstract

Engineered TCR-T Cell Immunotherapy in Anticancer Precision Medicine: Pros and Cons

Cited by 75 publications

References 104 publications

Prognostic Biomarkers in Uveal Melanoma: The Status Quo, Recent Advances and Future Directions

Prognostic Biomarkers in Uveal Melanoma: The Status Quo, Recent Advances and Future Directions

Implications of Antigen Selection on T Cell-Based Immunotherapy

Genetically Modified T Cells for Esophageal Cancer Therapy: A Promising Clinical Application

Contact Info

Product

Resources

About