Your search keyword '"t-cell receptor"' showing total 231 results

1. T-Cell Receptors Cross-Reactive to Coronaviral Epitopes Homologous to the SPR Peptide.

Author

Serdyuk, Yana V., Zornikova, Ksenia V., Dianov, Dmitry V., Ivanova, Nataliia O., Davydova, Vassa D., Fefelova, Ekaterina I., Nenasheva, Tatiana A., Sheetikov, Saveliy A., and Bogolyubova, Apollinariya V.

Subjects

*COVID-19, *SARS-CoV-2, *PEPTIDES, *COVID-19 pandemic, *IMMUNE response

Abstract

The COVID-19 pandemic caused by the rapid spread of the novel coronavirus SARS-CoV-2, has promoted an interest in studying the T-cell immune response. It was found that the polyclonal and cross-reactive T-cell response against seasonal coronaviruses and other SARS-CoV-2 strains reduced disease severity. We investigated the immunodominant T-cell epitope SPRWYFYYYL from the nucleocapsid protein of SARS-CoV-2. The immune response to this epitope is characterized by the formation of highly homologous (convergent) receptors that have been found in the T-cell receptor (TCR) repertoires of different individuals. This epitope belongs to a group of highly conserved peptides that are rarely mutated in novel SARS-CoV-2 strains and are homologous to the epitopes of seasonal coronaviruses. It has been suggested that the cross-reactive response to homologous peptides contributes to the reduction of COVID-19 severity. However, some investigators have questioned this hypothesis, suggesting that the low affinity of the cross-reactive receptors reduces the strength of the immune response. The aim of this study was to evaluate the effect of amino acid substitutions in the SPR epitope on its binding affinity to specific TCRs. For this, we performed antigen-dependent cellular expansions were performed using samples from four COVID-19-transfected donors and sequenced their TCR repertoires. The resulting SPR-specific repertoire of β-chains in TCRs had a greater sequence diversity than the repertoire of α-chains. However, the TCR repertoires of all four donors contained public receptors, three of which were cloned and used to generate the Jurkat E6-1 TPR cell line. Only one of these receptors was activated by the SPR peptide and recognized with the same affinity by its mutant homologue LPRWYFYYY from seasonal coronaviruses. This indicates that the presence of the mutation did not affect the strength of the immune response, which may explain why the cross-reactive response to the SPR epitope is so frequent and contributes positively to COVID-19 infection. [ABSTRACT FROM AUTHOR]

Published

2024

2. Characteristics of T cell premature senescence in maintenance hemodialysis patients.

Author

Wu, Wangshu, Song, Ahui, Xie, Kewei, Lu, Jiayue, Zhao, Bingru, Qian, Cheng, Wang, Minzhou, Min, Lulin, Hong, Wenkai, Pang, Huihua, Lu, Renhua, and Gu, Leyi

Subjects

*T-cell exhaustion, *HEMODIALYSIS patients, *P16 gene, *HDL cholesterol, *T cell receptors

Abstract

Background: Uremia-associated immunodeficiency, mainly characterized by T cell dysfunction, exists in patients on maintenance hemodialysis (MHD) and promotes systemic inflammation. However, T cell senescence, one of the causes of T cell dysfunction, has not been clearly revealed yet. In this cross-sectional research, we aimed to study the manifestation of T cell premature senescence in MHD patients and further investigate the associated clinical factors. Methods: 76 MHD patients including 33 patients with cardiovascular diseases (CVD) and 28 patients with arteriovenous fistula (AVF) event history were enrolled in this study. Complementarity determining region 3 (CDR3) of T cell receptor (TCR) was analyzed by immune repertoire sequencing (IR-Seq). CD28- T cell subsets and expression of senescence marker p16 and p21 genes were detected by multicolor flow cytometry and RT-qPCR, respectively. Results: MHD patients had significantly decreased TCR diversity (P < 0.001), increased CDR3 clone proliferation (P = 0.001) and a left-skewed CDR3 length distribution. The proportion of CD4 + CD28- T cells increased in MHD patients (P = 0.014) and showed a negative correlation with TCR diversity (P = 0.001). p16 but not p21 expression in T cells was up-regulated in MHD patients (P = 0.039). Patients with CVD exhibited increased expression of p16 and p21 genes (P = 0.010 and 0.004, respectively), and patients with AVF events showed further TCR diversity and evenness reduction (P = 0.002 and 0.017, respectively) compared to patients without the comorbidities. Moreover, age, average convection volume, total cholesterol, high-density lipoprotein cholesterol and transferrin saturation were associated with TCR diversity or CD4 + CD28- T cell proportion (P < 0.05). Conclusions: MHD patients undergo T cell premature senescence characterized by significant TCR diversity reduction and repertoire skew, as well as accumulation of the CD4 + CD28- subset and up-regulation of p16 gene. Patients with CVD or AVF events show higher level of immunosenescence. Furthermore, T cell senescence in MHD patients is associated with blood cholesterol and uremic toxin retention, suggesting potential intervention strategies in the future. [ABSTRACT FROM AUTHOR]

Published

2024

3. Expression, Purification, and Crystallization of the Vγ9Vδ2 T-cell Receptor Recognizing Protein/Peptide Antigens.

Author

Cheng, Chaofei, Zhao, Zhendong, and Liu, Guangzhi

Subjects

*PEPTIDES, *PROTEIN receptors, *T cells, *MYCOBACTERIAL diseases, *CRYSTALLIZATION, *HEAT shock proteins, *T cell receptors, *MOLECULAR recognition

Abstract

γδ T cells, especially Vγ9Vδ2 T cells, play an important role in mycobacterial infection. We have identified some Vγ9Vδ2 T cells that recognize protein/peptide antigens derived from mycobacteria, which may induce protective immune responses to mycobacterial infection. To clarify the structural basis of the molecular recognition mechanism, we tried many methods to express the Vγ9Vδ2 T-cell receptor (TCR). The Vγ9Vδ2 TCR was not expressed well in a prokaryotic expression system or a baculovirus expression system, even after extensive optimization. In a mammalian cell expression system, the Vγ9Vδ2 TCR was expressed in the form of a soluble heterodimer, which was suitable for crystal screening. Reduced-temperature cultivation (cold shock) increased the yield of the recombinant TCR. The recombinant purified TCR was used for crystal trials, and crystals that could be used for X-ray diffraction were obtained. Although we have not yet determined the crystal structure of the Vγ9Vδ2 TCR, we have established a procedure for Vγ9Vδ2 TCR expression and purification, which is useful for basic research and potentially for clinical application. [ABSTRACT FROM AUTHOR]

Published

2023

4. Specific Genetic Polymorphisms Contributing in Differential Binding of Gliadin Peptides to HLA-DQ and TCR to Elicit Immunogenicity in Celiac Disease.

Author

Banerjee, Pratibha, Chaudhary, Ramprasad, Singh, Atul Kumar, Parulekar, Pratima, Kumar, Shashank, and Senapati, Sabyasachi

Subjects

*GLIADINS, *GENETIC polymorphisms, *CELIAC disease, *IMMUNE response, *PEPTIDES, *BINDING sites

Abstract

Immunogenicity of gliadin peptides in celiac disease (CD) is majorly determined by the pattern of molecular interactions with HLA-DQ and T-cell receptors (TCR). Investigation of the interactions between immune-dominant gliadin peptides, DQ protein, and TCR are warranted to unravel the basis of immunogenicity and variability contributed by the genetic polymorphisms. Homology modeling of HLA and TCR done using Swiss Model and iTASSER, respectively. Molecular interactions of eight common deamidated immune-dominant gliadin with HLA-DQ allotypes and specific TCR gene pairs were evaluated. Docking of the three structures was performed with ClusPro2.0 and ProDiGY was used to predict binding energies. Effects of known allelic polymorphisms and reported susceptibility SNPs were predicted on protein–protein interactions. CD susceptible allele, HLA-DQ2.5 was shown to have considerable binding affinity to 33-mer gliadin (ΔG = − 13.9; Kd = 1.5E − 10) in the presence of TRAV26/TRBV7. Higher binding affinity was predicted (ΔG = − 14.3, Kd = 8.9E − 11) when TRBV28 was replaced with TRBV20 paired with TRAV4 suggesting its role in CD predisposition. SNP rs12722069 at HLA-DQ8 that codes Arg76α forms three H-bonds with Glu12 and two H-bonds with Asn13 of DQ2 restricted gliadin in the presence of TRAV8-3/TRBV6. None of the HLA-DQ polymorphisms was found to be in linkage disequilibrium with reported CD susceptibility markers. Haplotypic presentations of rs12722069-G, rs1130392-C, rs3188043-C and rs4193-A with CD reported SNPs were observed in sub-ethnic groups. Highly polymorphic sites of HLA alleles and TCR variable regions could be utilized for better risk prediction models in CD. Therapeutic strategies by identifying inhibitors or blockers targeting specific gliadin:HLA-DQ:TCR binding sites could be investigated. [ABSTRACT FROM AUTHOR]

Published

2023

5. Revolutionizing cancer treatment: a comprehensive review of CAR-T cell therapy.

Author

Dabas, Preeti and Danda, Adithi

Abstract

Chimeric antigen receptor (CAR)-T cell therapy is a promising new treatment for cancer that involves genetically modifying a patient's T-cells to recognize and attack cancer cells. This review provides an overview of the latest discoveries and clinical trials related to CAR-T cell therapy, as well as the concept and applications of the therapy. The review also discusses the limitations and potential side effects of CAR-T cell therapy, including the high cost and the risk of cytokine release syndrome and neurotoxicity. While CAR-T cell therapy has shown promising results in the treatment of hematologic malignancies, ongoing research is needed to improve the efficacy and safety of the therapy and expand its use to solid tumors. With continued research and development, CAR-T cell therapy has the potential to revolutionize cancer treatment and improve outcomes for patients with cancer. [ABSTRACT FROM AUTHOR]

Published

2023

6. Single‐cell profiling of muscle‐infiltrating T cells in idiopathic inflammatory myopathies

Author

Alexandra Argyriou, Begum Horuluoglu, Angeles Shunashy Galindo‐Feria, Juan Sebastian Diaz‐Boada, Merel Sijbranda, Antonella Notarnicola, Lara Dani, Annika vanVollenhoven, Daniel Ramsköld, Inger Nennesmo, Maryam Dastmalchi, Ingrid E Lundberg, Lina‐Marcela Diaz‐Gallo, and Karine Chemin

Subjects

HOBIT, idiopathic inflammatory myopathies, muscle, T‐cell receptor, tissue resident memory T cells, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract Idiopathic inflammatory myopathies (IIM) are rare autoimmune systemic diseases characterized by muscle weakness and the presence of muscle‐infiltrating T cells. IIM represent a clinical challenge due to heterogeneity of symptoms and variability of response to immunosuppressive treatment. Here, we performed in‐depth single‐cell sequencing on muscle‐infiltrating T cells and peripheral blood memory T cells in six patients with recently diagnosed IIM. We identified tissue resident memory T‐cell (TRM) signatures including the expression of HOBIT, XCL1 and CXCR6 in the muscle biopsies of all patients with IIM. Clonally expanded T‐cell clones were mainly found among cytotoxic and TRM implying their role in the disease pathogenesis. Finally, identical expanded T‐cell clones persisting at follow‐up in the muscle tissue of two patients suggest their involvement in disease chronicity. Our study reveals a muscle tissue resident memory T‐cell signature in patients with IIM and a transcriptomic map to identify novel therapeutic targets in IIM.

Published

2023

7. Clinical features, laboratory characteristics, and outcome of ETP and TCRA/D aberrations in pediatric patients with T-acute lymphoblastic leukemia.

Author

Ashry, Mona S. El, Radwan, Enas, Abdellateif, Mona S., Arafah, Omar, and Hassan, Naglaa M.

Subjects

CHILD patients, LYMPHOBLASTIC leukemia, LEUCOCYTES, FLUORESCENCE in situ hybridization, GENE amplification

Abstract

Background: T-cell acute lymphoblastic leukemia (T-ALL) is an aggressive malignancy with few accepted prognostic factors that limit the efficiency of therapy. The aim of the current study was to assess the clinical and laboratory features of T-cell receptor (TCR) aberrations and early T-cell precursor (ETP) subtype as well as their outcome to therapy. Methods: Sixty-three newly diagnosed pediatric T-ALL patients were assessed for the ETP status using immunophenotyping. Screening of TCRA/D aberrations was done by fluorescent in situ hybridization (FISH). The data were correlated to the patients' clinical features, response to treatment, and survival rates. Results: Seven patients (11%) had ETP-ALL. The ETP-ALL patients were older (P = 0.013), presented with lower white blood cell (WBC) count (P = 0.001) and lower percentage of peripheral blood (PB) blast cells (P = 0.037), more likely to have hyperdiploid karyotype (P = 0.009), and had been associated with TCRA/D gene amplification (P = 0.014) compared to other T-ALL patients. Of note, the same associations had been significantly observed in patients with TCRA/D gene amplification. Patients with TCRA/D amplification frequently coincided with TCRβ aberrations (P = 0.025). TCR-β aberrations were significantly associated with negative MRD at the end of induction compared to TCR-β-negative patients. There was a nonsignificant trend of ETP-positive cases to have lower overall survival (OS) (P = 0.06). Patients with TCR aberrations had no significant differences regarding disease-free survival (DFS) or OS rates compared to those with normal TCR. Conclusion: ETP-ALL patients tend to have increased mortalities. There was no significant impact of TCR aberrations on the survival rates of the patients. [ABSTRACT FROM AUTHOR]

Published

2023

8. Recombinant Human Cyclophilin A in Combination with Adoptive T-cell Therapy Improves the Efficacy of Cancer Immunotherapy in Experimental Models in vivo.

Author

Kalinina, Anastasiia A., Kazansky, Dmitry B., and Khromykh, Ludmila M.

Subjects

*CYCLOPHILINS, *CYTOTOXIC T cells, *T cells, *TRANSGENIC mice, *IMMUNE response, *IMMUNOTHERAPY

Abstract

Adoptive T-cell therapy (ACT) is successfully applied in cancer treatment; however, its efficiency can be limited by a low viability, short persistence time, and loss of functional activity of T-cells after adoptive transfer. The search for novel immunomodulators that can improve the viability, expansion, and functions of T-cells after their infusion with the minimal side effects could contribute to the development of more efficient and safe ACT strategies. Recombinant human cyclophilin A (rhCypA) is of particular interest in this respect, as it exhibits pleiotropic immunomodulatory activity and stimulates both innate and adaptive anti-tumor immunity. Here, we evaluated the effect of rhCypA on the efficacy of ACT in the mouse EL4 lymphoma model. Lymphocytes from transgenic 1D1a mice with an inborn pool of EL4-specific T-cells were used as a source of tumor-specific T-cells for ACT. In models of immunocompetent and immunodeficient transgenic mice, the course (3 days) rhCypA administration was shown to significantly stimulate EL4 rejection and prolong the overall survival of tumor-bearing mice after adoptive transfer of lowered doses of transgenic 1D1a cells. Our studies showed that rhCypA significantly improved the efficacy of ACT by enhancing the effector functions of tumor-specific cytotoxic T-cells. These findings open up the prospects for the development of innovative strategies of adoptive T-cell immunotherapy for cancer using rhCypA as an alternative to existing cytokine therapies. [ABSTRACT FROM AUTHOR]

Published

2023

9. T-cell receptor diversity in minimal change disease in the NEPTUNE study.

Author

Liu, Shiying, Bush, William S., Miskimen, Kristy, Gonzalez-Vicente, Agustin, Bailey, Jessica N. Cooke, Konidari, Ioanna, McCauley, Jacob L., Sedor, John R., O'Toole, John F., and Crawford, Dana C.

Subjects

*DISEASE progression, *SEQUENCE analysis, *CELL receptors, *HYPOTHESIS, *IMMUNITY, *DESCRIPTIVE statistics, *RESEARCH funding, *T cells, *LONGITUDINAL method, *FOCAL segmental glomerulosclerosis, *DISEASE remission

Abstract

Background: Minimal change disease (MCD) is the major cause of childhood idiopathic nephrotic syndrome, which is characterized by massive proteinuria and debilitating edema. Proteinuria in MCD is typically rapidly reversible with corticosteroid therapy, but relapses are common, and children often have many adverse events from the repeated courses of immunosuppressive therapy. The pathobiology of MCD remains poorly understood. Prior clinical observations suggest that abnormal T-cell function may play a central role in MCD pathogenesis. Based on these observations, we hypothesized that T-cell responses to specific exposures or antigens lead to a clonal expansion of T-cell subsets, a restriction in the T-cell repertoire, and an elaboration of specific circulating factors that trigger disease onset and relapses. Methods: To test these hypotheses, we sequenced T-cell receptors in fourteen MCD, four focal segmental glomerulosclerosis (FSGS), and four membranous nephropathy (MN) patients with clinical data and blood samples drawn during active disease and during remission collected by the Nephrotic Syndrome Study Network (NEPTUNE). We calculated several T-cell receptor diversity metrics to assess possible differences between active disease and remission states in paired samples. Results: Median productive clonality did not differ between MCD active disease (0.0083; range: 0.0042, 0.0397) and remission (0.0088; range: 0.0038, 0.0369). We did not identify dominant clonotypes in MCD active disease, and few clonotypes were shared with FSGS and MN patients. Conclusions: While these data do not support an obvious role of the adaptive immune system T-cells in MCD pathogenesis, further study is warranted given the limited sample size. A higher resolution version of the Graphical abstract is available as Supplementary information. [ABSTRACT FROM AUTHOR]

Published

2023

10. Chemical Complementarity of Blood-Sourced, Breast Cancer-Related TCR CDR3s and the CMV UL29 and IE1 Antigens is Associated with Worse Overall Survival.

Author

Neerumalla, Pooja, Jain, Rahul, Aboujaoude, Michael. T., Hudock, Tabitha R., Song, Joanna J., Cao, Bryan H., Chobrutskiy, Andrea, Chobrutskiy, Boris I., and Blanck, George

Subjects

*CYTOMEGALOVIRUS diseases, *ANTIGEN receptors, *OVERALL survival, *BREAST cancer, *IMMUNOCOMPROMISED patients

Abstract

Cytomegalovirus (CMV) infection is common and becomes a particular concern in immunocompromised patients. Understanding the potential role CMV plays in breast cancer patients’ disease progression is important for providing more patient-specific treatments. In this study, we analyzed whether a breast cancer patient’s blood-sourced T-cell receptor (TCR) complementarity determining-3 (CDR3) amino acid (AA) sequences could provide an indication of the impact of a systemic CMV infection. Specifically, we assessed the chemical complementarity of patient TCR CDR3 AAs and CMV antigens to determine whether patients with greater complementarity also represented different survival probabilities. Initially, we examined five distinct CMV antigens, of which two, IE1 and UL29, represented TCR (TRA+ RB)-CDR3-CMV antigen complementarity scores (CSs) whereby cases representing the upper 50th percentile of CSs had a worse overall survival (log-rank p = 5.034E-3, for IE1). Then, an analysis of CSs representing previously identified, TCR IE1 epitopes indicated that greater TRB CDR3-IE1 epitope complementarities represented a worse OS (log-rank p = 0.0111). These results raise the question of whether a systemic, anti-CMV response leads to increased systemic inflammation, which is either directly or indirectly supportive of tumor growth; or are patients succumbing to a direct impact of CMV functions on tumor growth or metastasis? [ABSTRACT FROM AUTHOR]

Published

2024

11. Preclinical development of T-cell receptor-engineered T-cell therapy targeting the 5T4 tumor antigen on renal cell carcinoma.

Author

Xu, Yuexin, Morales, Alicia J., Cargill, Michael J., Towlerton, Andrea M. H., Coffey, David G., Warren, Edus H., and Tykodi, Scott S.

Subjects

*TUMOR antigens, *RENAL cell carcinoma, *GENETIC vectors, *T cells, *RNA sequencing, *TROPHOBLASTIC tumors

Abstract

5T4 (trophoblast glycoprotein, TPBG) is a transmembrane tumor antigen expressed on more than 90% of primary renal cell carcinomas (RCC) and a wide range of human carcinomas but not on most somatic adult tissues. The favorable expression pattern has encouraged the development and clinical testing of 5T4-targeted antibody and vaccine therapies. 5T4 also represents a compelling and unexplored target for T-cell receptor (TCR)-engineered T-cell therapy. Our group has previously isolated high-avidity CD8+ T-cell clones specific for an HLA-A2-restricted 5T4 epitope (residues 17–25; 5T4p17). In this report, targeted single-cell RNA sequencing was performed on 5T4p17-specific T-cell clones to sequence the highly variable complementarity-determining region 3 (CDR3) of T-cell receptor α chain (TRA) and β chain (TRB) genes. Full-length TRA and TRB sequences were cloned into lentiviral vectors and transduced into CD8+ T-cells from healthy donors. Redirected effector T-cell function against 5T4p17 was measured by cytotoxicity and cytokine release assays. Seven unique TRA-TRB pairs were identified. All seven TCRs exhibited high expression on CD8+ T-cells with transduction efficiencies from 59 to 89%. TCR-transduced CD8+ T-cells demonstrated redirected cytotoxicity and cytokine release in response to 5T4p17 on target-cells and killed 5T4+/HLA-A2+ kidney-, breast-, and colorectal-tumor cell lines as well as primary RCC tumor cells in vitro. TCR-transduced CD8+ T-cells also detected presentation of 5T4p17 in TAP1/2-deficient T2 target-cells. TCR-transduced T-cells redirected to recognize the 5T4p17 epitope from a broadly shared tumor antigen are of interest for future testing as a cellular immunotherapy strategy for HLA-A2+ subjects with 5T4+ tumors. [ABSTRACT FROM AUTHOR]

Published

2019

12. T-Zell-Immunreaktionen bei chronisch entzündlichen Erkrankungen der nasalen Schleimhäute.

Author

Klimek, L., Casper, I., Siemer, S., Wollenberg, B., Stauber, R., and Koennecke, M.

Abstract

Copyright of HNO is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2019

13. T-cell receptor-β V and J usage, in combination with particular HLA class I and class II alleles, correlates with cancer survival patterns.

Author

Callahan, Blake M., Yavorski, John M., Tu, Yaping N., Tong, Wei Lue, Kinskey, Jacob C., Clark, Kendall R., Fawcett, Timothy J., and Blanck, George

Subjects

*CANCER genetics, *HLA class II antigens, *TUMOR immunology, *T-cell receptor genes, *EXOMES, *ALLELES

Abstract

Class I and class II HLA proteins, respectively, have been associated with subsets of V(D)J usage resulting from recombination of the T-cell receptor (TCR) genes. Additionally, particular HLA alleles, in combination with dominant TCR V(D)J recombinations, have been associated with several autoimmune diseases. The recovery of TCR recombination reads from tumor specimen exome files has allowed rapid and extensive assessments of V(D)J usage, likely for cancer resident T-cells, across relatively large cancer datasets. The results from this approach, in this report, have permitted an extensive alignment of TCR-β VDJ usage and HLA class I and II alleles. Results indicate the correlation of both better and worse cancer survival rates with particular TCR-β, V and J usage-HLA allele combinations, with differences in median survival times ranging from 7 to 130 months, depending on the cancer and the specific TCR-β V and J usage/HLA class allele combination. [ABSTRACT FROM AUTHOR]

Published

2018

14. Human c-SRC kinase (CSK) overexpression makes T cells dummy.

Author

Inderberg, Else Marit, Mensali, Nadia, Oksvold, Morten P., Fallang, Lars-Egil, Fåne, Anne, Skorstad, Gjertrud, Stenvik, Grethe-Elisabeth, Progida, Cinzia, Bakke, Oddmund, Kvalheim, Gunnar, Myklebust, June H., and Wälchli, Sébastien

Subjects

*CANCER immunotherapy, *GENETIC overexpression, *CELLULAR therapy, *T cell receptors, *PROTEIN kinases, *CELLULAR signal transduction

Abstract

Adoptive cell therapy with T-cell receptor (TCR)-engineered T cells represents a powerful method to redirect the immune system against tumours. However, although TCR recognition is restricted to a specific peptide-MHC (pMHC) complex, increasing numbers of reports have shown cross-reactivity and off-target effects with severe consequences for the patients. This demands further development of strategies to validate TCR safety prior to clinical use. We reasoned that the desired TCR signalling depends on correct pMHC recognition on the outside and a restricted clustering on the inside of the cell. Since the majority of the adverse events are due to TCR recognition of the wrong target, we tested if blocking the signalling would affect the binding. By over-expressing the c-SRC kinase (CSK), a negative regulator of LCK, in redirected T cells, we showed that peripheral blood T cells inhibited anti-CD3/anti-CD28-induced phosphorylation of ERK, whereas TCR proximal signalling was not affected. Similarly, overexpression of CSK together with a therapeutic TCR prevented pMHC-induced ERK phosphorylation. Downstream effector functions were also almost completely blocked, including pMHC-induced IL-2 release, degranulation and, most importantly, target cell killing. The lack of effector functions contrasted with the unaffected TCR expression, pMHC recognition, and membrane exchange activity (trogocytosis). Therefore, co-expression of CSK with a therapeutic TCR did not compromise target recognition and binding, but rendered T cells incapable of executing their effector functions. Consequently, we named these redirected T cells “dummy T cells” and propose to use them for safety validation of new TCRs prior to therapy. [ABSTRACT FROM AUTHOR]

Published

2018

15. T Lymphocytes with Modified Specificity in the Therapy of Malignant Diseases.

Author

Vdovin, A., Bykova, N., and Efimov, G.

Subjects

*T cells, *CANCER treatment, *LYMPHOCYTES, *CANCER cells, *IMMUNE system

Abstract

Immunotherapy is one of the most rapidly progressing and promising fields in antitumor therapy. It is based on the idea of using immune cells of patient or healthy donors for elimination of malignant cells. T lymphocytes play a key role in cell-mediated immunity including the response to tumors. Recently developed approaches of altering antigen specificity of T cells consist of their genetic modification (introduction of additional T cell receptor or chimeric antigen receptor), as well as the use of bispecific molecules that crosslink target and effector cells. These approaches are used to retarget T lymphocytes with arbitrary specificity against tumor antigens in the context of antitumor immunotherapy. The high potential of T cell immunotherapy was demonstrated in a number of clinical trials. In the future, it is possible to develop approaches to the therapy of a wide spectrum of tumors. The selection of the optimal antigen is the main challenge in successful T cell immunotherapy, as it largely determines the effectiveness of the treatment, as well as the risk of side effects. In this review we discuss potential methods of modification of T cell specificity and targets for immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2017

16. T-Cell Receptor-Engineered Cells for the Treatment of Hematologic Malignancies.

Author

Hossain, Nasheed, Chapuis, Aude, and Walter, Roland

Abstract

Recent attention in adoptive immunotherapy for hematologic malignancies has focused on lymphocytes expressing chimeric antigen receptors. An alternative technique to redirect the immune system toward cancer cells involves the use of T-cells carrying an engineered tumor-recognizing T-cell receptor (TCR). This approach allows targeting of surface or intracellular/nuclear proteins as long as they are processed and presented on the cell surface by human leukocyte antigen molecules. Several trials in advanced solid tumors, particularly melanoma and synovial sarcoma, support the validity of this strategy, although tumor responses have often been short-lived. Emerging data from patients with multiple myeloma and myeloid neoplasms suggest that the benefit of TCR-modified cells may extend to blood cancers. Methodological refinements may be necessary to increase the in vivo persistence and functionality of these cells. Particularly with affinity-enhanced TCRs, however, more effective therapies may increase the potential for serious toxicity due to the unexpected on- or off-target reactivity. [ABSTRACT FROM AUTHOR]

Published

2016

17. Backbone resonance assignment of N15, N30 and D10 T cell receptor β subunits.

Author

Mallis, Robert, Reinherz, Ellis, Wagner, Gerhard, and Arthanari, Haribabu

Abstract

The αβT Cell receptor (TCR) governs T cell immunity through its interaction with peptide bound to major histocompatibility complex molecules (pMHC). Previously, soluble ectodomain constructs have been used to elucidate the binding mode of the TCR for the MHC. However, the full heterodimeric αβTCR has proven difficult to produce reproducibly in recombinant systems to the extent seen in the routine production of novel antibodies. Particularly, the route of production in E. coli, which is most convenient for isotopic labeling of proteins, is challenging for a wide range of αβTCR, including N15αβ, N30αβ, but not D10αβ. With the aim of understanding the TCR-pMHC interaction through the use of dynamic binding measurements, we set out to produce TCRβ subunits with which we could investigate binding with pMHC. The TCRβ constructs are more readily produced and refolded than their αβ counterparts and have proven to be an effective model of preTCR in pMHC binding studies. As a first step towards characterizing potential interactions with protein ligands, we have assigned the backbone resonances of three TCRβ subunits, N15β, N30β and D10β. [ABSTRACT FROM AUTHOR]

Published

2016

18. Immunoscoring by correlating MHC class II and TCR expression: high level immune functions represented by the KIRP dataset of TCGA.

Author

Butler, Shanitra and Blanck, George

Subjects

*MAJOR histocompatibility complex, *CANCER cells, *CANCER genetics, *NUCLEOTIDE sequence, *GENE expression, *RENAL cancer diagnosis, *STATISTICAL correlation, *BIOMARKERS

Abstract

The Cancer Genome Atlas (TCGA) is primarily oriented towards revealing the status of cancer cells but TCGA RNASeq data have the potential of representing gene expression for a variety of cells that are included during RNA preparation, i.e., cells that cannot be removed from the microenvironment during cancer sample isolation. Thus, we seek to determine whether RNASeq data can be used to pioneer greater precision for immunoscoring. We obtained the RNASeq results for HLA class II genes, the class II transactivator (CIITA) and T-cell receptor (TCR) alpha segments. The data indicated strong degrees of correlation of HLA class II expression with TCR expression. Furthermore, biomarkers of professional antigen-presenting cells also correlated with TCR expression, with the kidney renal papillary cell carcinoma (KIRP) dataset indicative of the highest level, immune function microenvironment. These analyses indicate that an immune function signature, with probable internal HLA class II-TCR verifications, can be obtained from individual TCGA samples; this in turn indicates that such signatures might provide a basis for correlations with prognosis or for convenient indications of therapy options, such as tumor-infiltrating lymphocyte availability for ex-vivo amplification. Although tumor immunoscoring has been proposed, the above analysis represents the first immunoscoring approach that correlates antigen presentation capacity with TCR mRNA expression. [ABSTRACT FROM AUTHOR]

Published

2016

19. Epigenetic Control of T-Cell Receptor Locus Rearrangements in Normal and Aberrant Conditions.

Author

del Blanco, Beatriz, Angulo, Úrsula, and Hernández-Munain, Cristina

Abstract

V(D)J recombination is the process responsible for the exclusive expression of one antigen receptor form, either T-cell receptor (TCR) or immunoglobulin (Ig), per individual T or B lymphocyte, respectively. This process is, therefore, essential for adaptive immune responses in vertebrates and it consists of the assembly of disperse gene segments present at the TCR and Ig loci to obtain a genetic structure that is able to encode a functional protein. V(D)J recombination is highly regulated during lymphocyte development and depends on the activation of accessibility control elements (ACEs) to direct the recruitment of the specific endonuclease RAG-1/2 to its site-specific target sequences that flank the gene segments. The RAG-1/2-mediated DNA cleavage at these loci is controlled by changes in the epigenome. These changes are derived from chromatin modification, transcriptional elongation, the location of the loci within the nucleus, and the three-dimensional architecture of the loci, which is controlled by functional interplay among ACEs and their bound trans-factors. This epigenetic control ultimately leads to the juxtapositioning or synapsis of two gene segments that are normally distantly located and the recombination reaction itself. This process must be completed without any errors to avoid the potential risk of generating aberrant translocations that could result in the generation of leukemia. This chapter summarizes the advances in this area at the TCR loci and the importance of regulating this potentially risky process during thymocyte development. [ABSTRACT FROM AUTHOR]

Published

2014

20. Indispensable epigenetic control of thymic epithelial cell development and function by polycomb repressive complex 2

Author

Rushika C. Wirasinha, Hong Ying Teh, Adam E. Handel, Stephen R. Daley, Benoit Roch, Saulius Žuklys, Stuart H. Orkin, Thomas Barthlott, Jean-Pierre de Villartay, Katrin Hafen, and Georg A. Holländer

Subjects

0301 basic medicine, CD4-Positive T-Lymphocytes, Male, Lineage (genetic), Science, TEC, T cell, T-Lymphocytes, education, Receptors, Antigen, T-Cell, General Physics and Astronomy, Autoimmunity, Mice, Transgenic, macromolecular substances, Thymus Gland, CD8-Positive T-Lymphocytes, General Biochemistry, Genetics and Molecular Biology, Article, Epigenesis, Genetic, 03 medical and health sciences, 0302 clinical medicine, Antigen, medicine, Animals, Cell Lineage, Epigenetics, Multidisciplinary, Thymocytes, biology, T-cell receptor, Polycomb Repressive Complex 2, hemic and immune systems, Cell Differentiation, Epithelial Cells, General Chemistry, Epigenetics in immune cells, Cell biology, Thymus, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, Clonal selection, biology.protein, Female, PRC2, tissues, 030217 neurology & neurosurgery, Function (biology)

Abstract

Thymic T cell development and T cell receptor repertoire selection are dependent on essential molecular cues provided by thymic epithelial cells (TEC). TEC development and function are regulated by their epigenetic landscape, in which the repressive H3K27me3 epigenetic marks are catalyzed by polycomb repressive complex 2 (PRC2). Here we show that a TEC-targeted deficiency of PRC2 function results in a hypoplastic thymus with reduced ability to express antigens and select a normal repertoire of T cells. The absence of PRC2 activity reveals a transcriptomically distinct medullary TEC lineage that incompletely off-sets the shortage of canonically-derived medullary TEC whereas cortical TEC numbers remain unchanged. This alternative TEC development is associated with the generation of reduced TCR diversity. Hence, normal PRC2 activity and placement of H3K27me3 marks are required for TEC lineage differentiation and function and, in their absence, the thymus is unable to compensate for the loss of a normal TEC scaffold., Development of the T cells requires functions from thymic epithelial cells, whose development and function are epigenetically regulated. Here the authors show that inactivation of the polycomb repressive complex 2 (PRC2) alters the H3K27me3 configuration, reduces TEC functions, reveals a specific TEC subset, and hampers T cell development.

Published

2021

21. Primer on Immunoendocrinology.

Author

Jasinski, Jean and Eisenbarth, George S.

Abstract

This book on immunoendocrinology deals primarily with -autoimmune disorders. The study of endocrine autoimmune diseases has played a prominent role in advancing the understanding of autoimmunity including creation of the first models of induced autoimmune disease (1), demonstration that autoimmunity can cause human pathology (2), and characterization of remarkable syndromes linking multiple autoimmune diseases, as well as the first discovery of genes contributing to multiple diseases such mutations of the AIRE (Autoimmune Regulator) gene (3  ) of APS-1 (Autoimmune Polyendocrine Syndrome) and a specific polymorphism (R620W) of the PTPN22 gene associated with type 1 diabetes and rheumatoid arthritis (4, 5  ). Autoimmunity can be driven primarily by autoantibodies (e.g., targeting of the TSH-receptor by antibodies in Graves΄ disease) or predominantly by T cells (e.g., Type 1A diabetes), but in general, both humoral and cellular autoimmunity occur together. Autoimmune endocrine disorders may affect single organs, a few organs, or many organs. Regardless of the number of organs affected, the underlying autoimmune disease mechanisms are similar with potential variation in the probability of loss of tolerance. In general, persons suffering from rare single organ-specific autoimmune diseases tend to develop multi-organ autoimmunity over time. [ABSTRACT FROM AUTHOR]

Published

2011

22. Genetically Engineered Antigen Specificity in T Cells for Adoptive Immunotherapy.

Author

Powell Jr, Daniel J. and Levine, Bruce L.

Abstract

Antigen specificity has been genetically conferred to human T cells for therapy through the transfer of sequences encoding antigen-specific T-cell receptors (TCRs) or through the antigen-specific antibody-based chimeric antigen receptors (CARs). By either method, the advantage of the adoptive transfer of modified T cells over immunotherapies developed to date such as vaccines or cytokines alone is that T cells have the ability to directly traffic to the site of tumor or infection, to multiply at that site, and to persist in a memory state for months to years. [ABSTRACT FROM AUTHOR]

Published

2011

23. Mechanisms and Implications of Immunodominance in CD8+ T-Cell Responses.

Author

Perreault, Claude

Abstract

Immunodominant Major Histocompatibility Complex class I (MHC I)- associated epitopes suppress T-cell responses against cryptic epitopes. That is, when confronted with complex antigens, CD8+ T cells respond to only a few ˵immunodominant″ epitopes and neglect other ˵cryptic″ peptides that would otherwise be immunogenic when presented alone. Immunodominant epitopes are better immunogens than cryptic epitopes. Compared with T cells specific for cryptic epitopes, CD8+ T cells that recognize immunodominant epitopes interact with their antigen with higher avidity, are primed after a shorter duration of antigen presentation, expand more swiftly and extensively, and generate more potent effector function. Furthermore, by curtailing the duration of Ag presentation [through deletion or exhaustion of antigen presenting cells (APCs)], immunodominant CD8+ effector T cells selectively impair priming against cryptic epitopes. Immunodominance results in one major advantage and one potential drawback: that is, immunodominance favors expansion of the fittest effector T cells but may enhance the risk of immune escape by antigen-loss variants. Targeting immunodominant epitopes is probably crucial not only for success of immune responses against pathogens but also in cancer immunotherapy. Indeed, CD8+ T cells targeted to immunodominant but not cryptic minor histocompatibility antigens can eradicate leukemia and melanoma in mice. In this chapter, I will review the current state-of-the-art regarding T-cell immunodominance and discuss key elements of ongoing and future research in this area. [ABSTRACT FROM AUTHOR]

Published

2011

24. Molecular Techniques in Hematopathology.

Author

Boyanton Jr, Bobby L. and Rushton, Jennifer R.

Abstract

The discipline of hematopathology traditionally relies upon morphologic evaluation, cytochemical stains, immunohistochemistry, flow cytometry, and karyotypic analysis to classify hematolymphoid neoplasms. Although these time-honored methods still comprise the primary diagnostic arsenal of the pathologist, the last few decades have borne witness to the widespread acceptance of molecular techniques to classify these neoplasms. No longer considered ancillary, molecular analyses have led to a greater understanding of the biological and clinical heterogeneity of hematolymphoid neoplasms, and now form the primary diagnostic criteria for many diagnoses as set forth by the World Health Organization [1]. They also provide extremely sensitive and specific methods for prognostic marker detection and minimal residual disease monitoring. These techniques have evolved rapidly over the last decade from Southern blot and hybridization assays to polymerase chain reaction and its variants to gene expression profiling and single-nucleotide polymorphism analysis, and more recently to microarray technology and whole-genome analysis. Despite technological advancements, molecular techniques are critically dependent upon the nature of nucleic acids retrieved from the specimen. Results cannot be correctly interpreted if the quantity and/or the integrity of nucleic acids are not optimal for the desired molecular application. As such, the purpose of this chapter is twofold. First, issues pertaining to specimen collection, handling and processing, and nucleic acid extraction, stability, and storage are reviewed. Second, molecular techniques commonly utilized in hematopathology are reviewed. Cytogenetics, fluorescent in situ hybridization (FISH), and microarray techniques are discussed in Chapter 2. [ABSTRACT FROM AUTHOR]

Published

2010

25. Multiple Sclerosis and Other Demyelinating Diseases.

Author

Soldan, Samantha S., Wu, Gregory, Markowitz, Clyde, and Kolson, Dennis L.

Abstract

Multiple sclerosis (MS) is the most common idiopathic demyelinating disease of the central nervous system (CNS). Although partially effective treatments are now available, MS represents a major target for research into the development of disease-modifying therapies that specifically focus on the neuroimmune pathways of myelin and tissue damage that currently are incompletely understood. Multiple sclerosis is considered to be an example of development of autoimmunity to self-antigens within the CNS through multiple initiating events that include infections and other environmental factors. The direct or indirect induction of immune responses against CNS antigens includes chemotaxis of T cells, B cells, and monocytes, and production of immunoglobulin responses, each of which can act as an effector of myelin damage that occurs in distinct histological patterns. Because a specific cause for MS has not been identified, much MS research has focused on CNS immune responses triggered by unidentified insults that in turn trigger inflammation-mediated cascades of myelin and cellular damage that are likely relevant to other neurodegenerative diseases. This chapter discusses current the epidemiology, etiology, pathophysiology, animal models, virus models and recent advances in the neuroimmunology of MS from the perspective of the potential for development of newer therapies for MS and other inflammatory CNS diseases. [ABSTRACT FROM AUTHOR]

Published

2008

26. Adoptive T-cell therapy for hematological malignancies using T cells gene-modified to express tumor antigen-specific receptors.

Author

Fujiwara, Hiroshi

Abstract

The functional properties of the adoptive immune response mediated by effector T lymphocytes are decisively regulated by their T-cell receptors (TCRs). Transfer of genes encoding target antigen-specific receptors enables polyclonal T cells to redirect toward cancer cells and virally infected cells expressing those defined antigens. Using this technology, a large population of redirected T cells displaying uniform therapeutic properties has been produced, powerfully advancing their clinical application as 'cellular drugs' for adoptive immunotherapy against cancer. Clinically, anticancer adoptive immunotherapy using these genetically engineered T cells has an impressive and proven track record. Notable examples include the dramatic benefit of chimeric antigen receptor gene-modified T cells redirected towards B-cell lineage antigen CD19 in patients with chronic lymphocytic leukemia, and the impressive outcomes in the use of TCR gene-modified T cells redirected towards NY-ESO-1, a representative cancer-testis antigen, in patients with advanced melanoma and synovial cell sarcoma. In this review, we briefly overview the current status of this treatment option in the context of hematological malignancy, and discuss a number of challenges that still pose an obstacle to the full effectiveness of this strategy. [ABSTRACT FROM AUTHOR]

Published

2014

27. Cytotoxic human peripheral blood-derived γδT cells kill glioblastoma cell lines: implications for cell-based immunotherapy for patients with glioblastoma.

Author

Nakazawa, Tsutomu, Nakamura, Mitsutoshi, Park, Young, Motoyama, Yasushi, Hironaka, Yasuo, Nishimura, Fumihiko, Nakagawa, Ichiro, Yamada, Shuichi, Matsuda, Ryosuke, Tamura, Kentaro, Sugimoto, Tadashi, Takeshima, Yasuhiro, Marutani, Akiko, Tsujimura, Takahiro, Ouji, Noriko, Ouji, Yukiteru, Yoshikawa, Masahide, and Nakase, Hiroyuki

Abstract

Glioblastoma (GBM) is a highly aggressive brain tumor for which novel therapeutic approaches, such as immunotherapy, are urgently needed. Zoledronate (ZOL), an inhibitor of osteoclastic activity, is known to stimulate peripheral blood-derived γδT cells and sensitize tumors to γδT cell-mediated killing. To investigate the feasibility of γδT cell-based immunotherapy for patients with GBM, we focused on the killing of GBM cell lines by γδT cells and the molecular mechanisms involved in these cell-cell interactions. Peripheral blood mononuclear cells were expanded in ZOL and interleukin (IL)-2 for 14 days, and γδT cells were enriched in the expanded cells by the immunomagnetic depletion of αβT cells. Gliomas are resistant to NK cells but susceptible to lymphokine-activated killer cells and some cytotoxic T lymphocytes. When the γδT cell-mediated killing of three GBM cell lines (U87MG, U138MG and A172 cells) and an NK-sensitive leukemia cell line (K562 cells) were tested, 32 % U87MG, 15 % U138MG, 1 % A172, and 50 % K562 cells were killed at an effector:target ratio of 5:1. The γδT cell-mediated killing of all three GBM cell lines was significantly enhanced by ZOL and this ZOL-enhanced killing was blocked by an anti-T cell receptor (TcR) antibody. These results indicated that TcR γδ is crucial for the recognition of ZOL-treated GBM cells by γδT cells. Since the low level killing of GBM cells by the γδT cells was enhanced by ZOL, γδT cell-targeting therapy in combination with ZOL treatment could be effective for patients with GBM. [ABSTRACT FROM AUTHOR]

Published

2014

28. Human cancer germline antigen-specific cytotoxic T cell: What can we learn from patient

Author

Yanchun Peng, Tao Dong, and M Abd Hamid

Subjects

0301 basic medicine, Cytotoxicity, Immunologic, Cellular immunity, medicine.medical_treatment, Immunology, Receptors, Antigen, T-Cell, immune check point receptor, chemical and pharmacologic phenomena, Cancer immunotherapy, Review Article, Germline, 03 medical and health sciences, Epitopes, 0302 clinical medicine, Antigens, Neoplasm, Neoplasms, immune therapy, medicine, Immunology and Allergy, Cytotoxic T cell, Humans, business.industry, T-cell receptor, Cancer, hemic and immune systems, medicine.disease, CTL, 030104 developmental biology, Infectious Diseases, Germ Cells, 030220 oncology & carcinogenesis, Cancer research, cancer antigen, T cell receptor, business, CD8, cytotoxic T cell

Abstract

In this review, we will highlight the importance of cancer germline antigen-specific cytotoxic CD8+ T lymphocytes (CTL) and the factors affecting antitumor CTL responses. In light of cancer immunotherapy, we will emphasis the need to further understand the features, characteristics, and actions of modulatory receptors of human cancer germline-specific CTLs, in order to determine the optimal conditions for antitumor CTL responses.

Published

2020

29. Characteristics of New Monomolecular Chimeric T-Cell Receptors to Carcinoembryonic Antigen.

Author

Bozhenko, V. K., Shramova, E. I., Shishkin, A. M., Ivanov, A. V., Khokhlova, E. V., Lebedin, Yu. S., and Shkoporov, A. N.

Subjects

*CHIMERIC proteins, *T cell receptors, *CARCINOEMBRYONIC antigen, *GENETIC code, *IMMUNOGLOBULINS, *IMMUNOTHERAPY

Abstract

We described two original genetic constructs encoding chimeric monomolecular T-cell receptors, where the effector T-cell receptor fragment was linked with the antigen-recognizing part consisting of two variable fragments of two different antibodies to carcinoembryonic antigen. Following transfection, these receptors were expressed on the cell surface and bound carcinoembryonic antigen. Human peripheral blood lymphocytes transfected with the above constructs demonstrated high cytotoxic activity against HCT116 cells expressing carcinoembryonic antigen. [ABSTRACT FROM AUTHOR]

Published

2013

30. Adoptive Zelltherapien in der Hämatologie und Onkologie.

Author

Thomas, S., Hauptrock, B., Theobald, M., and Herr, W.

Abstract

Copyright of Der Onkologe is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2012

31. T cells specific for lipid antigens.

Author

Mori, Lucia and Libero, Gennaro

Abstract

Lipid-specific T cells are important participants in human immune responses. Recognition of lipid antigens contributes to host defense against pathogens that can cause debilitating diseases, including mycobacterial, viral, and parasitic infections. Lipid-specific T cells also play important roles in various autoimmune diseases, atherosclerosis, and in tumor surveillance. A better understanding of the mechanisms that regulate lipid-reactive T-cell functions will enable the development of novel therapies across a wide range of diseases. In recent years, our laboratory has investigated lipid antigen specificities, mechanisms of lipid antigen presentation, molecular interaction of lipid antigens with CD1 antigen-presenting molecules, and the pathogenic and regulatory functions of lipid-specific T cells in a variety of disease settings. In this review, we present recent data that illustrate the critical role played by lipid-specific immune responses in host protection, with a particular focus on human studies. [ABSTRACT FROM AUTHOR]

Published

2012

32. Widespread expressions of immunoglobulin superfamily proteins in cancer cells.

Author

Lee, Gregory, Zhu, Mingang, Ge, Bixia, and Potzold, Suzanne

Subjects

*CANCER immunotherapy, *T cell receptors, *EPITOPES, *IMMUNOGLOBULINS, *CELL adhesion molecules, *ANTINEOPLASTIC agents, *CANCER cell growth, *MONOCLONAL antibodies, *CONFERENCES & conventions

Abstract

RP215 monoclonal antibody (Mab) was shown to recognize a carbohydrate-associated epitope of cancer cell-expressed glycoproteins, known as CA215. Extensive MALDI-TOF MS analysis was performed to search for the molecular identity of CA215. Besides immunoglobulin (Ig) heavy chains, homology to human T-cell receptors (TCR) and Ig-like cell adhesion molecules was also detected. By using RT-PCR and cDNA sequencing, it was observed that as many as 80% of cancer cell lines showed significant levels of gene expressions of TCR-α and TCR-β. Selected Ig-like cell adhesion molecules such as CD47, CD54, CD58 and CD 147 were also highly expressed among all the cell lines tested. In contrast, co-receptors and co-stimulators of TCR such as CD3, CD4 and CD8 were rarely expressed demonstrating the non-functional nature of TCR in cancer cells. Results of immunohistochemical staining and Western blot assays of cancer cell lines as well as cancerous tissue sections were consistent with these observations. Anti-TCR and anti-human IgG antibodies were shown to induce complement-dependent cytotoxicity and apoptosis of cultured cancer cells indicating the surface nature of Ig-like proteins. Based on these experimental observations, it was hypothesized that the expressions of these immunoglobulin superfamily (IgSF) proteins may be relevant to the immune protection and proliferations of cancer cells during carcinogenesis or cancer progression. Surface-bound TCR-like proteins as well as immunoglobulins may be the potential targets for RP215-based anti-cancer drugs. [ABSTRACT FROM AUTHOR]

Published

2012

33. Mechanisms controlling granule-mediated cytolytic activity of cytotoxic T lymphocytes.

Author

Anikeeva, Nadia and Sykulev, Yuri

Abstract

Cytotoxic T lymphocytes (CTL) play a critical role in immunity against viruses and cancer. The antigen receptor or T-cell receptor (TCR) on CTL determines the specificity toward target cells. The CD8 co-receptor functions in concert with the TCR to enhance TCR-mediated signaling, accounting for the remarkable sensitivity and swift signaling kinetics of the CTL response. The latter ensures efficient delivery and release of lytic granules, resulting in sensitive and rapid destruction of target cells. [ABSTRACT FROM AUTHOR]

Published

2011

34. Conformational studies of immunodominant myelin basic protein 1-11 analogues using NMR and molecular modeling.

Author

Laimou, Despina, Lazoura, Eliada, Troganis, Anastassios, Matsoukas, Minos-Timotheos, Deraos, Spyros, Katsara, Maria, Matsoukas, John, Apostolopoulos, Vasso, and Tselios, Theodore

Subjects

*MYELIN basic protein, *NUCLEAR magnetic resonance, *MOLECULAR dynamics, *PEPTIDES, *DIMETHYL sulfoxide, *MAJOR histocompatibility complex, *CONFORMATIONAL analysis

Abstract

Τwo dimensional nuclear magnetic resonance studies complimented by molecular dynamics simulations were conducted to investigate the conformation of the immunodominant epitope of acetylated myelin basic protein residues 1-11 (Ac-MBP) and its altered peptide ligands, mutated at position 4 to an alanine (Ac-MBP[4A]) or a tyrosine residue (Ac-MBP[4Y]). Conformational analysis of the three analogues indicated that they adopt an extended conformation in DMSO solution as no long distance NOE connectivities were observed and seem to have a similar conformation when bound to the active site of the major histocompatibility complex (MHC II). The interaction of each peptide with MHC class II I-A was further investigated in order to explore the molecular mechanism of experimental autoimmune encephalomyelitis induction/inhibition in mice. The present findings indicate that the Gln residue, which serves as a T-cell receptor (TCR) contact site in the TCR/peptide/I-A complex, has a different orientation in the mutated analogues especially in the Ac-MBP[4A] peptide. In particular the side chain of Gln is not solvent exposed as for the native Ac-MBP and it is not available for interaction with the TCR. [ABSTRACT FROM AUTHOR]

Published

2011

35. In vitro generated anti-tumor T lymphocytes exhibit distinct subsets mimicking in vivo antigen-experienced cells.

Author

Yang, Shicheng, Luca, Gattinoni, Liu, Fang, Ji, Yun, Yu, Zhiya, Restifo, Nicholas, Rosenberg, Steven, and Morgan, Richard

Subjects

*T cells, *TUMOR antigens, *PHENOTYPES, *CYTOKINES, *TUMOR immunology, *GENETIC vectors, *CANCER treatment, *GENE therapy, *LENTIVIRUSES

Abstract

The T-lymphocyte pool can be subdivided into naïve (Tn), effector memory (Tem), and central memory (Tcm) T cells. In this study, we characterized in vitro short-term cultured anti-tumor human T lymphocytes generated by lentiviral transduction with an anti-tumor antigen TCR vector. Within 2 weeks of in vitro culture, the cultured T cells showed a Tcm-like phenotype illustrated by a high percentage of CD62L and CD45RO cells. When the cells were sorted into populations that were CD45RO+/CD62L-(Tem), CD45RO+/CD62L+(Tcm), or CD45RO/CD62L+(Tn) and co-cultured with antigen-matched tumor lines, the magnitude of cytokine release from these populations for IFNγ (Tn < Tcm < Tem) and IL-2 (Tn > Tcm > Tem) mimicked the types of immune cell responses observed in vivo . In comparing cell-mediated effector function, Tn were found to be deficient (relative to Tcm and Tem) in the ability to form conjugates with tumor cells and subsequent lytic activity. Moreover, analysis of the gene expression profiles of the in vitro cultured and sorted T-cell populations also demonstrated patterns consistent with their in vivo counterparts. When Tcm and Tem were tested for the ability to survive in vivo, Tcm displayed significantly increased engraftment and persistence in NOD/SCID/γc mice. In general, a large percentage of in vitro generated anti-tumor T lymphocytes mimic a Tcm-like phenotype (based on phenotype, effector function, and increased persistence in vivo), which suggests that these Tcm-like cultured T cells may be optimal for adoptive immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2011

36. Stage-specific functions of E-proteins at the β-selection and T-cell receptor checkpoints during thymocyte development.

Author

Jones, Mary and Zhuang, Yuan

Abstract

The E-protein transcription factors E2A and HEB function in a lineage- and stage-specific manner to orchestrate many critical events throughout lymphocyte development. The function of E-proteins in both B- and T-lymphocyte development has been extensively studied through the use of single-gene knockout animals. Unlike B cells, which rely primarily on E2A alone, T cells are regulated by the combinatorial expression of both E2A and HEB. Therefore, many of the roles of E-proteins during T-cell development may be masked in single-gene knockout studies due to the compensatory function of E2A and HEB. More recently, our laboratory has established double-conditional knockout models to eliminate both E2A and HEB in a stage-specific manner throughout T-cell development. These models, in combination with other complimentary genetic approaches, have identified new E-protein functions at each of the two major T-cell developmental checkpoints. Here, we will discuss how E-proteins function to regulate the expression of T-cell receptor components and cell cycle at the β-selection checkpoint, and how they control positive selection, survival, and lineage-specific gene expression at the subsequent T-cell receptor checkpoint. [ABSTRACT FROM AUTHOR]

Published

2011

37. Receptor signaling in immune cell development and function.

Author

Zhong, Xiao-Ping, Shin, Jinwook, Gorentla, Balachandra, O'Brien, Tommy, Srivatsan, Sruti, Xu, Li, Chen, Yong, Xie, Danli, and Pan, Hongjie

Abstract

Immune cell development and function must be tightly regulated through cell surface receptors to ensure proper responses to pathogen and tolerance to self. In T cells, the signal from the T-cell receptor is essential for T-cell maturation, homeostasis, and activation. In mast cells, the high-affinity receptor for IgE transduces signal that promotes mast cell survival and induces mast cell activation. In dendritic cells and macrophages, the toll-like receptors recognize microbial pathogens and play critical roles for both innate and adaptive immunity against pathogens. Our research explores how signaling from these receptors is transduced and regulated to better understand these immune cells. Our recent studies have revealed diacylglycerol kinases and TSC1/2-mTOR as critical signaling molecules/regulators in T cells, mast cells, dendritic cells, and macrophages. [ABSTRACT FROM AUTHOR]

Published

2011

38. Orchestrating T-cell receptor α gene assembly through changes in chromatin structure and organization.

Author

Shih, Han-Yu, Hao, Bingtao, and Krangel, Michael

Abstract

V(D)J recombination is regulated through changes in chromatin structure that allow recombinase proteins access to recombination signal sequences and through changes in three-dimensional chromatin organization that bring pairs of distant recombination signal sequences into proximity. The Tcra/Tcrd locus is complex and undergoes distinct recombination programs in double negative and double positive thymocytes that lead to the assembly of Tcrd and Tcra genes, respectively. Our studies provide insights into how locus chromatin structure is regulated and how changes in locus chromatin structure can target and then retarget the recombinase to create developmental progressions of recombination events. Our studies also reveal distinct locus conformations in double negative and double positive thymocytes and suggest how these conformations may support the distinct recombination programs in the two compartments. [ABSTRACT FROM AUTHOR]

Published

2011

39. Inhibition of Lck enhances glucocorticoid sensitivity and apoptosis in lymphoid cell lines and in chronic lymphocytic leukemia.

Author

Harr, M. W., Caimi, P. F., McColl, K. S., Zhong, F., Patel, S. N., Barr, P. M., and Distelhorst, C. W.

Subjects

*LYMPHOCYTIC leukemia, *GLUCOCORTICOIDS, *ADRENOCORTICAL hormones, *THERAPEUTICS, *T cells, *LEUKEMIA treatment

Abstract

Glucocorticoids are used as part of front-line therapy to treat lymphoid malignancy because of their remarkable ability to induce apoptosis. Yet, in T cells, glucocorticoid-induced apoptosis is readily inhibited by lymphocyte activation and signaling. We have previously shown that the Src family kinase, Lck (lymphocyte cell-specific tyrosine kinase), which is predominantly expressed in T cells, interacts with IP3 receptors to facilitate calcium signaling. Here, we discovered that dexamethasone downregulates Lck, which, in turn, suppresses lymphocyte activation by inhibiting pro-survival calcium oscillations. Moreover, stable expression of shRNAs that selectively targeted Lck or treatment with the Src inhibitor dasatinib (BMS-354825) enhanced apoptosis induction by dexamethasone. To investigate the effect of Lck inhibition in a primary leukemia model, we employed chronic lymphocytic leukemia (CLL) cells that aberrantly expressed Lck and were relatively insensitive to dexamethasone. Lck expression was correlated with resistance to dexamethasone in CLL cells, and its inhibition by dasatinib or other inhibitors markedly enhanced glucocorticoid sensitivity. Collectively, these data indicate that Lck protects cells from glucocorticoid-induced apoptosis and its inhibition enhances sensitivity to dexamethasone. Small-molecule inhibitors of Lck, such as dasatinib, may function to reverse glucocorticoid resistance in some lymphoid malignancies. [ABSTRACT FROM AUTHOR]

Published

2010

40. Production of a Soluble Disulfide Bond-Linked TCR in the Cytoplasm of Escherichia coli trxB gor Mutants.

Author

Liddy, Nathaniel, Molloy, Peter, Bennett, Alan, Boulter, Jonathan, Jakobsen, Bent, and Li, Yi

Abstract

Previously, we have described the use of phage display to generate high affinity disulfide bond-linked T cell receptors (TCRs). The affinities of the mutant TCRs were analysed after refolding of separately expressed α and β chains from Escherichia coli inclusion bodies. This approach is only suitable for the analysis of small numbers of TCR variants. An attractive alternative would be soluble expression within the bacterial periplasm, but the generic production of TCRs within the E. coli periplasm has so far not proved successful. Here we show that functional, soluble TCR can be produced within the cytoplasm of trxB gor mutant E. coli strains, with maximum yields of 3.4 mg/l. We also investigated the effect of coexpressing the folding modulators Skp and DsbC finding that the TCR expression levels were largely unaffected by these chaperones. Importantly, we demonstrated that the amount of protein purified from 50 ml starter cultures was sufficient to show functionality of the TCR by specific antigen binding in both ELISA and surface plasmon resonance (SPR) assays. This TCR production method has the potential to allow rapid and medium throughput analysis of affinity-matured TCRs selected from TCR phage display libraries. [ABSTRACT FROM AUTHOR]

Published

2010

41. Backbone resonance assignment of Staphylococcal Enterotoxin H.

Author

Saline, Maria, Orekhov, Vladislav, Lindkvist-Petersson, Karin, and Karlsson, B.

Abstract

The staphylococcal enterotoxin H (SEH; 217 aa, 25 kD) belongs to a family of superantigens that cause a massive immune response upon simultaneous binding to the T cell receptor (TCR) and the major histocompatibility complex class II. The SEH-TCR interaction is weak and amenable to studies using NMR methodology. Essentially, 2 mg of U{2H, 13C,15N}-labeled SEH was used for the complete sequential backbone assignment of SEH at 900 MHz. The protein secondary structure inferred from the chemical shift index (Cα and Cβ) is in very good agreement with the secondary structure elements of the X-ray structure. [ABSTRACT FROM AUTHOR]

Published

2010

42. PCR-based clonality assessment in patients with lymphocytic leukaemias: a single-institution experience.

Author

CIKOTA, BOJANA M., TUKIĆ, LJILJANA J., TARABAR, OLIVERA T., STAMATOVIĆ, DRAGANA T., ELEZ, MARIJA N., and MAGIĆ, ZVONKO M.

Subjects

*DIAGNOSTIC use of polymerase chain reaction, *LYMPHOCYTIC leukemia, *HUMAN cloning, *BONE marrow, *BLOOD testing, *LYMPHOPROLIFERATIVE disorders, *DIAGNOSIS

Abstract

PCR-based clonality testing can be performed in all lymphoproliferations by analysing gene rearrangements of antigen receptors, rearrangements that are unique for each kind of lymphocyte. Reactive lymphoproliferations have polyclonally rearranged Ig/TCR genes, whereas malignant proliferations (leukaemias and lymphomas) show clonal rearrangements. The aim of this study was to assess the clinical benefits of clonality testing with previously evaluated consensus primers in leukaemia patients. The study included peripheral blood and bone marrow samples of 67 leukaemia patients (32 B-CLL, 24 B-ALL and 11 T-ALL). Clonality testing was based on PCR amplification of rearranged IgH and TCR genes. During diagnosis, monoclonal pattern was found in all analysed B-CLL and T-ALL samples. Testing in B-ALL patients showed positive results in all bone marrow and one peripheral blood samples. Results of clonality testing in B-CLL patients during follow-up were concordant between peripheral blood and bone marrow. Obtained results corresponded to clinical course in all but one patient. In B-ALL group, results of molecular testing in peripheral blood and bone marrow confirmed remission estimated according to clinical criteria in all except one patient. Before any clinical sign of relapse, monoclonal pattern was found in six/seven patients by bone marrow and in three/seven patients by peripheral blood analysis, respectively. Results of molecular monitoring in T-ALL patients did not confirme clinical evaluation in two patients. Obtained results indicate high accuracy of re-evaluated primers for clonality assessment in ALL and CLL patients at the time of diagnosis. Results of clonality testing in B-ALL patients indicate that bone marrow analysis has higher sensitivity compared to analysis of peripheral blood. [ABSTRACT FROM AUTHOR]

Published

2009

43. The Major Players in Adaptive Immunity.

Author

Ahmed, Asma, Saha, Banishree, Patwardhan, Anand, Shivaprasad, Shwetha, and Nandi, Dipankar

Subjects

IMMUNE system, IMMUNE response, IMMUNOLOGY, CARCINOGENS, HAZARDOUS substances, ALLERGENS, IMMUNOGLOBULINS, B cells

Abstract

Our immune system, by and large, does a fine job in protecting us from opportunistic and infectious microbes, potential carcinogens and allergens. It is therefore crucial to understand the organization of the immune network. This article focuses on some important features and key players involved in adaptive immune response. The first part of the article dealt with the humoral immune response mediated mainly by immunoglobulins produced by the B cells. The second part deals with T cells, the Major Histocompatibility Complex (MHC)-encoded molecules, and Recombination Activating Genes (RAG) responsible for generating diverse B-cell receptors (BCR) and T-cell receptors (TCR). With the advent of newer and smarter infectious agents, it is important to understand the working of the immune network as more research in this area may facilitate the development of better protective strategies. [ABSTRACT FROM AUTHOR]

Published

2009

44. Rapid αβ TCR-mediated responses in γδ T cells transduced with cancer-specific TCR genes.

Author

Hiasa, A., Nishikawa, H., Hirayama, M., Kitano, S., Okamoto, S., Chono, H., Yu, SS, Mineno, J., Tanaka, Y., Minato, N., Kato, I., and Shiku, H.

Subjects

*T cells, *CANCER, *GENES, *IMMUNE response, *THERAPEUTICS

Abstract

Adoptive T-cell transfer of in vitro cultured T cells derived from cancer patients with naturally developed immune responses has met with some success as an immunotherapeutic approach, although only a limited number of patients showed spontaneous immune responses. To find alternative ways, such as cancer-specific T-cell receptor (TCR) gene transfer, in preparation for sufficient numbers of antigen-specific T cells is an important issue in the field of adoptive T-cell therapy. Given the inherent disadvantage of αβ TCR transfer to other αβ T cells, namely the possible formation of mixed TCR heterodimers with endogenous α or β TCR, we employed γδ T cells as a target for retroviral transfer of cancer-specific TCR and examined whether γδ T cells were useful as an alternative population for TCR transfer. Although retroviral transduction to γδ T cells with TCR αβ genes alone, isolated from a MAGE-A4143–151-specific αβ CD8+ cytotoxic T lymphocyte (CTL) clone, did not provide sufficient affinity to recognize major histocompatibility (MHC)–peptide complexes due to the lack of CD8 co-receptor, γδ T cells co-transduced with TCR αβ and CD8 αβ genes acquired cytotoxicity against tumor cells and produced cytokines in both αβ- and γδ-TCR-dependent manners. Furthermore, αβ TCR and CD8-transduced γδ T cells, stimulated either through αβ TCR or γδ TCR, rapidly responded to target cells compared with conventional αβ T cells, reminiscent of γδ T cells. We propose αβ TCR-transduced γδ T cells as an alternative strategy for adoptive T-cell transfer.Gene Therapy (2009) 16, 620–628; doi:10.1038/gt.2009.6; published online 26 February 2009 [ABSTRACT FROM AUTHOR]

Published

2009

45. Characterization of MHC class-I restricted TCRαβ+ CD4− CD8− double negative T cells recognizing the gp100 antigen from a melanoma patient after gp100 vaccination.

Author

Voelkl, Simon, Moore, Tamson V., Rehli, Michael, Nishimura, Michael I., Mackensen, Andreas, and Fischer, Karin

Subjects

*IMMUNE response, *MELANOMA, *CANCER, *T cells, *LYMPHOCYTES

Abstract

The immune attack against malignant tumors require the concerted action of CD8+ cytotoxic T lymphocytes (CTL) as well as CD4+ T helper cells. The contribution of T cell receptor (TCR) αβ+ CD4− CD8− double-negative (DN) T cells to anti-tumor immune responses is widely unknown. In previous studies, we have demonstrated that DN T cells with a broad TCR repertoire are present in humans in the peripheral blood and the lymph nodes of healthy individuals. Here, we characterize a human DN T cell clone (T4H2) recognizing an HLA-A2-restricted melanoma-associated antigenic gp100-peptide isolated from the peripheral blood of a melanoma patient. Antigen recognition by the T4H2 DN clone resulted in specific secretion of IFN-γ and TNF. Although lacking the CD8 molecule the gp100-specifc DN T cell clone was able to confer antigen-specific cytotoxicity against gp100-loaded target cells as well as HLA-A2+ gp100 expressing melanoma cells. The cytotoxic capacity was found to be perforin/granzymeB-dependent. Together, these data indicate that functionally active antigen-specific DN T cells recognizing MHC class I-restricted tumor-associated antigen (TAA) may contribute to anti-tumor immunity in vivo. [ABSTRACT FROM AUTHOR]

Published

2009

46. T cell CD3 receptor zeta (TCRζ)-chain expression in children with idiopathic nephrotic syndrome.

Author

Aviles, Diego H., Vehaskari, Matti V., Culotta, Kirk S., Manning, Jennifer, Ochoa, Augusto C., and Zea, Arnold H.

Subjects

*NEPHROTIC syndrome in children, *KIDNEY diseases, *JUVENILE diseases, *INFECTION, *T cells, *MESSENGER RNA

Abstract

Children with idiopathic nephrotic syndrome (INS) have an increased risk of developing life-threatening infections. Several studies have demonstrated functional abnormalities in the T lymphocytes of patients with nephrotic syndrome. Although T cells are activated in INS during relapse, as indicated by an increased expression of interleukin (IL)-2 receptor, these cells have a decreased ability to proliferate. The T-cell receptor (TCR) plays an important role in signal transduction and T cell activation, with the TCR-zeta (TCRζ) chain being a key element in early signaling. We measured the expression of the TCRζ chain in patients with INS (steroid resistant and steroid sensitive) during relapse and remission by flow cytometry and by PCR ELISA. The results showed a significant decrease in the expression of the TCRζ chain at both the protein and mRNA level in INS patients during relapse as compared with normal controls ( p < 0.05). In contrast, when patients with INS achieved remission, the expression of TCRζ normalized and was similar to that expressed in normal controls. Therefore, a decreased expression of the TCRζ chain may explain the abnormal function of T cells in patients with INS, and it may also contribute to the increased risk for infections seen in these patients. [ABSTRACT FROM AUTHOR]

Published

2009

47. Different Allelic Distribution of a Single SNP Between Sexes in Humans.

Author

Tripputi, P., Cigognini, D., Bianchi, S., and Fedele, L.

Subjects

*CHROMOSOME polymorphism, *ALLELES, *T cell receptors, *SEX-linkage (Genetics), SEX differences (Biology)

Abstract

We searched for a difference in allele distribution between males and females of a single nucleotide polymorphism located in the human beta T-cell receptor, in 500 subjects (200 males and 300 females). Genotype analysis gave the following results: among the males, 114 (57%) were heterozygous for the T/C polymorphism, 52 (26%) were homozygous (T/T), and 34 (17%) were homozygous (C/C). Among the females, 142 (47.3%) were heterozygous, 73 (24.3%) were homozygous (T/T), and 85 (28.3%) were homozygous (C/C). The allele frequency was significantly different between sexes (χ2 = 8.799, P = 0.012). [ABSTRACT FROM AUTHOR]

Published

2008

48. Development of optimal bicistronic lentiviral vectors facilitates high-level TCR gene expression and robust tumor cell recognition.

Author

Yang, S, Cohen, C J, Peng, P D, Zhao, Y, Cassard, L, Yu, Z, Zheng, Z, Jones, S, Restifo, N P, Rosenberg, S A, and Morgan, R A

Subjects

*LENTIVIRUSES, *CANCER treatment, *GENE therapy, *GENE expression, *CELL receptors, *PEPTIDES

Abstract

In human gene therapy applications, lentiviral vectors may have advantages over γ-retroviral vectors in several areas, including the ability to transduce nondividing cells, resistance to gene silencing and a potentially safer integration site profile. However, unlike γ-retroviral vectors it has been problematic to drive the expression of multiple genes efficiently and coordinately with approaches such as internal ribosome entry sites or dual promoters. Using different 2A peptides, lentiviral vectors expressing two-gene T-cell receptors directed against the melanoma differentiation antigens gp100 and MART-1 were constructed. We demonstrated that addition of amino-acid spacer sequences (GSG or SGSG) before the 2A sequence is a prerequisite for efficient synthesis of biologically active T-cell receptors and that addition of a furin cleavage site followed by a V5 peptide tag yielded optimal T-cell receptor gene expression. Furthermore, we determined that the furin cleavage site was recognized in lymphocytes and accounted for removal of residual 2A peptides at the post-translational level with an efficiency of 20–30%, which could not be increased by addition of multiple furin cleavage sites. The novel bicistronic lentiviral vector developed herein afforded robust anti-melanoma activities to engineered peripheral blood lymphocytes, including cytokine secretion, cell proliferation and lytic activity. Such optimal vectors may have immediate applications in cancer gene therapy.Gene Therapy (2008) 15, 1411–1423; doi:10.1038/gt.2008.90; published online 22 May 2008 [ABSTRACT FROM AUTHOR]

Published

2008

49. Long-term phenotypic, functional and genetic stability of cancer-specific T-cell receptor (TCR) αβ genes transduced to CD8+ T cells.

Author

Hiasa, A., Hirayama, M., Nishikawa, H., Kitano, S., Nukaya, I., Yu, S. S., Mineno, J., Kato, I., and Shiku, H.

Subjects

*T cell receptors, *CD antigens, *CELL lines, *INTERFERONS, *LEUCOCYTES

Abstract

In adoptive T-cell transfer as an intervention for malignant diseases, retroviral transfer of T-cell receptor (TCR) genes derived from CD8+ cytotoxic T-lymphocyte (CTL) clones provides an opportunity to generate a large number of T cells with the same antigen specificity. We cloned the TCR-αβ genes from a human leukocyte antigen (HLA)-A*2402-restricted CTL clone specific for MAGE-A4143–151. The TCR-αβ genes were transduced to 99.2% of non-TCR expressing SupT1, a human T-cell line, and to 12.7–32.6% of polyclonally activated CD8+ T cells by retroviral transduction. As expected, TCR-αβ gene-modified CD8+ T cells showed cytotoxic activity and interferon-γ production in response to peptide-loaded T2-A*2402 and tumor cell lines expressing both MAGE-A4 and HLA-A*2402. A total of 24 clones were established from TCR-αβ gene-transduced peripheral blood mononuclear cells and all clones were functional on a transduced TCR-dependent manner. Four clones were kept in culture over 6 months for analyses in detail. The transduced TCR-αβ genes were stably maintained phenotypically, functionally and genetically. Our results indicate that TCR-transduced αβ T cells by retroviral transduction represent an efficient and promising strategy for adoptive T-cell transfer for long term.Gene Therapy (2008) 15, 695–699; doi:10.1038/sj.gt.3303099; published online 21 February 2008 [ABSTRACT FROM AUTHOR]

Published

2008

50. Induction of tolerance and immunity by redirected B cell-specific cytolytic T lymphocytes.

Author

Nguyen, P., Duthoit, C. T., and Geiger, T. L.

Subjects

*T-cell receptor genes, *EPITOPES, *LYMPHOCYTES, *IMMUNITY, *LIGANDS (Biochemistry), *CLINICAL trials

Abstract

Chimeric receptors bearing ligand recognition domains linked to signaling regions from the T-cell receptor can redirect T lymphocytes against non-MHC-restricted targets. Cytolytic T lymphocytes (CTL) expressing these chimeric receptors are being tested in preclinical and clinical trials for activity in cancer, infectious diseases and autoimmunity. The chimeric receptors may incorporate antigenic epitopes previously unrecognized by the immune system. Whether a receptor-specific antibody response develops to these neoantigens and whether such a response inhibits therapeutic cell activity is unknown. We hypothesized that upon engagement of a chimeric receptor-specific B cell, receptor-modified CTL will be activated, lysing the B cell and inducing tolerance to the chimeric receptor rather than immunity. We demonstrate that receptor-modified CTL are indeed stimulated by cognate receptor-specific B cells, proliferate and produce cytokines in response and kill the B cells in vitro and in vivo. However, this is insufficient to induce full B-cell tolerance. Modified CTL induce a chimeric receptor-specific antibody response independent of any other source of antigen. Nevertheless, the CTL retain substantial activity even in the presence of saturating doses of receptor-specific antibody. Thus antichimeric receptor antibody responses need to be considered in the clinical use of chimeric receptor-modified T cells. However, the inhibitory activity of these antibodies may in cases be limited.Gene Therapy (2007) 14, 1739–1749; doi:10.1038/sj.gt.3303045; published online 11 October 2007 [ABSTRACT FROM AUTHOR]

Published

2007