Your search keyword '"Riddell SR"' showing total 11 results

1. Dual Targeting with CAR T Cells to Limit Antigen Escape in Multiple Myeloma.

Author

Simon S and Riddell SR

Abstract

Adoptive T-cell therapy targeting a single tumor antigen can induce remissions of hematologic cancers but relapses often occur due to the outgrowth of tumor cells with absent or low expression of the antigen. Strategies to simultaneousy target multiple antigens are needed to fully capitalize on the promise of this therapeutic strategy. In this issue of Blood Cancer Discovery , Fernández de Larrea and colleagues demonstrate in preclinical models of multiple myeloma that targeting BCMA and GPRC5D simultaneously with T cells engineered to express chimeric antigen receptors specific for these antigens may prevent tumor cell escape. See related article by Fernández de Larrea et al., p. 146 ., Competing Interests: S.R. Riddell reports grants and personal fees from Lyell Immunopharma and personal fees from Juno Therapeutics/a BMS company outside the submitted work; in addition, S.R. Riddell has a patent for “Combination Therapies for Treatment of BCMA-related cancers and autoimmune disorders” pending and licensed to Juno Therapeutics, a BMS company. No potential conflicts of interest were disclosed by the other author., (©2020 American Association for Cancer Research.)

Published

2020

2. Systemic Interferon-γ Increases MHC Class I Expression and T-cell Infiltration in Cold Tumors: Results of a Phase 0 Clinical Trial.

Author

Zhang S, Kohli K, Black RG, Yao L, Spadinger SM, He Q, Pillarisetty VG, Cranmer LD, Van Tine BA, Yee C, Pierce RH, Riddell SR, Jones RL, and Pollack SM

Subjects

Adult, Aged, Antigens, Neoplasm immunology, Biomarkers, Biopsy, Cytokines, Female, Humans, Immunophenotyping, Liposarcoma, Myxoid etiology, Liposarcoma, Myxoid immunology, Liposarcoma, Myxoid pathology, Liposarcoma, Myxoid therapy, Lymphocytes, Tumor-Infiltrating pathology, Male, Middle Aged, Sarcoma, Synovial etiology, Sarcoma, Synovial immunology, Sarcoma, Synovial pathology, Sarcoma, Synovial therapy, Young Adult, Histocompatibility Antigens Class I genetics, Histocompatibility Antigens Class I immunology, Interferon-gamma metabolism, Lymphocytes, Tumor-Infiltrating immunology, Lymphocytes, Tumor-Infiltrating metabolism, T-Lymphocytes immunology, T-Lymphocytes metabolism

Abstract

Interferon-γ (IFNγ) has been studied as a cancer treatment with limited evidence of clinical benefit. However, it could play a role in cancer immunotherapy combination treatments. Despite high expression of immunogenic cancer-testis antigens, synovial sarcoma (SS) and myxoid/round cell liposarcoma (MRCL) have a cold tumor microenvironment (TME), with few infiltrating T cells and low expression of major histocompatibility complex class I (MHC-I). We hypothesized that IFNγ treatment could drive inflammation in a cold TME, facilitating further immunotherapy. We conducted a phase 0 clinical trial treating 8 SS or MRCL patients with weekly systemic IFNγ. We performed pre- and posttreatment biopsies. IFNγ changed the SS and MRCL TME, inducing tumor-surface MHC-I expression and significant T-cell infiltration ( P < 0.05). Gene-expression analysis suggested increased tumor antigen presentation and less exhausted phenotypes of the tumor-infiltrating T cells. Newly emergent antigen-specific humoral and/or T-cell responses were found in 3 of 7 evaluable patients. However, increased expression of PD-L1 was observed on tumor-infiltrating myeloid cells and in some cases tumor cells. These findings suggest that systemic IFNγ used to convert SS and MRCL into "hot" tumors will work in concert with anti-PD-1 therapy to provide patient benefit., (©2019 American Association for Cancer Research.)

Published

2019

3. Endogenous CD4 + T Cells Recognize Neoantigens in Lung Cancer Patients, Including Recurrent Oncogenic KRAS and ERBB2 ( Her2 ) Driver Mutations.

Author

Veatch JR, Jesernig BL, Kargl J, Fitzgibbon M, Lee SM, Baik C, Martins R, Houghton AM, and Riddell SR

Subjects

Aged, Carcinoma, Non-Small-Cell Lung genetics, Carcinoma, Non-Small-Cell Lung immunology, Cell Line, Tumor, Computational Biology methods, Female, Gene Expression, Humans, Lung Neoplasms diagnosis, Lung Neoplasms therapy, Lymphocyte Activation, Lymphocytes, Tumor-Infiltrating immunology, Lymphocytes, Tumor-Infiltrating metabolism, Male, Middle Aged, Neoplasm Staging, RNA, Messenger, Transcriptome, Antigens, Neoplasm immunology, CD4-Positive T-Lymphocytes immunology, CD4-Positive T-Lymphocytes metabolism, Lung Neoplasms genetics, Lung Neoplasms immunology, Mutation, Proto-Oncogene Proteins p21(ras) genetics, Receptor, ErbB-2 genetics

Abstract

T cells specific for neoantigens encoded by mutated genes in cancers are increasingly recognized as mediators of tumor destruction after immune-checkpoint inhibitor therapy or adoptive cell transfer. Much of the focus has been on identifying epitopes presented to CD8 + T cells by class I MHC. However, CD4 + class II MHC-restricted T cells have been shown to have an important role in antitumor immunity. Unfortunately, the vast majority of neoantigens recognized by CD8 + or CD4 + T cells in cancer patients result from random mutations and are patient-specific. Here, we screened the blood of 5 non-small cell lung cancer (NSCLC) patients for T-cell responses to candidate mutation-encoded neoepitopes. T-cell responses were detected to 8.8% of screened antigens, with 1 to 7 antigens identified per patient. A majority of responses were to random, patient-specific mutations. However, CD4 + T cells that recognized the recurrent KRAS G12V and the ERBB2 ( Her2 ) internal tandem duplication (ITD) oncogenic driver mutations, but not the corresponding wild-type sequences, were identified in two patients. Two different T-cell receptors (TCR) specific for KRAS G12V and one T-cell receptor specific for Her2 -ITD were isolated and conferred antigen specificity when transfected into T cells. Deep sequencing identified the Her2 -ITD-specific TCR in the tumor but not nonadjacent lung. Our results showed that CD4 + T-cell responses to neoantigens, including recurrent driver mutations, can be derived from the blood of NSCLC patients. These data support the use of adoptive transfer or vaccination to augment CD4 + neoantigen-specific T cells and elucidate their role in human antitumor immunity., (©2019 American Association for Cancer Research.)

Published

2019

4. Chimeric Antigen Receptor T Cell-Mediated Neurotoxicity in Nonhuman Primates.

Author

Taraseviciute A, Tkachev V, Ponce R, Turtle CJ, Snyder JM, Liggitt HD, Myerson D, Gonzalez-Cuyar L, Baldessari A, English C, Yu A, Zheng H, Furlan SN, Hunt DJ, Hoglund V, Finney O, Brakke H, Blazar BR, Berger C, Riddell SR, Gardner R, Kean LS, and Jensen MC

Subjects

Animals, Cell Line, Tumor, Cyclophosphamide adverse effects, Disease Models, Animal, Humans, K562 Cells, Macaca mulatta, Neurotoxicity Syndromes etiology, Transplantation, Autologous, Antigens, CD20 immunology, Cyclophosphamide administration & dosage, Immunotherapy, Adoptive adverse effects, Neurotoxicity Syndromes immunology, Receptors, Antigen, T-Cell immunology

Abstract

Chimeric antigen receptor (CAR) T-cell immunotherapy has revolutionized the treatment of refractory leukemias and lymphomas, but is associated with significant toxicities, namely cytokine release syndrome (CRS) and neurotoxicity. A major barrier to developing therapeutics to prevent CAR T cell-mediated neurotoxicity is the lack of clinically relevant models. Accordingly, we developed a rhesus macaque (RM) model of neurotoxicity via adoptive transfer of autologous CD20-specific CAR T cells. Following cyclophosphamide lymphodepletion, CD20 CAR T cells expand to 272 to 4,450 cells/μL after 7 to 8 days and elicit CRS and neurotoxicity. Toxicities are associated with elevated serum IL6, IL8, IL1RA, MIG, and I-TAC levels, and disproportionately high cerebrospinal fluid (CSF) IL6, IL2, GM-CSF, and VEGF levels. During neurotoxicity, both CD20 CAR and non-CAR T cells accumulate in the CSF and in the brain parenchyma. This RM model demonstrates that CAR T cell-mediated neurotoxicity is associated with proinflammatory CSF cytokines and a pan-T cell encephalitis. Significance: We provide the first immunologically relevant, nonhuman primate model of B cell-directed CAR T-cell therapy-mediated CRS and neurotoxicity. We demonstrate CAR and non-CAR T-cell infiltration in the CSF and in the brain during neurotoxicity resulting in pan-encephalitis, accompanied by increased levels of proinflammatory cytokines in the CSF. Cancer Discov; 8(6); 750-63. ©2018 AACR. This article is highlighted in the In This Issue feature, p. 663 ., (©2018 American Association for Cancer Research.)

Published

2018

5. Endothelial Activation and Blood-Brain Barrier Disruption in Neurotoxicity after Adoptive Immunotherapy with CD19 CAR-T Cells.

Author

Gust J, Hay KA, Hanafi LA, Li D, Myerson D, Gonzalez-Cuyar LF, Yeung C, Liles WC, Wurfel M, Lopez JA, Chen J, Chung D, Harju-Baker S, Özpolat T, Fink KR, Riddell SR, Maloney DG, and Turtle CJ

Subjects

Humans, Treatment Outcome, Antigens, CD19 immunology, Blood-Brain Barrier metabolism, Immunotherapy, Adoptive methods, Receptors, Antigen, T-Cell metabolism

Abstract

Lymphodepletion chemotherapy followed by infusion of CD19-targeted chimeric antigen receptor-modified T (CAR-T) cells can be complicated by neurologic adverse events (AE) in patients with refractory B-cell malignancies. In 133 adults treated with CD19 CAR-T cells, we found that acute lymphoblastic leukemia, high CD19 + cells in bone marrow, high CAR-T cell dose, cytokine release syndrome, and preexisting neurologic comorbidities were associated with increased risk of neurologic AEs. Patients with severe neurotoxicity demonstrated evidence of endothelial activation, including disseminated intravascular coagulation, capillary leak, and increased blood-brain barrier (BBB) permeability. The permeable BBB failed to protect the cerebrospinal fluid from high concentrations of systemic cytokines, including IFNγ, which induced brain vascular pericyte stress and their secretion of endothelium-activating cytokines. Endothelial activation and multifocal vascular disruption were found in the brain of a patient with fatal neurotoxicity. Biomarkers of endothelial activation were higher before treatment in patients who subsequently developed grade ≥4 neurotoxicity. Significance: We provide a detailed clinical, radiologic, and pathologic characterization of neurotoxicity after CD19 CAR-T cells, and identify risk factors for neurotoxicity. We show endothelial dysfunction and increased BBB permeability in neurotoxicity and find that patients with evidence of endothelial activation before lymphodepletion may be at increased risk of neurotoxicity. Cancer Discov; 7(12); 1404-19. ©2017 AACR. See related commentary by Mackall and Miklos, p. 1371 This article is highlighted in the In This Issue feature, p. 1355 ., (©2017 American Association for Cancer Research.)

Published

2017

6. Preserved Activity of CD20-Specific Chimeric Antigen Receptor-Expressing T Cells in the Presence of Rituximab.

Author

Rufener GA, Press OW, Olsen P, Lee SY, Jensen MC, Gopal AK, Pender B, Budde LE, Rossow JK, Green DJ, Maloney DG, Riddell SR, and Till BG

Subjects

Animals, Antigens, CD20 drug effects, Antigens, CD20 metabolism, Antineoplastic Agents administration & dosage, Cell Proliferation drug effects, Combined Modality Therapy, Cytokines biosynthesis, Cytotoxicity, Immunologic drug effects, Dose-Response Relationship, Drug, Humans, Immunotherapy, Adoptive methods, Lymphoma, B-Cell immunology, Mice, Inbred NOD, Mice, SCID, Rituximab administration & dosage, T-Lymphocyte Subsets immunology, T-Lymphocyte Subsets transplantation, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, Antigens, CD20 immunology, Antineoplastic Agents pharmacology, Lymphoma, B-Cell therapy, Receptors, Antigen, T-Cell metabolism, Rituximab pharmacology, T-Lymphocyte Subsets drug effects

Abstract

CD20 is an attractive immunotherapy target for B-cell non-Hodgkin lymphomas, and adoptive transfer of T cells genetically modified to express a chimeric antigen receptor (CAR) targeting CD20 is a promising strategy. A theoretical limitation is that residual serum rituximab might block CAR binding to CD20 and thereby impede T cell-mediated anti-lymphoma responses. The activity of CD20 CAR-modified T cells in the presence of various concentrations of rituximab was tested in vitro and in vivo CAR-binding sites on CD20(+) tumor cells were blocked by rituximab in a dose-dependent fashion, although at 37°C blockade was incomplete at concentrations up to 200 μg/mL. T cells with CD20 CARs also exhibited modest dose-dependent reductions in cytokine secretion and cytotoxicity, but not proliferation, against lymphoma cell lines. At rituximab concentrations of 100 μg/mL, CAR T cells retained ≥50% of baseline activity against targets with high CD20 expression, but were more strongly inhibited when target cells expressed low CD20. In a murine xenograft model using a rituximab-refractory lymphoma cell line, rituximab did not impair CAR T-cell activity, and tumors were eradicated in >85% of mice. Clinical residual rituximab serum concentrations were measured in 103 lymphoma patients after rituximab therapy, with the median level found to be only 38 μg/mL (interquartile range, 19-72 μg/mL). Thus, despite modest functional impairment in vitro, the in vivo activity of CD20-targeted CAR T cells remains intact at clinically relevant levels of rituximab, making use of these T cells clinically feasible. Cancer Immunol Res; 4(6); 509-19. ©2016 AACR, (©2016 American Association for Cancer Research.)

Published

2016

7. Safety of targeting ROR1 in primates with chimeric antigen receptor-modified T cells.

Author

Berger C, Sommermeyer D, Hudecek M, Berger M, Balakrishnan A, Paszkiewicz PJ, Kosasih PL, Rader C, and Riddell SR

Subjects

Animals, Cell Movement immunology, Cell Survival immunology, Cytokines blood, Genetic Engineering methods, Genetic Vectors, Humans, Immunotherapy, Adoptive methods, Macaca mulatta, Models, Animal, Receptors, Antigen, T-Cell genetics, Receptors, Antigen, T-Cell metabolism, Retroviridae genetics, Transduction, Genetic, Immunotherapy, Adoptive adverse effects, Receptor Tyrosine Kinase-like Orphan Receptors metabolism, T-Lymphocytes immunology

Abstract

Genetic engineering of T cells for adoptive transfer by introducing a tumor-targeting chimeric antigen receptor (CAR) is a new approach to cancer immunotherapy. A challenge for the field is to define cell surface molecules that are both preferentially expressed on tumor cells and can be safely targeted with T cells. The orphan tyrosine kinase receptor ROR1 is a candidate target for T-cell therapy with CAR-modified T cells (CAR-T cells) because it is expressed on the surface of many lymphatic and epithelial malignancies and has a putative role in tumor cell survival. The cell surface isoform of ROR1 is expressed in embryogenesis but absent in adult tissues except for B-cell precursors and low levels of transcripts in adipocytes, pancreas, and lung. ROR1 is highly conserved between humans and macaques and has a similar pattern of tissue expression. To determine if low-level ROR1 expression on normal cells would result in toxicity or adversely affect CAR-T cell survival and/or function, we adoptively transferred autologous ROR1 CAR-T cells into nonhuman primates. ROR1 CAR-T cells did not cause overt toxicity to normal organs and accumulated in bone marrow and lymph node sites, where ROR1-positive B cells were present. The findings support the clinical evaluation of ROR1 CAR-T cells for ROR1(+) malignancies and demonstrate the utility of nonhuman primates for evaluating the safety of immunotherapy with engineered T cells specific for tumor-associated molecules that are homologous between humans and nonhuman primates., (©2014 American Association for Cancer Research.)

Published

2015

8. The nonsignaling extracellular spacer domain of chimeric antigen receptors is decisive for in vivo antitumor activity.

Author

Hudecek M, Sommermeyer D, Kosasih PL, Silva-Benedict A, Liu L, Rader C, Jensen MC, and Riddell SR

Subjects

Animals, Antigens, CD19 immunology, Burkitt Lymphoma immunology, Cell Death immunology, Cell Line, Tumor, Cytotoxicity, Immunologic, Genetic Engineering methods, Genetic Vectors, Humans, Immunoglobulin G immunology, Immunophenotyping methods, Lentivirus genetics, Lung immunology, Lymphocyte Activation immunology, Mice, Inbred NOD, Mice, SCID, Protein Structure, Tertiary, Recombinant Fusion Proteins immunology, Signal Transduction immunology, Structure-Activity Relationship, Xenograft Model Antitumor Assays, Burkitt Lymphoma therapy, Immunotherapy, Adoptive methods, Receptors, Antigen, T-Cell immunology, T-Lymphocytes immunology

Abstract

The use of synthetic chimeric antigen receptors (CAR) to redirect T cells to recognize tumor provides a powerful new approach to cancer immunotherapy; however, the attributes of CARs that ensure optimal in vivo tumor recognition remain to be defined. Here, we analyze the influence of length and composition of IgG-derived extracellular spacer domains on the function of CARs. Our studies demonstrate that CD19-CARs with a long spacer from IgG4 hinge-CH2-CH3 are functional in vitro but lack antitumor activity in vivo due to interaction between the Fc domain within the spacer and the Fc receptor-bearing myeloid cells, leading to activation-induced T-cell death. We demonstrate that in vivo persistence and antitumor effects of CAR-T cells with a long spacer can be restored by modifying distinct regions in the CH2 domain that are essential for Fc receptor binding. Our studies demonstrate that modifications that abrogate binding to Fc receptors are crucial for CARs in which a long spacer is obligatory for tumor recognition as shown here for a ROR1-specific CAR. These results demonstrate that the length and composition of the extracellular spacer domain that lacks intrinsic signaling function can be decisive in the design of CARs for optimal in vivo activity., (©2014 American Association for Cancer Research.)

Published

2015

9. Cytotoxic T-cell cytokines put cancer under arrest.

Author

Riddell SR

Subjects

Animals, Female, Humans, Male, CD8-Positive T-Lymphocytes immunology, Cell Cycle Checkpoints, Cyclin-Dependent Kinase Inhibitor p27 metabolism, Cytokines immunology, Immunotherapy, Adoptive, Indoles therapeutic use, Interferon-gamma immunology, Melanoma therapy, Neoplasm Metastasis therapy, S-Phase Kinase-Associated Proteins metabolism, Sulfonamides therapeutic use, T-Lymphocytes, Cytotoxic immunology

Published

2015

10. Recognition and killing of brain tumor stem-like initiating cells by CD8+ cytolytic T cells.

Author

Brown CE, Starr R, Martinez C, Aguilar B, D'Apuzzo M, Todorov I, Shih CC, Badie B, Hudecek M, Riddell SR, and Jensen MC

Subjects

AC133 Antigen, Animals, Antigen Presentation, Antigens, CD biosynthesis, Antigens, CD immunology, Brain Neoplasms pathology, Cell Death immunology, Cell Line, Tumor, Glioma pathology, Glycoproteins biosynthesis, Glycoproteins immunology, HLA-A2 Antigen immunology, Humans, Mice, Mice, Inbred NOD, Mice, SCID, Neoplastic Stem Cells pathology, Peptides immunology, Transplantation, Heterologous, Brain Neoplasms immunology, Glioma immunology, Neoplastic Stem Cells immunology, T-Lymphocytes, Cytotoxic immunology

Abstract

Solid tumors contain a subset of stem-like cells that are resistant to the cytotoxic effects of chemotherapy/radiotherapy, but their susceptibility to cytolytic T lymphocyte (CTL) effector mechanisms has not been well characterized. Using a panel of early-passage human brain tumor stem/initiating cell (BTSC) lines derived from high-grade gliomas, we show that BTSCs are subject to immunologic recognition and elimination by CD8(+) CTLs. Compared with serum-differentiated CD133(low) tumor cells and established glioma cell lines, BTSCs are equivalent with respect to expression levels of HLA class I and ICAM-1, similar in their ability to trigger degranulation and cytokine synthesis by antigen-specific CTLs, and equally susceptible to perforin-dependent CTL-mediated cytolysis. BTSCs are also competent in the processing and presentation of antigens as evidenced by the killing of these cells by CTL when antigen is endogenously expressed. Moreover, we show that CTLs can eliminate all BTSCs with tumor-initiating activity in an antigen-specific manner in vivo. Current models predict that curative therapies for many cancers will require the elimination of the stem/initiating population, and these studies lay the foundation for developing immunotherapeutic approaches to eradicate this tumor population.

Published

2009

11. Recognition of breast cancer cells by CD8+ cytotoxic T-cell clones specific for NY-BR-1.

Author

Wang W, Epler J, Salazar LG, and Riddell SR

Subjects

Antigen Presentation, Antigens, Neoplasm biosynthesis, Antigens, Neoplasm genetics, Breast Neoplasms genetics, Cell Line, Tumor, Clone Cells, Dendritic Cells immunology, Female, HLA-A Antigens immunology, HLA-A2 Antigen, Humans, Peptide Fragments immunology, Transfection, Antigens, Neoplasm immunology, Breast Neoplasms immunology, Epitopes, T-Lymphocyte immunology, T-Lymphocytes, Cytotoxic immunology

Abstract

Immunotherapy for breast cancer using cytotoxic T cells (CTL) is hindered by the lack of well-characterized breast cancer antigens that are expressed in most breast tumor cells and recognized by CD8+ CTL. A recently described breast tissue differentiation antigen, NY-BR-1, is expressed in >80% breast tumors and elicits a humoral response in a subset of breast cancer patients. To identify potential NY-BR-1 epitopes that are recognized by CTL, CD8+ T cells were stimulated in vitro with autologous dendritic cells pulsed with NY-BR-1 peptides that were predicted to bind to HLA-A2. In multiple normal female donors and breast cancer patients, specific CD8+ CTL responses were detected by enzyme-linked immunospot assay against several NY-BR-1 peptides after two cycles of stimulation. CD8+ CTL clones against three NY-BR-1 epitopes were isolated and recognized peptide-pulsed target cells with high avidity. T-cell clones specific for one of the NY-BR-1 epitopes (p904) also recognized breast tumor cells expressing NY-BR-1, NY-BR-1(-) cells transfected with a cDNA encoding the NY-BR-1 protein, and autologous dendritic cells pulsed with opsonized NY-BR-1+ breast tumor cells. Taken together, these results show that the p904 epitope derived from NY-BR-1 is efficiently processed and presented endogenously and identify NY-BR-1 as a promising target for T-cell-based immunotherapy for breast cancer.

Published

2006