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56. Foreword

Author

Stephen Gottschalk

Published
2011

58. Harnessing T Cells to Target Pediatric Acute Myeloid Leukemia: CARs, BiTEs, and Beyond

Author

Rebecca Epperly, Stephen Gottschalk, and Mireya Paulina Velasquez

Subjects
acute myeloid leukemia, immunotherapy, chimeric antigen receptor, car, bispecific antibodies, bite, dart, Pediatrics, RJ1-570
Abstract

Outcomes for pediatric patients with acute myeloid leukemia (AML) remain poor, highlighting the need for improved targeted therapies. Building on the success of CD19-directed immune therapy for acute lymphocytic leukemia (ALL), efforts are ongoing to develop similar strategies for AML. Identifying target antigens for AML is challenging because of the high expression overlap in hematopoietic cells and normal tissues. Despite this, CD123 and CD33 antigen targeted therapies, among others, have emerged as promising candidates. In this review we focus on AML-specific T cell engaging bispecific antibodies and chimeric antigen receptor (CAR) T cells. We review antigens being explored for T cell-based immunotherapy in AML, describe the landscape of clinical trials upcoming for bispecific antibodies and CAR T cells, and highlight strategies to overcome additional challenges facing translation of T cell-based immunotherapy for AML.

Published
2020
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59. Foreign or Domestic CARs: Receptor Ligands as Antigen-Binding Domains

Author

Donald R. Shaffer, Penghui Zhou, and Stephen Gottschalk

Subjects
chimeric antigen receptor, adoptive immunotherapy, immunology, cancer, Medicine
Abstract

Chimeric antigen receptors (CARs) are increasingly being used in clinical trials to treat a variety of malignant conditions and recent results with CD19-specific CARs showing complete tumor regressions has sparked the interest of researchers and the public alike. Traditional CARs have been generated using single-chain variable fragments (scFv), often derived from murine monoclonal antibodies, for antigen specificity. As the clinical experience with CAR T cells grows, so does the potential for unwanted immune responses against the foreign transgene. Strategies that may reduce the immunogenicity of CAR T cells are humanization of the scFv and the use of naturally occurring receptor ligands as antigen-binding domains. Herein, we review the experience with alternatively designed CARs that contain receptor ligands rather than scFv. While most of the experiences have been in the pre-clinical setting, clinical data is also emerging.

Published
2014
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60. A vaccine that co-targets tumor cells and cancer associated fibroblasts results in enhanced antitumor activity by inducing antigen spreading.

Author

Stephen Gottschalk, Feng Yu, Minjun Ji, Sunitha Kakarla, and Xiao-Tong Song

Subjects
Medicine, Science
Abstract

Dendritic cell (DC) vaccines targeting only cancer cells have produced limited antitumor activity in most clinical studies. Targeting cancer-associated fibroblasts (CAFs) in addition to cancer cells may enhance antitumor effects, since CAFs, the central component of the tumor stroma, directly support tumor growth and contribute to the immunosuppressive tumor microenvironment. To co-target CAFs and tumor cells we developed a new compound DC vaccine that encodes an A20-specific shRNA to enhance DC function, and targets fibroblast activation protein (FAP) expressed in CAFs and the tumor antigen tyrosine-related protein (TRP)2 (DC-shA20-FAP-TRP2). DC-shA20-FAP-TRP2 vaccination induced robust FAP- and TRP2-specific T-cell responses, resulting in greater antitumor activity in the B16 melanoma model in comparison to monovalent vaccines or a vaccine encoding antigens and a control shRNA. DC-shA20-FAP-TRP2 vaccination enhanced tumor infiltration of CD8-positive T cells, and induced antigen-spreading resulting in potent antitumor activity. Thus, co-targeting of tumor cells and CAFs results in the induction of broad-based tumor-specific T-cell responses and has the potential to improve current vaccine approaches for cancer.

Published
2013
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61. TanCAR: A Novel Bispecific Chimeric Antigen Receptor for Cancer Immunotherapy

Author

Zakaria Grada, Meenakshi Hegde, Tiara Byrd, Donald R Shaffer, Alexia Ghazi, Vita S Brawley, Amanda Corder, Kurt Schönfeld, Joachim Koch, Gianpietro Dotti, Helen E Heslop, Stephen Gottschalk, Winfried S Wels, Matthew L Baker, and Nabil Ahmed

Subjects
bispecific chimeric antigen receptor, CAR, cancer immunotherapy, molecular modeling, T-cell therapy, Therapeutics. Pharmacology, RM1-950
Abstract

Targeted T cells are emerging as effective non-toxic therapies for cancer. Multiple elements, however, contribute to the overall pathogenesis of cancer through both distinct and redundant mechanisms. Hence, targeting multiple cancer-specific markers simultaneously could result in better therapeutic efficacy. We created a functional chimeric antigen receptor'the TanCAR, a novel artificial molecule that mediates bispecific activation and targeting of T cells. We demonstrate the feasibility of cumulative integration of structure and docking simulation data using computational tools to interrogate the design and predict the functionality of such a complex bispecific molecule. Our prototype TanCAR induced distinct T cell reactivity against each of two tumor restricted antigens, and produced synergistic enhancement of effector functions when both antigens were simultaneously encountered. Furthermore, the TanCAR preserved the cytolytic ability of T cells upon loss of one of the target molecules and better controlled established experimental tumors by recognition of both targets in an animal disease model. This proof-of-concept approach can be used to increase the specificity of effector cells for malignant versus normal target cells, to offset antigen escape or to allow for targeting the tumor and its microenvironment.

Published
2013
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62. Crosstalk between medulloblastoma cells and endothelium triggers a strong chemotactic signal recruiting T lymphocytes to the tumor microenvironment.

Author

Vita S Salsman, Kevin K H Chow, Donald R Shaffer, Huseyin Kadikoy, Xiao-Nan Li, Claudia Gerken, Laszlo Perlaky, Leonid S Metelitsa, Xiuhua Gao, Meena Bhattacharjee, Karen Hirschi, Helen E Heslop, Stephen Gottschalk, and Nabil Ahmed

Subjects
Medicine, Science
Abstract

Cancer cells can live and grow if they succeed in creating a favorable niche that often includes elements from the immune system. While T lymphocytes play an important role in the host response to tumor growth, the mechanism of their trafficking to the tumor remains poorly understood. We show here that T lymphocytes consistently infiltrate the primary brain cancer, medulloblastoma. We demonstrate, both in vitro and in vivo, that these T lymphocytes are attracted to tumor deposits only after the tumor cells have interacted with tumor vascular endothelium. Macrophage Migration Inhibitory Factor (MIF)" is the key chemokine molecule secreted by tumor cells which induces the tumor vascular endothelial cells to secrete the potent T lymphocyte attractant "Regulated upon Activation, Normal T-cell Expressed, and Secreted (RANTES)." This in turn creates a chemotactic gradient for RANTES-receptor bearing T lymphocytes. Manipulation of this pathway could have important therapeutic implications.

Published
2011
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64. Preferential expansion of CD8+ CD19-CAR T cells postinfusion and the role of disease burden on outcome in pediatric B-ALL

Author

Aimee C. Talleur, Amr Qudeimat, Jean-Yves Métais, Deanna Langfitt, Ewelina Mamcarz, Jeremy Chase Crawford, Sujuan Huang, Cheng Cheng, Caitlin Hurley, Renee Madden, Akshay Sharma, Ali Suliman, Ashok Srinivasan, M. Paulina Velasquez, Esther A. Obeng, Catherine Willis, Salem Akel, Seth E. Karol, Hiroto Inaba, Allison Bragg, Wenting Zheng, Sheng M. Zhou, Sarah Schell, MaCal Tuggle-Brown, David Cullins, Sagar L Patil, Ying Li, Paul G. Thomas, Caitlin Zebley, Benjamin Youngblood, Ching-Hon Pui, Timothy Lockey, Terrence L. Geiger, Michael M. Meagher, Brandon M. Triplett, and Stephen Gottschalk

Subjects
Lymphoma, B-Cell, Receptors, Chimeric Antigen, Cost of Illness, T-Lymphocytes, Antigens, CD19, Humans, Hematology, CD8-Positive T-Lymphocytes, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Burkitt Lymphoma
Abstract

T cells expressing CD19-specific chimeric antigen receptors (CD19-CARs) have potent antileukemia activity in pediatric and adult patients with relapsed and/or refractory B-cell acute lymphoblastic leukemia (B-ALL). However, not all patients achieve a complete response (CR), and a significant percentage relapse after CD19-CAR T-cell therapy due to T-cell intrinsic and/or extrinsic mechanisms. Thus, there is a need to evaluate new CD19-CAR T-cell products in patients to improve efficacy. We developed a phase 1/2 clinical study to evaluate an institutional autologous CD19-CAR T-cell product in pediatric patients with relapsed/refractory B-ALL. Here we report the outcome of the phase 1 study participants (n = 12). Treatment was well tolerated, with a low incidence of both cytokine release syndrome (any grade, n = 6) and neurotoxicity (any grade, n = 3). Nine out of 12 patients (75%) achieved a minimal residual disease-negative CR in the bone marrow (BM). High disease burden (≥40% morphologic blasts) before CAR T-cell infusion correlated with increased side effects and lower response rate, but not with CD19-CAR T-cell expansion. After infusion, CD8+ CAR T cells had a proliferative advantage over CD4+ CAR T cells and at peak expansion, had an effector memory phenotype with evidence of antigen-driven differentiation. Patients that proceeded to allogeneic hematopoietic cell transplantation (AlloHCT) had sustained, durable responses. In summary, the initial evaluation of our institutional CD19-CAR T-cell product demonstrates safety and efficacy while highlighting the impact of pre-infusion disease burden on outcomes. This trial was registered at www.clinicaltrials.gov as #NCT03573700.

Published
2022

65. Long-term follow-up for the development of subsequent malignancies in patients treated with genetically modified IECs

Author

David H. M. Steffin, Ibrahim N. Muhsen, LaQuisa C. Hill, Carlos A. Ramos, Nabil Ahmed, Meenakshi Hegde, Tao Wang, Mengfen Wu, Stephen Gottschalk, Sarah B. Whittle, Premal D. Lulla, Maksim Mamonkin, Bilal Omer, Rayne H. Rouce, Andras Heczey, Leonid S. Metelitsa, Bambi J. Grilley, Catherine Robertson, Virginia Torrano, Natalia Lapteva, Adrian P. Gee, Cliona M. Rooney, Malcolm K. Brenner, and Helen E. Heslop

Subjects
Adult, Hematologic Neoplasms, Neoplasms, Immunology, Leukocytes, Mononuclear, Humans, Cell Biology, Hematology, Child, Biochemistry, Follow-Up Studies, Retrospective Studies
Abstract

Subsequent malignancies are well-documented complications in long-term follow-up of cancer patients. Recently, genetically modified immune effector (IE) cells have shown benefit in hematologic malignancies and are being evaluated in clinical trials for solid tumors. Although the short-term complications of IE cells are well described, there is limited literature summarizing long-term follow-up, including subsequent malignancies. We retrospectively reviewed data from 340 patients treated across 27 investigator-initiated pediatric and adult clinical trials at our center. All patients received IE cells genetically modified with γ-retroviral vectors to treat relapsed and/or refractory hematologic or solid malignancies. In a cumulative 1027 years of long-term follow-up, 13 patients (3.8%) developed another cancer with a total of 16 events (4 hematologic malignancies and 12 solid tumors). The 5-year cumulative incidence of a first subsequent malignancy in the recipients of genetically modified IE cells was 3.6% (95% confidence interval, 1.8% to 6.4%). For 11 of the 16 subsequent tumors, biopsies were available, and no sample was transgene positive by polymerase chain reaction. Replication-competent retrovirus testing of peripheral blood mononuclear cells was negative in the 13 patients with subsequent malignancies tested. Rates of subsequent malignancy were low and comparable to standard chemotherapy. These results suggest that the administration of IE cells genetically modified with γ retroviral vectors does not increase the risk for subsequent malignancy.

Published
2022

67. Supplementary Data from Common Trajectories of Highly Effective CD19-Specific CAR T Cells Identified by Endogenous T-cell Receptor Lineages

Author

Paul G. Thomas, Jeremy Chase Crawford, Stephen Gottschalk, Aimee C. Talleur, Brandon M. Triplett, Michael M. Meagher, Catherine Willis, Timothy Lockey, Scott R. Olsen, Sanchit Trivedi, Pratibha Kottapalli, M. Paulina Velasquez, Janice M. Riberdy, Mikhail V. Pogorelyy, Jean-Yves Métais, E. Kaitlynn Allen, Anastasia A. Minervina, Robert C. Mettelman, Deanna Langfitt, Ching-Heng Chou, Hyunjin Kim, and Taylor L. Wilson

Abstract

Supplementary Data from Common Trajectories of Highly Effective CD19-Specific CAR T Cells Identified by Endogenous T-cell Receptor Lineages

Published
2023

68. Data from Antitumor Effects of CAR T Cells Redirected to the EDB Splice Variant of Fibronectin

Author

Stephen Gottschalk, Giedre Krenciute, Heather Tillman, Shondra M. Pruett-Miller, Shaina N. Porter, Jinghui Zhang, Deanna Langfitt, Alejandro Allo Anido, Timothy I. Shaw, Elizabeth Wickman, and Jessica Wagner

Abstract

Chimeric antigen receptor (CAR) T-cell therapy has had limited success in early-phase clinical studies for solid tumors. Lack of efficacy is most likely multifactorial, including a limited array of targetable antigens. We reasoned that targeting the cancer-specific extra domain B (EDB) splice variant of fibronectin might overcome this limitation because it is abundantly secreted by cancer cells and adheres to their cell surface. In vitro, EDB-CAR T cells recognized and killed EDB-positive tumor cells. In vivo, 1 × 106 EDB-CAR T cells had potent antitumor activity in both subcutaneous and systemic tumor xenograft models, resulting in a significant survival advantage in comparison with control mice. EDB-CAR T cells also targeted the tumor vasculature, as judged by IHC and imaging, and their antivascular activity was dependent on the secretion of EDB by tumor cells. Thus, targeting tumor-specific splice variants such as EDB with CAR T cells is feasible and has the potential to improve the efficacy of CAR T-cell therapy.

Published
2023

69. Supplementary Data from A Costimulatory CAR Improves TCR-based Cancer Immunotherapy

Author

Cliona M. Rooney, Caroline Arber, Stephen Gottschalk, Thomas Shum, Chris DeRenzo, Lauren Scherer, Stacey Van Pelt, Silvana Perconti, Candise Tat, Cicilyn Xie, Nazila Nouraee, Sandhya Sharma, Mai Huynh, Rachel Daum, Thomas Pfeiffer, Mara G. Cardenas, and Bilal Omer

Abstract

Supplementary Data from A Costimulatory CAR Improves TCR-based Cancer Immunotherapy

Published
2023

70. Data from A Costimulatory CAR Improves TCR-based Cancer Immunotherapy

Author

Cliona M. Rooney, Caroline Arber, Stephen Gottschalk, Thomas Shum, Chris DeRenzo, Lauren Scherer, Stacey Van Pelt, Silvana Perconti, Candise Tat, Cicilyn Xie, Nazila Nouraee, Sandhya Sharma, Mai Huynh, Rachel Daum, Thomas Pfeiffer, Mara G. Cardenas, and Bilal Omer

Abstract

T-cell receptors (TCR) recognize intracellular and extracellular cancer antigens, allowing T cells to target many tumor antigens. To sustain proliferation and persistence, T cells require not only signaling through the TCR (signal 1), but also costimulatory (signal 2) and cytokine (signal 3) signaling. Because most cancer cells lack costimulatory molecules, TCR engagement at the tumor site results in incomplete T-cell activation and transient antitumor effects. To overcome this lack of signal 2, we genetically modified tumor-specific T cells with a costimulatory chimeric antigen receptor (CoCAR). Like classical CARs, CoCARs combine the antigen-binding domain of an antibody with costimulatory endodomains to trigger T-cell proliferation, but CoCARs lack the cytotoxic CD3ζ chain to avoid toxicity to normal tissues. We first tested a CD19-targeting CoCAR in combination with an HLA-A*02:01-restricted, survivin-specific transgenic TCR (sTCR) in serial cocultures with leukemia cells coexpressing the cognate peptide–HLA complex (signal 1) and CD19 (signal 2). The CoCAR enabled sTCR+ T cells to kill tumors over a median of four additional tumor challenges. CoCAR activity depended on CD19 but was maintained in tumors with heterogeneous CD19 expression. In a murine tumor model, sTCR+CoCAR+ T cells improved tumor control and prolonged survival compared with sTCR+ T cells. We further evaluated the CoCAR in Epstein–Barr virus–specific T cells (EBVST). CoCAR-expressing EBVSTs expanded more rapidly than nontransduced EBVSTs and delayed tumor progression in an EBV+ murine lymphoma model. Overall, we demonstrated that the CoCAR can increase the activity of T cells expressing both native and transgenic TCRs and enhance antitumor responses.

Published
2023

72. Supplemental Figure 3 from Constitutive Signaling from an Engineered IL7 Receptor Promotes Durable Tumor Elimination by Tumor-Redirected T Cells

Author

Cliona M. Rooney, Stephen Gottschalk, Leonid S. Metelitsa, Malcolm K. Brenner, Hao Liu, Paul Castillo, Robin Parihar, Daofeng Liu, Tim Sauer, Zhongzhen Yi, Kathan Parikh, Dimitrios L. Wagner, Robert L. Kruse, Haruko Tashiro, Bilal Omer, and Thomas Shum

Abstract

Supplementary Figure 3: C7R signaling does not change phenotypic composition of GD2-CAR T-cells during culture.

Published
2023

73. Data from A Chimeric GM-CSF/IL18 Receptor to Sustain CAR T-cell Function

Author

Stephen Gottschalk, Deanna Langfitt, Sagar L. Patil, Matthew Bell, Laurens G.L. Sand, and Shannon Lange

Abstract

The inability of chimeric antigen receptor (CAR) T cells to sustain their effector function after repeated exposure to tumor cells is a major obstacle to their success in patients with solid tumors. To overcome this limitation, we designed a novel chimeric cytokine receptor to create an autocrine loop that links activation-dependent GM-CSF production by CAR T cells to IL18 receptor signaling (GM18). Expression of GM18 in CAR T cells enhanced their effector function in an antigen- and activation-dependent manner. In repeat stimulation assays, which mimic chronic antigen exposure, CAR.GM18 T cells had a significantly greater ability to expand and produce cytokines in comparison with their unmodified counterparts targeting EPHA2 or HER2. In vivo, CAR.GM18 T cells induced tumor regression at cell doses at which standard CAR T cells were ineffective in two solid tumor xenograft models. Thus, our study highlights the potential of hijacking cytokines that are physiologically secreted by T cells to bolster their antitumor activity.Significance:We designed a chimeric cytokine receptor (GM18) that links CAR T-cell activation to MYD88 signaling. GM18 endows CAR T cells with sustained effector function in the setting of chronic antigen exposure, resulting in potent antitumor activity in preclinical solid tumor models.This article is highlighted in the In This Issue feature, p. 1601

Published
2023

74. Supplementary Figures from Inducible Activation of MyD88 and CD40 in CAR T Cells Results in Controllable and Potent Antitumor Activity in Preclinical Solid Tumor Models

Author

Stephen Gottschalk, David M. Spencer, Giedre Krenciute, Phuong Nguyen, Claudia Gerken, and Melinda Mata

Abstract

Supplemental Figure 1: Activation of iCO molecules in T cells enhances NF-κB signaling;Supplemental Figure 2: Activation of iCO molecules enhances cytokine production in T cells;Supplemental Figure 3: CID dose-dependent IL2 production of HER2ζ.iCO T cells can be controlled by CID;Supplemental Figure 4: iCO activation enhances pro-inflammatory cytokine secretion of HER2ζ.iCO T cells;Supplemental Figure 5: Signal 1 is critical for HER2ζ.iCO T-cell effector function;Supplemental Figure 6: HER2ζ.iCO and HER2.CD28ζ T-cell lines have similar T-cell subset composition;Supplemental Figure 7: HER2ζ.iCO T cells have reduced PD-1 surface expression;Supplemental Figure 8: Recurrent tumors from HER2ζ.iCO T-cell + CID and HER2.CD28 ζ T-cell treated mice express HER2;Supplemental Figure 9: HER2ζ.iCO and HER2.CD28ζ T-cell lines have similar T-cell subset composition in vivo;Supplemental Figure 10: Anatomic location of tumors in treated mice;Supplemental Figure 11: Chemokine secretion of A549 cells, and chemokine receptor expression of T cells;Supplemental Figure 12: PD-L1 expression in tumor cell lines;Supplemental Figure 13: Generation of T-cells expressing HER2.CD28ζ.iCO;Supplemental Figure 14: iCO activation enhances expansion and pro-inflammatory cytokine secretion of HER2ζ.iCO and HER2.CD28ζ.iCO T-cells;Supplemental Figure 15: iCO activation enhances cytolytic activity of HER2ζ.iCO and HER2.CD28ζ.iCO T-cells; Supplemental Figure 16: Second CID injection eliminates recurrent tumors in 2/3 mice

Published
2023

75. CIR-17-0171 Supplementary Data from CD28 and 41BB Costimulation Enhances the Effector Function of CD19-Specific Engager T Cells

Author

Stephen Gottschalk, Hao Liu, Meng-Fen Wu, Phuong Nguyen, Aarohi Thakkar, Abishek Vaidya, Arpad Szoor, and Mireya Paulina Velasquez

Abstract

S1: T-cell immunophenotyping by flow cytometry. S2: Determination of TSCM presence in PBMC and NT T-cells by flow cytometry. S3: CD19-ENGT-cells and CD19-ENGT-cells expressing CD80 and/or 41BBL kill Nalm 6 cells efficiently. S4: Experimental set up of Serial Killing Assay. S5: CD19- ENG.41BBL/CD80 T-cells have improved ability to sequentially kill CD19 target cells. S6: CD19-ENG T-cells expressing CD80 or 41BBL and CD80 have improved ability to sequentially kill CD19 target cells. S7: Nalm 6 express PD-L1 after exposure to IFNgamma. S8: CD19 ENG.41BBL/CD80 T-cells expand in vivo and persist long-term at low levels.

Published
2023

77. Supplemental Figure 6 from Constitutive Signaling from an Engineered IL7 Receptor Promotes Durable Tumor Elimination by Tumor-Redirected T Cells

Author

Cliona M. Rooney, Stephen Gottschalk, Leonid S. Metelitsa, Malcolm K. Brenner, Hao Liu, Paul Castillo, Robin Parihar, Daofeng Liu, Tim Sauer, Zhongzhen Yi, Kathan Parikh, Dimitrios L. Wagner, Robert L. Kruse, Haruko Tashiro, Bilal Omer, and Thomas Shum

Abstract

Supplementary Figure 6: Efficient retroviral transduction of T-cells with Î"34, C7R, GD2-CAR, and GD2-CAR.C7R constructs.

Published
2023

78. Supplemental Figure 5 from Constitutive Signaling from an Engineered IL7 Receptor Promotes Durable Tumor Elimination by Tumor-Redirected T Cells

Author

Cliona M. Rooney, Stephen Gottschalk, Leonid S. Metelitsa, Malcolm K. Brenner, Hao Liu, Paul Castillo, Robin Parihar, Daofeng Liu, Tim Sauer, Zhongzhen Yi, Kathan Parikh, Dimitrios L. Wagner, Robert L. Kruse, Haruko Tashiro, Bilal Omer, and Thomas Shum

Abstract

Supplementary Figure 5: C7R does not significantly increase intracranial EphA2-CAR T-cell expansion against U373 tumors

Published
2023

79. Data from B7-H3 Specific CAR T Cells for the Naturally Occurring, Spontaneous Canine Sarcoma Model

Author

Seth M. Pollack, Beverly Torok-Storb, Peter F. Moore, Stephen Gottschalk, Michael C. Jensen, Stanley R. Riddell, Alexander I. Salter, Bernard Seguin, Himaly Shinglot, Juliana Chi Kei Ng, Weiqing Jing, Ali Zhang, Amy B. Heimberger, Borislav A. Alexiev, Brian C. Schulte, Kraig Abrams, Brett A. Schroeder, Amanda Koehne, Cassandra Miller, Brian J. Hayes, Karan Kohli, R. Graeme Black, and Shihong Zhang

Abstract

One obstacle for human solid tumor immunotherapy research is the lack of clinically relevant animal models. In this study, we sought to establish a chimeric antigen receptor (CAR) T-cell treatment model for naturally occurring canine sarcomas as a model for human CAR T-cell therapy.Canine CARs specific for B7-H3 were constructed using a single-chain variable fragment derived from the human B7-H3–specific antibody MGA271, which we confirmed to be cross-reactive with canine B7-H3. After refining activation, transduction, and expansion methods, we confirmed target killing in a tumor spheroid three-dimensional assay. We designed a B7-H3 canine CAR T-cell and achieved consistently high levels of transduction efficacy, expansion, and in vitro tumor killing. Safety of the CAR T cells were confirmed in two purposely bred healthy canine subjects following lymphodepletion by cyclophosphamide and fludarabine. Immune response, clinical parameters, and manifestation were closely monitored after treatments and were shown to resemble that of humans. No severe adverse events were observed.In summary, we demonstrated that similar to human cancers, B7-H3 can serve as a target for canine solid tumors. We successfully generated highly functional canine B7-H3–specific CAR T-cell products using a production protocol that closely models human CAR T-cell production procedure. The treatment regimen that we designed was confirmed to be safe in vivo. Our research provides a promising direction to establish in vitro and in vivo models for immunotherapy for canine and human solid tumor treatment.

Published
2023

80. Data from CD28 and 41BB Costimulation Enhances the Effector Function of CD19-Specific Engager T Cells

Author

Stephen Gottschalk, Hao Liu, Meng-Fen Wu, Phuong Nguyen, Aarohi Thakkar, Abishek Vaidya, Arpad Szoor, and Mireya Paulina Velasquez

Abstract

T cells expressing CD19-specific chimeric antigen receptors (CARs) with endodomains that encode a signaling domain derived from CD3ζ and CD28 or 41BB have potent antitumor activity in early-phase clinical studies for B-cell malignancies. Besides CD19-specific CARs, other approaches are actively being pursued to redirect T cells to CD19, including recombinant bispecific T-cell engager (BiTE) proteins or T cells genetically modified to express BiTEs [engager (ENG) T cells]. As BiTEs provide no costimulation, we investigated here if provision of costimulation through CD28 and 41BB enhances the effector function of CD19-ENG T cells. CD19-ENG T cells expressing CD80 and 41BBL on their cell surface (CD19-ENG.41BBL/CD80 T cells) were generated by retroviral transduction. CD19-ENG.41BBL/CD80 T cells retained their antigen specificity and had superior effector function compared with both unmodified T cells and CD19-ENG T cells expressing either CD80, 41BBL, or no costimulatory molecule, as judged by cytokine (IFNγ and IL2) production, T-cell proliferation, and their ability to sequentially kill target cells. In vivo, CD19-ENG.41BBL/CD80 T cells had superior antileukemia activity in the BV173 xenograft model, resulting in a survival advantage in comparison to CD19-ENG T cells. Thus, provision of costimulation is critical for the effector function of ENG T cells. Cancer Immunol Res; 5(10); 860–70. ©2017 AACR.

Published
2023

81. Supplemental Figures 1 - 8 from Transgenic Expression of IL15 Improves Antiglioma Activity of IL13Rα2-CAR T Cells but Results in Antigen Loss Variants

Author

Stephen Gottschalk, Irina V. Balyasnikova, Gianpietro Dotti, Hao Liu, Meng-Fen Wu, Zhongzhen Yi, Brooke L. Prinzing, and Giedre Krenciute

Abstract

Supplementary Figure 1: IL13Rα2-CAR and/or IL15 expression does not change T-cell phenotype. Supplementary Figure 2: Cell surface expression of IL13Rα2. Supplementary Figure 3: IL15 improves cell viability in the absence of exogenous cytokines. Supplementary Figure 4: Transgene expression is upregulated upon T cell activation. Supplemental Figure 5: IL13Rα2-CAR.IL15 T cells display activation-dependent IL15 production and greater proliferative capacity. Supplementary Figure 6: CID induces cell death in T cells genetically modified with retroviral vector encoding iC9.dNFGR.IL15. Supplemental Figure 7: Addition of exogenous IL15 increases CAR T-cell expansion in vitro. Supplementary Figure 8: IL13Rα2 or HER2 antigen loss variants are not killed by IL13Rα2- or HER2-CAR T cells.

Published
2023

82. Supplementary Figure from B7-H3 Specific CAR T Cells for the Naturally Occurring, Spontaneous Canine Sarcoma Model

Author

Seth M. Pollack, Beverly Torok-Storb, Peter F. Moore, Stephen Gottschalk, Michael C. Jensen, Stanley R. Riddell, Alexander I. Salter, Bernard Seguin, Himaly Shinglot, Juliana Chi Kei Ng, Weiqing Jing, Ali Zhang, Amy B. Heimberger, Borislav A. Alexiev, Brian C. Schulte, Kraig Abrams, Brett A. Schroeder, Amanda Koehne, Cassandra Miller, Brian J. Hayes, Karan Kohli, R. Graeme Black, and Shihong Zhang

Abstract

Supplementary Figure from B7-H3 Specific CAR T Cells for the Naturally Occurring, Spontaneous Canine Sarcoma Model

Published
2023

83. Data from Transgenic Expression of IL15 Improves Antiglioma Activity of IL13Rα2-CAR T Cells but Results in Antigen Loss Variants

Author

Stephen Gottschalk, Irina V. Balyasnikova, Gianpietro Dotti, Hao Liu, Meng-Fen Wu, Zhongzhen Yi, Brooke L. Prinzing, and Giedre Krenciute

Abstract

Glioblastoma (GBM) is the most aggressive primary brain tumor in adults and is virtually incurable with conventional therapies. Immunotherapy with T cells expressing GBM-specific chimeric antigen receptors (CAR) is an attractive approach to improve outcomes. Although CAR T cells targeting GBM antigens, such as IL13 receptor subunit α2 (IL13Rα2), HER2, and EGFR variant III (EGFRvIII), have had antitumor activity in preclinical models, early-phase clinical testing has demonstrated limited antiglioma activity. Transgenic expression of IL15 is an appealing strategy to enhance CAR T-cell effector function. We tested this approach in our IL13Rα2-positive glioma model in which limited IL13Rα2-CAR T-cell persistence results in recurrence of antigen-positive gliomas. T cells were genetically modified with retroviral vectors encoding IL13Rα2-CARs or IL15 (IL13Rα2-CAR.IL15 T cells). IL13Rα2-CAR.IL15 T cells recognized glioma cells in an antigen-dependent fashion, had greater proliferative capacity, and produced more cytokines after repeated stimulations in comparison with IL13Rα2-CAR T cells. No autonomous IL13Rα2-CAR.IL15 T-cell proliferation was observed; however, IL15 expression increased IL13Rα2-CAR T-cell viability in the absence of exogenous cytokines or antigen. In vivo, IL13Rα2-CAR.IL15 T cells persisted longer and had greater antiglioma activity than IL13Rα2-CAR T cells, resulting in a survival advantage. Gliomas recurring after 40 days after T-cell injection had downregulated IL13Rα2 expression, indicating that antigen loss variants occur in the setting of improved T-cell persistence. Thus, CAR T cells for GBM should not only be genetically modified to improve their proliferation and persistence, but also to target multiple antigens.Summary: Glioblastoma responds imperfectly to immunotherapy. Transgenic expression of IL15 in T cells expressing CARs improved their proliferative capacity, persistence, and cytokine production. The emergence of antigen loss variants highlights the need to target multiple tumor antigens. Cancer Immunol Res; 5(7); 571–81. ©2017 AACR.

Published
2023

84. Supplemental Figure 1 from Constitutive Signaling from an Engineered IL7 Receptor Promotes Durable Tumor Elimination by Tumor-Redirected T Cells

Author

Cliona M. Rooney, Stephen Gottschalk, Leonid S. Metelitsa, Malcolm K. Brenner, Hao Liu, Paul Castillo, Robin Parihar, Daofeng Liu, Tim Sauer, Zhongzhen Yi, Kathan Parikh, Dimitrios L. Wagner, Robert L. Kruse, Haruko Tashiro, Bilal Omer, and Thomas Shum

Abstract

Supplementary Figure 1: CD34-IL7R* (C7R) is stably expressed in T-cells and enhances constitutive STAT5 activation relative to IL7R*.

Published
2023

85. Supplemental Figure 4 from Constitutive Signaling from an Engineered IL7 Receptor Promotes Durable Tumor Elimination by Tumor-Redirected T Cells

Author

Cliona M. Rooney, Stephen Gottschalk, Leonid S. Metelitsa, Malcolm K. Brenner, Hao Liu, Paul Castillo, Robin Parihar, Daofeng Liu, Tim Sauer, Zhongzhen Yi, Kathan Parikh, Dimitrios L. Wagner, Robert L. Kruse, Haruko Tashiro, Bilal Omer, and Thomas Shum

Abstract

Supplementary Figure 4: C7R prolongs survival of GD2-CAR T-cells but does not support autonomous cell expansion.

Published
2023

86. Supplemental Table 1 from Constitutive Signaling from an Engineered IL7 Receptor Promotes Durable Tumor Elimination by Tumor-Redirected T Cells

Author

Cliona M. Rooney, Stephen Gottschalk, Leonid S. Metelitsa, Malcolm K. Brenner, Hao Liu, Paul Castillo, Robin Parihar, Daofeng Liu, Tim Sauer, Zhongzhen Yi, Kathan Parikh, Dimitrios L. Wagner, Robert L. Kruse, Haruko Tashiro, Bilal Omer, and Thomas Shum

Abstract

Supplemental Table 1: Differential gene expression in GD2-CAR.C7R T-cells compared to GD2-CAR T-cells.

Published
2023

87. Supplemental Figure 2 from Constitutive Signaling from an Engineered IL7 Receptor Promotes Durable Tumor Elimination by Tumor-Redirected T Cells

Author

Cliona M. Rooney, Stephen Gottschalk, Leonid S. Metelitsa, Malcolm K. Brenner, Hao Liu, Paul Castillo, Robin Parihar, Daofeng Liu, Tim Sauer, Zhongzhen Yi, Kathan Parikh, Dimitrios L. Wagner, Robert L. Kruse, Haruko Tashiro, Bilal Omer, and Thomas Shum

Abstract

Supplementary Figure 2: Efficient retroviral transduction of C7R and Î"34 in both CD4 and CD8 selected T-cells.

Published
2023

92. Data from Armed Oncolytic Adenovirus–Expressing PD-L1 Mini-Body Enhances Antitumor Effects of Chimeric Antigen Receptor T Cells in Solid Tumors

Author

Masataka Suzuki, Malcolm Brenner, Stephen Gottschalk, Bhakti Rana, Caroline Porter, Norihiro Watanabe, Amanda Rosewell Shaw, and Kiyonori Tanoue

Abstract

Chimeric antigen receptor–modified T cells (CAR T cells) produce proinflammatory cytokines that increase expression of T-cell checkpoint signals such as PD-L1, which may inhibit their functionality against solid tumors. In this study, we evaluated in human tumor xenograft models the proinflammatory properties of an oncolytic adenovirus (Onc.Ad) with a helper-dependent Ad (HDAd) that expresses a PD-L1 blocking mini-antibody (mini-body; HDPDL1) as a strategy to enhance CAR T-cell killing. Coadministration of these agents (CAd-VECPDL1) exhibited oncolytic effects with production of PD-L1 mini-body locally at the tumor site. On their own, HDPDL1 exhibited no antitumor effect and CAd-VECPDL1 alone reduced tumors only to volumes comparable to Onc.Ad treatment. However, combining CAd-VECPDL1 with HER2.CAR T cells enhanced antitumor activity compared with treatment with either HER2.CAR T cells alone or HER2.CAR T cells plus Onc.Ad. The benefits of locally produced PD-L1 mini-body by CAd-VECPDL1 could not be replicated by infusion of anti-PD-L1 IgG plus HER2.CAR T cells and coadministration of Onc.Ad in an HER2+ prostate cancer xenograft model. Overall, our data document the superiority of local production of PD-L1 mini-body by CAd-VECPDL1 combined with administration of tumor-directed CAR T cells to control the growth of solid tumors. Cancer Res; 77(8); 2040–51. ©2017 AACR.

Published
2023

98. Supplemental Figure 1 from Armed Oncolytic Adenovirus–Expressing PD-L1 Mini-Body Enhances Antitumor Effects of Chimeric Antigen Receptor T Cells in Solid Tumors

Author

Masataka Suzuki, Malcolm Brenner, Stephen Gottschalk, Bhakti Rana, Caroline Porter, Norihiro Watanabe, Amanda Rosewell Shaw, and Kiyonori Tanoue

Abstract

Cancer cells express HER2 and PD-L1 expression is induced in the presence of recombinant IFN�, and HER2.CAR T-cells express PD-1 in the presence of target cells.

Published
2023

99. B7-H3 Specific CAR T Cells for the Naturally Occurring, Spontaneous Canine Sarcoma Model

Author

Shihong Zhang, R. Graeme Black, Karan Kohli, Brian J. Hayes, Cassandra Miller, Amanda Koehne, Brett A. Schroeder, Kraig Abrams, Brian C. Schulte, Borislav A. Alexiev, Amy B. Heimberger, Ali Zhang, Weiqing Jing, Juliana Chi Kei Ng, Himaly Shinglot, Bernard Seguin, Alexander I. Salter, Stanley R. Riddell, Michael C. Jensen, Stephen Gottschalk, Peter F. Moore, Beverly Torok-Storb, and Seth M. Pollack

Subjects
Cancer Research, B7 Antigens, Dogs, Receptors, Chimeric Antigen, Oncology, Cell Line, Tumor, T-Lymphocytes, Animals, Humans, Sarcoma, Xenograft Model Antitumor Assays
Abstract

One obstacle for human solid tumor immunotherapy research is the lack of clinically relevant animal models. In this study, we sought to establish a chimeric antigen receptor (CAR) T-cell treatment model for naturally occurring canine sarcomas as a model for human CAR T-cell therapy. Canine CARs specific for B7-H3 were constructed using a single-chain variable fragment derived from the human B7-H3–specific antibody MGA271, which we confirmed to be cross-reactive with canine B7-H3. After refining activation, transduction, and expansion methods, we confirmed target killing in a tumor spheroid three-dimensional assay. We designed a B7-H3 canine CAR T-cell and achieved consistently high levels of transduction efficacy, expansion, and in vitro tumor killing. Safety of the CAR T cells were confirmed in two purposely bred healthy canine subjects following lymphodepletion by cyclophosphamide and fludarabine. Immune response, clinical parameters, and manifestation were closely monitored after treatments and were shown to resemble that of humans. No severe adverse events were observed. In summary, we demonstrated that similar to human cancers, B7-H3 can serve as a target for canine solid tumors. We successfully generated highly functional canine B7-H3–specific CAR T-cell products using a production protocol that closely models human CAR T-cell production procedure. The treatment regimen that we designed was confirmed to be safe in vivo. Our research provides a promising direction to establish in vitro and in vivo models for immunotherapy for canine and human solid tumor treatment.

Published
2022

100. Paediatric Strategy Forum for medicinal product development of chimeric antigen receptor T-cells in children and adolescents with cancer

Author

Elizabeth Fox, Michael Berntgen, Alfonso Quintás-Cardama, Veronique Minard-Colin, Susan L. Weiner, André Baruchel, Laura Pearce, Karsten Nysom, Andrew D.J. Pearson, Danielle H. Taylor, Christian M. Zwaan, Nirali N. Shah, Yousif Matloub, Ivan D. Horak, Gregory H. Reaman, Gilles Vassal, Koen Norga, Claudia Rossig, Dominik Karres, Lori A. Ehrlich, Martina Schüßler-Lenz, Alberto S. Pappo, Joe McDonough, Martina A. Sersch, Nick Richardson, Donna Ludwinski, Abraham Bassan, Eric Bleickardt, Nicole Scobie, Stephen Gottschalk, Rob Pieters, Sarah K. Tasian, Courtney Johnson, Teresa de Rojas, Malcolm A. Smith, Franca Ligas, Lynley V. Marshall, Shannon L. Maude, Brenda J. Weigel, Nick Bird, Najat Bouchkouj, Behzad K. Masouleh, Sarah Beaussant Cohen, Delphine Heenen, Rosanna Ricafort, G. Lesa, Linda Hanssens, Peter F. Bross, Carrie Brownstein, Crystal L. Mackall, Martin Pule, Douglas S. Hawkins, Jaroslav Sterba, and Maksim Mamonkin

Subjects
0303 health sciences, Cancer Research, medicine.medical_specialty, education.field_of_study, medicine.medical_treatment, Population, Immunotherapy, Disease, Chimeric antigen receptor, 3. Good health, Transplantation, Cell therapy, Clinical trial, 03 medical and health sciences, 0302 clinical medicine, Oncology, Drug development, hemic and lymphatic diseases, 030220 oncology & carcinogenesis, medicine, Intensive care medicine, education, 030304 developmental biology
Abstract

The seventh multi-stakeholder Paediatric Strategy Forum focused on chimeric antigen receptor (CAR) T-cells for children and adolescents with cancer. The development of CAR T-cells for patients with haematological malignancies, especially B-cell precursor acute lymphoblastic leukaemia (BCP-ALL), has been spectacular. However, currently, there are scientific, clinical and logistical challenges for use of CAR T-cells in BCP-ALL and other paediatric malignancies, particularly in acute myeloid leukaemia (AML), lymphomas and solid tumours. The aims of the Forum were to summarise the current landscape of CAR T-cell therapy development in paediatrics, too identify current challenges and future directions, with consideration of other immune effector modalities and ascertain the best strategies to accelerate their development and availability to children. Although the effect is of limited duration in about half of the patients, anti-CD19 CAR T-cells produce high response rates in relapsed/refractory BCP-ALL and this has highlighted previously unknown mechanisms of relapse. CAR T-cell treatment as first- or second-line therapy could also potentially benefit patients whose disease has high-risk features associated with relapse and failure of conventional therapies. Identifying patients with very early and early relapse in whom CAR T-cell therapy may replace haematopoietic stem cell transplantation and be definitive therapy versus those in whom it provides a more effective bridge to haematopoietic stem cell transplantation is a very high priority. Development of approaches to improve persistence, either by improving T cell fitness or using more humanised/fully humanised products and co-targeting of multiple antigens to prevent antigen escape, could potentially further optimise therapy. Many differences exist between paediatric B-cell non-Hodgkin lymphomas (B-NHL) and BCP-ALL. In view of the very small patient numbers with relapsed lymphoma, careful prioritisation is needed to evaluate CAR T-cells in children with Burkitt lymphoma, primary mediastinal B cell lymphoma and other NHL subtypes. Combination trials of alternative targets to CD19 (CD20 or CD22) should also be explored as a priority to improve efficacy in this population. Development of CD30 CAR T-cell immunotherapy strategies in patients with relapsed/refractory Hodgkin lymphoma will likely be most efficiently accomplished by joint paediatric and adult trials. CAR T-cell approaches are early in development for AML and T-ALL, given the unique challenges of successful immunotherapy actualisation in these diseases. At this time, CD33 and CD123 appear to be the most universal targets in AML and CD7 in T-ALL. The results of ongoing or planned first-in-human studies are required to facilitate further understanding. There are promising early results in solid tumours, particularly with GD2 targeting cell therapies in neuroblastoma and central nervous system gliomas that represent significant unmet clinical needs. Further understanding of biology is critical to success. The comparative benefits of autologous versus allogeneic CAR T-cells, T-cells engineered with T cell receptors T-cells engineered with T cell receptor fusion constructs, CAR Natural Killer (NK)-cell products, bispecific T-cell engager antibodies and antibody-drug conjugates require evaluation in paediatric malignancies. Early and proactive academia and multi-company engagement are mandatory to advance cellular immunotherapies in paediatric oncology. Regulatory advice should be sought very early in the design and preparation of clinical trials of innovative medicines, for which regulatory approval may ultimately be sought. Aligning strategic, scientific, regulatory, health technology and funding requirements from the inception of a clinical trial is especially important as these are very expensive therapies. The model for drug development for cell therapy in paediatric oncology could also involve a ‘later stage handoff’ to industry after early development in academic hands. Finally, and very importantly, strategies must evolve to ensure appropriate ease of access for children who need and could potentially benefit from these therapies.

Published
2022

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