Your search keyword '"Carl H. June"' showing total 370 results

1. Next-Generation CAR T-cell Therapies

Author

Regina M. Young, Nils W. Engel, Ugur Uslu, Nils Wellhausen, and Carl H. June

Subjects

Oncology, T-Lymphocytes, Antigens, CD19, Receptors, Antigen, T-Cell, Tumor Microenvironment, Humans, B-Cell Maturation Antigen, Multiple Myeloma, Immunotherapy, Adoptive, Article

Abstract

Summary:CD19- and B-cell maturation antigen (BCMA)–directed chimeric antigen receptor (CAR) T cells have enabled unprecedented responses in a subset of refractory patients with B-cell and plasma cell malignancies, leading to their approval by the FDA for the treatment of leukemia, lymphoma, and myeloma. These “living drugs” can become part of a synthetic immune system, persisting at least a decade in some patients. However, despite this tremendous impact, significant unmet treatment needs remain for patients with hematologic malignancies and solid cancers. In this perspective, we highlight recent innovations that advance the field toward production of a more potent and universal cellular immunotherapy of the future. Next-generation CAR T cells will incorporate advances in gene engineering and synthetic biology to enhance functionality and persistence, and reduce treatment-associated toxicities. The combination of autologous CAR T cells with various allogeneic cell treatment strategies designed to target the immunosuppressive tumor microenvironment will broaden the impact of future CAR T-cell therapies.

Published

2022

2. Potent suppression of neuroendocrine tumors and gastrointestinal cancers by CDH17CAR T cells without toxicity to normal tissues

Author

Zijie Feng, Xin He, Xuyao Zhang, Yuan Wu, Bowen Xing, Alison Knowles, Qiaonan Shan, Samuel Miller, Taylor Hojnacki, Jian Ma, Bryson W. Katona, Terence P. F. Gade, Jörg Schrader, David C. Metz, Carl H. June, and Xianxin Hua

Subjects

Mice, Neuroendocrine Tumors, Cancer Research, Receptors, Chimeric Antigen, Oncology, T-Lymphocytes, Animals, Humans, Xenograft Model Antitumor Assays, Gastrointestinal Neoplasms

Abstract

Gastrointestinal cancers (GICs) and neuroendocrine tumors (NETs) are often refractory to therapy after metastasis. Adoptive cell therapy using chimeric antigen receptor (CAR) T cells, though remarkably efficacious for treating leukemia, is yet to be developed for solid tumors such as GICs and NETs. Here we isolated a llama-derived nanobody, VHH1, and found that it bound cell surface adhesion protein CDH17 upregulated in GICs and NETs. VHH1-CAR T cells (CDH17CARTs) killed both human and mouse tumor cells in a CDH17-dependent manner. CDH17CARTs eradicated CDH17-expressing NETs and gastric, pancreatic and colorectal cancers in either tumor xenograft or autochthonous mouse models. Notably, CDH17CARTs do not attack normal intestinal epithelial cells, which also express CDH17, to cause toxicity, likely because CDH17 is localized only at the tight junction between normal intestinal epithelial cells. Thus, CDH17 represents a class of previously unappreciated tumor-associated antigens that is 'masked' in healthy tissues from attack by CAR T cells for developing safer cancer immunotherapy.

Published

2022

3. A randomized phase 2 trial of idiotype vaccination and adoptive autologous T-cell transfer in patients with multiple myeloma

Author

Cha Soung-chul, Veerabhadran Baladandayuthapani, Qaiser Bashir, Naseem Kerr, Sheetal S Rao, Beryl Tross, Carl H. June, Edward A. Stadtmauer, Szymon Jakub Szymura, Adam D. Cohen, Neeraj Saini, Robert Z. Orlowski, Michael Popescu, Karen Dengel, Zhe Wang, Medhavi Honhar, Bruce L. Levine, Elizabeth J. Shpall, Kunhwa Kim, Richard E. Champlin, Aaron Anderson, Alfred L. Garfall, Muzaffar H. Qazilbash, Tiantian Zhang, Dan T. Vogl, Larry W. Kwak, and Heather Lin

Subjects

CD4-Positive T-Lymphocytes, Male, Idiotype, Clinical Trials and Observations, T cell, Immunology, chemical and pharmacologic phenomena, CD8-Positive T-Lymphocytes, Cancer Vaccines, Transplantation, Autologous, complex mixtures, Biochemistry, Disease-Free Survival, Memory T Cells, Immune system, Immunologic Factors, Humans, Medicine, Autografts, Multiple myeloma, business.industry, Vaccination, hemic and immune systems, Cell Biology, Hematology, medicine.disease, Adoptive Transfer, Survival Rate, medicine.anatomical_structure, Hemocyanins, Toxicity, Female, Blood Commentary, Immunotherapy, Cancer vaccine, Multiple Myeloma, business, CD8

Abstract

We hypothesized that combining adoptively transferred autologous T cells with a cancer vaccine strategy would enhance therapeutic efficacy by adding antimyeloma idiotype (Id)–keyhole limpet hemocyanin (KLH) vaccine to vaccine-specific costimulated T cells. In this randomized phase 2 trial, patients received either control (KLH only) or Id-KLH vaccine, autologous transplantation, vaccine-specific costimulated T cells expanded ex vivo, and 2 booster doses of assigned vaccine. In 36 patients (KLH, n = 20; Id-KLH, n = 16), no dose-limiting toxicity was seen. At last evaluation, 6 (30%) and 8 patients (50%) had achieved complete remission in KLH-only and Id-KLH arms, respectively (P = .22), and no difference in 3-year progression-free survival was observed (59% and 56%, respectively; P = .32). In a 594 Nanostring nCounter gene panel analyzed for immune reconstitution (IR), compared with patients receiving KLH only, there was a greater change in IR genes in T cells in those receiving Id-KLH relative to baseline. Specifically, upregulation of genes associated with activation, effector function induction, and memory CD8+ T-cell generation after Id-KLH but not after KLH control vaccination was observed. Similarly, in responding patients across both arms, upregulation of genes associated with T-cell activation was seen. At baseline, all patients had greater expression of CD8+ T-cell exhaustion markers. These changes were associated with functional Id-specific immune responses in a subset of patients receiving Id-KLH. In conclusion, in this combination immunotherapy approach, we observed significantly more robust IR in CD4+ and CD8+ T cells in the Id-KLH arm, supporting further investigation of vaccine and adoptive immunotherapy strategies. This trial was registered at www.clinicaltrials.gov as #NCT01426828.

Published

2022

4. Better living through chemistry: CRISPR/Cas engineered T cells for cancer immunotherapy

Author

Saar Gill, Nils Wellhausen, Sangya Agarwal, Carl H. June, and Philipp C. Rommel

Subjects

Gene Editing, T-Lymphocytes, Transgene, T cell, medicine.medical_treatment, Immunology, T-cell receptor, Computational biology, Immunotherapy, Adoptive, Article, Chimeric antigen receptor, medicine.anatomical_structure, Genome editing, Cancer immunotherapy, Neoplasms, medicine, Humans, Immunology and Allergy, CRISPR, Immunotherapy, CRISPR-Cas Systems, Function (biology)

Abstract

T cells engineered to express transgenes such as chimeric antigen receptors (CAR) or modified T cell receptors (TCR) represent a new pillar of cancer therapy. Use of CRISPR/Cas gene-editing tools now allows even stronger and more precise control over the fate and function of engineered T cell therapies, including multiplex genome editing to facilitate use of off-the-shelf allogeneic T cells and novel approaches which have the potential to overcome some of the limitations of canonical Cas9-mediated DNA cleavage. This review summarizes the CRISPR/Cas techniques that have been used in preclinical research and outlines those that currently being tested in clinical trials.

Published

2022

5. CAR T cells produced in vivo to treat cardiac injury

Author

Joel G. Rurik, István Tombácz, Amir Yadegari, Pedro O. Méndez Fernández, Swapnil V. Shewale, Li Li, Toru Kimura, Ousamah Younoss Soliman, Tyler E. Papp, Ying K. Tam, Barbara L. Mui, Steven M. Albelda, Ellen Puré, Carl H. June, Haig Aghajanian, Drew Weissman, Hamideh Parhiz, and Jonathan A. Epstein

Subjects

Heart Failure, Male, Receptors, Chimeric Antigen, Multidisciplinary, Heart Diseases, Myocardium, T-Lymphocytes, Membrane Proteins, Fibroblasts, CD5 Antigens, Adoptive Transfer, Fibrosis, Immunotherapy, Adoptive, Trogocytosis, Mice, Inbred C57BL, Mice, HEK293 Cells, Endopeptidases, Liposomes, Animals, Humans, Nanoparticles, RNA, Messenger, Cell Engineering, Spleen

Abstract

Making CAR T cells in vivo Cardiac fibrosis is the stiffening and scarring of heart tissue and can be fatal. Rurik et al . designed an immunotherapy strategy to generate transient chimeric antigen receptor (CAR) T cells that can recognize the fibrotic cells in the heart (see the Perspective by Gao and Chen). By injecting CD5-targeted lipid nanoparticles containing the messenger RNA (mRNA) instructions needed to reprogram T lymphocytes, the researchers were able to generate therapeutic CAR T cells entirely inside the body. Analysis of a mouse model of heart disease revealed that the approach was successful in reducing fibrosis and restoring cardiac function. The ability to produce CAR T cells in vivo using modified mRNA may have a number of therapeutic applications. —PNK

Published

2022

6. CAR T-cell Therapy Meets Clonal Hematopoiesis

Author

Ugur Uslu and Carl H. June

Subjects

Biological Products, Antigens, CD19, Receptors, Antigen, T-Cell, Humans, Neurotoxicity Syndromes, Lymphoma, Large B-Cell, Diffuse, General Medicine, In Focus, Clonal Hematopoiesis, Immunotherapy, Adoptive

Abstract

To explore the role of clonal hematopoiesis (CH) in chimeric antigen receptor (CAR) T-cell therapy outcomes, we performed targeted deep sequencing on buffy coats collected during the 21 days before lymphodepleting chemotherapy from 114 large B-cell lymphoma patients treated with anti-CD19 CAR T cells. We detected CH in 42 (36.8%) pretreatment samples, most frequently in PPM1D (19/114) and TP53 (13/114) genes. Grade ≥3 immune effector cell-associated neurotoxicity syndrome (ICANS) incidence was higher in CH-positive patients than CH-negative patients (45.2% vs. 25.0%, P = 0.038). Higher toxicities with CH were primarily associated with DNMT3A, TET2, and ASXL1 genes (DTA mutations). Grade ≥3 ICANS (58.9% vs. 25%, P = 0.02) and ≥3 cytokine release syndrome (17.7% vs. 4.2%, P = 0.08) incidences were higher in DTA-positive than in CH-negative patients. The estimated 24-month cumulative incidence of therapy-related myeloid neoplasms after CAR T-cell therapy was higher in CH-positive than CH-negative patients [19% (95% CI, 5.5-38.7) vs. 4.2% (95% CI, 0.3-18.4), P = 0.028].Our study reveals that CH mutations, especially those associated with inflammation (DNMT3A, TET2, and ASXL1), are associated with severe-grade neurotoxicities in lymphoma patients receiving anti-CD19 CAR T-cell therapy. Further studies to investigate the mechanisms and interventions to improve toxicities in the context of CH are warranted. See related content by Uslu and June, p. 382. This article is highlighted in the In This Issue feature, p. 369.

Published

2022

7. Orthogonal Design of Experiments for Optimization of Lipid Nanoparticles for mRNA Engineering of CAR T Cells

Author

Carl H. June, Margaret M. Billingsley, David Mai, Alex G. Hamilton, Michael J. Mitchell, Savan K. Patel, Kelsey L. Swingle, and Neil C. Sheppard

Subjects

Messenger RNA, Chemistry, T-Lymphocytes, Mechanical Engineering, Electroporation, T cell, Excipient, Bioengineering, General Chemistry, Transfection, Condensed Matter Physics, Article, Chimeric antigen receptor, Cell biology, medicine.anatomical_structure, Liposomes, Cancer cell, medicine, Humans, Nanoparticles, General Materials Science, RNA, Messenger, Cytotoxicity, medicine.drug

Abstract

Viral engineered chimeric antigen receptor (CAR) T cell therapies are potent, targeted cancer immunotherapies, but their permanent CAR expression can lead to severe adverse effects. Nonviral messenger RNA (mRNA) CAR T cells are being explored to overcome these drawbacks, but electroporation, the most common T cell transfection method, is limited by cytotoxicity. As a potentially safer nonviral delivery strategy, here, sequential libraries of ionizable lipid nanoparticle (LNP) formulations with varied excipient compositions were screened in comparison to a standard formulation for improved mRNA delivery to T cells with low cytotoxicity, revealing B10 as the top formulation with a 3-fold increase in mRNA delivery. When compared to electroporation in primary human T cells, B10 LNPs induced comparable CAR expression with reduced cytotoxicity while demonstrating potent cancer cell killing. These results demonstrate the impact of excipient optimization on LNP performance and support B10 LNPs as a potent mRNA delivery platform for T cell engineering.

Published

2021

8. In vivo gene immunotherapy for cancer

Author

David Mai, Carl H. June, and Neil C. Sheppard

Subjects

Neoplasms, Genetic Vectors, Humans, Immunotherapy, Genetic Therapy, General Medicine, Precision Medicine

Abstract

Cancer is becoming increasingly understood not only as a disease of pathological cells but also as one of immune hypofunction. The heterogenous and patient-specific nature of cancer further underscores the need for personalized cellular therapies, which are currently produced ex vivo. Gene-modulating approaches, such as therapeutic RNAs and improved viral vectors, now bring us closer toward strategies for mitigating disease, particularly for diseases that benefit from altering gene or transgene expression profiles in pathological or therapeutic immune cells. An advancing toolbox of technologies and trends toward simplifying personalized therapies foreshadow opportunities for direct, in vivo precision medicine against cancer.

Published

2022

9. CAR T therapy extends its reach to autoimmune diseases

Author

Daniel J. Baker and Carl H. June

Subjects

Receptors, Chimeric Antigen, Humans, Lupus Erythematosus, Systemic, General Biochemistry, Genetics and Molecular Biology, Autoimmune Diseases

Abstract

CAR T therapy has revolutionized the treatment of hematologic cancers. In their recent Nature Medicine paper, Mackensen et al. report the use of CAR T cells to treat systemic lupus erythematosus in five patients. This provides enthusiasm to further explore CAR T therapy beyond oncology.

Published

2022

10. Single-cell antigen-specific landscape of CAR T infusion product identifies determinants of CD19-positive relapse in patients with ALL

Author

Zhiliang Bai, Steven Woodhouse, Ziran Zhao, Rahul Arya, Kiya Govek, Dongjoo Kim, Stefan Lundh, Alev Baysoy, Hongxing Sun, Yanxiang Deng, Yang Xiao, David M. Barrett, Regina M. Myers, Stephan A. Grupp, Carl H. June, Rong Fan, Pablo G. Camara, and J. Joseph Melenhorst

Subjects

Proteomics, Receptors, Chimeric Antigen, Multidisciplinary, Recurrence, Antigens, CD19, Humans, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Immunotherapy, Adoptive

Abstract

A notable number of acute lymphoblastic leukemia (ALL) patients develop CD19-positive relapse within 1 year after receiving chimeric antigen receptor (CAR) T cell therapy. It remains unclear if the long-term response is associated with the characteristics of CAR T cells in infusion products, hindering the identification of biomarkers to predict therapeutic outcomes. Here, we present 101,326 single-cell transcriptomes and surface protein landscape from the infusion products of 12 ALL patients. We observed substantial heterogeneity in the antigen-specific activation states, among which a deficiency of T helper 2 function was associated with CD19-positive relapse compared with durable responders (remission, >54 months). Proteomic data revealed that the frequency of early memory T cells, rather than activation or coinhibitory signatures, could distinguish the relapse. These findings were corroborated by independent functional profiling of 49 patients, and an integrative model was developed to predict the response. Our data unveil the molecular mechanisms that may inform strategies to boost specific T cell function to maintain long-term remission.

Published

2022

11. A phase I trial of cyclosporine for hospitalized patients with COVID-19

Author

Emily A. Blumberg, Julia Han Noll, Pablo Tebas, Joseph A. Fraietta, Ian Frank, Amy Marshall, Anne Chew, Elizabeth A. Veloso, Alison Carulli, Walter Rogal, Avery L. Gaymon, Aliza H. Schmidt, Tiffany Barnette, Renee Jurek, Rene Martins, Briana M. Hudson, Kalyan Chavda, Christina M. Bailey, Sarah E. Church, Hooman Noorchashm, Wei-Ting Hwang, Carl H. June, and Elizabeth O. Hexner

Subjects

Oxygen, SARS-CoV-2, Cyclosporine, Cytokines, Humans, General Medicine, COVID-19 Drug Treatment

Abstract

BACKGROUNDCOVID-19 remains a global health emergency with limited treatment options, lagging vaccine rates, and inadequate healthcare resources in the face of an ongoing calamity. The disease is characterized by immune dysregulation and cytokine storm. Cyclosporine A (CSA) is a calcineurin inhibitor that modulates cytokine production and may have direct antiviral properties against coronaviruses.METHODSTo test whether a short course of CSA was safe in patients with COVID-19, we treated 10 hospitalized, oxygen-requiring, noncritically ill patients with CSA (starting at a dose of 9 mg/kg/d). We evaluated patients for clinical response and adverse events, measured serum cytokines and chemokines associated with COVID-19 hyperinflammation, and conducted gene-expression analyses.RESULTSFive participants experienced adverse events, none of which were serious; transaminitis was most common. No participant required intensive care unit-level care, and all patients were discharged alive. CSA treatment was associated with significant reductions in serum cytokines and chemokines important in COVID-19 hyperinflammation, including CXCL10. Following CSA administration, we also observed a significant reduction in type I IFN gene expression signatures and other transcriptional profiles associated with exacerbated hyperinflammation in the peripheral blood cells of these patients.CONCLUSIONShort courses of CSA appear safe and feasible in patients with COVID-19 who require oxygen and may be a useful adjunct in resource-limited health care settings.TRIAL REGISTRATIONThis trial was registered on ClinicalTrials.gov (Investigational New Drug Application no. 149997; ClinicalTrials.gov NCT04412785).FUNDINGThis study was internally funded by the Center for Cellular Immunotherapies.

Published

2022

12. Off-the-shelf CAR T cells to treat cancer

Author

Sofia Castelli, Regina M. Young, and Carl H. June

Subjects

Neoplasms, T-Lymphocytes, Receptors, Antigen, T-Cell, Humans, Cell Biology, Immunotherapy, Adoptive, Molecular Biology

Published

2022

13. Engineered cellular immunotherapies in cancer and beyond

Author

Amanda V. Finck, Tatiana Blanchard, Christopher P. Roselle, Giulia Golinelli, and Carl H. June

Subjects

Receptors, Chimeric Antigen, Neoplasms, T-Lymphocytes, Humans, General Medicine, Immunotherapy, Immunotherapy, Adoptive, General Biochemistry, Genetics and Molecular Biology, Article

Abstract

This year marks the tenth anniversary of cell therapy with chimeric antigen receptor (CAR)-modified T cells for refractory leukemia. The widespread commercial approval of genetically engineered T cells for a variety of blood cancers offers hope for patients with other types of cancer, and the convergence of human genome engineering and cell therapy technology holds great potential for generation of a new class of cellular therapeutics. In this Review, we discuss the goals of cellular immunotherapy in cancer, key challenges facing the field and exciting strategies that are emerging to overcome these obstacles. Finally, we outline how developments in the cancer field are paving the way for cellular immunotherapeutics in other diseases.

Published

2022

14. Anti-CD19 CAR T cells in combination with ibrutinib for the treatment of chronic lymphocytic leukemia

Author

Saar Gill, Vanessa Vides, Noelle V. Frey, Elizabeth O. Hexner, Susan Metzger, Megan O'Brien, Wei-Ting Hwang, Jennifer L. Brogdon, Megan M. Davis, Joseph A. Fraietta, Avery L. Gaymon, Whitney L. Gladney, Simon F. Lacey, Anne Lamontagne, Anthony R. Mato, Marcela V. Maus, J. Joseph Melenhorst, Edward Pequignot, Marco Ruella, Maksim Shestov, John C. Byrd, Stephen J. Schuster, Donald L. Siegel, Bruce L. Levine, Carl H. June, and David L. Porter

Subjects

Neoplasm, Residual, Pyrimidines, hemic and lymphatic diseases, T-Lymphocytes, Antigens, CD19, Humans, Pyrazoles, Hematology, Prospective Studies, Leukemia, Lymphocytic, Chronic, B-Cell, Disease-Free Survival

Abstract

In chronic lymphocytic leukemia (CLL) patients who achieve a complete remission (CR) to anti-CD19 chimeric antigen receptor T cells (CART-19), remissions are remarkably durable. Preclinical data suggesting synergy between CART-19 and the Bruton’s tyrosine kinase (BTK) inhibitor ibrutinib prompted us to conduct a prospective single-center phase 2 trial in which we added autologous anti-CD19 humanized binding domain T cells (huCART-19) to ibrutinib in patients with CLL not in CR despite ≥6 months of ibrutinib. The primary endpoints were safety, feasibility, and achievement of a CR within 3 months. Of 20 enrolled patients, 19 received huCART-19. The median follow-up for all infused patients was 41 months (range, 0.25-58 months). Eighteen patients developed cytokine release syndrome (CRS; grade 1-2 in 15 of 18 subjects), and 5 developed neurotoxicity (grade 1-2 in 4 patients, grade 4 in 1 patient). While the 3-month CR rate among International Working Group on CLL (iwCLL)-evaluable patients was 44% (90% confidence interval [CI], 23-67%), at 12 months, 72% of patients tested had no measurable residual disease (MRD). The estimated overall and progression-free survival at 48 months were 84% and 70%, respectively. Of 15 patients with undetectable MRD at 3 or 6 months, 13 remain in ongoing CR at the last follow-up. In patients with CLL not achieving a CR despite ≥6 months of ibrutinib, adding huCART-19 mediated a high rate of deep and durable remissions. ClinicalTrials.gov number, NCT02640209.

Published

2022

15. Diagnostic biomarkers to differentiate sepsis from cytokine release syndrome in critically ill children

Author

Simon F. Lacey, Caroline Diorio, Edward M. Behrens, David M. Barrett, David L. Porter, Fang Chen, Jenny Bush, Bruce L. Levine, Alena Orlenko, Edward Pequignot, J. Joseph Melenhorst, Jason H. Moore, Natalka Koterba, Pamela A. Shaw, Richard Aplenc, Donglan Zhang, Michele Paessler, David T. Teachey, Vanessa E. Gonzalez, Don L. Siegel, Hamid Bassiri, Stephan A. Grupp, Megan M. Davis, Nuala J. Meyer, Scott L. Weiss, Amanda M. DiNofia, Shannon L. Maude, and Carl H. June

Subjects

0301 basic medicine, Immunobiology and Immunotherapy, Critical Illness, T cell, Receptors, Antigen, T-Cell, CD19, Sepsis, 03 medical and health sciences, 0302 clinical medicine, Antigen, Refractory, otorhinolaryngologic diseases, medicine, Humans, Child, Receptor, biology, business.industry, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, Chimeric antigen receptor, Cytokine release syndrome, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Immunology, biology.protein, Cytokine Release Syndrome, business

Abstract

Chimeric antigen receptor (CAR) T-cells directed against CD19 have drastically altered outcomes for children with relapsed and refractory acute lymphoblastic leukemia (r/r ALL). Pediatric patients with r/r ALL treated with CAR-T are at increased risk of both cytokine release syndrome (CRS) and sepsis. We sought to investigate the biologic differences between CRS and sepsis and to develop predictive models which could accurately differentiate CRS from sepsis at the time of critical illness. We identified 23 different cytokines that were significantly different between patients with sepsis and CRS. Using elastic net prediction modeling and tree classification, we identified cytokines that were able to classify subjects as having CRS or sepsis accurately. A markedly elevated interferon γ (IFNγ) or a mildly elevated IFNγ in combination with a low IL1β were associated with CRS. A normal to mildly elevated IFNγ in combination with an elevated IL1β was associated with sepsis. This combination of IFNγ and IL1β was able to categorize subjects as having CRS or sepsis with 97% accuracy. As CAR-T therapies become more common, these data provide important novel information to better manage potential associated toxicities.

Published

2020

16. Long-Term Outcomes From a Randomized Dose Optimization Study of Chimeric Antigen Receptor Modified T Cells in Relapsed Chronic Lymphocytic Leukemia

Author

Xinhe Shan, Elizabeth O. Hexner, Noelle V. Frey, Daniel J. Landsburg, Simon F. Lacey, Carl H. June, Saar Gill, Sunita D. Nasta, Jakub Svoboda, Edward A. Stadtmauer, Anthony R. Mato, Alison W. Loren, Elizabeth Veloso, Avery L. Gaymon, Wei-Ting Hwang, Bruce L. Levine, Stephen J. Schuster, J. Joseph Melenhorst, David L. Porter, and Edward Pequignot

Subjects

Male, Cart, Oncology, Cancer Research, medicine.medical_specialty, T-Lymphocytes, Antigens, CD19, Dose-Response Relationship, Immunologic, Relapsed chronic lymphocytic leukemia, Immunotherapy, Adoptive, immune system diseases, Recurrence, Internal medicine, Long term outcomes, medicine, Humans, In patient, Aged, Receptors, Chimeric Antigen, business.industry, ORIGINAL REPORTS, Middle Aged, Leukemia, Lymphocytic, Chronic, B-Cell, Progression-Free Survival, Chimeric antigen receptor, Survival Rate, Dose optimization, Female, Refractory Chronic Lymphocytic Leukemia, Cytokine Release Syndrome, business

Abstract

PURPOSE To describe long-term outcomes of anti-CD19 chimeric antigen receptor T (CART) cells in patients with relapsed or refractory chronic lymphocytic leukemia (CLL). METHODS Between January 2013 and June 2016, 42 patients with relapsed or refractory CLL were enrolled in this study and 38 were infused with anti-CD19 CART cells (CART-19). Of these, 28 patients were initially randomly assigned to receive a low (5 × 107) or high (5 × 108) dose of CART-19, and 24 were evaluable for response assessment. After an interim analysis, 10 additional patients received the selected (high) dose and of these, eight were evaluable for response. Patients were followed for a median 31.5 months (range, 2 to 75 months). RESULTS At 4 weeks, the complete and overall responses for the 32 evaluable patients were 28% (90% CI, 16% to 44%) and 44% (90% CI, 29% to 60%), respectively. The median overall survival (OS) for all patients was 64 months; there was no statistically significant difference between low- and high-dose groups ( P = .84). Regardless of dose, prolonged survival was observed in patients who achieved a CR versus those who did not ( P = .035), with median OS not reached in patients with CR versus 64 months in those without CR. The median progression-free survival was 40.2 months in patients with CR and 1 month in those without a CR ( P < .0001). Toxicity was comparable in both dose groups. CONCLUSION In patients with advanced CLL, a 5 × 108 dose of CART-19 may be more effective than 5 × 107 CART-19 at inducing CR without excessive toxicity. Attainment of a CR after CART-19 infusion, regardless of cell dose, is associated with longer OS and progression-free survival in patients with relapsed CLL.

Published

2020

17. Cancer immunotherapy comes of age and looks for maturity

Author

Carl H. June, Amanda Finck, and Saar Gill

Subjects

0301 basic medicine, Cancer therapy, Receptor, ErbB-2, medicine.medical_treatment, Science, Programmed Cell Death 1 Receptor, General Physics and Astronomy, Cancer immunotherapy, 02 engineering and technology, Protein Engineering, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Neoplasms, Political science, medicine, Humans, CTLA-4 Antigen, lcsh:Science, Gene Editing, Oncolytic Virotherapy, Multidisciplinary, Extramural, business.industry, Comment, Antibodies, Monoclonal, Neoplasms therapy, General Chemistry, Public relations, 021001 nanoscience & nanotechnology, Maturity (finance), Cancer treatment, 030104 developmental biology, lcsh:Q, Immunotherapy, 0210 nano-technology, business

Abstract

As Nature Communications celebrates a 10-year anniversary, the field has witnessed the transition of cancer immunotherapy from a pipe dream to an established powerful cancer treatment modality. Here we discuss the opportunities and challenges for the future.

Published

2020

18. Harnessing CAR T-cell Insights to Develop Treatments for Hyperinflammatory Responses in Patients with COVID-19

Author

Carl H. June and Sangya Agarwal

Subjects

0301 basic medicine, Coronavirus disease 2019 (COVID-19), medicine.medical_treatment, Calcineurin Inhibitors, Pneumonia, Viral, Cell- and Tissue-Based Therapy, Receptors, Antigen, T-Cell, Lymphohistiocytosis, Hemophagocytic, Betacoronavirus, 03 medical and health sciences, 0302 clinical medicine, Antigen, Neoplasms, Immunopathology, medicine, Animals, Humans, Macrophage, In patient, In Focus, Pandemics, Repurposing, Inflammation, SARS-CoV-2, business.industry, Drug Repositioning, COVID-19, Macrophage Activation, Drug repositioning, 030104 developmental biology, Cytokine, Oncology, 030220 oncology & carcinogenesis, Immunology, Cytokines, Immunotherapy, Morbidity, Coronavirus Infections, business

Abstract

Summary: Cytokine release and macrophage activation contribute to immunopathology after SARS-CoV-2 infection. We discuss approaches to decrease the morbidity and mortality in patients with COVID-19 by repurposing existing drugs previously developed for cancer therapy.

Published

2020

19. Impaired Death Receptor Signaling in Leukemia Causes Antigen-Independent Resistance by Inducing CAR T-cell Dysfunction

Author

Nathan Singh, Xueqing Maggie Lu, Matthew D. Weitzman, Noelle V. Frey, Marco Ruella, Pranali Ravikumar, Shelley L. Berger, Sangya Agarwal, Olga Shestova, Stephan A. Grupp, Elena Orlando, Katharina E. Hayer, Seok Jae Hong, Shannon L. Maude, Shunichiro Kuramitsu, Ophir Shalem, Carl H. June, Raymone Pajarillo, Saar Gill, Karen Thudium Mueller, Charly R. Good, and Yong Gu Lee

Subjects

0301 basic medicine, Receptors, Chimeric Antigen, business.industry, Receptors, Death Domain, Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, Chimeric antigen receptor, 03 medical and health sciences, Leukemia, 030104 developmental biology, 0302 clinical medicine, Oncology, Antigen, 030220 oncology & carcinogenesis, medicine, Cancer research, Humans, Signal transduction, Receptor, business, Cytotoxicity, Gene, Progressive disease, Signal Transduction

Abstract

Primary resistance to CD19-directed chimeric antigen receptor T-cell therapy (CART19) occurs in 10% to 20% of patients with acute lymphoblastic leukemia (ALL); however, the mechanisms of this resistance remain elusive. Using a genome-wide loss-of-function screen, we identified that impaired death receptor signaling in ALL led to rapidly progressive disease despite CART19 treatment. This was mediated by an inherent resistance to T-cell cytotoxicity that permitted antigen persistence and was subsequently magnified by the induction of CAR T-cell functional impairment. These findings were validated using samples from two CAR T-cell clinical trials in ALL, where we found that reduced expression of death receptor genes was associated with worse overall survival and reduced T-cell fitness. Our findings suggest that inherent dysregulation of death receptor signaling in ALL directly leads to CAR T-cell failure by impairing T-cell cytotoxicity and promoting progressive CAR T-cell dysfunction. Significance: Resistance to CART19 is a significant barrier to efficacy in the treatment of B-cell malignancies. This work demonstrates that impaired death receptor signaling in tumor cells causes failed CART19 cytotoxicity and drives CART19 dysfunction, identifying a novel mechanism of antigen-independent resistance to CAR therapy. See related commentary by Green and Neelapu, p. 492.

Published

2020

20. Optimizing Chimeric Antigen Receptor T-Cell Therapy for Adults With Acute Lymphoblastic Leukemia

Author

Nirav N. Shah, Elizabeth O. Hexner, Selina M. Luger, Pamela A. Shaw, David L. Porter, Carl H. June, Simon F. Lacey, Alison W. Loren, J. Joseph Melenhorst, Joan Gilmore, Bruce L. Levine, Saar Gill, Stephan A. Grupp, Noelle V. Frey, Alexander E. Perl, Edward Pequignot, James K. Mangan, and Shannon L. Maude

Subjects

Adult, Male, 0301 basic medicine, Cancer Research, medicine.medical_treatment, Receptors, Antigen, T-Cell, Immunotherapy, Adoptive, Article, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Refractory, Antigen, medicine, Humans, Receptor, Survival rate, Aged, Chemotherapy, business.industry, Age Factors, Immunotherapy, Middle Aged, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Chimeric antigen receptor, Survival Rate, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, Female, Chimeric Antigen Receptor T-Cell Therapy, business

Abstract

PURPOSE The anti-CD19 chimeric antigen receptor T-cell therapy tisagenlecleucel (CTL019) has an 81% response rate in children with relapsed or chemotherapy refractory (r/r) B-cell acute lymphoblastic leukemia (ALL). Cytokine release syndrome (CRS) is a life-threatening treatment-related toxicity that limits the full therapeutic potential in adults. We report outcomes for adults with r/r ALL treated with an optimized CTL019 dosing and CRS management strategy. METHODS Adults with r/r B-cell ALL received CTL019 in 1 of 2 trials. Patients received lymphodepletion followed by CTL019 as either a one-time infusion or fractionated infusions split over 3 days (day 1, 10%; day 2, 30%; day 3, 60%), which allowed for day 2 and day 3 doses to be held for early CRS. Total planned CTL019 dose varied with adaptive protocol modifications in response to efficacy and CRS toxicity. RESULTS Thirty-five adults with r/r ALL received CTL019 in 1 of 3 dosing cohorts. The low-dose cohort (n = 9) received single or fractionated dosing and had manageable toxicity with a 33% complete remission (CR) rate. In the high-dose single infusion cohort, 3 of 6 patients with refractory CRS concurrent with culture-positive sepsis died, and 3 achieved CR. The 20 patients in the high-dose fractionated (HDF) cohort had a 90% CR rate and manageable CRS. The HDF cohort had the highest survival, with a 2-year overall survival of 73% (95% CI, 46% to 88%) and event-free survival of 49.5% (95% CI, 21% to 73%). CONCLUSION Fractionated dosing of CTL019 with intrapatient dose modification optimizes safety without compromising efficacy in adults with r/r ALL.

Published

2020

21. Ionizable Lipid Nanoparticle-Mediated mRNA Delivery for Human CAR T Cell Engineering

Author

Pranali Ravikumar, Michael J. Mitchell, Rui Zhang, Carl H. June, Margaret M. Billingsley, and Nathan Singh

Subjects

T-Lymphocytes, T cell, Bioengineering, 02 engineering and technology, Jurkat cells, Article, Viral vector, Drug Delivery Systems, Cell Line, Tumor, medicine, Humans, Cytotoxic T cell, General Materials Science, RNA, Messenger, Cell Engineering, Receptors, Chimeric Antigen, Chemistry, Mechanical Engineering, Electroporation, General Chemistry, 021001 nanoscience & nanotechnology, Condensed Matter Physics, Lipids, Coculture Techniques, Chimeric antigen receptor, Cell biology, medicine.anatomical_structure, Lipofectamine, Nanoparticles, 0210 nano-technology, Ex vivo

Abstract

Chimeric antigen receptor (CAR) T cell therapy relies on the ex vivo manipulation of patient T cells to create potent, cancer-targeting therapies, shown to be capable of inducing remission in patients with acute lymphoblastic leukemia and large B cell lymphoma. However, current CAR T cell engineering methods use viral delivery vectors, which induce permanent CAR expression and could lead to severe adverse effects. Messenger RNA (mRNA) has been explored as a promising strategy for inducing transient CAR expression in T cells to mitigate the adverse effects associated with viral vectors, but it most commonly requires electroporation for T cell mRNA delivery, which can be cytotoxic. Here, ionizable lipid nanoparticles (LNPs) were designed for ex vivo mRNA delivery to human T cells. A library of 24 ionizable lipids was synthesized, formulated into LNPs, and screened for luciferase mRNA delivery to Jurkat cells, revealing seven formulations capable of enhanced mRNA delivery over lipofectamine. The top-performing LNP formulation, C14—4, was selected for CAR mRNA delivery to primary human T cells. This platform induced CAR expression at levels equivalent to electroporation, with substantially reduced cytotoxicity. CAR T cells engineered via C14—4 LNP treatment were then compared to electroporated CAR T cells in a coculture assay with Nalm-6 acute lymphoblastic leukemia cells, and both CAR T cell engineering methods elicited potent cancer-killing activity. These results demonstrate the ability of LNPs to deliver mRNA to primary human T cells to induce functional protein expression, and indicate the potential of LNPs to enhance mRNA-based CAR T cell engineering methods.

Published

2020

22. Novel Redirected T Cell Immunotherapies for Advanced Prostate Cancer

Author

Naomi B. Haas, Stephen J. Forman, Vivek Narayan, Joseph A. Fraietta, Tanya B. Dorff, Peter Zang, Saul J. Priceman, and Carl H. June

Subjects

Oncology, Male, Cancer Research, medicine.medical_specialty, medicine.medical_treatment, T cell, T-Lymphocytes, Article, Prostate cancer, Internal medicine, Clinical investigation, Antibodies, Bispecific, medicine, Tumor Microenvironment, Humans, Tumor microenvironment, business.industry, Prostatic Neoplasms, Immunotherapy, medicine.disease, Differential toxicity, Chimeric antigen receptor, Clinical trial, medicine.anatomical_structure, business

Abstract

Immunotherapy has failed to achieve durable remissions in advanced prostate cancer patients. More potent T-cell–redirecting strategies may be needed to overcome the immunologically exclusive and suppressive tumor microenvironment. Clinical trials are underway, seeking to define the optimal target for T-cell redirection, such as PSMA, PSCA, or STEAP-1, as well as the optimal strategy, with CAR or bispecific antibodies. As results continue to emerge from these trials, understanding differential toxicity and efficacy of these therapies based on their targets and functional modifications will be key to advancing these promising therapies toward clinical practice. This review provides a unique depth and breadth of perspective regarding the diverse immunotherapy strategies currently under clinical investigation for men with advanced prostate cancer.

Published

2022

23. CD19-targeting CAR T cell immunotherapy outcomes correlate with genomic modification by vector integration

Author

Christopher L. Nobles, John K. Everett, Joseph A. Fraietta, Bruce L. Levine, Noelle V. Frey, Don L. Siegel, Shantan Reddy, Carl H. June, Stephan A. Grupp, J. Joseph Melenhorst, David L. Porter, Simon F. Lacey, Shannon L. Maude, Scott Sherrill-Mix, Saar Gill, and Frederic D. Bushman

Subjects

Male, 0301 basic medicine, Chronic lymphocytic leukemia, medicine.medical_treatment, T cell, Antigens, CD19, Genetic Vectors, Receptors, Antigen, T-Cell, Biology, Immunotherapy, Adoptive, CD19, Viral vector, Insertional mutagenesis, 03 medical and health sciences, 0302 clinical medicine, Antigen, hemic and lymphatic diseases, medicine, Humans, Gene, General Medicine, Immunotherapy, medicine.disease, Leukemia, Lymphocytic, Chronic, B-Cell, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Female, Research Article

Abstract

Chimeric antigen receptor–engineered T cells targeting CD19 (CART19) provide an effective treatment for pediatric acute lymphoblastic leukemia but are less effective for chronic lymphocytic leukemia (CLL), focusing attention on improving efficacy. CART19 harbor an engineered receptor, which is delivered through lentiviral vector integration, thereby marking cell lineages and modifying the cellular genome by insertional mutagenesis. We recently reported that vector integration within the host TET2 gene was associated with CLL remission. Here, we investigated clonal population structure and therapeutic outcomes in another 39 patients by high-throughput sequencing of vector-integration sites. Genes at integration sites enriched in responders were commonly found in cell-signaling and chromatin modification pathways, suggesting that insertional mutagenesis in these genes promoted therapeutic T cell proliferation. We also developed a multivariate model based on integration-site distributions and found that data from preinfusion products forecasted response in CLL successfully in discovery and validation cohorts and, in day 28 samples, reported responders to CLL therapy with high accuracy. These data clarify how insertional mutagenesis can modulate cell proliferation in CART19 therapy and how data on integration-site distributions can be linked to treatment outcomes.

Published

2019

24. CAR T-Cells Depend on the Coupling of NADH Oxidation with ATP Production

Author

Sophie Trefely, John Leferovich, Saba Ghassemi, Joshua D. Rabinowitz, Michael C. Milone, David Heo, Chong Xu, Roddy S. O’Connor, Carl H. June, Edmund K. Moon, Juan Carlos García-Cañaveras, Benjamin Philipson, and Nathaniel W. Snyder

Subjects

Adult, Male, Lactobacillus brevis NADH oxidase, QH301-705.5, T-Lymphocytes, Levilactobacillus brevis, Receptors, Antigen, T-Cell, Oxidative phosphorylation, Mice, SCID, armor CAR T-cells, Article, LDHA, chemistry.chemical_compound, Mice, Adenosine Triphosphate, In vivo, Mice, Inbred NOD, Multienzyme Complexes, Lactate dehydrogenase, medicine, Animals, Humans, NADH, NADPH Oxidoreductases, Biology (General), chemistry.chemical_classification, biology, Lactobacillus brevis, General Medicine, Hypoxia (medical), biology.organism_classification, NAD, Electron transport chain, Enzyme, Biochemistry, chemistry, Female, NAD+ kinase, medicine.symptom, Oxidation-Reduction

Abstract

The metabolic milieu of solid tumors provides a barrier to chimeric antigen receptor (CAR) T-cell therapies. Excessive lactate or hypoxia suppresses T-cell growth, through mechanisms including NADH buildup and the depletion of oxidized metabolites. NADH is converted into NAD+ by the enzyme Lactobacillus brevis NADH Oxidase (LbNOX), which mimics the oxidative function of the electron transport chain without generating ATP. Here we determine if LbNOX promotes human CAR T-cell metabolic activity and antitumor efficacy. CAR T-cells expressing LbNOX have enhanced oxygen as well as lactate consumption and increased pyruvate production. LbNOX renders CAR T-cells resilient to lactate dehydrogenase inhibition. But in vivo in a model of mesothelioma, CAR T-cell’s expressing LbNOX showed no increased antitumor efficacy over control CAR T-cells. We hypothesize that T cells in hostile environments face dual metabolic stressors of excessive NADH and insufficient ATP production. Accordingly, futile T-cell NADH oxidation by LbNOX is insufficient to promote tumor clearance.

Published

2021

25. PSMA-targeting TGFβ-insensitive armored CAR T cells in metastatic castration-resistant prostate cancer: a phase 1 trial

Author

Vivek, Narayan, Julie S, Barber-Rotenberg, In-Young, Jung, Simon F, Lacey, Andrew J, Rech, Megan M, Davis, Wei-Ting, Hwang, Priti, Lal, Erica L, Carpenter, Shannon L, Maude, Gabriela, Plesa, Neha, Vapiwala, Anne, Chew, Michael, Moniak, Ronnie A, Sebro, Michael D, Farwell, Amy, Marshall, Joan, Gilmore, Lester, Lledo, Karen, Dengel, Sarah E, Church, Tyler D, Hether, Jun, Xu, Mercy, Gohil, Thomas H, Buckingham, Stephanie S, Yee, Vanessa E, Gonzalez, Irina, Kulikovskaya, Fang, Chen, Lifeng, Tian, Kyle, Tien, Whitney, Gladney, Christopher L, Nobles, Hayley E, Raymond, Elizabeth O, Hexner, Donald L, Siegel, Frederic D, Bushman, Carl H, June, Joseph A, Fraietta, and Bruce L, Levine

Subjects

Male, Prostatic Neoplasms, Castration-Resistant, Receptors, Chimeric Antigen, Transforming Growth Factor beta, T-Lymphocytes, Tumor Microenvironment, Humans, Prostate-Specific Antigen, Immunotherapy, Adoptive

Abstract

Chimeric antigen receptor (CAR) T cells have demonstrated promising efficacy, particularly in hematologic malignancies. One challenge regarding CAR T cells in solid tumors is the immunosuppressive tumor microenvironment (TME), characterized by high levels of multiple inhibitory factors, including transforming growth factor (TGF)-β. We report results from an in-human phase 1 trial of castration-resistant, prostate cancer-directed CAR T cells armored with a dominant-negative TGF-β receptor (NCT03089203). Primary endpoints were safety and feasibility, while secondary objectives included assessment of CAR T cell distribution, bioactivity and disease response. All prespecified endpoints were met. Eighteen patients enrolled, and 13 subjects received therapy across four dose levels. Five of the 13 patients developed grade ≥2 cytokine release syndrome (CRS), including one patient who experienced a marked clonal CAR T cell expansion,98% reduction in prostate-specific antigen (PSA) and death following grade 4 CRS with concurrent sepsis. Acute increases in inflammatory cytokines correlated with manageable high-grade CRS events. Three additional patients achieved a PSA reduction of ≥30%, with CAR T cell failure accompanied by upregulation of multiple TME-localized inhibitory molecules following adoptive cell transfer. CAR T cell kinetics revealed expansion in blood and tumor trafficking. Thus, clinical application of TGF-β-resistant CAR T cells is feasible and generally safe. Future studies should use superior multipronged approaches against the TME to improve outcomes.

Published

2021

26. BET bromodomain protein inhibition reverses chimeric antigen receptor extinction and reinvigorates exhausted T cells in chronic lymphocytic leukemia

Author

Jamie E. DeNizio, Yan Wang, Simon F. Lacey, Vijay Bhoj, Tyler J. Reich, In-Young Jung, Regina M. Young, David L. Porter, John Scholler, Minnal Gupta, Julie K. Jadlowsky, Carl H. June, Todd Yoder, Christopher J. Ott, Megan M. Davis, Kathleen M. Haines, Irina Kulikovskaya, Golnaz Vahedi, Katherine T. Marcucci, Weimin Kong, Jun Xu, J. Joseph Melenhorst, John K. Everett, Joseph A. Fraietta, Marcela V. Maus, Erik F. Williams, Bruce L. Levine, Wenliang Wang, James E. Bradner, Rahul M. Kohli, Alexander Dimitri, Frederic D. Bushman, and Maria Fasolino

Subjects

T-Lymphocytes, T cell, Chronic lymphocytic leukemia, Antigens, CD19, Cell, chemical and pharmacologic phenomena, Immunotherapy, Adoptive, Oxidative Phosphorylation, Epigenesis, Genetic, Immune Tolerance, medicine, Humans, Gene silencing, Receptor, B cell, Receptors, Chimeric Antigen, Chemistry, Proteins, hemic and immune systems, Azepines, General Medicine, Triazoles, medicine.disease, Leukemia, Lymphocytic, Chronic, B-Cell, Chimeric antigen receptor, Bromodomain, medicine.anatomical_structure, Cancer research, Glycolysis, Immunologic Memory, Research Article

Abstract

Chimeric antigen receptor (CAR) T cells have induced remarkable antitumor responses in B cell malignancies. Some patients do not respond because of T cell deficiencies that hamper the expansion, persistence, and effector function of these cells. We used longitudinal immune profiling to identify phenotypic and pharmacodynamic changes in CD19-directed CAR T cells in patients with chronic lymphocytic leukemia (CLL). CAR expression maintenance was also investigated because this can affect response durability. CAR T cell failure was accompanied by preexisting T cell-intrinsic defects or dysfunction acquired after infusion. In a small subset of patients, CAR silencing was observed coincident with leukemia relapse. Using a small molecule inhibitor, we demonstrated that the bromodomain and extra-terminal (BET) family of chromatin adapters plays a role in downregulating CAR expression. BET protein blockade also ameliorated CAR T cell exhaustion as manifested by inhibitory receptor reduction, enhanced metabolic fitness, increased proliferative capacity, and enriched transcriptomic signatures of T cell reinvigoration. BET inhibition decreased levels of the TET2 methylcytosine dioxygenase, and forced expression of the TET2 catalytic domain eliminated the potency-enhancing effects of BET protein targeting in CAR T cells, providing a mechanism linking BET proteins and T cell dysfunction. Thus, modulating BET epigenetic readers may improve the efficacy of cell-based immunotherapies.

Published

2021

27. Bispecific Antibody Armed Metabolically Enhanced Headless CAR T Cells

Author

John Scholler, Dana L Schalk, Lawrence G. Lum, Archana Thakur, Edwin T. Bliemeister, Ewa Kubicka, and Carl H. June

Subjects

Cytotoxicity, Immunologic, 0301 basic medicine, Chemokine, Antigen Targeting, Receptor, ErbB-2, co-activated T cells, T-Lymphocytes, T cell, pancreatic cancer, Immunology, Breast Neoplasms, Immunotherapy, Adoptive, 03 medical and health sciences, breast cancer, Th1 cytokines, 0302 clinical medicine, Pancreatic cancer, Antibodies, Bispecific, Tumor Microenvironment, medicine, Humans, Immunology and Allergy, Secretion, Cytotoxicity, Original Research, activated T cells, Receptors, Chimeric Antigen, biology, Chemistry, headless CAR T cells, RC581-607, medicine.disease, Coculture Techniques, In vitro, ErbB Receptors, bispecific antibody, Phenotype, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, MCF-7 Cells, Cancer research, biology.protein, Cytokines, Tumor Hypoxia, Female, Cytokine secretion, Immunologic diseases. Allergy

Abstract

Adoptive T cell therapies for solid tumors is challenging. We generated metabolically enhanced co-activated-T cells by transducing intracellular co-stimulatory (41BB, ICOS or ICOS-27) and CD3ζ T cell receptor signaling domains followed by arming with bispecific antibodies (BiAbs) to produce armed “Headless CAR T cells” (hCART). Various hCART armed with BiAb directed at CD3ϵ and various tumor associated antigens were tested for: 1) specific cytotoxicity against solid tumors targets; 2) repeated and dual sequential cytotoxicity; 3) survival and cytotoxicity under in vitro hypoxic condition; and 4) cytokine secretion. The 41BBζ transduced hCART (hCART41BBζ) armed with HER2 BiAb (HER2 hCART41BBζ) or armed with EGFR BiAb (EGFR hCART41BBζ) killed multiple tumor lines significantly better than control T cells and secreted Th1 cytokines/chemokines upon tumor engagement at effector to target ratio (E:T) of 2:1 or 1:1. HER2 hCART serially killed tumor targets up to 14 days. Sequential targeting of EGFR or HER2 positive tumors with HER2 hCART41BBζ followed by EGFR hCART41BBζ showed significantly increased cytotoxicity compared single antigen targeting and continue to kill under in vitro hypoxic conditions. In summary, metabolically enhanced headless CAR T cells are effective serial killers of tumor targets, secrete cytokines and chemokines, and continue to kill under in vitro hypoxic condition.

Published

2021

28. Humanized CD19-Targeted Chimeric Antigen Receptor (CAR) T Cells in CAR-Naive and CAR-Exposed Children and Young Adults With Relapsed or Refractory Acute Lymphoblastic Leukemia

Author

Pamela A Shaw, Don L. Siegel, Andrew D. Fesnak, Christina Fasano, Kelly D. Getz, Richard Aplenc, Jennifer Brogdon, Amanda M. DiNofia, Allison Barz Leahy, Yimei Li, Megan M. Davis, Diane Baniewicz, Hongyan Liu, Lisa Wray, Carl H. June, David T. Teachey, Elizabeth O. Hexner, Stephan A. Grupp, Edward Pequignot, Bruce L. Levine, Colleen Callahan, Simon F. Lacey, Shannon L. Maude, Gerald Wertheim, Anne Chew, Chelsie Bartoszek, Regina M. Myers, Susan R. Rheingold, and David M. Barrett

Subjects

Adult, Male, Cancer Research, Adolescent, Lymphoblastic Leukemia, Antigens, CD19, Receptors, Antigen, T-Cell, Pilot Projects, CD19, Young Adult, Refractory, Medicine, Humans, Young adult, Child, Receptors, Chimeric Antigen, biology, business.industry, ORIGINAL REPORTS, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Chimeric antigen receptor, Oncology, Child, Preschool, Immunology, biology.protein, Female, Car t cells, business

Abstract

PURPOSE CD19-targeted chimeric antigen receptor (CAR)–modified T cells demonstrate unprecedented responses in B-cell acute lymphoblastic leukemia (B-ALL); however, relapse remains a substantial challenge. Short CAR T-cell persistence contributes to this risk; therefore, strategies to improve persistence are needed. METHODS We conducted a pilot clinical trial of a humanized CD19 CAR T-cell product (huCART19) in children and young adults with relapsed or refractory B-ALL (n = 72) or B-lymphoblastic lymphoma (n = 2), treated in two cohorts: with (retreatment, n = 33) or without (CAR-naive, n = 41) prior CAR exposure. Patients were monitored for toxicity, response, and persistence of huCART19. RESULTS Seventy-four patients 1-29 years of age received huCART19. Cytokine release syndrome developed in 62 (84%) patients and was grade 4 in five (6.8%). Neurologic toxicities were reported in 29 (39%), three (4%) grade 3 or 4, and fully resolved in all cases. The overall response rate at 1 month after infusion was 98% (100% in B-ALL) in the CAR-naive cohort and 64% in the retreatment cohort. At 6 months, the probability of losing huCART19 persistence was 27% (95% CI, 14 to 41) for CAR-naive and 48% (95% CI, 30 to 64) for retreatment patients, whereas the incidence of B-cell recovery was 15% (95% CI, 6 to 28) and 58% (95% CI, 33 to 77), respectively. Relapse-free survival at 12 and 24 months, respectively, was 84% (95% CI, 72 to 97) and 74% (95% CI, 60 to 90) in CAR-naive and 74% (95% CI, 56 to 97) and 58% (95% CI, 37 to 90) in retreatment cohorts. CONCLUSION HuCART19 achieved durable remissions with long-term persistence in children and young adults with relapsed or refractory B-ALL, including after failure of prior CAR T-cell therapy.

Published

2021

29. Phase I Study of Lentiviral-Transduced Chimeric Antigen Receptor-Modified T Cells Recognizing Mesothelin in Advanced Solid Cancers

Author

Lifeng Tian, Andrew R. Haas, Janos L. Tanyi, Whitney L. Gladney, Drew A. Torigian, Steven M. Albelda, Edmund K. Moon, Mark H. O'Hara, Bruce L. Levine, Gabriela Plesa, J. Joseph Melenhorst, Caitlin S. Farabaugh, Anne Marie Nelson, Maureen McGarvey, Carl H. June, Michael C. Soulen, Gregory L. Beatty, and Simon F. Lacey

Subjects

Male, T-Lymphocytes, medicine.medical_treatment, Cell, Immunotherapy, Adoptive, 0302 clinical medicine, Neoplasms, Drug Discovery, polycyclic compounds, 0303 health sciences, Receptors, Chimeric Antigen, biology, virus diseases, Middle Aged, medicine.anatomical_structure, Mesothelin, 030220 oncology & carcinogenesis, Molecular Medicine, Female, Original Article, Antibody, medicine.drug, Cyclophosphamide, Genetic Vectors, Receptors, Antigen, T-Cell, GPI-Linked Proteins, 03 medical and health sciences, Genetics, medicine, Humans, Molecular Biology, Aged, Neoplasm Staging, 030304 developmental biology, Pharmacology, business.industry, Lentivirus, fungi, Cancer, Genetic Therapy, Immunotherapy, medicine.disease, Chimeric antigen receptor, carbohydrates (lipids), biology.protein, Cancer research, Tomography, X-Ray Computed, Ovarian cancer, business, Biomarkers

Abstract

This phase I study investigated the safety and activity of lentiviral-transduced chimeric antigen receptor (CAR)-modified autologous T cells redirected against mesothelin (CART-meso) in patients with malignant pleural mesothelioma, ovarian carcinoma, and pancreatic ductal adenocarcinoma. Fifteen patients with chemotherapy-refractory cancer (n = 5 per indication) were treated with a single CART-meso cell infusion. CART-meso cells were engineered by lentiviral transduction with a construct composed of the anti-mesothelin single-chain variable fragment derived from the mouse monoclonal antibody SS1 fused to intracellular signaling domains of 4-1BB and CD3zeta. Patients received 1–3 × 10(7) or 1–3 × 10(8) CART-meso cells/m(2) with or without 1.5 g/m(2) cyclophosphamide. Lentiviral-transduced CART-meso cells were well tolerated; one dose-limiting toxicity (grade 4, sepsis) occurred at 1–3 × 10(7)/m(2) CART-meso without cyclophosphamide. The best overall response was stable disease (11/15 patients). CART-meso cells expanded in the blood and reached peak levels by days 6–14 but persisted transiently. Cyclophosphamide pre-treatment enhanced CART-meso expansion but did not improve persistence beyond 28 days. CART-meso DNA was detected in 7/10 tumor biopsies. Human anti-chimeric antibodies (HACA) were detected in the blood of 8/14 patients. CART-meso cells were well tolerated and expanded in the blood of all patients but showed limited clinical activity. Studies evaluating a fully human anti-mesothelin CAR are ongoing.

Published

2019

30. T-cell phenotypes associated with effective CAR T-cell therapy in postinduction vs relapsed multiple myeloma

Author

Joseph A. Fraietta, Edward A. Stadtmauer, Aaron P. Rapoport, Bruce L. Levine, Wei-Ting Hwang, Dan T. Vogl, Adam D. Cohen, Megan M. Davis, Carl H. June, Adam Waxman, Don L. Siegel, Alfred L. Garfall, Michael C. Milone, Ehren K. Dancy, and J. Joseph Melenhorst

Subjects

Adult, Oncology, medicine.medical_specialty, T cell, Refractory, Internal medicine, medicine, Humans, Multiple myeloma, Aged, Receptors, Chimeric Antigen, business.industry, Refractory Disease, Hematology, Middle Aged, medicine.disease, Stimulus Report, Phenotype, medicine.anatomical_structure, CAR T-cell therapy, Chimeric Antigen Receptor T-Cell Therapy, Car t cells, Multiple Myeloma, business, human activities

Abstract

Key points T cells from patients early in myeloma therapy exhibit better fitness for CAR T manufacturing than those from relapsed/refractory patients. CAR T cells may be more effective if manufactured from patients before onset of relapsed/refractory disease.

Published

2019

31. Emerging Cellular Therapies for Cancer

Author

Sonia Guedan, Carl H. June, and Marco Ruella

Subjects

Adoptive cell transfer, T-Lymphocytes, T cell, Immunology, Receptors, Antigen, T-Cell, Biology, medicine.disease_cause, Immunotherapy, Adoptive, Article, Autoimmunity, Synthetic biology, Antineoplastic Agents, Immunological, Immune system, Neoplasms, medicine, Animals, Humans, Immunology and Allergy, United States Food and Drug Administration, Cancer, medicine.disease, United States, Chimeric antigen receptor, Leukemia, medicine.anatomical_structure, Cancer research, Genetic Engineering

Abstract

Genetically engineered T cells are powerful new medicines, offering hope for curative responses in patients with cancer. Chimeric antigen receptor (CAR) T cells were recently approved by the US Food and Drug Administration and are poised to enter the practice of medicine for leukemia and lymphoma, demonstrating that engineered immune cells can serve as a powerful new class of cancer therapeutics. The emergence of synthetic biology approaches for cellular engineering provides a broadly expanded set of tools for programming immune cells for enhanced function. Advances in T cell engineering, genetic editing, the selection of optimal lymphocytes, and cell manufacturing have the potential to broaden T cell–based therapies and foster new applications beyond oncology, in infectious diseases, organ transplantation, and autoimmunity.

Published

2019

32. Immunotherapy for Glioblastoma: Adoptive T-cell Strategies

Author

Bryan D. Choi, Marcela V. Maus, Carl H. June, and John H. Sampson

Subjects

0301 basic medicine, Cancer Research, Adoptive cell transfer, T-Lymphocytes, medicine.medical_treatment, T cell, Cell- and Tissue-Based Therapy, Receptors, Antigen, T-Cell, Disease, Immunotherapy, Adoptive, Article, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antigen, medicine, Animals, Humans, Receptors, Chimeric Antigen, Brain Neoplasms, business.industry, Genetic Therapy, Immunotherapy, Combined Modality Therapy, Chimeric antigen receptor, Clinical trial, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Cancer research, Disease Susceptibility, Glioblastoma, business

Abstract

Glioblastoma (GBM) is a devastating disease with an extremely poor prognosis. Immunotherapy via adoptive cell transfer (ACT), especially with T cells engineered to express chimeric antigen receptors (CAR), represents a particularly promising approach. Despite the recent success of CAR T cells for blood cancers, the question remains whether this powerful anticancer therapy will ultimately work for brain tumors, and whether the primary immunologic challenges in this disease, which include antigenic heterogeneity, immune suppression, and T-cell exhaustion, can be adequately addressed. Here, we contextualize these concepts by reviewing recent developments in ACT for GBM, with a special focus on pioneering clinical trials of CAR T-cell therapy.

Published

2019

33. Tisagenlecleucel Model‐Based Cellular Kinetic Analysis of Chimeric Antigen Receptor–T Cells

Author

Karen Thudium Mueller, Pai Hsi Huang, Rakesh Awasthi, Michael Boyer, Mimi Leung, Lori Tomassian, Sweta Shah, Theodore W. Laetsch, Carl H. June, Andrew M. Stein, Michael A. Pulsipher, Patricia A. Wood, Bruce L. Levine, John E. Levine, Keith J. August, and Stephan A. Grupp

Subjects

Adult, Male, Adolescent, Receptors, Antigen, T-Cell, Antibodies, Monoclonal, Humanized, Immunotherapy, Adoptive, Article, CD19, Cell therapy, Young Adult, chemistry.chemical_compound, Clinical Trials, Phase II as Topic, Tocilizumab, Antigen, Refractory, medicine, Humans, Doubling time, Pharmacology (medical), Child, biology, business.industry, Research, lcsh:RM1-950, Articles, Models, Theoretical, Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, Chimeric antigen receptor, Cytokine release syndrome, lcsh:Therapeutics. Pharmacology, chemistry, Child, Preschool, Modeling and Simulation, Cancer research, biology.protein, Female, Lymphoma, Large B-Cell, Diffuse, business, Half-Life

Abstract

Tisagenlecleucel is a chimeric antigen receptor–T cell therapy that facilitates the killing of CD19+ B cells. A model was developed for the kinetics of tisagenlecleucel and the impact of therapies for treating cytokine release syndrome (tocilizumab and corticosteroids) on expansion. Data from two phase II studies in pediatric and young adult relapsed/refractory B cell acute lymphoblastic leukemia were pooled to evaluate this model and evaluate extrinsic and intrinsic factors that may impact the extent of tisagenlecleucel expansion. The doubling time, initial decline half‐life, and terminal half‐life for tisagenlecleucel were 0.78, 4.3, and 220 days, respectively. No impact of tocilizumab or corticosteroids on the expansion rate was observed. This work represents the first mixed‐effect model‐based analysis of chimeric antigen receptor–T cell therapy and may be clinically impactful as future studies examine prophylactic interventions in patients at risk of higher grade cytokine release syndrome and the effects of these interventions on chimeric antigen receptor–T cell expansion.

Published

2019

34. Clinical Pharmacology of Tisagenlecleucel in B-cell Acute Lymphoblastic Leukemia

Author

Michael A. Pulsipher, Carl H. June, Jason Hamilton, Shannon L. Maude, Michael Boyer, Rakesh Awasthi, Bruce L. Levine, Keith J. August, Lori Tomassian, Mimi Leung, Theodore W. Laetsch, Andrew M. Stein, Edward Waldron, Sweta Shah, Tetiana Taran, Denise Sickert, Karen Thudium Mueller, Abhijit Chakraborty, Stephan A. Grupp, Patricia A. Wood, and John E. Levine

Subjects

Adult, Male, 0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Adolescent, medicine.medical_treatment, Antigens, CD19, Cell- and Tissue-Based Therapy, Receptors, Antigen, T-Cell, Cmax, Immunotherapy, Adoptive, Article, law.invention, Mice, Young Adult, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Tocilizumab, Antigen, law, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma, Internal medicine, medicine, Animals, Humans, Lymphocyte Count, Transgenes, Child, Clinical pharmacology, business.industry, Immunogenicity, Genetic Therapy, Immunotherapy, Prognosis, medicine.disease, Chimeric antigen receptor, Immunity, Humoral, Cytokine release syndrome, Treatment Outcome, 030104 developmental biology, chemistry, Child, Preschool, 030220 oncology & carcinogenesis, Female, business

Abstract

Purpose: Tisagenlecleucel is an anti-CD19 chimeric antigen receptor (CAR19) T-cell therapy approved for the treatment of children and young adults with relapsed/refractory (r/r) B-cell acute lymphoblastic leukemia (B-ALL). Patients and Methods: We evaluated the cellular kinetics of tisagenlecleucel, the effect of patient factors, humoral immunogenicity, and manufacturing attributes on its kinetics, and exposure-response analysis for efficacy, safety and pharmacodynamic endpoints in 79 patients across two studies in pediatric B-ALL (ELIANA and ENSIGN). Results: Using quantitative polymerase chain reaction to quantify levels of tisagenlecleucel transgene, responders (N = 62) had ≈2-fold higher tisagenlecleucel expansion in peripheral blood than nonresponders (N = 8; 74% and 104% higher geometric mean Cmax and AUC0-28d, respectively) with persistence measurable beyond 2 years in responding patients. Cmax increased with occurrence and severity of cytokine release syndrome (CRS). Tisagenlecleucel continued to expand and persist following tocilizumab, used to manage CRS. Patients with B-cell recovery within 6 months had earlier loss of the transgene compared with patients with sustained clinical response. Clinical responses were seen across the entire dose range evaluated (patients ≤50 kg: 0.2 to 5.0 × 106/kg; patients >50 kg: 0.1 to 2.5 × 108 CAR-positive viable T cells) with no relationship between dose and safety. Neither preexisting nor treatment-induced antimurine CAR19 antibodies affected the persistence or clinical response. Conclusions: Response to tisagenlecleucel was associated with increased expansion across a wide dose range. These results highlight the importance of cellular kinetics in understanding determinants of response to chimeric antigen receptor T-cell therapy.

Published

2018

35. Chimeric antigen receptor (CAR) T therapies for the treatment of hematologic malignancies: clinical perspective and significance

Author

Crystal L. Mackall, Renier J. Brentjens, Madhav V. Dhodapkar, David G. Maloney, Stephan A. Grupp, Michael R. Bishop, Marcela V. Maus, Michael Boyiadzis, Carl H. June, Sattva S. Neelapu, David L. Porter, and James N. Kochenderfer

Subjects

0301 basic medicine, Cancer Research, Lymphoma, T-Lymphocytes, T cell, Immunology, Receptors, Antigen, T-Cell, Review, Bioinformatics, Immunotherapy, Adoptive, lcsh:RC254-282, Food and drug administration, 03 medical and health sciences, 0302 clinical medicine, Antigens, Neoplasm, Animals, Humans, Immunology and Allergy, Medicine, Chimeric antigen receptor, Tisagenlecleucel, Pharmacology, Clinical Trials as Topic, Receptors, Chimeric Antigen, Leukemia, business.industry, Genetically engineered, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Treatment Outcome, 030104 developmental biology, medicine.anatomical_structure, Oncology, Hematologic Neoplasms, 030220 oncology & carcinogenesis, New disease, Molecular Medicine, Axicabtagene ciloleucel, Car t cells, Genetic Engineering, business

Abstract

Chimeric Antigen Receptor (CAR) T cell therapies – adoptive T cell therapies that have been genetically engineered for a new antigen-specificity - have displayed significant success in treating patients with hematologic malignancies, leading to three recent US Food and Drug Administration approvals. Based on the promise generated from these successes, the field is rapidly evolving to include new disease indications and CAR designs, while simultaneously reviewing and optimizing toxicity and management protocols. As such, this review provides expert perspective on the significance and clinical considerations of CAR T cell therapies in order to provide timely information to clinicians about this revolutionary new therapeutic class.

Published

2018

36. Human epigenetic and transcriptional T cell differentiation atlas for identifying functional T cell-specific enhancers

Author

Josephine R. Giles, Sasikanth Manne, Elizabeth Freilich, Derek A. Oldridge, Amy E. Baxter, Sangeeth George, Zeyu Chen, Hua Huang, Lakshmi Chilukuri, Mary Carberry, Lydia Giles, Nan-Ping P. Weng, Regina M. Young, Carl H. June, Lynn M. Schuchter, Ravi K. Amaravadi, Xiaowei Xu, Giorgos C. Karakousis, Tara C. Mitchell, Alexander C. Huang, Junwei Shi, and E. John Wherry

Subjects

Epigenomics, Infectious Diseases, Immunology, Immunology and Allergy, Humans, Cell Differentiation, CD8-Positive T-Lymphocytes, Lymphocyte Activation, Chromatin, Article, Epigenesis, Genetic

Abstract

The clinical benefit of T cell immunotherapies remains limited by incomplete understanding of T cell differentiation and dysfunction. We generated an epigenetic and transcriptional atlas of T cell differentiation from healthy humans that included exhausted CD8 T cells and applied this resource in three ways. First, we identified modules of gene expression and chromatin accessibility, revealing molecular coordination of differentiation after activation and between central memory and effector memory. Second, we applied this healthy molecular framework to three settings - a neoadjuvant anti-PD1 melanoma trial, a basal cell carcinoma scATAC-seq data set, and autoimmune disease-associated SNPs - yielding insights into disease-specific biology. Third, we predicted genome-wide cis-regulatory elements and validated this approach for key effector genes using CRISPR interference, providing functional annotation and demonstrating the ability to identify targets for non-coding cellular engineering. These studies define epigenetic and transcriptional regulation of human T cells and illustrate the utility of interrogating disease in the context of a healthy T cell atlas.

Published

2021

37. Decade-long leukaemia remissions with persistence of CD4

Author

J Joseph, Melenhorst, Gregory M, Chen, Meng, Wang, David L, Porter, Changya, Chen, McKensie A, Collins, Peng, Gao, Shovik, Bandyopadhyay, Hongxing, Sun, Ziran, Zhao, Stefan, Lundh, Iulian, Pruteanu-Malinici, Christopher L, Nobles, Sayantan, Maji, Noelle V, Frey, Saar I, Gill, Alison W, Loren, Lifeng, Tian, Irina, Kulikovskaya, Minnal, Gupta, David E, Ambrose, Megan M, Davis, Joseph A, Fraietta, Jennifer L, Brogdon, Regina M, Young, Anne, Chew, Bruce L, Levine, Donald L, Siegel, Cécile, Alanio, E John, Wherry, Frederic D, Bushman, Simon F, Lacey, Kai, Tan, and Carl H, June

Subjects

CD4-Positive T-Lymphocytes, Leukemia, Receptors, Chimeric Antigen, Time Factors, Antigens, CD19, Humans, Cell Separation, CD8-Positive T-Lymphocytes, Immunotherapy, Adoptive

Abstract

The adoptive transfer of T lymphocytes reprogrammed to target tumour cells has demonstrated potential for treatment of various cancers

Published

2021

38. Single-cell multiomics dissection of basal and antigen-specific activation states of CD19-targeted CAR T cells

Author

Regina M. Myers, Carl H. June, David M. Barrett, Stephan A. Grupp, Rong Fan, J. Joseph Melenhorst, Pablo G. Camara, Dong-Joo Kim, Marcela V. Maus, Stefan Lundh, Steven Woodhouse, and Zhiliang Bai

Subjects

0301 basic medicine, Cytotoxicity, Immunologic, Cancer Research, medicine.medical_treatment, T-Lymphocytes, Cell, receptors, Lymphocyte Activation, Immunotherapy, Adoptive, Mice, 0302 clinical medicine, Immunotherapy Biomarkers, Immunology and Allergy, Cytotoxic T cell, RNA-Seq, RC254-282, Receptors, Chimeric Antigen, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Leukemia, medicine.anatomical_structure, Phenotype, Oncology, 030220 oncology & carcinogenesis, translational medical research, Molecular Medicine, immunotherapy, Single-Cell Analysis, Immunology, Antigens, CD19, Biology, CD19, 03 medical and health sciences, Downregulation and upregulation, Cell Line, Tumor, medicine, Animals, Humans, Pharmacology, Gene Expression Profiling, Immunotherapy, medicine.disease, Chimeric antigen receptor, Coculture Techniques, 030104 developmental biology, MRNA Sequencing, chimeric antigen, Case-Control Studies, Cancer research, biology.protein, NIH 3T3 Cells, Transcriptome

Abstract

BackgroundAutologous T cells engineered to express a chimeric antigen receptor (CAR) specific for CD19 molecule have transformed the therapeutic landscape in patients with highly refractory leukemia and lymphoma, and the use of donor-generated allogeneic CAR T is paving the way for further breakthroughs in the treatment of cancer. However, it remains unknown how the intrinsic heterogeneities of these engineered cells mediate therapeutic efficacy and whether allogeneic products match the effectiveness of autologous therapies.MethodsUsing single-cell mRNA sequencing in conjunction with CITE-seq, we performed multiomics characterization of CAR T cells generated from healthy donor and patients with acute lymphoblastic leukemia. CAR T cells used in this study were manufactured at the University of Pennsylvania through lentiviral transduction with a CD19-4-1BB-CD3ζ construct. Besides the baseline condition, we engineered NIH-3T3 cells with human CD19 or mesothelin expression to conduct ex vivo antigen-specific or non-antigen stimulation of CAR T cells through 6-hour coculture at a 1:1 ratio.ResultsWe delineated the global cellular and molecular CAR T landscape and identified that transcriptional CAR tonic signaling was regulated by a mixture of early activation, exhaustion signatures, and cytotoxic activities. On CD19 stimulation, we illuminated the disparities of CAR T cells derived from different origins and found that donor CAR T had more pronounced activation level in correlation with the upregulation of major histocompatibility complex class II genes compared with patient CAR T cells. This finding was independently validated in additional datasets from literature. Furthermore, GM-CSF(CSF2) expression was found to be associated with functional gene productions, but it induced little impact on the CAR T activation.ConclusionsThrough integrated multiomics profiling and unbiased canonical pathway analyses, our results unveil heterogeneities in the transcriptional, phenotypic, functional, and metabolic profiles of donor and patient CAR T cells, providing mechanistic basis for ameliorating clinical outcomes and developing next-generation ‘off- the-shelf’ allogeneic products.

Published

2021

39. Gut microbiome correlates of response and toxicity following anti-CD19 CAR T cell therapy

Author

Melody Smith, Anqi Dai, Guido Ghilardi, Kimberly V. Amelsberg, Sean M. Devlin, Raymone Pajarillo, John B. Slingerland, Silvia Beghi, Pamela S. Herrera, Paul Giardina, Annelie Clurman, Emmanuel Dwomoh, Gabriel Armijo, Antonio L. C. Gomes, Eric R. Littmann, Jonas Schluter, Emily Fontana, Ying Taur, Jae H. Park, Maria Lia Palomba, Elizabeth Halton, Josel Ruiz, Tania Jain, Martina Pennisi, Aishat Olaide Afuye, Miguel-Angel Perales, Craig W. Freyer, Alfred Garfall, Shannon Gier, Sunita Nasta, Daniel Landsburg, James Gerson, Jakub Svoboda, Justin Cross, Elise A. Chong, Sergio Giralt, Saar I. Gill, Isabelle Riviere, David L. Porter, Stephen J. Schuster, Michel Sadelain, Noelle Frey, Renier J. Brentjens, Carl H. June, Eric G. Pamer, Jonathan U. Peled, Andrea Facciabene, Marcel R. M. van den Brink, and Marco Ruella

Subjects

Receptors, Chimeric Antigen, Antigens, CD19, Humans, Neurotoxicity Syndromes, General Medicine, Prospective Studies, Immunotherapy, Adoptive, Article, General Biochemistry, Genetics and Molecular Biology, Gastrointestinal Microbiome, Retrospective Studies

Abstract

Anti-CD19 chimeric antigen receptor (CAR) T cell therapy has led to unprecedented responses in patients with high-risk hematologic malignancies. However, up to 60% of patients still experience disease relapse and up to 80% of patients experience CAR-mediated toxicities, such as cytokine release syndrome or immune effector cell-associated neurotoxicity syndrome. We investigated the role of the intestinal microbiome on these outcomes in a multicenter study of patients with B cell lymphoma and leukemia. We found in a retrospective cohort (n = 228) that exposure to antibiotics, in particular piperacillin/tazobactam, meropenem and imipenem/cilastatin (P-I-M), in the 4 weeks before therapy was associated with worse survival and increased neurotoxicity. In stool samples from a prospective cohort of CAR T cell recipients (n = 48), the fecal microbiome was altered at baseline compared to healthy controls. Stool sample profiling by 16S ribosomal RNA and metagenomic shotgun sequencing revealed that clinical outcomes were associated with differences in specific bacterial taxa and metabolic pathways. Through both untargeted and hypothesis-driven analysis of 16S sequencing data, we identified species within the class Clostridia that were associated with day 100 complete response. We concluded that changes in the intestinal microbiome are associated with clinical outcomes after anti-CD19 CAR T cell therapy in patients with B cell malignancies.

Published

2021

40. Production of Human CRISPR-Engineered CAR-T Cells

Author

Nils Wellhausen, Sangya Agarwal, Bruce L. Levine, and Carl H. June

Subjects

General Immunology and Microbiology, Cas9, medicine.medical_treatment, Genetic enhancement, General Chemical Engineering, General Neuroscience, Immunotherapy, Biology, Immunotherapy, Adoptive, Chimeric antigen receptor, CD19, General Biochemistry, Genetics and Molecular Biology, Viral vector, Cell biology, Genome editing, Neoplasms, medicine, biology.protein, CRISPR, Humans, Clustered Regularly Interspaced Short Palindromic Repeats

Abstract

Adoptive cell therapies using chimeric antigen receptor T cells (CAR-T cells) have demonstrated remarkable clinical efficacy in patients with hematological malignancies and are currently being investigated for various solid tumors. CAR-T cells are generated by removing T cells from a patient's blood and engineering them to express a synthetic immune receptor that redirects the T-cells to recognize and eliminate target tumor cells. Gene editing of CAR-T cells has the potential to improve safety of current CAR-T cell therapies and further increase the efficacy of CAR-T cells. Here, we describe methods for the activation, expansion, and characterization of human CRISPR-engineered CD19 directed CAR-T cells. This comprises transduction of the CAR lentiviral vector and use of single guide RNA (sgRNA) and Cas9 endonuclease to target genes of interest in T cells. The methods described in this protocol can be universally applied to other CAR constructs and target genes beyond the ones used for this study. Furthermore, this protocol discusses strategies for gRNA design, lead gRNA selection and target gene knockout validation to reproducibly achieve high-efficiency, multiplex CRISPR-Cas9 engineering of clinical grade human T cells.

Published

2021

41. CD19-targeted chimeric antigen receptor T-cell therapy for CNS relapsed or refractory acute lymphocytic leukaemia: a post-hoc analysis of pooled data from five clinical trials

Author

Regina M. Myers, Yimei Li, Amanda M. DiNofia, Susan R. Rheingold, Colleen Callahan, Diane Baniewicz, Haley Newman, Hongyan Liu, Richard Aplenc, Joseph G Dolan, Lisa Wray, Stephan A. Grupp, Carl H. June, Shannon L. Maude, Kaitlin Devine, and Allison Barz Leahy

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, Antigens, CD19, Gastroenterology, Immunotherapy, Adoptive, Article, Central Nervous System Neoplasms, Young Adult, Refractory, Recurrence, Internal medicine, Post-hoc analysis, medicine, Humans, Young adult, Receptors, Chimeric Antigen, business.industry, Incidence (epidemiology), Infant, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, Clinical trial, Cytokine release syndrome, medicine.anatomical_structure, Child, Preschool, Chimeric Antigen Receptor T-Cell Therapy, Female, Bone marrow, business

Abstract

Summary Background CNS relapse of acute lymphocytic leukaemia is difficult to treat. Durable remissions of relapsed or refractory B-cell acute lymphocytic leukaemia have been observed following treatment with CD19-directed chimeric antigen receptor (CAR) T cells; however, most trials have excluded patients with active CNS disease. We aimed to assess the safety and activity of CAR T-cell therapy in patients with a history of CNS relapsed or refractory B-cell acute lymphocytic leukaemia. Methods In this post-hoc analysis, we included 195 patients (aged 1–29 years; 110 [56%] male and 85 [44%] female) with relapsed or refractory CD19-positive acute lymphocytic leukaemia or lymphocytic lymphoma from five clinical trials (Pedi CART19, 13BT022, ENSIGN, ELIANA, and 16CT022) done at the Children's Hospital of Philadelphia (Philadelphia, PA, USA), in which participants received CD19-directed CAR T-cell therapy between April 17, 2012, and April 16, 2019. The trials required control of CNS disease at enrolment and infusion and excluded treatment in the setting of acute neurological toxic effects (>grade 1 in severity) or parenchymal lesions deemed to increase the risk of neurotoxicity. 154 patients from Pedi CART19, ELIANA, ENSIGN, and 16CT022 received tisagenlecleucel and 41 patients from the 13BT022 trial received the humanised CD19-directed CAR, huCART19. We categorised patients into two strata on the basis of CNS status at relapse or within the 12 months preceding CAR T-cell infusion—either CNS-positive or CNS-negative disease. Patients with CNS-positive disease were further divided on the basis of morphological bone marrow involvement—either combined bone marrow and CNS involvement, or isolated CNS involvement. Endpoints were the proportion of patients with complete response at 28 days after infusion, Kaplan-Meier analysis of relapse-free survival and overall survival, and the incidence of cytokine release syndrome and neurotoxicity. Findings Of all 195 patients, 66 (34%) were categorised as having CNS-positive disease and 129 (66%) as having CNS-negative disease, and 43 (22%) were categorised as having isolated CNS involvement. The median length of follow-up was 39 months (IQR 25–49) in the CNS-positive stratum and 36 months (18–49) in the CNS-negative stratum. The proportion of patients in the CNS-positive stratum with a complete response at 28 days after infusion was similar to that in the CNS-negative stratum (64 [97%] of 66 vs 121 [94%] of 129; p=0·74), with no significant difference in relapse-free survival (60% [95% CI 49–74] vs 60% [51–71]; p=0·50) or overall survival (83% [75–93] vs 71% [64–79]; p=0·39) at 2 years between the two groups. Overall survival at 2 years was significantly higher in patients with isolated CNS involvement compared with those with bone marrow involvement (91% [82–100] vs 71% [64–78]; p=0·046). The incidence and severity of neurotoxicity (any grade, 53 [41%] vs 38 [58%]; grade 1, 24 [19%] vs 20 [30%]; grade 2, 14 [11%] vs 10 [15%]; grade 3, 12 [9%] vs 6 [9%], and grade 4, 3 [2%] vs 2 [3%]; p=0·20) and cytokine release syndrome (any grade, 110 [85%] vs 53 [80%]; grade 1, 12 [9%] vs 2 [3%]; grade 2, 61 [47%] vs 38 [58%]; grade 3, 18 [14%] vs 7 [11%] and grade 4, 19 [15%] vs 6 [9%]; p=0·26) did not differ between the CNS-negative and the CNS-positive disease strata. Interpretation Tisagenlecleucel and huCART19 are active at clearing CNS disease and maintaining durable remissions in children and young adults with CNS relapsed or refractory B-cell acute lymphocytic leukaemia or lymphocytic lymphoma, without increasing the risk of severe neurotoxicity; although care should be taken in the timing of therapy and disease control to mitigate this risk. These preliminary findings support the use of these CAR T-cell therapies for patients with CNS relapsed or refractory B-cell acute lymphocytic leukaemia. Funding Children's Hospital of Philadelphia Frontier Program.

Published

2021

42. Five-Year Outcomes for Refractory B-Cell Lymphomas with CAR T-Cell Therapy

Author

Elise A, Chong, Marco, Ruella, Stephen J, Schuster, and Carl H, June

Subjects

Oncology, medicine.medical_specialty, medicine.medical_treatment, Antigens, CD19, Follicular lymphoma, 030204 cardiovascular system & hematology, Immunotherapy, Adoptive, CD19, 03 medical and health sciences, 0302 clinical medicine, Antigen, Refractory, immune system diseases, hemic and lymphatic diseases, Internal medicine, medicine, Humans, 030212 general & internal medicine, Progression-free survival, B cell, Receptors, Chimeric Antigen, biology, business.industry, General Medicine, Immunotherapy, medicine.disease, Progression-Free Survival, Lymphoma, medicine.anatomical_structure, Treatment Outcome, biology.protein, Lymphoma, Large B-Cell, Diffuse, business, Follow-Up Studies

Abstract

Long-Term Follow-up of CAR T-Cell–Treated Lymphoma Progression-free survival at 5 years was 31% in patients with diffuse large B-cell lymphoma and 43% in patients with follicular lymphoma. A total ...

Published

2021

43. The Safety of Bridging Radiation with Anti-BCMA CAR T-Cell Therapy for Multiple Myeloma

Author

Edward A. Stadtmauer, S.H. Manjunath, John P. Plastaras, Adam D. Cohen, Bruce L. Levine, Alfred L. Garfall, Michael C. Milone, Carl H. June, Ima Paydar, Simon F. Lacey, Joshua Jones, W. Tristram Arscott, Amit Maity, R.J.L. Maxwell, J. Joseph Melenhorst, and Megan M. Davis

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Future studies, Cyclophosphamide, Immunotherapy, Adoptive, Article, Antigen, immune system diseases, Internal medicine, medicine, Humans, B-Cell Maturation Antigen, Multiple myeloma, Retrospective Studies, Receptors, Chimeric Antigen, business.industry, Refractory Multiple Myeloma, medicine.disease, Chimeric antigen receptor, Toxicity, CAR T-cell therapy, business, Multiple Myeloma, medicine.drug

Abstract

Purpose: B-cell maturation antigen (BCMA)-targeted chimeric antigen receptor (CAR) T cells (CART-BCMA) are a promising treatment for relapsed/refractory multiple myeloma (r/rMM). We evaluated the safety and feasibility of bridging radiation (RT) in subjects treated on a phase I trial of CART-BCMA. Experimental Design: Twenty-five r/rMM subjects were treated in three cohorts with two doses of CART-BCMA cells ± cyclophosphamide. We retrospectively analyzed toxicity, response, and CART manufacturing data based on RT receipt. Results: Thirteen subjects received no RT Conclusions: Bridging-RT appeared safe and feasible with CART-BCMA therapy in our r/rMM patients, though larger future studies are needed to draw definitive conclusions.

Published

2021

44. Re: Human Chimeric Antigen Receptor Macrophages for Cancer Immunotherapy

Author

Benjamin A. Garcia, Saar Gill, Dylan M. Marchione, Konrad Gabrusiewicz, Kimberly Veliz, Xueqing Maggie Lu, Nicholas R. Anderson, Olga Shestova, Miriam Y. Kim, Feng Shen, Stephen R. Wallace, Michael Klichinsky, Xinhe Shan, Carl H. June, Roddy S. O’Connor, Kristin Blouch, Maksim Shestov, Marco Ruella, Yumi Yashiro-Ohtani, Miroslaw Kozlowski, Martha Zeeman, Katherine D. Cummins, Maggie Schmierer, Andrew Best, Nicholas E. Petty, and Saad S. Kenderian

Subjects

Lung Neoplasms, Cell Survival, T cell, Urology, medicine.medical_treatment, Antigen presentation, Biomedical Engineering, Bioengineering, Biology, Applied Microbiology and Biotechnology, Immunotherapy, Adoptive, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Antigen, Cancer immunotherapy, Cell Line, Tumor, Neoplasms, medicine, Macrophage, Animals, Humans, 030304 developmental biology, 0303 health sciences, Tumor microenvironment, Microscopy, Video, business.industry, Macrophages, Immunotherapy, Neoplasms, Experimental, Chimeric antigen receptor, medicine.anatomical_structure, Humanized mouse, Cancer research, Molecular Medicine, business, 030217 neurology & neurosurgery, Biotechnology

Abstract

Chimeric antigen receptor (CAR) T cell therapy has shown promise in hematologic malignancies, but its application to solid tumors has been challenging1–4. Given the unique effector functions of macrophages and their capacity to penetrate tumors5, we genetically engineered human macrophages with CARs to direct their phagocytic activity against tumors. We found that a chimeric adenoviral vector overcame the inherent resistance of primary human macrophages to genetic manipulation and imparted a sustained pro-inflammatory (M1) phenotype. CAR macrophages (CAR-Ms) demonstrated antigen-specific phagocytosis and tumor clearance in vitro. In two solid tumor xenograft mouse models, a single infusion of human CAR-Ms decreased tumor burden and prolonged overall survival. Characterization of CAR-M activity showed that CAR-Ms expressed pro-inflammatory cytokines and chemokines, converted bystander M2 macrophages to M1, upregulated antigen presentation machinery, recruited and presented antigen to T cells and resisted the effects of immunosuppressive cytokines. In humanized mouse models, CAR-Ms were further shown to induce a pro-inflammatory tumor microenvironment and boost anti-tumor T cell activity. Primary macrophages engineered to express chimeric antigen receptors have anti-tumor activity in humanized mice.

Published

2021

45. An NK-like CAR T cell transition in CAR T cell dysfunction

Author

Keisuke Watanabe, Charly R. Good, Kenichi Ishiyama, Greg Donahue, Marco Ruella, Lewis L. Lanier, Simon F. Lacey, Nathan Singh, Janos L. Tanyi, Austin K. Rennels, Shunichiro Kuramitsu, Yujie Ma, Lifeng Tian, Shelley L. Berger, Karl M. Glastad, Mark H. O'Hara, Regina M. Young, Parisa Samareh, Zhen Zhang, Edmund K. Moon, Carl H. June, M. Angela Aznar, Philipp C. Rommel, Steven M. Albelda, Katherine A. Alexander, Sangya Agarwal, Stephen J. Schuster, Max W. Richardson, Nils Wellhausen, and Sonia Guedan

Subjects

Male, medicine.medical_treatment, T-Lymphocytes, Mice, Nude, Mice, SCID, Biology, CD8-Positive T-Lymphocytes, Immunotherapy, Adoptive, General Biochemistry, Genetics and Molecular Biology, Article, SOXC Transcription Factors, SOX4, Mice, Antigen, Cell Line, Tumor, Cell transfer therapy, medicine, Animals, Humans, Transcription factor, Fatigue, Mice, Knockout, Receptors, Chimeric Antigen, T-cell receptor, Immunotherapy, Chimeric antigen receptor, Neoplasm Proteins, Killer Cells, Natural, Pancreatic Neoplasms, Phenotype, HEK293 Cells, Cancer research, Inhibitor of Differentiation Proteins, human activities, CD8

Abstract

Summary Chimeric antigen receptor (CAR) T cell therapy has achieved remarkable success in hematological malignancies but remains ineffective in solid tumors, due in part to CAR T cell exhaustion in the solid tumor microenvironment. To study dysfunction of mesothelin-redirected CAR T cells in pancreatic cancer, we establish a robust model of continuous antigen exposure that recapitulates hallmark features of T cell exhaustion and discover, both in vitro and in CAR T cell patients, that CAR dysregulation is associated with a CD8+ T-to-NK-like T cell transition. Furthermore, we identify a gene signature defining CAR and TCR dysregulation and transcription factors, including SOX4 and ID3 as key regulators of CAR T cell exhaustion. Our findings shed light on the plasticity of human CAR T cells and demonstrate that genetic downmodulation of ID3 and SOX4 expression can improve the efficacy of CAR T cell therapy in solid tumors by preventing or delaying CAR T cell dysfunction.

Published

2020

46. A rational mouse model to detect on-target, off-tumor CAR T cell toxicity

Author

Tong Da, Elizabeth L. Buza, John Scholler, Carl H. June, Caroline Sands, Yangbing Zhao, Joseph A. Fraietta, Kathleen Graham, and Mauro Castellarin

Subjects

0301 basic medicine, Receptor, ErbB-2, T-Lymphocytes, T cell, medicine.medical_treatment, Receptors, Antigen, T-Cell, Biology, Immunotherapy, Adoptive, Interferon-gamma, Mice, 03 medical and health sciences, 0302 clinical medicine, Antigen, Cancer immunotherapy, immune system diseases, In vivo, Cell Line, Tumor, parasitic diseases, mental disorders, medicine, Animals, Humans, Potency, Receptors, Chimeric Antigen, virus diseases, General Medicine, Xenograft Model Antitumor Assays, Chimeric antigen receptor, 3. Good health, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Gene Expression Regulation, Liver, nervous system, 030220 oncology & carcinogenesis, Toxicity, Cancer research, Animal studies, Single-Chain Antibodies, Research Article

Abstract

Off-tumor targeting of human antigens is difficult to predict in preclinical animal studies and can lead to serious adverse effects in patients. To address this, we developed a mouse model with stable and tunable human Her2 (hHer2) expression on normal hepatic tissue and compared toxicity between affinity-tuned Her2 chimeric antigen receptor T cells (CARTs). In mice with hHer2-high livers, both the high-affinity (HA) and low-affinity (LA) CARTs caused lethal liver damage due to immunotoxicity. In mice with hHer2-low livers, LA-CARTs exhibited less liver damage and lower systemic levels of IFN-γ than HA-CARTs. We then compared affinity-tuned CARTs for their ability to control a hHer2-positive tumor xenograft in our model. Surprisingly, the LA-CARTs outperformed the HA-CARTs with superior antitumor efficacy in vivo. We hypothesized that this was due, in part, to T cell trafficking differences between LA and HA-CARTs and found that the LA-CARTs migrated out of the liver and infiltrated the tumor sooner than the HA-CARTs. These findings highlight the importance of T cell targeting in reducing toxicity of normal tissue and also in preventing off-tumor sequestration of CARTs, which reduces their therapeutic potency. Our model may be useful to evaluate various CARTs that have conditional expression of more than 1 single-chain variable fragment (scFv).

Published

2020

47. The immunostimulatory RNA RN7SL1 enables CAR-T cells to enhance autonomous and endogenous immune function

Author

Daniel Y. Lee, Lexus R. Johnson, Carl H. June, Darwin Ye, Jacqueline S. Eacret, and Andy J. Minn

Subjects

T-Lymphocytes, Melanoma, Experimental, Biology, CD8-Positive T-Lymphocytes, General Biochemistry, Genetics and Molecular Biology, Extracellular Vesicles, Immune system, Antigen, Interferon, Cell Line, Tumor, medicine, Animals, Humans, Immunologic Factors, Myeloid Cells, Antigens, Receptors, Chimeric Antigen, RIG-I, Pattern recognition receptor, Immunity, Dendritic cell, Dendritic Cells, Chimeric antigen receptor, Cell biology, Mice, Inbred C57BL, Receptors, Pattern Recognition, Cancer cell, DEAD Box Protein 58, RNA, Immunotherapy, Interferons, Peptides, Immunocompetence, Immunologic Memory, medicine.drug

Abstract

Summary Poor tumor infiltration, development of exhaustion, and antigen insufficiency are common mechanisms that limit chimeric antigen receptor (CAR)-T cell efficacy. Delivery of pattern recognition receptor agonists is one strategy to improve immune function; however, targeting these agonists to immune cells is challenging, and off-target signaling in cancer cells can be detrimental. Here, we engineer CAR-T cells to deliver RN7SL1, an endogenous RNA that activates RIG-I/MDA5 signaling. RN7SL1 promotes expansion and effector-memory differentiation of CAR-T cells. Moreover, RN7SL1 is deployed in extracellular vesicles and selectively transferred to immune cells. Unlike other RNA agonists, transferred RN7SL1 restricts myeloid-derived suppressor cell (MDSC) development, decreases TGFB in myeloid cells, and fosters dendritic cell (DC) subsets with costimulatory features. Consequently, endogenous effector-memory and tumor-specific T cells also expand, allowing rejection of solid tumors with CAR antigen loss. Supported by improved endogenous immunity, CAR-T cells can now co-deploy peptide antigens with RN7SL1 to enhance efficacy, even when heterogenous CAR antigen tumors lack adequate neoantigens.

Published

2020

48. Nanomaterials for T-cell cancer immunotherapy

Author

Ningqiang, Gong, Neil C, Sheppard, Margaret M, Billingsley, Carl H, June, and Michael J, Mitchell

Subjects

Drug Delivery Systems, Receptors, Chimeric Antigen, Neoplasms, T-Lymphocytes, Cell- and Tissue-Based Therapy, Tumor Microenvironment, Animals, Humans, Immunotherapy, Cancer Vaccines, Nanostructures

Abstract

T-cell-based immunotherapies hold promise for the treatment of many types of cancer, with three approved products for B-cell malignancies and a large pipeline of treatments in clinical trials. However, there are several challenges to their broad implementation. These include insufficient expansion of adoptively transferred T cells, inefficient trafficking of T cells into solid tumours, decreased T-cell activity due to a hostile tumour microenvironment and the loss of target antigen expression. Together, these factors restrict the number of therapeutically active T cells engaging with tumours. Nanomaterials are uniquely suited to overcome these challenges, as they can be rationally designed to enhance T-cell expansion, navigate complex physical barriers and modulate tumour microenvironments. Here, we present an overview of nanomaterials that have been used to overcome clinical barriers to T-cell-based immunotherapies and provide our outlook of this emerging field at the interface of cancer immunotherapy and nanomaterial design.

Published

2020

49. Enhanced cytotoxicity against solid tumors by bispecific antibody-armed CD19 CAR T cells: a proof-of-concept study

Author

John Scholler, Dana L Schalk, Carl H. June, Archana Thakur, and Lawrence G. Lum

Subjects

0301 basic medicine, Cancer Research, Receptor, ErbB-2, medicine.medical_treatment, Antigens, CD19, Lymphocyte Activation, Immunotherapy, Adoptive, Proof of Concept Study, CD19, Article, Cell therapy, 03 medical and health sciences, 0302 clinical medicine, Pancreatic cancer, Neoplasms, Antibodies, Bispecific, medicine, Humans, Cytotoxicity, B cell, biology, Chemistry, General Medicine, medicine.disease, Chimeric antigen receptor, ErbB Receptors, 030104 developmental biology, medicine.anatomical_structure, Cytokine, Oncology, Cell culture, 030220 oncology & carcinogenesis, Cancer research, biology.protein

Abstract

PURPOSE: Although adoptive cell therapy with chimeric antigen receptor (CAR)-engineered T cells has shown durable clinical efficacy in patients with CD19(+) B-cell malignancies, the application of this approach to solid tumors is challenging. The goal of this proof-of-concept study was to investigate whether loading of CD19-CAR T cells (CART19) with anti-HER2 or anti-EGFR bispecific antibodies (BiAb) will target HER2+/EGFR+ CD19- targets and signal the intracellular domain of CAR without engaging antigen-specific CD19 ScFv of CAR T cells. METHODS: We used CART19 armed with anti-CD3 (OKT3) × anti-HER2 BiAb (HER2Bi) or anti-CD3 (OKT3) × anti-EGFR BiAb (EGFRBi) to evaluate the cytotoxicity directed at HER2 or EGFR expressing cancer cell lines compared with unarmed CART19 measured by short-term (51)Cr release assay and long-term real-time cell analysis using xCelligence. We also determined the differences in exhaustion or effector phenotypes and cytokine profiles during the short- and long-term cytotoxicity assays. RESULTS: Specific cytotoxicity was exhibited by CART19 armed with HER2Bi or EGFRBi against multiple tumor cell lines. Armed CART19 and armed activated T cells (ATC) showed comparable specific cytotoxicity that ranged between 10 and 90% against breast, pancreatic, ovarian, prostate, and lung cancer cell lines at 10:1 E/T ratio. Serial killing (repeated killing) by HER2Bi-armed CART19 ranged between 80 and 100% at 10:1 E/T ratio against MCF-7 cells up to 19 days (up to 4(th) round of repeated killing) measured by a real-time cell analysis without CART19 becoming exhausted. CONCLUSIONS: HER2Bi- or EGFRBi-armed CART19 exhibited specific cytotoxicity against multiple HER2(+)/EGFR+/CD19(−) tumor targets in overnight and long-term serial killing assays. CART19 showed improved survival and were resistant to exhaustion after prolonged repeated exposure to tumor cells.

Published

2020

50. AACR Calls on Congress to Take Immediate Action against COVID-19 and Protect Patients with Cancer during the Pandemic

Author

Karen E. Knudsen, Cory Abate-Shen, Charles Swanton, Gordon B. Mills, Adriana Albini, David A. Tuveson, René Bernards, Lillian L. Siu, Carl H. June, Elaine R. Mardis, Margaret Foti, Philip D. Greenberg, Antoni Ribas, Keith T. Flaherty, William N. Hait, Martine F. Roussel, Martine Piccart, Elizabeth M. Jaffee, Edison T. Liu, and Marcia Cruz-Correa

Subjects

American Cancer Society, medicine.medical_specialty, Biomedical Research, Coronavirus disease 2019 (COVID-19), business.industry, Pneumonia, Viral, Cancer, COVID-19, medicine.disease, Research Personnel, Telemedicine, United States, Oncology, Action (philosophy), Cancer Survivors, Neoplasms, Pandemic, medicine, Humans, Intensive care medicine, business, Coronavirus Infections, Pandemics, Societies, Medical

Abstract

On March 30, 2020, the AACR Board of Directors provided a letter to the U.S. Congressional leadership on behalf of its members in response to the COVID-19 public health emergency.

Published

2020