Showing total 396 results

1. Real-world survival analysis by tumor mutational burden in non-small cell lung cancer: a multisite U.S. study

Author

Connor Willis, Hillevi Bauer, Trang H. Au, Jyothi Menon, Sudhir Unni, Dao Tran, Zachary Rivers, Wallace Akerley, Matthew B. Schabath, Firas Badin, Ashley Sekhon, Malini Patel, Bing Xia, Beth Gustafson, John L. Villano, John-Michael Thomas, Solomon J. Lubinga, Michael A. Cantrell, Diana Brixner, and David Stenehjem

Subjects

Lung Neoplasms, Receptor Protein-Tyrosine Kinases, Survival Analysis, B7-H1 Antigen, Cohort Studies, ErbB Receptors, Oncology, tumor biomarkers, Carcinoma, Non-Small-Cell Lung, Mutation, Biomarkers, Tumor, Humans, lung neoplasma, immunotherapy, Prospective Studies, Research Paper

Abstract

Background: Tumor mutational burden (TMB) is a potential biomarker to predict tumor response to immuno-oncology agents in patients with metastatic non-small cell lung cancer (NSCLC). Materials and Methods: A multi-site cohort study evaluated patients diagnosed with stage IV NSCLC between 2012 and 2019 who had received comprehensive genomic profiling (CGP) and any NSCLC-related treatment at 9 U.S. cancer centers. Baseline characteristics and clinical outcomes were compared between patients with TMB 10 showed a significant association towards longer overall survival (OS) (HR: 0.43, 95% CI: 0.21–0.88, p = 0.02) and progression-free survival (PFS) (HR: 0.43, 95% CI: 0.21–0.85, p = 0.02) in patients treated with first-line immunotherapy and tested by Foundation Medicine or Caris at treatment initiation. Conclusions: TMB levels greater than or equal to 10 mut/Mb, when tested by Foundation Medicine or Caris at treatment initiation, were significantly associated with improved OS and PFS among patients treated with first-line immunotherapy-containing regimens. Additional prospective research is warranted to validate this biomarker along with PD-L1 expression.

Published

2022

2. Low tumour-infiltrating lymphocyte density in primary and recurrent glioblastoma

Author

Kelsey Maddison, Moira C. Graves, Sam Faulkner, Michael Fay, Paul A. Tooney, Nikola A. Bowden, and Ricardo E. Vilain

Subjects

Tumour infiltrating lymphocyte, medicine.medical_treatment, CD3, Cell, immune microenvironment, chemical and pharmacologic phenomena, Medicine, tumour recurrence, tumour-infiltrating lymphocytes, biology, business.industry, Recurrent glioblastoma, glioblastoma, hemic and immune systems, Immunotherapy, medicine.disease, Immune checkpoint, medicine.anatomical_structure, Oncology, programmed cell death 1, Cancer research, biology.protein, business, CD8, Research Paper, Glioblastoma

Abstract

Immunotherapies targeting tumour-infiltrating lymphocytes (TILs) that express the immune checkpoint molecule programmed cell death-1 (PD-1) have shown promise in preclinical glioblastoma models but have had limited success in clinical trials. To assess when glioblastoma is most likely to benefit from immune checkpoint inhibitors we determined the density of TILs in primary and recurrent glioblastoma. Thirteen cases of matched primary and recurrent glioblastoma tissue were immunohistochemically labelled for CD3, CD8, CD4 and PD-1, and TIL density assessed. CD3+ TILs were observed in all cases, with the majority of both primary (69.2%) and recurrent (61.5%) tumours having low density of TILs present. CD8+ TILs were observed at higher densities than CD4+ TILs in both tumour groups. PD-1+ TILs were sparse and present in only 25% of primary and 50% of recurrent tumours. Quantitative analysis of TILs demonstrated significantly higher CD8+ TIL density at recurrence (p = 0.040). No difference was observed in CD3+ (p = 0.191), CD4+ (p = 0.607) and PD-1+ (p = 0.070) TIL density between primary and recurrent groups. This study shows that TILs are present at low densities in both primary and recurrent glioblastoma. Furthermore, PD-1+ TILs were frequently absent, which may provide evidence as to why anti-PD-1 immunotherapy trials have been largely unsuccessful in glioblastoma.

Published

2021

3. Nanoparticle T cell engagers for the treatment of acute myeloid leukemia

Author

Chaelee Park, Barbara Muz, Ola Adebayo, Kinan Alhallak, Berit Lubben, John F. DiPersio, Hannah Bash, Jessica Yavner, Abdel Kareem Azab, Jennifer Sun, Samuel Achilefu, and Amanda Jeske

Subjects

business.industry, medicine.drug_class, medicine.medical_treatment, T cell, CD33, Myeloid leukemia, Immunotherapy, acute myeloid leukemia, medicine.disease, Monoclonal antibody, Isotype, Leukemia, medicine.anatomical_structure, Oncology, hemic and lymphatic diseases, T cell engagers, medicine, Cancer research, nanoparticles, Bone marrow, 3D tissue culture model, business, neoplasms, Research Paper

Abstract

Acute myeloid leukemia (AML) is the most common type of leukemia and has a 5-year survival rate of 25%. The standard-of-care for AML has not changed in the past few decades. Promising immunotherapy options are being developed for the treatment of AML; yet, these regimens require highly laborious and sophisticated techniques. We create nanoTCEs using liposomes conjugated to monoclonal antibodies to enable specific binding. We also recreate the bone marrow niche using our 3D culture system and use immunocompromised mice to enable use of human AML and T cells with nanoTCEs. We show that CD33 is ubiquitously present on AML cells. The CD33 nanoTCEs bind preferentially to AML cells compared to Isotype. We show that nanoTCEs effectively activate T cells and induce AML killing in vitro and in vivo. Our findings suggest that our nanoTCE technology is a novel and promising immuno-therapy for the treatment of AML and provides a basis for supplemental investigations for the validation of using nanoTCEs in larger animals and patients.

Published

2021

4. A platform for locoregional T-cell immunotherapy to control HNSCC recurrence following tumor resection

Author

Shay Sharon, Jason R. Baird, Rom Leidner, Marka R. Crittenden, Michael J. Gough, Shelly Bambina, Nardy Casap, Tiffany C. Blair, Shawn M. Jensen, Gwen Kramer, and R. Bryan Bell

Subjects

Oncology, medicine.medical_specialty, business.industry, medicine.medical_treatment, T cell, Head and neck cancer, biomaterial, Immunotherapy, medicine.disease, intratumoral, Lymphatic system, Immune system, medicine.anatomical_structure, Antigen, T-cell, Internal medicine, medicine, Carcinoma, Adjuvant therapy, head and neck cancer, immunotherapy, business, Research Paper

Abstract

Surgical resection of head and neck squamous-cell carcinoma (HNSCC) is associated with high rates of local and distant recurrence, partially mitigated by adjuvant therapy. A pre-existing immune response in the patient's tumor is associated with better outcomes following treatment with conventional therapies, but improved options are needed for patients with poor anti-tumor immunity. We hypothesized that local delivery of tumor antigen-specific T-cells into the resection cavity following surgery would direct T-cells to residual antigens in the margins and draining lymphatics and present a platform for T-cell-targeted immunotherapy. We loaded T-cells into a biomaterial that conformed to the resection cavity and demonstrated that it could release T-cells that retained their functional activity in-vitro, and in a HNSCC model in-vivo. Locally delivered T-cells loaded in a biomaterial were equivalent in control of established tumors to intravenous adoptive T-cell transfer, and resulted in the systemic circulation of tumor antigen-specific T-cells as well as local accumulation in the tumor. We demonstrate that adjuvant therapy with anti-PD1 following surgical resection was ineffective unless combined with local delivery of T-cells. These data demonstrate that local delivery of tumor-specific T-cells is an efficient option to convert tumors that are unresponsive to checkpoint inhibitors to permit tumor cures.

Published

2021

5. Immunotherapy in Xeroderma Pigmentosum: a case of advanced cutaneous squamous cell carcinoma treated with cemiplimab and a literature review

Author

Gianluca Avallone, Maria Teresa Fierro, Martina Merli, Andrea Agostini, Virginia Caliendo, Amelia Barcellini, Pietro Quaglino, Simone Ribero, Luca Mastorino, Francesca Valvo, Viviana Vitolo, and Marco Rubatto

Subjects

0301 basic medicine, medicine.medical_specialty, Cutaneous squamous cell carcinoma, Xeroderma pigmentosum, medicine.drug_class, medicine.medical_treatment, Monoclonal antibody, 03 medical and health sciences, 0302 clinical medicine, Nasal region, hadrontherapy, medicine, Advanced squamous cell carcinoma, Cemiplimab, Hadrontherapy, Immunotherapy, Xeroderma Pigmentosum, business.industry, Genetic disorder, Genodermatosis, xeroderma pigmentosum, medicine.disease, advanced squamous cell carcinoma, Dermatology, Radiation therapy, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, immunotherapy, cemiplimab, business, Research Paper

Abstract

Xeroderma Pigmentosum (XP) is a rare genetic disorder with a poor prognosis due to high photosensitivity in affected patients. Herein, we describe the first case of the use of cemiplimab in a patient with XP, a 19-year-old girl presented with locally advanced squamous cell carcinoma of the right periorbital and nasal region. This treatment has been undertaken after a cycle of proton beam radiotherapy. Besides, it is reported a description of the few cases in the literature describing the effectiveness of immunotherapy on skin cancers in XP-patients. This case is in line with those reported, underlining how anti-PD1 monoclonal antibodies may be a promising treatment in this genodermatosis.

Published

2021

6. Testosterone deficiency in men receiving immunotherapy for malignant melanoma

Author

Varun Monga, Sarah L. Mott, William W. Terry, Madeline Peters, and Amy M. Pearlman

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, Hypophysitis, medicine.medical_treatment, Ipilimumab, Hypopituitarism, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, melanoma, medicine, cancer, Endocrine system, Stage (cooking), business.industry, Melanoma, androgens, Cancer, Immunotherapy, medicine.disease, 030104 developmental biology, testosterone deficiency, 030220 oncology & carcinogenesis, immunotherapy, business, Research Paper, medicine.drug

Abstract

Immunotherapy has been established as a standard of care for patients with malignant melanoma, however, the long-term side-effects of immunotherapy are still emerging. Studies over the last decade have documented increasing reports of endocrine dysfunction following the initiation of immunotherapy. Our study aimed to detect the proportion of men who have low testosterone before, during, and or/after receiving immunotherapy for malignant melanoma, and to determine the proportion of men who receive testosterone replacement therapy after detection of low testosterone. We performed retrospective chart review of patients with malignant melanoma treated with immunotherapy. Low testosterone was identified in 34 out of 49 patients at some point during their treatment with immunotherapy. Despite low testosterone levels in two-thirds of patients, only three patients were treated with testosterone replacement therapy. In addition to laboratory evidence of low testosterone, patients were also symptomatic as 43 out of 49 patients reported fatigue to their providers. Four patients developed hypophysitis and subsequent hypopituitarism, all of whom were receiving Ipilimumab. We conclude that patients with stage 3 or 4 melanoma treated with immunotherapy appear to be at an increased risk of developing testosterone deficiency during their treatment.

Published

2021

7. Intratumoral immunotherapy with STING agonist, ADU-S100, induces CD8+ T-cell mediated anti-tumor immunity in an esophageal adenocarcinoma model

Author

Juliann E. Kosovec, Laila Babar, Shahin Ayazi, Gene Grant Finley, Ali H. Zaidi, Soyoung Lee, Blair A. Jobe, Ashten N. Omstead, Madison Salvitti, Ronan J. Kelly, Ping Zheng, Ajay Goel, and Anastasia Gorbunova

Subjects

0301 basic medicine, Agonist, PD-L1, esophageal adenocarcinoma, medicine.drug_class, medicine.medical_treatment, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Interferon, medicine, biology, business.industry, CD8+ T-cells, Immunotherapy, Sting, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Tumor necrosis factor alpha, business, CD8, IFNβ, medicine.drug, Research Paper, STING

Abstract

Background: Esophageal adenocarcinoma (EAC) is a deadly disease with limited treatment options. STING is a transmembrane protein that activates transcription of interferon genes, resulting in stimulation of APCs and enhanced CD8+ T-cell infiltration. The present study evaluates STING agonists, alone and in combination with radiation to determine durable anticancer activity in solid tumors. Materials and Methods: Esophagojejunostomy was performed on rats to induce reflux leading to the development of EAC. At 32 weeks post operatively, rats received intratumorally either 50 μg STING (ADU-S100) or placebo (PBS), +/– 16Gy radiation. Drug activity was evaluated by pre- and post- treatment MRI, histology, immunofluorescence and RT-PCR. Results: Mean MRI tumor volume decreased by 30.1% and 50.8% in ADU-S100 and ADU-S100 + radiation animals and increased by 76.7% and 152.4% in placebo and placebo + radiation animals, respectively (P < 0.0001). Downstream gene expression, pre- to on- and post- treatment, demonstrated significant upregulation of IFNβ, TNFα, IL-6, and CCL-2 in the treatment groups vs. placebo. On- or post- treatment, radiation alone, ADU-S100 alone, and ADU-S100 + radiation groups demonstrated enhanced PD-LI expression, induced by upregulation of CD8+ T-cells (p < 0.01). Conclusions: ADU-S100 +/– radiation exhibits potent antitumor activity and a promising immunomodulatory profile in a de novo EAC.

Published

2021

8. Improved therapeutic efficacy of unmodified anti-tumor antibodies by immune checkpoint blockade and kinase targeted therapy in mouse models of melanoma

Author

Rolando Perez-Lorenzo, Raphael Clynes, Angela M. Christiano, and S. Erjavec

Subjects

0301 basic medicine, anti-tumor antibodies, medicine.medical_treatment, Targeted therapy, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antigen, medicine, melanoma, business.industry, Melanoma, FOXP3, Cancer, Immunotherapy, medicine.disease, targeted therapy, Immune checkpoint, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, immunotherapy, combination therapies, business, Research Paper

Abstract

The use of specific anti-tumor antibodies has transformed the solid cancer therapeutics landscape with the relative successes of therapies such as anti-HER2 in breast cancer, and anti-EGFR in HNSCC and colorectal cancer. However, these therapies result in toxicity and the emergence of resistant tumors. Here, we showed that removing immune suppression and enhancing stimulatory signals increased the anti-tumor activity of unmodified TA99 antibodies (anti-TYRP1) with a significant reduction of growth of solid tumors and lung metastases in mouse models of melanoma. Immune checkpoint blockade enhanced the efficacy of TA99, which was associated with greater CD8+/Foxp3+, NK1.1+ and dendritic cell infiltrates, suggestive of an increased anti-tumor innate and adaptive immune responses. Further, MEK inhibition in melanoma cell lines increased the expression of melanosomal antigens in vitro, and combining TA99 and MEKi in vivo resulted in enhanced tumor control. Moreover, we found an improved therapeutic effect when YUMM tumor-bearing mice were treated with TA99 combined with MEKi and immune checkpoint blockade (anti-PD1 and anti-CTLA4). Our findings suggest that MEKi induced an increased expression of tumor-associated antigens, which in combination with anti-tumor antibodies, generated a robust adaptive anti-tumor response that was sustained by immune checkpoint inhibition therapy. We postulate that combining anti-tumor antibodies with standard-of-care strategies such as immune checkpoint blockade or targeted therapy, will improve therapeutic outcomes in cancer.

Published

2021

9. Targeting an engineered cytokine with interleukin-2 and interleukin-15 activity to the neovasculature of solid tumors

Author

Marco Bertolini, Marco Stringhini, Michael R. Mortensen, Dario Neri, Jacqueline Mock, and Marco Catalano

Subjects

Interleukin 2, Biodistribution, EDB of fibronectin, biology, Chemistry, medicine.medical_treatment, engineered cytokine, Immunotherapy, Fusion protein, Fibronectin, Cytokine, Oncology, antibody-cytokine fusion proteins, Interleukin 15, medicine, biology.protein, Cancer research, immunotherapy, Antibody, immunocytokines, Research Paper, medicine.drug

Abstract

There is a growing interest in the antibody-based delivery of cytokines to the tumor environment as a means to boost the anti-cancer activity of tumor-resident T cells and NK cells. Here, we describe the expression and characterization of fusion proteins, featuring the L19 antibody (specific to the alternatively-spliced EDB domain of fibronectin) and an engineered cytokine with interleukin-2 and interleukin-15 properties. The cytokine moiety was fused either at the N-terminal or at the C-terminal extremity and both fusion proteins showed a selective tumor accumulation in a quantitative biodistribution experiment. The N-terminal fusion inhibited tumor growth in immunocompetent mice bearing F9 carcinomas or WEHI-164 sarcomas when used as single agent. The anticancer activity was compared to the one of the same cytokine payload used as recombinant protein or fused to an anti-hen egg lysozyme antibody, serving as negative control of irrelevant specificity in the mouse. These results indicate that the antibody-based delivery of engineered cytokines to the tumor neovasculature may mediate a potent anticancer activity.

Published

2020

10. Evaluations of CRC2631 toxicity, tumor colonization, and genetic stability in the TRAMP prostate cancer model

Author

Austen A. Barnett, Robert A. Kazmierczak, Yves C. Chabu, Bakul Dhagat-Mehta, Li Lee, Elke Gülden, Clintin P. Davis-Stober, and Lixin Ma

Subjects

0301 basic medicine, cancer targeting, medicine.medical_treatment, salmonella, TRAMP, Metastasis, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Immune system, Cancer immunotherapy, Prostate, medicine, business.industry, Cancer, Immunotherapy, prostate cancer, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Cancer research, immunotherapy, business, Research Paper, Tramp

Abstract

Conventional cancer chemotherapies are not fully efficacious and do not target tumors, leading to significant treatment-related morbidities. A number of genetically attenuated cancer-targeting bacteria are being developed to safely target tumors in vivo. Here we report the toxicological, tumor-targeting, and efficacy profiles of Salmonella enterica serovar Typhimurium CRC2631 in a syngeneic and autochthonous TRAMP model of aggressive prostate cancer. CRC2631 preferentially colonize primary and metastatic tumors in the TRAMP animals. In addition, longitudinal whole genome sequencing studies of CRC2631 recovered from prostate tumor tissues demonstrate that CRC2631 is genetically stable. Moreover, tumor-targeted CRC2631 generates an anti-tumor immune response. Combination of CRC2631 with checkpoint blockade reduces metastasis burden. Collectively, these findings demonstrate a potential for CRC2631 in cancer immunotherapy strategies.

Published

2020

11. Clonality and antigen-specific responses shape the prognostic effects of tumor-infiltrating T cells in ovarian cancer

Author

Sacha Gnjatic, Sebastiano Battaglia, Harlan Robins, J. Brian Szender, Anthony Miliotto, Ryan O. Emerson, Jianmin Wang, Junko Matsuzaki, Shashikant Lele, Kunle Odunsi, Wiam Bshara, Carl Morrison, Takemasa Tsuji, Amit A. Lugade, Kevin H. Eng, and Song Liu

Subjects

0301 basic medicine, business.industry, Repertoire, medicine.medical_treatment, chemical and pharmacologic phenomena, Immunotherapy, medicine.disease, tumor immunity, 03 medical and health sciences, Serous fluid, ovarian cancer, 030104 developmental biology, 0302 clinical medicine, Immune system, Oncology, Antigen, 030220 oncology & carcinogenesis, T-cell repertoire, Monoclonal, medicine, Cancer research, business, Ovarian cancer, CD8, Research Paper

Abstract

CD8+ tumor-infiltrating lymphocytes (TILs) are not all specific for tumor antigens, but can include bystander TILs that are specific for cancer-irrelevant epitopes, and it is unknown whether the T-cell repertoire affects prognosis. To delineate the complexity of anti-tumor T-cell responses, we utilized a computational method for de novo assembly of sequences from CDR3 regions of 369 high-grade serous ovarian cancers from TCGA, and then applied deep TCR-sequencing for analyses of paired tumor and peripheral blood specimens from an independent cohort of 99 ovarian cancer patients. Strongly monoclonal T-cell repertoires were associated with favorable prognosis (PFS, HR = 0.65, 0.50–0.84, p = 0.003; OS, HR = 0.61, 0.44–0.83, p = 0.006) in TCGA cohort. In the validation cohort, we discovered that patients with low T-cell infiltration but low diversity or focused repertoires had clinical outcomes almost indistinguishable from highly-infiltrated tumors (median 21.0 months versus 15.9 months, log-rank p = 0.945). We also found that the degree of divergence of the peripheral repertoire from the TIL repertoire, and the presence of detectable spontaneous anti-tumor immune responses are important determinants of clinical outcome. We conclude that the prognostic significance of TILs in ovarian cancer is dictated by T-cell clonality, degree of overlap with peripheral repertoire, and the presence of detectable spontaneous anti-tumor immune response in the patients. These immunological phenotypes defined by the TCR repertoire may provide useful insights for identifying “TIL-low” ovarian cancer patients that may respond to immunotherapy.

Published

2020

12. Th1 cytokines in conjunction with pharmacological Akt inhibition potentiate apoptosis of breast cancer cells in vitro and suppress tumor growth in vivo

Author

Gary K. Koski, Brian J. Czerniecki, and Loral E Showalter

Subjects

0301 basic medicine, business.industry, medicine.medical_treatment, Cancer, Active immunotherapy, Dendritic cell, Immunotherapy, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Breast cancer, breast cancer, Oncology, In vivo, Apoptosis, 030220 oncology & carcinogenesis, Cancer research, Medicine, immunotherapy, business, Protein kinase B, Research Paper, Akt kinase

Abstract

Targeted drug approaches have been a major focus for developing new anticancer therapies. Although many such agents approved in the last 20 years have improved outcomes, almost all have underperformed expectations. The full potential of such agents may yet be obtained through novel combinations. Previously, we showed that anti-estrogen drugs combined with a dendritic cell-based anti-HER-2 vaccine known to induce strong Th1-polarized immunity dramatically improved clinical response rates in patients with HER-2pos/ERpos early breast cancer. Here, we show that the small molecule Akt antagonist MK-2206, when combined with the Th1 cytokines IFN-gamma and TNF-alpha, maximize indicators of apoptotic cell death in a panel of phenotypically-diverse human breast cancer lines. These findings were mirrored by other, structurally-unrelated Akt-targeting drugs that work through different mechanisms. Interestingly, we found that MK-2206, as well as the other Akt antagonist drugs, also had a tendency to suppress Th1 cytokine expression in stimulated human and murine lymphocytes, potentially complicating their use in conjunction with active immunotherapy. After verifying that MK-2206 plus IFN-gamma could show similar combined effects against breast cancer lines, even in the absence of TNF-alpha, we tested in a rodent HER-2pos breast cancer model either a HER-2-based DC vaccine, or recombinant IFN-gamma with or without MK-2206 administration. We found that for MK-2206, co-administration of recombinant IFN-gamma outperformed co-administration of DC vaccination for slowing tumor growth kinetics. These findings suggest a combined therapy approach for Akt-targeting drugs that incorporates recombinant Interferon-gamma and is potentially translatable to humans.

Published

2020

13. Rapid onset type 1 diabetes with anti-PD-1 directed therapy

Author

Sandip Pravin Patel, Karen Yun, Gregory A. Daniels, Kathryn A. Gold, and Karen C. McCowen

Subjects

0301 basic medicine, medicine.medical_specialty, Diabetic ketoacidosis, endocrine system diseases, type 1 diabetes, medicine.medical_treatment, Oncology and Carcinogenesis, Autoimmune Disease, 03 medical and health sciences, diabetic ketoacidosis, 0302 clinical medicine, Internal medicine, Diabetes mellitus, diabetic ketoacidosis (DKA), immune-related adverse event, medicine, immune-related adverse event (irAE), Adverse effect, Prospective cohort study, Metabolic and endocrine, Type 1 diabetes, business.industry, Prevention, Insulin, Diabetes, Autoantibody, nutritional and metabolic diseases, medicine.disease, Good Health and Well Being, 030104 developmental biology, Oncology, 5.1 Pharmaceuticals, 030220 oncology & carcinogenesis, immunotherapy, PD-1 inhibitors, Development of treatments and therapeutic interventions, Nivolumab, business, Research Paper

Abstract

Type 1 diabetes is a rare immune-related adverse event (irAE) caused by checkpoint inhibitors with serious risk for diabetic ketoacidosis (DKA). Using our electronic medical record, we identified 1327 adult patients who received PD-(L)1 or CTLA-4 inhibitors from 2013 to 2018. Of the patients who received immunotherapy, 5 (0.38%) patients were found to have type 1 diabetes, all of whom presented with DKA requiring insulin at 20 to 972 days from their first anti-PD-(L)1 dose. All patients were treated with anti-PD-1 therapy (nivolumab or pembrolizumab). Four patients had new onset diabetes with mean HbA1c of 9.1% on DKA presentation and persistent elevations over time. Two patients who tested positive for glutamic acid decarboxylase (GAD) antibodies presented with DKA at 20 and 106 days from first anti-PD-1 administration whereas patients who were autoantibody negative had DKA more than a year later. Type 1 diabetes occurs within a wide time frame after anti-PD-1 initiation and commences with an abrupt course. Our case series suggests that monitoring glycemia in patients on PD-1 inhibitors is not predictive for diabetes occurrence. GAD autoantibodies could portend earlier onset for diabetes, although further prospective studies are needed to elucidate their diagnostic utility and contribution in therapeutic interception.

Published

2020

14. Entinostat augments NK cell functions via epigenetic upregulation of IFIT1-STING-STAT4 pathway

Author

Nathan J. Schloemer, Subramaniam Malarkannan, John M Idso, Jeffrey Knipstein, Shunhua Lao, Monica S. Thakar, and Robert Burns

Subjects

0301 basic medicine, Entinostat, medicine.drug_class, Histone deacetylase inhibitor, NK cells, NKG2D, Chromatin, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, IRF1, Oncology, chemistry, Downregulation and upregulation, Cell culture, 030220 oncology & carcinogenesis, medicine, Cancer research, rhabdomyosarcoma, immunotherapy, Histone deacetylase, histone deacetylase inhibitor, Ewing sarcoma, Research Paper

Abstract

Histone deacetylase inhibitors (HDACi) are an emerging cancer therapy; however, their effect on natural killer (NK) cell-mediated anti-tumor responses remain unknown. Here, we evaluated the impact of a benzamide HDACi, entinostat, on human primary NK cells as well as tumor cell lines. Entinostat significantly upregulated the expression of NKG2D, an essential NK cell activating receptor. Independently, entinostat augmented the expression of ULBP1, HLA, and MICA/B on both rhabdomyosarcoma and Ewing sarcoma cell lines. Additionally, entinostat increased both cytotoxicity and IFN-γ production in human NK cells following coculture with these tumor cells. Mechanistically, entinostat treatment resulted in increased chromatin accessibility to the promoter region for interferon-induced protein with tetratricopeptide repeats 1 (IFIT1) gene and thereby increasing the transcript and protein levels of IFIT1 that augmented the IFIT1-mediated IRF1, STAT4, and STING pathways. Corresponding transcriptome analysis revealed enrichment of IRF1 and STAT4 and gene sets responsible for NK cell-mediated IFN-γ production and cytotoxicity, respectively. Our results show a novel mechanism by which entinostat initiates an IFIT1-STING-mediated potentiation of STAT4 via IRF1 to augment NK cell-mediated anti-tumor responses.

Published

2020

15. Lymph nodes may be a source for immunetherapy in gastric cancer

Author

Paulo Pimentel Assumpção, Erika Couto Canelas, Ana Karyssa Mendes Anaissi, Samia Demachki, Sidney Santos, Aline Maria Pereira Cruz Ramos, Geraldo Ishak, João Felipe Acioli, and Paula Baraúna de Assumpção

Subjects

Tissue microarray, business.industry, gastric cancer, medicine.medical_treatment, Cancer, Immunotherapy, medicine.disease, Immune system, Oncology, Antigen, lymph nodes, Cancer cell, Cancer research, Medicine, immunotherapy, Lymph, business, Immunostaining, Research Paper

Abstract

Background adoptive immunotherapy is a promising cancer therapy. Immune cells are capable of recognizing and destroying cancer cells and represent a powerful strategy, however, this approach remains technically complicated, due to the need to select and isolate immune cells from these, present cancer antigens to those cells, expanding and reinjecting them. Lymph nodes recovered during gastric cancer surgery may represent an option for immunotherapy, since they harbor an enormous amount of immune cells, which have already been presented to cancer antigens. The advantage of selecting only cancer-negative lymph has not been determined yet. The status of immune checkpoints in the immune cells within the lymph nodes was analyzed in order to try to solve this problem. Materials and methods Tissue microarrays were constructed and automated immunostaining for PD-1 and PD-L1 was performed on 143 lymph nodes from 70 patients with gastric adenocarcinoma. Results In positive nodes, PD-L1 was only positivity in cancer cells (6%) and PD-1 was positive for B lymphocytes (60%), T lymphocytes (70%) and one case in cancer cells (2.5%). In negative nodes, most cases were positive for PD-1 in B (73.1%) and T (71.65%) lymphocytes. Conclusions Expression of PD-1 and PD-L1 in gastric cancer lymph nodes was demonstrated for the first time. PD-1 is expressed in positive and negative nodes, which could activate the PD-1 pathway. Lymphocytes from tumor-free lymph nodes were negative for PD-L1, and this might represent an advantage for selecting these lymph nodes as a potential source of immune cells for adoptive immunotherapy.

Published

2020

16. Hyperprogression and impact of tumor growth kinetics after PD1/PDL1 inhibition in head and neck squamous cell carcinoma

Author

Nicolas Gadot, Jean-Yves Blay, Pierre Saintigny, Carole Crozes, Frédéric Bérard, Thibaut Garrivier, Charles Mastier, Jérôme Fayette, Philippe Ceruse, Andy Karabajakian, and Philippe Zrounba

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, medicine.medical_treatment, Immune checkpoint inhibitors, Salvage treatment, Disease, programmed cell death 1 receptor, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Tumor growth, business.industry, Significant difference, Immunotherapy, medicine.disease, Head and neck squamous-cell carcinoma, 030104 developmental biology, kinetics, 030220 oncology & carcinogenesis, squamous cell carcinoma of head and neck, immunotherapy, business, Progressive disease, Research Paper

Abstract

Background: Hyperprogressive disease (HPD) rate in head and neck squamous cell carcinoma (HNSCC) patients treated with immune checkpoint inhibitors (ICI) was determined using tumor growth kinetics (TGK) and compared with rapidly progressive screen-failure (SF) patients. The impact of TGK on outcomes with salvage chemotherapy (SCT) was also evaluated. Results: HPD was found in 22/120 (18%) patients. Median TGK before the onset of immunotherapy (TGKpre) was 2.7 for SF patients and 4.8 for HPD patients, with no significant difference (p = 0.17). Disease control rate after initial progressive disease on ICI was 86% with SCT in case of tumor growth deceleration vs 39% in case of tumor growth acceleration. Conclusions: HPD was frequent, but TGK of HPD patients treated with ICI did not differ from SF patients, suggesting that there is no relevant causal relationship between HPD and ICI. After initial PD with ICI, tumor growth deceleration was associated with better outcomes, indicating that TGKR might be useful to detect late responders, meriting prospective investigations. Materials and Methods: TGK ratio (TGKR) was defined as the ratio of TGK on ICI (TGKpost) to TGKpre. HPD was defined as TGKR ≥ 2. TGKR >1 indicated tumor growth acceleration, while 0 < TGKR < 1 indicated tumor deceleration.

Published

2020

17. Radiation induces iatrogenic immunosuppression by indirectly affecting hematopoiesis in bone marrow

Author

Dennis E. Hallahan, Xiaowei Wang, Vaishali Kapoor, Grant A. Challen, Joseph R. Krambs, Dinesh Thotala, Kaylan Griffith, Nathan Wong, Subhajit Ghosh, Daniel C. Link, and Andrea Collins

Subjects

0301 basic medicine, medicine.medical_treatment, T cell, chemical and pharmacologic phenomena, mass cytometry RNA sequencing, 03 medical and health sciences, 0302 clinical medicine, Immune system, medicine, Progenitor cell, business.industry, Immunosuppression, hemic and immune systems, Immunotherapy, lymphopenia, radiation, Haematopoiesis, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Cancer research, Bone marrow, Stem cell, business, Research Paper

Abstract

The immune system plays a vital role in cancer therapy, especially with the advent of immunotherapy. Radiation therapy induces iatrogenic immunosuppression referred to as radiation-induced lymphopenia (RIL). RIL correlates with significant decreases in the overall survival of cancer patients. Although the etiology and severity of lymphopenia are known, the mechanism(s) of RIL are largely unknown. We found that irradiation not only had direct effects on circulating lymphocytes but also had indirect effects on the spleen, thymus, and bone marrow. We found that irradiated cells traffic to the bone marrow and bring about the reduction of hematopoietic stem cells (HSC) and progenitor cells. Using mass cytometry analysis (CyTOF) of the bone marrow, we found reduced expression of CD11a, which is required for T cell proliferation and maturation. RNA Sequencing and gene set enrichment analysis of the bone marrow cells following irradiation showed down-regulation of genes involved in hematopoiesis. Identification of CD11a and hematopoietic genes involved in iatrogenic immune suppression can help identify mechanisms of RIL.

Published

2020

18. Prognostic and predictive factors associated with ipilimumab-related adverse events: a retrospective analysis of 11 NCI-sponsored phase I clinical trials

Author

Jing Wei, Aman Chauhan, Jianrong Wu, Charles A. Kunos, Mary Cook, and Tanvir Kabir

Subjects

Oncology, medicine.medical_specialty, co-administered agents, business.industry, Incidence (epidemiology), toxicity, Cancer, Ipilimumab, medicine.disease, immune checkpoint inhibitors, Clinical trial, Cancer Therapy Evaluation Program, Internal medicine, Toxicity, Medicine, immunotherapy, Biostatistics, business, Adverse effect, Research Paper, metastatic melanoma, medicine.drug

Abstract

// Aman Chauhan 1 , Tanvir Kabir 2 , Jianrong Wu 3 , Jing Wei 4 , Mary Cook 1 and Charles A. Kunos 5 1 Division of Medical Oncology, University of Kentucky, Lexington, KY, USA 2 College of Medicine, University of Kentucky, Lexington, KY, USA 3 Markey Cancer Center, Biostatistics and Bioinformatics Shared Resource Facility, University of Kentucky, Lexington, KY, USA 4 Department of Statistics, University of Kentucky, Lexington, KY, USA 5 Cancer Therapy Evaluation Program, National Cancer Institute, Bethesda, MD, USA Correspondence to: Aman Chauhan, email: Aman.Chauhan@uky.edu Keywords: immunotherapy; toxicity; co-administered agents; metastatic melanoma; immune checkpoint inhibitors Received: December 16, 2019 Accepted: March 14, 2020 Published: April 21, 2020 ABSTRACT Background: We review factors impacting ipilimumab-associated adverse events through the experience from National Cancer Institute (NCI)-sponsored phase I immunotherapy clinical trials. Materials and Methods: Attributable ipilimumab-related adverse events from NCI-sponsored phase I immunotherapy clinical trials were queried retrospectively by anonymized patient experience reports for observed adverse events like decreased hematological cell counts, blood electrolytes or proteins, or reduced patient performance status. The prevalence of ipilimumab-related toxicity was associated by patient to the duration of ipilimumab exposure, radiographic responses, progression-free survival, and overall survival. Results: 373 patients from 11 phase 1 ipilimumab clinical trials were analyzed. Patients experiencing at least one grade 3 or 4 adverse event associated with observed radiographic response were included. The average number of grade 3/4 adverse events in responders was 1.167 versus 0.645 in non-responders ( p = 0.001). Patient performance status did not significantly impact observed toxicity grade. Pretherapy lymphocyte count or chemistries were not associated with ipilimumab-associated toxicity. The number of agents combined with ipilimumab on trial was associated with average number of grade 3/4 toxicities–ipilimumab monotherapy (0.631) versus ipilimumab + 1 agent (0.877) versus ipilimumab + 2 agents (1.408) ( p = 0.014). Number of low grade (grade 1/2) toxicities was associated with duration of treatment, Pearson correlation coefficient r = 0.456 ( p < 0.0001); whereas the number of high grade (grade 3/4) toxicities was not, r = 0.032 ( p = 0.546). Conclusions: Ipilimumab-attributed grade 3/4 toxicity was associated with therapeutic response. The number of co-administered agents added to ipilimumab significantly raised the likelihood of toxicity. Extended duration of treatment increased the incidence of low but not high-grade toxicity.

Published

2020

19. A phase II study of axalimogene filolisbac for patients with previously treated, unresectable, persistent/recurrent loco-regional or metastatic anal cancer

Author

Van K. Morris, Hope E. Uronis, Marwan Fakih, Patrick McKay Boland, Manik Amin, Howard S. Hochster, and Cathy Eng

Subjects

0301 basic medicine, medicine.medical_specialty, medicine.medical_treatment, Phases of clinical research, Disease, Malignancy, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, phase II clinical trial, Internal medicine, Clinical endpoint, medicine, Papillomaviridae, Adverse effect, anal neoplasms, papillomaviridae, biology, business.industry, Incidence (epidemiology), Immunotherapy, biology.organism_classification, medicine.disease, Listeria monocytogenes, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, immunotherapy, business, Research Paper

Abstract

Squamous cell carcinoma of the anorectal canal (SCCA) is a rare HPV-related malignancy that is steadily increasing in incidence. A high unmet need exists for patients with persistent loco-regional and metastatic disease. Axalimogene filolisbac (ADXS11-001) is an investigational immunotherapy that stimulates tumor-specific responses against HPV-associated cancers, and has demonstrated benefit in metastatic cervical cancer. We conducted this single-arm, multicenter, phase 2 trial in patients with persistent/recurrent, loco-regional or metastatic SCCA. Patients received ADXS11-001, 1 × 109 colony-forming units intravenously every 3 weeks. A Simon 2-stage design was used to test primary co-endpoints of overall response rate (ORR) and 6-month progression-free survival (PFS) rate. Study would proceed to full enrollment if ORR ≥ 10% or 6-month PFS rate ≥ 20%. Thirty-six patients were treated; 29 patients were evaluable for response. One patient had a prolonged partial response (3.4% ORR). The 6-month PFS rate was 15.5%. Grade 3 adverse event were noted in 10 patients, with the majority being cytokine-release symptoms; one grade 4 adverse event was noted. No grade 5 adverse events occurred. ADXS11-001 was safe and well-tolerated in patients with SCCA. However, this study did not meet either primary endpoint. ADXS11-001 may be more beneficial when administered in combination with other cytotoxic or targeted agents.

Published

2020

20. Targeting PI3Kβ alone and in combination with chemotherapy or immunotherapy in tumors with PTEN loss

Author

Argun Akcakanat, Filip Janku, Kurt W. Evans, Erkan Yuca, Ming Zhao, Ecaterina Ileana Dumbrava, Funda Meric-Bernstam, and Nicci Owusu-Brackett

Subjects

0301 basic medicine, medicine.medical_treatment, AZD8186, chemotherapy, PI3Kβ, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, In vivo, medicine, PTEN, Viability assay, PTEN loss, Chemotherapy, biology, Cell growth, Immunotherapy, 3. Good health, 030104 developmental biology, Oncology, Paclitaxel, chemistry, Apoptosis, 030220 oncology & carcinogenesis, Cancer research, biology.protein, immunotherapy, Research Paper

Abstract

Background: PTEN-deficient tumors are dependent on PI3Kβ activity, making PI3Kβ a compelling target. We evaluated the efficacy of PI3Kβ inhibitor AZD8186 on tumors with PTEN loss. Results: In vitro cell viability assay and immunoblotting demonstrated that PTEN loss was significantly correlated with AZD8186 sensitivity in triple negative breast cancer (TNBC) cell lines. Colony formation assay confirmed sensitivity of PTEN-deficient cell lines to AZD8186. AZD8186 inhibited PI3K signaling in PTEN loss TNBC cells. AZD8186 in combination with paclitaxel, eribulin had synergistic effects on growth inhibition in PTEN loss cells. AZD8186 promoted apoptosis in PTEN loss cells which was synergized by paclitaxel. In vivo, AZD8186 had limited activity as a single agent, but enhanced antitumor activity when combined with paclitaxel in MDA-MB-436 and MDA-MB-468 cell-line xenografts. AZD8186 significantly enhanced antitumor efficacy of anti-PD1 antibodies in the PTEN-deficient BP murine melanoma xenograft model, but not in the PTEN-wild-type CT26 xenograft model. Methods: In vitro, cell proliferation and colony formation assays were performed to determine cell sensitivity to AZD8186. Immunoblotting was performed to assess PTEN expression and PI3K signaling activity. FACS was performed to evaluate apoptosis. In vivo, antitumor efficacy of AZD8186 and its combinations were evaluated. Conclusions: AZD8186 has single agent efficacy in PTEN-deficient TNBC cell lines in vitro, but has limited single agent efficacy in vivo. However, AZD8186 has enhanced efficacy when combined with paclitaxel and anti-PD1 in vivo. Further study is needed to determine optimal combination therapies for PTEN-deficient solid tumors.

Published

2020

21. Identification of biomarkers of immune checkpoint blockade efficacy in recurrent or refractory solid tumor malignancies

Author

Michael T. Tetzlaff, Jiexin Zhang, Richard K. Yang, Mark J. Routbort, Kenna R. Mills Shaw, Russell Broaddus, Scott Kopetz, L. Jeffrey Medeiros, Yun Qing, Fatima Zahra Jelloul, Jack Lee, and Peng Wang

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, Multivariate analysis, medicine.drug_class, medicine.medical_treatment, Gene mutation, Monoclonal antibody, histology, 03 medical and health sciences, 0302 clinical medicine, Refractory, Internal medicine, Genotype, medicine, TMB, business.industry, biomarkers, Immunotherapy, mutations, Immune checkpoint, 3. Good health, Blockade, 030104 developmental biology, 030220 oncology & carcinogenesis, immunotherapy, business, Research Paper

Abstract

Patients with advanced solid malignancies recurrent or resistant to standard therapy have limited treatment options. The role of molecular biomarkers for predicting immune checkpoint blockade (ICB) efficacy are not well characterized in these patients. Tumor mutational profiles of 490 patients with a variety of advanced solid tumors enrolled in a prospective protocol were analyzed to identify prognostic and predictive biomarkers. ICB therapy was defined as treatment with any CTLA-4, PD-1, and/or PD-L1 monoclonal antibody. ICB treatment was associated with significantly improved overall survival compared to non-ICB therapy. Multivariate regression analysis including the two variables of tumor mutation burden (TMB) and ICB, and their interaction term, showed favorable survival associated with ICB, unfavorable survival associated with TMB without ICB treatment, and improved outcome with increasing TMB in ICB treated patients. Tumor TP53 mutation was associated with worse survival, but these patients still benefitted from ICB. A more comprehensive multivariate analysis including cancer type, specific gene mutations, and TMB revealed that ICB treatment was an independent predictor of improved overall survival. Therefore, ICB-based therapeutic trials are beneficial in patients with advanced solid malignancies, but the most benefit may be restricted to patients with the right combination of TMB and specific tumor histology and genotype.

Published

2020

22. Toxoplasma gondii GRA8-derived peptide immunotherapy improves tumor targeting of colorectal cancer

Author

Wooic Son, Chul-Su Yang, Daeun Lee, Seok-Jun Mun, Donggyu Kim, Jae-Sung Kim, and Euni Cho

Subjects

0301 basic medicine, SIRT3, business.industry, Immunogenicity, medicine.medical_treatment, tumor-targeting, Immunotherapy, Mitochondrion, mitochondria, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Toxoplasma gondii GRA8 peptide, Oncology, In vivo, 030220 oncology & carcinogenesis, Drug delivery, Cancer cell, Cancer research, medicine, business, Protein kinase A, metabolism, Research Paper

Abstract

// Jae-Sung Kim 1 , 2 , Daeun Lee 1 , Donggyu Kim 1 , Seok-Jun Mun 1 , 2 , Euni Cho 1 , 2 , Wooic Son 1 and Chul-Su Yang 1 , 2 1 Department of Molecular and Life Science, Hanyang University, Ansan 15588, S. Korea 2 Department of Bionano Technology, Hanyang University, Seoul 04673, S. Korea Correspondence to: Chul-Su Yang, email: chulsuyang@hanyang.ac.kr Keywords: Toxoplasma gondii GRA8 peptide; mitochondria; tumor-targeting; metabolism Received: October 17, 2019 Accepted: December 19, 2019 Published: January 07, 2020 ABSTRACT Targeted tumor and efficient, specific biological drug delivery in vivo has been one of the main challenges in protein-based cancer-targeted therapies. Mitochondria are potential therapeutic targets for various anti-cancer drugs. We have previously reported that protein kinase Cα-mediated phosphorylation of Toxoplasma gondii GRA8 is required for mitochondrial trafficking and regulating the interaction of the C-terminal of GRA8 with ATP5A1/SIRT3 in mitochondria. Furthermore, SIRT3 facilitates ATP5A1 deacetylation, mitochondrial activation, and subsequent antiseptic activity in vivo . Herein we developed a recombinant acidity-triggered rational membrane (ATRAM)-conjugated multifunctional GRA8 peptide (rATRAM-G8-M/AS) comprising ATRAM as the cancer-targeting cell-penetrating peptide, and essential/minimal residues for mitochondrial targeting or ATP5A1/SIRT3 binding. This peptide construct showed considerably improved potency about cancer cell death via mitochondria activity and biogenesis compared with rGRA8 alone in HCT116 human carcinoma cells, reaching an IC 50 value of up to 200-fold lower in vitro and 500-fold lower in vivo . Notably, rATRAM-G8-M/AS treatment showed significant therapeutic effects in a mouse xenograft model through mitochondrial metabolic resuscitation, and it produced negligible immunogenicity and immune responses in vivo . Thus, these results demonstrate that rATRAM-G8-M/AS represents a useful therapeutic strategy against tumors, particularly colon cancer. This strategy represents an urgently needed paradigm shift for therapeutic intervention.

Published

2020

23. EGFR806-CAR T cells selectively target a tumor-restricted EGFR epitope in glioblastoma

Author

Ali C. Ravanpay, Cindy A. Chang, Michelle Cecchini, Adam Johnson, Michael C. Jensen, Virginia Hoglund, Nicholas A Vitanza, Juliane Gust, Lisa S. Rolczynski, Rimas J. Orentas, and Rithun Mukherjee

Subjects

0301 basic medicine, mAb806, Chemistry, T cell, EGFR, glioblastoma, CAR T cell, medicine.disease, Chimeric antigen receptor, Epitope, Granzyme B, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Oncology, Antigen, 030220 oncology & carcinogenesis, Glioma, Cancer research, medicine, Cytokine secretion, immunotherapy, Induced pluripotent stem cell, Research Paper

Abstract

Targeting solid tumor antigens with chimeric antigen receptor (CAR) T cell therapy requires tumor specificity and tolerance toward variability in antigen expression levels. Given the relative paucity of unique cell surface proteins on tumor cells for CAR targeting, we have focused on identifying tumor-specific epitopes that arise as a consequence of target protein posttranslational modification. We designed a CAR using a mAb806-based binder, which recognizes tumor-specific untethered EGFR. The mAb806 epitope is also exposed in the EGFRvIII variant transcript. By varying spacer domain elements of the CAR, we structurally tuned the CAR to recognize low densities of EGFR representative of non-gene amplified expression levels in solid tumors. The appropriately tuned short-spacer 2nd generation EGFR806-CAR T cells showed efficient in vitro cytokine secretion and glioma cell lysis, which was competitively blocked by a short peptide encompassing the mAb806 binding site. Unlike the nonselective Erbitux-based CAR, EGFR806-CAR T cells did not target primary human fetal brain astrocytes expressing wild-type EGFR, but showed a similar level of activity compared to Erbitux-CAR when the tumor-specific EGFRvIII transcript variant was overexpressed in astrocytes. EGFR806-CAR T cells successfully treated orthotopic U87 glioma implants in NSG mice, with 50% of animals surviving to 90 days. With additional IL-2 support, all tumors were eradicate without recurrence after 90 days. In a novel human induced pluripotent stem cell (iPSC)-derived teratoma xenograft model, EGFR806-CAR T cells infiltrated but were not activated in EGFR+ epidermal cell nests as assessed by Granzyme B expression. These results indicate that EGFR806-CAR T cells effectively and selectively target EGFR-expressing tumor cells.

Published

2019

24. Hyperprogression of a mismatch repair-deficient colon cancer in a humanized mouse model following administration of immune checkpoint inhibitor pembrolizumab

Author

Zehra Ordulu, Andrew George, Kelsey E. Huntington, Ilyas Sahin, Lanlan Zhou, Wafik S. El-Deiry, and Shengliang Zhang

Subjects

cancer immunotherapy, biology, Colorectal cancer, business.industry, medicine.medical_treatment, hyperprogressive disease (HPD), Pembrolizumab, Immunotherapy, medicine.disease, Immune checkpoint, immune checkpoint inhibitors, Oncology, Cancer immunotherapy, Humanized mouse, biology.protein, medicine, Cancer research, Mdm2, Cytotoxic T cell, humanized mouse, hyperprogression (HP), business, Research Paper

Abstract

Immunotherapy is an established treatment modality in oncology. However, in addition to primary or acquired therapy resistance with immune checkpoint blockade (ICB), hyperprogressive disease (HPD) or hyperprogression (HP) with acceleration of tumor growth occurs in a subset of patients receiving ICB therapy. A validated and predictive animal model would help investigate HPD/HP to develop new approaches for this challenging clinical entity. Using human cytotoxic T-cell line TALL-104 injected intraperitoneally into immunodeficient NCRU-nude athymic mice bearing mismatch repair-deficient (MMR-d) human colon carcinoma HCT116 p53-null (but not wild-type p53) tumor xenograft, we observed accelerated tumor growth after PD-1 blockade with pembrolizumab administration. There was increased colon tumor cell proliferation as determined by immunohistochemical Ki67 staining of tumor sections. There was no increase in MDM2 or MDM4/MDMX in the p53-null HCT116 cells versus the wild-type p53-expressing isogenic tumor cells, suggesting the effects in this model may be MDM2 or MDM4/MDMX-independent. Human cytokine profiling revealed changes in IFN-γ, TRAIL-R2/TNFRSF10B, TRANCE/TNFSF11/RANK L, CCL2/JE/MCP-1, Chitinase 3-like 1, IL-4 and TNF-α. This represents a novel humanized HPD mouse model with a link to deficiency of the p53 pathway of tumor suppression in the setting of MMR-d. Our novel humanized preclinical TALL-104/p53-null HCT116 mouse model implicates p53-deficiency in an MMR-d tumor as a possible contributor to HPD/HP and may help with evaluating therapeutic strategies in cancer immunotherapy to extend clinical benefits of ICB's in a broader patient population.

Published

2021

25. Multipeptide stimulated PBMCs generate T

Author

Trupti, Vardam-Kaur, Latha B, Pathangey, Daniel J, McCormick, P Leif, Bergsagel, Peter A, Cohen, and Sandra J, Gendler

Subjects

multiple myeloma, CD4/CD8 T cells, peptides, cellular therapy, immunotherapy, Research Paper

Abstract

Multiple Myeloma (MM) patients suffer disease relapse due to the development of therapeutic resistance. Increasing evidence suggests that immunotherapeutic strategies can provide durable responses. Here we evaluate the possibility of adoptive cell transfer (ACT) by generating ex vivo T cells from peripheral blood mononuclear cells (PBMCs) isolated from MM patients by employing our previously devised protocols. We designed peptides from antigens (Ags) including cancer testis antigens (CTAs) that are over expressed in MM. We exposed PBMCs from different healthy donors (HDs) to single peptides. We observed reproducible Ag-specific cluster of differentiation 4+ (CD4+) and CD8+ T cell responses on exposure of PBMCs to different single peptide sequences. These peptide sequences were used to compile four different peptide cocktails. Naïve T cells from PBMCs from MM patients or HDs recognized the cognate Ag in all four peptide cocktails, leading to generation of multiclonal Ag-specific CD4+ and CD8+ effector and central memory T (TEM and TCM, respectively) cells which produced interferon-gamma (IFN-γ), granzyme B and perforin on secondary restimulation. Furthermore, this study demonstrated that immune cells from MM patients are capable of switching metabolic programs to induce effector and memory responses. Multiple peptides and cocktails were identified that induce IFN-γ+, T1-type, metabolically active T cells, thereby paving the way for feasibility testing of ACT in phase I clinical trials.

Published

2021

26. Evaluation of a ConvitVax/anti-PD-1 combined immunotherapy for breast cancer treatment

Author

Ana Federica Convit, Eglys González-Marcano, María José Godoy-Calderón, and Jeismar M. Carballo

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, medicine.medical_treatment, Cell, autologous tumor cells vaccine, 03 medical and health sciences, breast cancer, 0302 clinical medicine, Breast cancer, Cancer immunotherapy, Internal medicine, medicine, combination immunotherapies, cancer immunotherapy, business.industry, Anti pd 1, Immunotherapy, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, anti-PD-1, Immunohistochemistry, Tumor necrosis factor alpha, business, Infiltration (medical), Research Paper

Abstract

// Maria Jose Godoy-Calderon 1 , 2 , Eglys Gonzalez-Marcano 1 , 2 , Jeismar Carballo 2 and Ana Federica Convit 1 , 2 1 Unidad Experimental de Inmunoterapia, Fundacion Jacinto Convit, Caracas, Venezuela 2 Jacinto Convit World Organization, Inc., Palo Alto, CA, USA Correspondence to: Maria Jose Godoy-Calderon, email: publicaciones@jacintoconvit.org Keywords: combination immunotherapies; cancer immunotherapy; breast cancer; autologous tumor cells vaccine; anti-PD-1 Received: May 29, 2019 Accepted: September 24, 2019 Published: November 12, 2019 ABSTRACT Breast cancer therapies using checkpoints alone have not been highly effective. Based on previous experiences using the ConvitVax, an autologous tumor cells/bacillus Calmette-Guerin (BCG)/formalin-based vaccine, in breast cancer and the potential success of combined therapies, we sought to ascertain whether the ConvitVax combined with anti-PD-1 enhances the antitumor effect in a 4T1 breast cancer model. Animals received four weekly injections of either PBS (G1), ConvitVax (200 μg cell homogenate, 0.0625 mg BCG, 0.02% formalin) (G2), 50 μg anti-PD-1 (G3), or ConvitVax plus anti-PD-1 (200 μg cell homogenate, 0.0625 mg BCG, 0.02% formalin, 50 μg anti-PD-1) (G4). Five weeks post tumor induction all mice were euthanized, tumors extracted and evaluated pathologically and by immunohistochemistry. The combination group (G4) showed 10% more tumor necrosis, greater infiltration of PD-1 + cells and lower infiltration of TAMs, evidencing that the combination of ConvitVax and anti-PD-1 can improve the antitumor effect of the vaccine. Using a higher anti-PD-1 dose and administering each treatment at different times could further potentiate the effect of our therapy. Given the vaccine’s low cost and simple preparation, its use in combination with checkpoints or other target-specific compounds may lead to a highly effective personalized breast cancer immunotherapy.

Published

2019

27. Secretome of pleural effusions associated with non-small cell lung cancer (NSCLC) and malignant mesothelioma: therapeutic implications

Author

James D. Luketich, Vera S. Donnenberg, and Albert D. Donnenberg

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, Pleural effusion, medicine.medical_treatment, non-small cell lung cancer (NSCLC), Cell therapy, 03 medical and health sciences, 0302 clinical medicine, pleural effusion, Internal medicine, medicine, Mesothelioma, non-small cell lung cancer, IL-6, biology, business.industry, Cancer, Immunotherapy, medicine.disease, cytokines, Chimeric antigen receptor, respiratory tract diseases, 3. Good health, 030104 developmental biology, 030220 oncology & carcinogenesis, malignant mesothelioma, biology.protein, Antibody, business, Research Paper

Abstract

// Albert D. Donnenberg 1 , 2 , 3 , James D. Luketich 2 , 4 and Vera S. Donnenberg 2 , 3 , 4 1 University of Pittsburgh School of Medicine, Department of Medicine, Pittsburgh, PA, USA 2 UPMC Hillman Cancer Centers, Pittsburgh, PA, USA 3 McGowan Institute for Regenerative Medicine, Pittsburgh, PA, USA 4 University of Pittsburgh School of Medicine, Department of Cardiothoracic Surgery, Pittsburgh, PA, USA Correspondence to: Albert D. Donnenberg, email: donnenbergad@upmc.edu Vera S. Donnenberg, email: donnenbergvs@upmc.edu Keywords: pleural effusion; non-small cell lung cancer; malignant mesothelioma; cytokines; IL-6 Received: August 07, 2019 Accepted: September 24, 2019 Published: November 05, 2019 ABSTRACT Introduction: We compared the secretome of metastatic (non-small cell lung cancer (NSCLC)) and primary (mesothelioma) malignant pleural effusions, benign effusions and the published plasma profile of patients receiving chimeric antigen receptor T cells (CAR-T), to determine factors unique to neoplasia in pleural effusion (PE) and those accompanying an efficacious peripheral anti-tumor immune response. Materials and Methods: Cryopreserved cell-free PE fluid from 101 NSCLC patients, 8 mesothelioma and 13 with benign PE was assayed for a panel of 40 cytokines/chemokines using the Luminex system. Results: Profiles of benign and malignant PE were dominated by high concentrations of sIL-6Rα, CCL2/MCP1, CXCL10/IP10, IL-6, TGFβ1, CCL22/MDC, CXCL8/IL-8 and IL-10. Malignant PE contained significantly higher ( p < 0.01, Bonferroni-corrected) concentrations of MIP1β, CCL22/MDC, CX3CL1/fractalkine, IFNα2, IFNγ, VEGF, IL-1α and FGF2. When grouped by function, mesothelioma PE had lower effector cytokines than NSCLC PE. Comparing NSCLC PE and published plasma levels of CAR-T recipients, both were dominated by sIL-6Rα and IL-6 but NSCLC PE had more VEGF, FGF2 and TNFα, and less IL-2, IL-4, IL-13, IL-15, MIP1α and IFNγ. Conclusions: An immunosuppressive, wound-healing environment characterizes both benign and malignant PE. A dampened effector response (IFNα2, IFNγ, MIP1α, TNFα and TNFβ) was detected in NSCLC PE, but not mesothelioma or benign PE. The data indicate that immune effectors are present in NSCLC PE and suggest that the IL-6/sIL-6Rα axis is a central driver of the immunosuppressive, tumor-supportive pleural environment. A combination localized antibody-based immunotherapy with or without cellular therapy may be justified in this uniformly fatal condition.

Published

2019

28. Extramammary Paget disease shows differential expression of B7 family members B7-H3, B7-H4, PD-L1, PD-L2 and cancer/testis antigens NY-ESO-1 and MAGE-A

Author

Travis J. Hollmann, Maryam Pourmaleki, Jonathan H. Young, Marcia Edelweiss, Dennis S. Chi, Sarah Chiang, Lev Roshal, Ingo K. Mellinghoff, Klaus J. Busam, Yanyun Li, Nicholas D. Socci, and Mianlei Zhang

Subjects

0301 basic medicine, Surgical margin, medicine.medical_treatment, 03 medical and health sciences, 0302 clinical medicine, Antigen, PD-L1, cancer/testis antigens, medicine, B7 family, biology, business.industry, Cancer, Immunotherapy, medicine.disease, 3. Good health, extramammary paget disease, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Cancer/testis antigens, Adenocarcinoma, immunotherapy, NY-ESO-1, business, Research Paper, targetable molecules

Abstract

Extramammary Paget disease (EMPD) is a rare cutaneous adenocarcinoma of the anogenital region most commonly treated with surgical excision. Surgical margin clearance is often problematic and recurrence rates remain high indicating the need for additional therapeutic options. Topical immunomodulators have been used with reported success suggesting EMPD may respond to other immunotherapies. This study investigates EMPD protein expression of targetable B7 family members and cancer/testis antigens (CTAs) B7-H3, B7-H4, PD-L1, PD-L2, MAGE-A, and NY-ESO-1 and components of antigen presenting machinery B2M and MHC-I. Fifty-seven specimens from 48 patients (31 female and 17 male), representing in situ, invasive, and metastatic disease of primary and secondary origin were stained and scored (627 total slides). The percentage of cases expressing each immune regulatory molecule in the in situ followed by invasive tumor components was: B7-H3 (94, 90), B7-H4 (82, 78), PD-L1 (6, 10), MAGE-A (39, 50), NY-ESO-1 (16, 20), B2M (100, 89), and MHC-I (78, 79). PD-L2 was negative in all cases. There was high correlation between marker expression within the in situ and invasive tumor components of the same case. B7-H4 was preferentially expressed in primary cutaneous EMPD. Co-expression of B7 family members B7-H3 and B7-H4 was found within the in situ and invasive tumor components of 74% and 48% of cases, respectively. These findings provide an initial characterization of EMPD tumor cell expression of B7-H3, B7-H4, PD-L1, PD-L2, MAGE-A, and NY-ESO-1 and indicate the potential for new immunotherapeutic options for patients with EMPD.

Published

2019

29. Clinicopathological correlation of immune response in human cancers

Author

Yuexin Liu

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, medicine.medical_treatment, Clinicopathological correlation, immunogenicity, Spearman's rank correlation coefficient, immune response, Correlation, 03 medical and health sciences, 0302 clinical medicine, Immune system, Internal medicine, medicine, cancer, Immune gene, business.industry, Immunogenicity, clinicopathological characteristics, Histology, Immunotherapy, 3. Good health, 030104 developmental biology, 030220 oncology & carcinogenesis, business, Research Paper

Abstract

// Yuexin Liu 1 1 Department of Bioinformatics and Computational Biology, The University of Texas MD Anderson Cancer Center, Houston, Texas, USA Correspondence to: Yuexin Liu, email: yliu8@mdanderson.org Keywords: clinicopathological characteristics; immune response; immunogenicity; cancer Received: August 01, 2019 Accepted: September 24, 2019 Published: October 08, 2019 ABSTRACT Background: The clinicopathologic association of tumor immune response is largely unknown. We systematically investigated this matter in human cancers. Results: Different cancer types exhibited distinct immune gene profiling. Four cancer types exhibited a significant and positive correlation of immune response with patient age. Significant but inconsistent correlation of immune response was observed with gender, surgical stage, and TNM stage in a small number of cancer types. In contrast, the histological grade appears to have much stronger and more consistent association with immune response as compared to the other clinicopathologic factors. Specifically, patients with high grade had significantly higher immune responses than those with low grade in 5 out of 12 analyzed cancer types. In addition, both histological and molecular classifications had a significant and strong association with tumor immune response. Methods: t-distributed stochastic neighbor embedding was used to assess similarity of immune gene profiling in human cancers. The Mann-Whitney or Kruskal-Wallis test was, respectively, used to compare the tumor immune response in two or more groups that were stratified by patient clinicopathological characteristics, such as gender, grade, stage (including surgical and TNM stage), histology, and molecular subtypes. Spearman correlation with student’s t -test was used to examine the association of patient age with immune response. Multiple tests with the Benjamini-Hochberg correction also were performed. Conclusions: Tumor grade should be taken into account in selection of patient candidates for immunotherapy. Prospective verification is needed before use of the findings for clinical practice.

Published

2019

30. Oncologist uptake of comprehensive genomic profile guided targeted therapy

Author

Jeffrey M. Conroy, Grace K. Dy, Mateusz Opyrchal, Sean T. Glenn, Patrick McKay Boland, Antonios Papanicolau-Sengos, Mark Gardner, Shashikant Lele, S.N. Akers, Carl Morrison, Amy P. Early, Paul DePietro, Peter J. Frederick, Marc S. Ernstoff, Kunle Odunsi, Igor Puzanov, Hongbin Chen, Stephen B. Edge, Mary Nesline, Anne Grand'Maison, Felicia L. Lenzo, and Gurkamal Chatta

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, medicine.medical_treatment, clinical decision making, Targeted therapy, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Medical history, comprehensive genomic profiling, business.industry, Cancer, Immunotherapy, Guideline, targeted therapy, medicine.disease, real world data, 030104 developmental biology, 030220 oncology & carcinogenesis, Cohort, Genomic Profile, next-generation sequencing, business, Research Paper, Companion diagnostic

Abstract

We describe the extent to which comprehensive genomic profiling (CGP) results were used by oncologists to guide targeted therapy selection in a cohort of solid tumor patients tested as part of standard care at Roswell Park Comprehensive Cancer Center June 2016–June 2017, with adequate follow up through September 2018 (n = 620). Overall, 28.4% of CGP tests advised physicians about targeted therapy use supported by companion diagnostic or practice guideline evidence. Post-test targeted therapy uptake was highest for patients in active treatment at the time of order (86% versus 76% of treatment naïve patients), but also took longer to initiate (median 50 days versus 7 days for treatment naïve patients), with few patients (2.6%) receiving targeted agents prior to testing. 100% of patients with resistance variants did not receive targeted agents. Treatment naïve patients received immunotherapy as the most common alternative. When targeted therapy given off-label or in a trial was the best CGP option, (7%) of patients received it. Our data illustrate the appropriate and heterogeneous use of CGP by oncologists as a longitudinal treatment decision tool based on patient history and treatment needs, and that some patients may benefit from testing prior to initiation of other standard treatments.

Published

2019

31. The landscape of novel and complementary targets for immunotherapy: an analysis of gene expression in the tumor microenvironment

Author

Elizabeth B. Perry, Stephen G. Gaffney, Jeffrey P. Townsend, Ping-Min Chen, Susan M. Kaech, and Andrew E. Greenstein

Subjects

0301 basic medicine, cancer genomics, Tumor microenvironment, CD96, medicine.medical_treatment, Cancer, Immunotherapy, Biology, medicine.disease, Immune checkpoint, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Oncology, TIGIT, 030220 oncology & carcinogenesis, Gene expression, T lymphocyte, Cancer research, medicine, tumor microenvironment, immunotherapy, RNA-seq, Gene, Research Paper

Abstract

Background: Immunotherapies targeting immune checkpoint proteins CTLA-4, PD-1, and PD-L1 have saved lives, but these therapies have only been effective in some patients. Patients positive for expression of immune checkpoint proteins in the tumor microenvironment show better response to immune checkpoint inhibitors. Consequently, knowledge of which genes are consistently expressed in lymphocytes within the tumor microenvironment can convey potentially effective and complementary new immunotherapy targets. Results: We identified 54 genes that have higher co-expression with the pan T-cell marker CD3E than CTLA4 or PDCD1. In a dataset of 26 patients who received anti-PD-1 therapy, we observed that co-expression between CD3E and PDCD1 was higher among responders than non-responders, supporting our correlation-based approach. Conclusions: The genes highlighted in these analyses, which include CD6, TIGIT, CD96, and SLAMF6, warrant further investigation of their therapeutic potential. Methods: We analyzed and ranked genes that were co-expressed with the pan T-cell marker CD3E in 9,601 human tumors, spanning 31 cancer types. To further identify targets that may be complementary to existing PD-1 therapy, we examined and ranked genes with high CD3E co-expression and relatively low PDCD1 co-expression.

Published

2019

32. CD90low MSCs modulate intratumoral immunity to confer antitumor activity in a mouse model of ovarian cancer

Author

Richard T. Penson, Yang Zeng, Yanan Du, Mark C. Poznansky, Chongzhao Ran, Binghao Li, Huabiao Chen, Wei Liu, and Tao Li

Subjects

0301 basic medicine, mesenchymal stem cells, Tumor microenvironment, medicine.medical_treatment, Mesenchymal stem cell, Immunotherapy, Biology, CCL5, 3. Good health, CD90, 03 medical and health sciences, ovarian cancer, 030104 developmental biology, 0302 clinical medicine, Immune system, Cytokine, Oncology, 030220 oncology & carcinogenesis, TLR4, medicine, Cancer research, CXCL10, immunotherapy, Research Paper

Abstract

Both anti-tumoral and pro-tumoral effects of mesenchymal stem cells (MSCs) in preclinical treatment of ovarian cancer have been controversially demonstrated. In this study, we profiled the phenotypes of mouse compact bone-derived MSCs (CB-MSCs) and bone marrow-derived MSCs (BM-MSCs) and found that CB-MSCs expressed lower CD90 compared to BM-MSCs. We examined gene expression of immune regulating cytokines of CB-MSCs in 2D and 3D culture and under stimulation with TLR4 agonist LPS or immune activator VIC-008. Our data showed that when CB-MSCs were cultured in simulated in vivo 3D condition, CD90 expression was further decreased. Moreover, gene expressions of immune activating cytokines IL-12, IL-21, IFNγ and a pro-inflammatory cytokine CXCL10 in CB-MSCs were increased in 3D culture whereas gene expression of anti-inflammatory cytokines IL-10 and CCL5 were downregulated. Stimulation of CB-MSCs by LPS or VIC-008 presented similar profile of the cytokine gene expressions to that in 3D culture which might benefit the anti-tumor efficacy of CD90low MSCs. The anti-tumor effects of CD90low CB-MSCs alone or in combination with VIC-008 were evaluated in a syngeneic orthotopic mouse model of ovarian cancer. Treatment that combines CB-MSCs and VIC-008 significantly decreased tumor growth and prolonged mouse survival. This was associated with the increase of activated anti-tumoral CD4+ and CD8+ T cells and the decrease of Treg cells in the tumor microenvironment. Taken together, our study demonstrates the synergistic anti-tumoral efficacy by application of CB-MSCs combined with immune activator VIC-008 and provides new insight into CD90low MSCs as a new anti-tumor arsenal.

Published

2019

33. A DNA telomerase vaccine for canine cancer immunotherapy

Author

Pascal Clayette, Anne-Sophie Pailhes-Jimenez, Anna Kostrzak, Thomas Bestetti, Marion Julithe, Christine Kreuz, Simon Wain-Hobson, Pierre Langlade-Demoyen, Gabriel Chamel, Jessie Thalmensi, Christelle Liard, Emmanuèle Bourges, Ludovic Bourré, Elodie Pliquet, Marie Escande, Olivier Keravel, and Thierry Huet

Subjects

DNA vaccine, 0301 basic medicine, Telomerase, medicine.medical_treatment, DNA vaccination, 03 medical and health sciences, 0302 clinical medicine, Cancer immunotherapy, medicine, cancer, Telomerase reverse transcriptase, business.industry, Electro-Gene-Transfer, ELISPOT, Cancer, Immunotherapy, medicine.disease, 030104 developmental biology, Oncology, canine TERT, 030220 oncology & carcinogenesis, Cancer research, immunotherapy, Cancer vaccine, business, Research Paper

Abstract

Telomerase reverse transcriptase (TERT) is highly expressed in more than 90% of canine cancer cells and low to absent in normal cells. Given that immune tolerance to telomerase is easily broken both naturally and experimentally, telomerase is an attractive tumor associated antigen for cancer immunotherapy. Indeed, therapeutic trials using human telomerase peptides have been performed. We have developed an immunogenic yet catalytically inactive human telomerase DNA construct that is in clinical trials with patients presenting solid tumors. Paralleling this human construct, we have developed a canine telomerase DNA vaccine, called pDUV5. When administered intradermally to mice combined with electrogene transfer, pDUV5 induced canine TERT specific cytotoxic T-cells as measured by IFN-γ ELISpot assay. Intradermal vaccination of healthy dogs with 400 μg of pDUV5 generated strong, broad and long lasting TERT specific cellular immune responses. In vitro immunization with cTERT peptides revealed the maintenance of cTERT specific T-cells in PBMCs from tumor bearing dogs showing that this repertoire was not depleted. This study highlights the potential of pDUV5 as a cancer vaccine and supports its evaluation for the treatment of spontaneous canine tumors.

Published

2019

34. Phase I study of local radiation and tremelimumab in patients with inoperable locally recurrent or metastatic breast cancer

Author

Ben X. Wang, Pamela S. Ohashi, Anthony Fyles, Linh T. Nguyen, Di Maria Jiang, Srikala S. Sridhar, Adrian G. Sacher, Robert Rottapel, and Benjamin G. Neel

Subjects

0301 basic medicine, medicine.medical_specialty, medicine.medical_treatment, Peripheral blood mononuclear cell, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, breast cancer, Median follow-up, Internal medicine, medicine, business.industry, Immunotherapy, medicine.disease, Rash, Metastatic breast cancer, 3. Good health, radiation, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, anti-CTLA-4, Toxicity, immunotherapy, medicine.symptom, business, Tremelimumab, medicine.drug, Research Paper

Abstract

Immunotherapy has shown modest activity in metastatic breast cancer (MBC). In this phase I dose escalation study, we assessed safety of tremelimumab, a humanized anti-CTLA4 monoclonal antibody, at starting dose 3 mg/kg, on the third day of palliative radiotherapy (2000cGy in 5 daily fractions) in patients with MBC. Primary objective was to determine the maximum tolerated dose (MTD) of tremelimumab combined with RT. Secondary objective was to assess response. Among 6 patients enrolled between July 2010 and October 2011, 5 had hormone receptor-positive MBC, 1 had triple negative MBC. Median age was 45 years. Common toxicities included lymphopenia (83%), fatigue (50%) and rash (33%). One dose-limiting toxicity occurred at 6 mg/kg, however the trial closed before MTD could be determined. One patient discontinued treatment due to a pathological fracture. Best response was stable disease (SD), 1 patient had SD for >6 months. Median follow up was 27.0 months. Median OS was 50.8 months, with 1 patient surviving >8 years. Peripheral blood mononuclear cell (PBMC) profiles showed increasing proliferating (Ki67+) Treg cells 1 week post treatment in 5 patients. Overall, tremelimumab at 3 mg/kg combined with RT appears to be a tolerable treatment strategy. Further studies are needed to optimize this combination approach.

Published

2019

35. PD-L1 checkpoint blockade delivered by retroviral replicating vector confers anti-tumor efficacy in murine tumor models

Author

Anthony W. Munday, William P. Accomando, Cynthia Burrascano, Sophie Viaud, Daniel Mendoza, Marin V. Miner, Kader Yagiz, Leah Mitchell, Ali Haghighi, Amy H. Lin, Dawn Gammon, Harry E. Gruber, Douglas J. Jolly, Fernando Lopez Espinoza, Simon Bergqvist, Maria Rodriguez-Aguirre, and Andrew Hofacre

Subjects

PD-L1, 0301 basic medicine, medicine.drug_class, medicine.medical_treatment, chemical and pharmacologic phenomena, Monoclonal antibody, 03 medical and health sciences, 0302 clinical medicine, Immune system, PD-1, medicine, Single-chain variable fragment, Vector (molecular biology), biology, business.industry, Immunotherapy, single chain variable fragment, retroviral replicating vector, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer cell, biology.protein, Cancer research, immunotherapy, Antibody, business, Research Paper

Abstract

Immune checkpoint inhibitors (CPIs) are associated with a number of immune-related adverse events and low response rates. We provide preclinical evidence for use of a retroviral replicating vector (RRV) selective to cancer cells, to deliver CPI agents that may circumvent such issues and increase efficacy. An RRV, RRV-scFv-PDL1, encoding a secreted single chain variable fragment targeting PD-L1 can effectively compete with PD-1 for PD-L1 occupancy. Cell binding assays showed trans-binding activity on 100% of cells in culture when infection was limited to 5% RRV-scFv-PDL1 infected tumor cells. Further, the ability of scFv PD-L1 to rescue PD-1/PD-L1 mediated immune suppression was demonstrated in a co-culture system consisting of human-derived immune cells and further demonstrated in several syngeneic mouse models including an intracranial tumor model. These tumor models showed that tumors infected with RRV-scFv-PD-L1 conferred robust and durable immune-mediated anti-tumor activity comparable or superior to systemically administered anti-PD-1 or anti PD-L1 monoclonal antibodies. Importantly, the nominal level of scFv-PD-L1 detected in serum is ∼50-150 fold less than reported for systemically administered therapeutic antibodies targeting immune checkpoints. These results support the concept that RRV-scFv-PDL1 CPI strategy may provide an improved safety and efficacy profile compared to systemic monoclonal antibodies of currently approved therapies.

Published

2019

36. Characterization of CD4+ T cells primed and boosted by MHCII primary uveal melanoma cell-based vaccines

Author

Margarete M Karg, Barbara Bock, Ludwig M. Heindl, Jonas Sommer, Anika Fischer, Jacobus J. Bosch, Imke Atreya, Sabine Britting, Andreas Mackensen, and Julia M Kittler

Subjects

0301 basic medicine, ICAM-1, Lymphocyte, medicine.medical_treatment, T cell, Melanoma Vaccine, 03 medical and health sciences, 0302 clinical medicine, Antigen, Medicine, Antigen-presenting cell, business.industry, T cell activation, FOXP3, Immunotherapy, CD4+ T cells, tumor immunity, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Cancer research, uveal melanoma, business, CD80, Research Paper

Abstract

Uveal melanoma is the most common primary malignancy of the eye in adults. Despite significant improvements in treatment of the primary tumor, to date none of these therapies prevent metastatic disease or improve overall survival. We are exploring immunotherapeutic options for metastatic uveal melanoma using MHC II uveal melanoma cell-based vaccines that target the activation of tumor-reactive CD4+ T cells. Previously, we showed that these uveal melanoma cell-based vaccines activate CD4+ T cells within total peripheral blood lymphocytes (PBMC). Since PBMC include professional antigen presenting cells, we now demonstrate that Mel202/DR1/CD80 vaccine cells directly activate a diverse repertoire of purified, naive CD4+ T cells. The activated CD4+ T cells proliferated, secreted high amounts of interferon gamma (IFNγ) and produced a heterogeneous profile of Th1, Th2 and Th17 cytokines. Analysis of the TCR-Vβ-repertoire showed that a polyclonal T cell response was induced, suggesting the capacity of vaccine-activated CD4+ T cells to target multiple tumor (neo)antigens. In addition, a subset of the responding CD4+ T cells expressed forkhead box protein P3 (FoxP3), indicating that although a regulatory component of the vaccine-activated CD4+ T cell response was induced, the anti-tumor vaccine response was not limited by these regulatory CD4+ T cells. Finally, Mel202/DR1/CD80 uveal melanoma vaccine cells expressed the intercellular adhesion molecule 1 (ICAM-1) that was pivotal for CD4+ T cell activation via lymphocyte function-associated antigen 1(LFA-1). In conclusion, MHC II uveal melanoma vaccines activate purified CD4+ T cells and may serve as a novel immunotherapy for uveal melanoma patients.

Published

2019

37. The immune checkpoint molecules PD-1, PD-L1, TIM-3 and LAG-3 in diffuse large B-cell lymphoma

Author

Hong Chang, Pallavi Galera, Andrew M. Evens, Vladislav V. Makarenko, Ravi Dashnamoorthy, Srimoyee Ghosh, and Benjamin J. Chen

Subjects

0301 basic medicine, medicine.medical_treatment, TIM-3, lymphoma, 03 medical and health sciences, 0302 clinical medicine, International Prognostic Index, LAG-3, medicine, immune checkpoint, Tumor microenvironment, business.industry, Tumor-infiltrating lymphocytes, Cancer, Immunotherapy, medicine.disease, Immune checkpoint, Lymphoma, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, immunotherapy, business, Diffuse large B-cell lymphoma, Research Paper

Abstract

Signaling through immune checkpoint receptors may lead to T-cell exhaustion and function as immune escape mechanisms in cancer. For diffuse large B-cell lymphoma (DLBCL), the mechanistic and prognostic importance of these markers on tumor cells and the tumor microenvironment remains unclear. We determined the immunohistochemical expression of PD-1, PD-L1, TIM-3, and LAG-3 on tumor cells and on tumor infiltrating lymphocytes (TILs) among 123 DLBCL patients. TIM-3 showed positive staining on tumor cells in 39% of DLBCL cases and PD-L1 expression was noted in 15% of cases. Both PD-1 and LAG-3 were positive on tumor cells in a minority of DLBCL cases (8.3% and 7.5%, respectively), but were more widely expressed on TILs in a correlated manner. With median follow-up of 44 months (n = 70, range 5-85), 4-year progression-free survival (PFS) and overall survival (OS) rates were significantly inferior among DLBCL patients with high vs low/negative TIM-3 expression (PFS: 23% [95% CI 7% to 46%] vs 60% [95% CI 43% to 74%], respectively, P = 0.008; OS: 30% [95% CI 10% to 53%] vs 74% [95% CI 58% to 85%], respectively, P = 0.006). Differences in OS remained significant when controlling for International Prognostic Index in Cox regression analyses (HR 3.49 [95% CI 1.40-6.15], P = 0.007). In addition, we observed that co-culture of DLBCL cell lines with primed T cells in the presence of anti-LAG-3 and anti-TIM-3 induced potent dose-dependent increases in in vitro cell death via AcellaTox and IL-2 ELISA assays, suggesting potent anti-tumor activity of these compounds.

Published

2019

38. Co-inhibitory T cell receptor KLRG1: human cancer expression and efficacy of neutralization in murine cancer models

Author

Evan Thompson, Steven A. Greenberg, Stefano V. Gulla, and Sek Won Kong

Subjects

0301 basic medicine, KLRG1, Colorectal cancer, medicine.medical_treatment, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, medicine, Cytotoxic T cell, biology, business.industry, Cancer, Immunotherapy, medicine.disease, Immune checkpoint, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, co-inhibitory receptor, murine cancer models, Cancer research, biology.protein, immunotherapy, Antibody, business, CD8, immune checkpoint receptor, Research Paper

Abstract

// Steven A. Greenberg 1, 2 , Sek Won Kong 2, 3 , Evan Thompson 4 and Stefano V. Gulla 4 1 Department of Neurology, Brigham and Women’s Hospital and Harvard Medical School, Boston, MA, USA 2 Computational Health Informatics Program, Boston Children’s Hospital, Boston, MA, USA 3 Department of Pediatrics, Harvard Medical School, Boston, MA, USA 4 Abcuro, Inc., Newton, MA, USA Correspondence to: Steven A. Greenberg, email: sagreenberg@bwh.harvard.edu Keywords: immune checkpoint receptor; immunotherapy; KLRG1; co-inhibitory receptor; murine cancer models Received: December 12, 2018 Accepted: January 21, 2019 Published: February 15, 2019 ABSTRACT Background: KLRG1 is a lymphocyte co-inhibitory, or immune checkpoint, receptor expressed predominantly on late-differentiated effector and effector memory CD8+ T and NK cells. Targeting of KLRG1 neutralization in murine cancer models has not previously been reported. Methods: We studied KLRG1 expression in human blood and tumor samples from available genomic datasets. Anti-KLRG1 neutralizing antibody was studied in the murine 4T1 breast cancer as monotherapy, and in the MC38 colon cancer and B16F10 melanoma models as combination therapy with anti-PD-1 antibody. Results: In human blood and tumor samples, KLRG1 expression is aligned with cytotoxic T and NK cell differentiation, and upregulated in human tumor samples after a variety of therapies, potentially contributing to adaptive resistance. In in vivo murine models, anti-KLRG1 antibody monotherapy in the 4T1 breast cancer model reduced lung metastases (decreased lung weights p=0.04; decreased nodule count p=0.002), while anti-KLRG1 + anti-PD-1 combination therapy in the MC38 colon cancer and B16F10 melanoma models produced synergistic benefit greater than anti-PD-1 alone for tumor volume (MC38 p=0.01; B16F10 p=0.007) and survival (MC38 p=0.02; B16F10 p=0.002). Conclusions: These studies provide the first evidence that inhibition of the KLRG1 pathway enhances immune control of cancer in murine models, and provide target validation for KLRG1 targeting of human cancer. The mechanism of efficacy of KLRG1 blockade in murine models remains to be determined.

Published

2019

39. Immune response characterization of endometrial cancer

Author

Yuexin Liu

Subjects

0301 basic medicine, medicine.medical_treatment, Biology, immune response, 03 medical and health sciences, 0302 clinical medicine, Immune system, tumor-infiltrating lymphocyte, Gene expression, medicine, STAT1, Tumor-infiltrating lymphocytes, Endometrial cancer, Immunotherapy, Gene signature, medicine.disease, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, endometrial cancer, Cancer research, biology.protein, prognosis, immunotherapy, Signal transduction, Research Paper

Abstract

Background The comprehensive characterization and prognostic relevance of immune activation in endometrial cancer remain largely unknown. Results We systematically reported a subset of endometrioid-type endometrial cancer characterized by multifaceted immune features such as low tumor purity, high leukocyte percentage, and striking CD8 lymphocytic infiltration with anti-tumor efficacy along with marked upregulation of immunosuppressive gene markers. We also showed that genes whose expression was significantly correlated with better survival were significantly enriched in the immune-related signaling pathways, suggesting that tumor-infiltrating lymphocytes give rise to a favorable prognosis in endometrial cancer. Furthermore, we showed that immune cell recruitment in this subset of tumors is likely due to the transcriptional activation of the STAT1 signaling network. Methods We obtained the multi-dimensional genomic data from publicly available databases and correlated them with the four gene expression-based subtypes we recently identified in endometrial cancer. Upstream regulator analysis was used to identify the most significantly enriched transcription regulators and Ingenuity pathway analysis was applied to determine enrichment of signaling pathways in survival-associated genes. Gene set enrichment analysis was performed on the 200-gene T-cell tumor infiltration gene signature comparing Cluster IV with the other three clusters combined. All statistical tests were two-sided, and a P value of less than 0.05 is considered significant across all analyses performed. Conclusion This study helps to identify patients with immune activation who are likely to benefit from emerging immune checkpoint inhibitors.

Published

2019

40. Accurate diagnosis of mismatch repair deficiency in colorectal cancer using high-quality DNA samples from cultured stem cells

Author

Fumihiko Kakizaki, Takehito Yamamoto, Tadayoshi Yamaura, Tomonori Morimoto, Hiroyuki Miyoshi, Koichiro Higasa, Fumihiko Matsuda, Yoshiharu Sakai, Hisatsugu Maekawa, Makoto Mark Taketo, and Kenji Kawada

Subjects

cancer stem cell, education.field_of_study, business.industry, Colorectal cancer, Population, Cancer, Microsatellite instability, colorectal cancer, medicine.disease, Primary tumor, digestive system diseases, Lynch syndrome, molecular oncology, Oncology, spheroid, Cancer stem cell, Cancer research, Medicine, DNA mismatch repair, immunotherapy, business, education, Research Paper

Abstract

Mismatch repair (MMR)-deficient or microsatellite instability (MSI) colorectal cancer includes two subtypes; Lynch syndrome and sporadic MSI cancer, both of which generate multiple neoantigens due to unrepaired mutations. Although such patients respond very well to immune checkpoint therapy, their diagnosis can be confused by low quality DNA samples owing to formalin fixation and/or low cancer cell content. Here we prepared high-quality DNA samples from in vitro-cultured cancer spheroids that consisted of the pure cell population. We evaluated their diagnostic power by on-chip electrophoresis, mutational burden assessment, and direct sequencing. Because formalin-fixed paraffin-embedded (FFPE) tissues are widely used as the DNA source, we compared such samples with spheroid DNA. Additionally, we performed immunohistochemistry (IHC) for MMR proteins on spheroids as well as primary tumor sections. Of 111 cases of colorectal cancer patients, we found seven MSI-high cases in which all diagnostic results agreed on spheroid-based assays, whereas the results with the FFPE DNA were less reliable though analyzable. Importantly, there was an MSS case that appeared as MSI by IHC on primary tumor sections. Based on these results, we propose to employ cultured cancer spheroids as the source of both DNA and IHC specimens for more reliable clinical diagnosis.

Published

2018

41. Human papilloma virus circulating tumor DNA assay predicts treatment response in recurrent/metastatic head and neck squamous cell carcinoma

Author

Molly E. Heft Neal, Francis P. Worden, Collin Brummel, Emily Bellile, Mark E. Prince, Ryan M. Spengler, Matthew E. Spector, Erin Sandford, Chandan Bhambhani, Muneesh Tewari, Catherine T. Haring, J. Chad Brenner, Paul L. Swiecicki, Brittany M. Jewell, Michelle Mierzwa, Apurva D. Bhangale, and Jonathan B. McHugh

Subjects

Oncology, circulating tumor DNA, medicine.medical_specialty, HPV, business.industry, oropharyngeal cancer, medicine.medical_treatment, Head and neck cancer, Disease, Immunotherapy, ctDNA, medicine.disease, Head and neck squamous-cell carcinoma, Clinical trial, Circulating tumor DNA, Tumor progression, Internal medicine, medicine, Digital polymerase chain reaction, head and neck cancer, business, Research Paper

Abstract

Despite the rising incidence of human papillomavirus related (HPV+) oropharyngeal squamous cell carcinoma (OPSCC), treatment of metastatic disease remains palliative. Even with new treatments such as immunotherapy, response rates are low and can be delayed, while even mild tumor progression in the face of an ineffective therapy can lead to rapid death. Real-time biomarkers of response to therapy could improve outcomes by guiding early change of therapy in the metastatic setting. Herein, we developed and analytically validated a new droplet digital PCR (ddPCR)-based assay for HPV16 circulating tumor DNA (ctDNA) and evaluated plasma HPV16 ctDNA for predicting treatment response in metastatic HPV+ OPSCC. We found that longitudinal changes HPV16 ctDNA correlate with treatment response and that ctDNA responses are observed earlier than conventional imaging (average 70 days, range: 35-166). With additional validation in multi-site studies, this assay may enable early identification of treatment failure, allowing patients to be directed promptly toward clinical trials or alternative therapies.

Published

2021

42. Discovery of peptide inhibitors targeting human programmed death 1 (PD-1) receptor

Author

Li Qiao, Xia Wang, Jiankun Lyu, Honglin Li, Xiaofeng Liu, Jiajia Meng, Lili Zhu, Zhenjiang Zhao, Quan Lina, and Zenghui He

Subjects

0301 basic medicine, T-Lymphocytes, medicine.medical_treatment, Programmed Cell Death 1 Receptor, Peptide, Lymphocyte Activation, Jurkat cells, B7-H1 Antigen, Jurkat Cells, 03 medical and health sciences, Cancer immunotherapy, medicine, Humans, Molecular Targeted Therapy, Receptor, chemistry.chemical_classification, human programmed death 1, peptide inhibitor, protein-protein interactions (PPIs), business.industry, Carcinoma, Peptide inhibitor, Computational Biology, Immunotherapy, Surface Plasmon Resonance, HCT116 Cells, Ligand (biochemistry), de novo peptide design, 030104 developmental biology, Oncology, chemistry, Immunology, Cancer research, immunotherapy, Programmed death 1, Peptides, business, Protein Binding, Signal Transduction, Research Paper

Abstract

// Qiao Li 1, * , Lina Quan 1, * , Jiankun Lyu 1 , Zenghui He 1 , Xia Wang 1 , Jiajia Meng 1 , Zhenjiang Zhao 1 , Lili Zhu 1 , Xiaofeng Liu 1 , Honglin Li 1 1 State Key Laboratory of Bioreactor Engineering, Shanghai Key Laboratory of New Drug Design, School of Pharmacy, East China University of Science and Technology, Shanghai, 200237, China * These Authors contributed equally to this work Correspondence to: Lili Zhu, email: zhulfl@ecust.edu.cn Xiaofeng Liu, email: xxffliu@gmail.com Honglin Li, email: hlli@ecust.edu.cn Keywords: immunotherapy, human programmed death 1, peptide inhibitor, protein-protein interactions (PPIs), de novo peptide design Received: June 06, 2016 Accepted: July 29, 2016 Published: August 12, 2016 ABSTRACT Blocking the interaction of human programmed death 1 (hPD-1) and its ligand hPD-L1 has been a promising immunotherapy in cancer treatment. In this paper, using a computational de novo peptide design method, we designed several hPD-1 binding peptides. The most potent peptide Ar5Y_4 showed a KD value of 1.38 ± 0.39 μM, comparable to the binding affinity of the cognate hPD-L1. A Surface Plasmon Resonance (SPR) competitive binding assay result indicated that Ar5Y_4 could inhibit the interaction of hPD-1/hPD-L1. Moreover, Ar5Y_4 could restore the function of Jurkat T cells which had been suppressed by stimulated HCT116 cells. Peptides described in this paper provide promising biologic candidates for cancer immunotherapy or diagnostics.

Published

2016

43. Predictors of immunotherapy benefit in Merkel cell carcinoma

Author

Gabriel J. Starrett, Manisha Thakuria, Glenn J. Hanna, Harita Dharaneeswaran, Ann W. Silk, James A. DeCaprio, Nicole R. LeBoeuf, and Alec Kacew

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, medicine.medical_treatment, precision medicine, Merkel cell polyomavirus, Disease, 03 medical and health sciences, 0302 clinical medicine, Merkel cell carcinoma, Internal medicine, medicine, genomics, cancer, Stage (cooking), biology, business.industry, Cancer, Odds ratio, Immunotherapy, biology.organism_classification, medicine.disease, Confidence interval, 030104 developmental biology, 030220 oncology & carcinogenesis, immunotherapy, business, Research Paper

Abstract

Merkel cell carcinoma is a rare cancer for which immune checkpoint blockade is standard-of-care for recurrent/metastatic disease. However, not all patients benefit from immunotherapy. A greater understanding of molecular mechanisms and predictive biomarkers are unmet needs. We retrospectively analyzed electronic health records and next-generation sequencing data of 45 patients treated at our institution from 2013 to 2020 to understand clinical and genomic correlates of benefit from immunotherapy. Our cohort predominantly included individuals with stage III disease at primary disease diagnosis and individuals with stage IV disease at recurrent/metastatic disease diagnosis. Most received immunotherapy as first-line treatment. 43% experienced objective response (median duration of response 24.2 months, 95% confidence interval 8.8-not reached). Median overall survival was 15.5 months (95% confidence interval 9.0-28.7) (median follow-up 25.2 months). Less advanced stage at primary disease diagnosis and shorter disease-free interval between completion of initial treatment and recurrence were each associated with greater odds of response (odds ratio of 0.06, p = 0.04 for stage; odds ratio 0.75, p = 0.05 for disease-free interval). Single-nucleotide variants in ARID2 and NTRK1 were associated with response (p = 0.05, without Bonferroni correction), while none of Merkel cell polyomavirus status, total mutational burden, ultraviolet mutational signatures, and copy-number alterations predicted outcomes. Patients with shorter disease-free interval may be particularly suitable immunotherapy candidates. Our molecular findings point to ARID2 and NTRK1 as potential predictive markers and/or therapeutic targets (e.g., with Trk inhibitors), although this association needs to be confirmed in a larger sample.

Published

2020

44. Immunotherapy of ovarian cancer with a monoclonal antibody specific for the extracellular domain of anti-Müllerian hormone receptor II

Author

Valerie Swank, Suparna Mazumder, Justin M. Johnson, Anton A. Komar, and Vincent K. Tuohy

Subjects

0301 basic medicine, Programmed cell death, endocrine system diseases, medicine.drug_class, medicine.medical_treatment, anti-Müllerian hormone receptor type II, Monoclonal antibody, 03 medical and health sciences, 0302 clinical medicine, Anti-Müllerian hormone receptor, medicine, Caspase, biology, business.industry, Immunotherapy, 4D12G1, medicine.disease, female genital diseases and pregnancy complications, ovarian cancer, 030104 developmental biology, Oncology, monoclonal antibody, Hormone receptor, Apoptosis, 030220 oncology & carcinogenesis, biology.protein, Cancer research, immunotherapy, business, Ovarian cancer, Research Paper

Abstract

Epithelial ovarian carcinoma (EOC) is the most prevalent and lethal form of ovarian cancer. The low five-year overall survival after EOC diagnosis indicates an urgent need for more effective ways to control this disease. Anti-Müllerian hormone receptor 2 (AMHR2) is an ovarian protein overexpressed in the majority of human EOCs. We have previously found that vaccination against the ovarian-specific extracellular domain of AMHR2 (AMHR2-ED) significantly inhibits growth of murine EOCs through an IgG-mediated mechanism that agonizes receptor signaling of a Bax/caspase-3 dependent proapoptotic cascade. To determine if a single monoclonal antibody (mAb) could inhibit growth of human EOC, we generated a panel of mAbs specific for recombinant human AMHR2-ED and characterized a candidate mAb for humanization and use in clinical trials. We found that our candidate 4D12G1 mAb is an IgG1 that shows high affinity antigen-specific binding to the 7-mer 20KTLGELL26 sequence of AMHR2-ED that facilitates induction of programmed cell death in EOC cells. Most importantly, the 4D12G1 mAb significantly inhibits growth of primary human EOCs in patient-derived xenografts (PDXs) by inducing direct apoptosis of EOC tumors. Our results support the view that a humanized 4D12G1 mAb may be a much needed and effective reagent for passive immunotherapy of human EOC.

Published

2020

45. First-in-human study of anticancer immunotherapy drug candidate mobilan: safety, pharmacokinetics and pharmacodynamics in prostate cancer patients

Author

Vasily I Kazey, Natalia V Eremina, Sergey V Mishugin, Roman V Leonenkov, Vadim L. Mett, Dmitry Pushkar, and Andrei V. Gudkov

Subjects

0301 basic medicine, medicine.medical_treatment, Metastasis, intratumor injection, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Immune system, Prostate, medicine, business.industry, Immunotherapy, prostate cancer, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, Cytokine, Oncology, TLR5, adenoviral vector, 030220 oncology & carcinogenesis, Pharmacodynamics, Cancer research, immunotherapy, business, mobilan, Research Paper

Abstract

Toll-like receptor 5 (TLR5) controls endogenous immune responses to pathogens and is a promising target for pharmacological stimulation of anti-tumor immunity. Mobilan is an innovative gene therapy agent consisting of a non-replicating bicistronic adenovirus directing constitutive expression of human Toll-like receptor 5 (TLR5) and the secreted flagellin-based TLR5 agonist, 502s. In mice, Mobilan injection into prostate tumors resulted in autocrine TLR5 signaling, immune system activation, and suppression of tumor growth and metastasis. Here we report a first-in-human placebo-controlled clinical study of Mobilan aimed at evaluating safety, tolerability, pharmacokinetics and pharmacodynamics of a single intra-prostate injection of Mobilan in early stage prostate cancer patients. Mobilan was safe and well-tolerated at all tested doses; thus, the maximum tolerated dose was not identified. Injection of Mobilan induced signs of self-resolving inflammation not present in placebo-injected patients, including transient elevation of PSA and cytokine (G-CSF, IL-6) levels, and increased lymphoid infiltration in prostate tissue. The highest dose of Mobilan (1011 viral particles) produced the best combination of safety and pharmacodynamic effects. Therefore, Mobilan is well-tolerated and induces the expected pharmacodynamic response in humans. These results support further clinical development of Mobilan as a novel immunotherapy for prostate cancer.

Published

2020

46. Extremely strong infiltration of WT1-specific CTLs into mouse tumor by the combination vaccine with WT1-specific CTL and helper peptides

Author

Haruo Sugiyama, Yoshihiro Oka, Naoki Hosen, Daisuke Motooka, Fumihiro Fujiki, Atsushi Kumanogoh, Daisuke Okuzaki, Akihiro Tsuboi, Jun Nakata, Yusuke Oji, Kana Hasegawa, Hiromu Hayashibara, Kanako Imafuku, Hiroko Nakajima, and Soyoko Morimoto

Subjects

medicine.medical_treatment, Priming (immunology), urologic and male genital diseases, 03 medical and health sciences, 0302 clinical medicine, wilms tumor 1 (WT1), medicine, Cytotoxic T cell, biology, Chemistry, urogenital system, CD44, resident memory T cells (TRM), Immunotherapy, female genital diseases and pregnancy complications, CTL, helper vaccine, Oncology, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Peptide vaccine, tumor infiltrating lymphocytes (TIL), Cancer vaccine, cancer vaccine, CD8, 030215 immunology, Research Paper

Abstract

In immunotherapy by cancer antigen-derived peptide vaccine, vaccination of cytotoxic T lymphocyte (CTL) peptide alone is common, while it remains unclear whether the addition of helper peptide vaccine to the CTL peptide vaccine is of great advantage for the enhancement of tumor immunity. In the present study, combination vaccine of Wilms' tumor gene 1(WT1) protein-derived CTL and helper peptides induced the strong infiltration of WT1-specific CD8+ T cells into mouse tumor at frequencies of 8.8%, resulting in the formation of multiple microscopic necrotic lesions in the tumor, whereas the frequencies of WT1-specific CD8+ T cell infiltration into the tumor in the vaccination of the CTL peptide alone were only 0.32%. The majority of the infiltrated WT1-specific CD8+ T cells was effector phenotype T cells, but importantly, WT1-specific CD8+CD44+CD62L+CD103+ resident memory T cells, which could differentiate into a lot of effector phenotype T cells, existed in the tumor of mice vaccinated with the both WT1 peptides. Furthermore, T-cell receptor repertoire analysis showed the oligoclonality of these tumor infiltrating WT1 tetramer+ CD8+ T cells, and 3 clones occupied about half of them. These results indicated that WT1-specific CD4+ T cells played an essential role not only in the priming and activation of WT1-specific CD8+ T cells, but also in trafficking and infiltration of the CD8+ T cells into tumors. These results should provide us with the concept that in the clinical setting, combination vaccine of WT1-specific CTL and helper peptides would be more advantageous than the CTL peptide vaccine alone.

Published

2018

47. Enhanced expression of PD-L1 in non-muscle-invasive bladder cancer after treatment with Bacillus Calmette-Guerin

Author

Takeshi Kishida, Mitsuyo Yoshihara, Tetsuro Sasada, Kahori Shoji, Susumu Umemoto, Yoshiyasu Nakamura, Satoshi Wada, Yohei Miyagi, Akihito Hashizume, and Tomoyuki Yokose

Subjects

PD-L1, medicine.medical_treatment, 030232 urology & nephrology, 03 medical and health sciences, 0302 clinical medicine, medicine, immune checkpoint, Bacillus Calmette-Guerin, Bladder cancer, Tissue microarray, biology, business.industry, CD8, Immunotherapy, medicine.disease, Immune checkpoint, Oncology, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Immunohistochemistry, Antibody, business, non-muscle-invasive bladder cancer, Research Paper

Abstract

Immune checkpoint molecules, such as PD-1/PD-L1, are reported to be closely associated with suppression of antitumor immunity, and their inhibitors have been used to treat various cancers including bladder cancer. However, there have been only a few studies investigating the effects of Bacillus Calmette-Guerin (BCG) administration on expression of the immune checkpoint molecules in bladder cancer. The current study examined the expression of PD-L1 and PD-L2 before and after BCG in non-muscle-invasive bladder cancer (NMIBC) patients. Tissue microarrays of 22 BCG-resistant NMIBC patients were stained by immunohistochemistry with antibodies against PD-L1, PD-L2, and CD8, and were compared between before and after BCG. The expression levels of PD-L1, but not of PD-L2, were significantly increased after BCG treatment on tumor cells (p < 0.001) and tumor-infiltrating inflammatory cells (p = 0.030) within tumor tissues, as well as on inflammatory cells within non-tumor normal tissues (p = 0.003). Although CD8+ T cells were significantly increased within tumor tissues (p = 0.005) and non-tumor normal tissues (p = 0.007) after BCG treatment, they might be not effective for anti-tumor immunity. This study demonstrated for the first time that expression of PD-L1, which might contribute to the immune escape mechanism, was enhanced on tumor tissue after BCG treatment in BCG-resistant NMIBC patients. Our finding thus propose that immunotherapy with anti-PD-1/PD-L1 antibodies could be feasible as combination treatment with BCG or as secondary treatment at relapse after BCG in NMIBC patients.

Published

2018

48. Establishment of a novel platform cell line for efficient and precise evaluation of T cell receptor functional avidity

Author

Haruo Sugiyama, Yoshiki Kobayashi, Miki Inatome, Hiroko Nakajima, Nao Aoyama, Yoshihiro Oka, Jun Nakata, Kenta Kondo, Sumiyuki Nishida, Yuya Nishida, Akihiro Tsuboi, Naoki Hosen, Soyoko Morimoto, Fumihiro Fujiki, and Yusuke Oji

Subjects

0301 basic medicine, Reporter gene, Chemistry, Cell growth, medicine.medical_treatment, T-cell receptor, hemic and immune systems, chemical and pharmacologic phenomena, Immunotherapy, Cell biology, WT1, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Oncology, Antigen, medicine, Cytotoxic T cell, Avidity, TCR functional avidity, CD8, TCR, TCR-engineered T-cell therapy, 030215 immunology, Research Paper

Abstract

Adoptive T-cell therapy with T cell receptor (TCR) -engineered T cells is an attractive strategy for cancer treatment and the success in this therapy is dependent on the functional avidity of the transduced TCRs against targeted tumor antigens. Therefore, the establishment of the methodology of the efficient and precise evaluation of TCR functional avidity has been awaited. Here, we show a novel platform cell line, named 2D3, which enables the functional avidity of transduced TCRs to be evaluated efficiently and precisely. In the 2D3, the precise TCR functional avidity of transduced TCRs is easily evaluable by the expression of green fluorescent protein (GFP) reporter gene driven by nuclear factor of activated T cells (NFAT) activation via TCR signaling. Four different TCRs of HLA-A*24:02-restricted Wilms' tumor gene 1 (WT1)-specific CD8+ cytotoxic T lymphocytes (CTLs) were transduced into 2D3 cells and the functional avidities of these four TCRs were evaluated. The evaluated functional avidity of these TCRs positively correlated with cell proliferation, cytokine production, and WT1-specific cytotoxicity of the TCR-transduced CD8+ T cells in response to WT1 antigen. These results showed that 2D3 cell line was a novel and stable tool useful for the efficient and precise evaluation of the functional avidity of isolated and transduced TCRs in developing TCR-based immunotherapy.

Published

2018

49. Identification of a novel HLA-A24-restricted cytotoxic T lymphocyte epitope peptide derived from mesothelin in pancreatic cancer

Author

Hiroki Yamaue, Satoshi Wada, Ken Shirabe, Tetsuro Sasada, Mariko Tsukagoshi, Seiko Hirono, Erica Yada, Hiroyuki Kuwano, and Shintaro Yoshida

Subjects

0301 basic medicine, endocrine system diseases, medicine.medical_treatment, pancreatic cancer, Biology, Epitope, 03 medical and health sciences, 0302 clinical medicine, Antigen, Pancreatic cancer, medicine, Cytotoxic T cell, Mesothelin, Immunotherapy, mesothelin, medicine.disease, CTL, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, biology.protein, immunotherapy, Cancer vaccine, epitope peptide, cancer vaccine, Research Paper

Abstract

Pancreatic cancer involves highly malignant tumors, and the development of new therapeutic strategies is critical. Mesothelin is overexpressed in infiltrating pancreatic cancer cells and plays an important role in the invasion and migration processes. In this study, we focused on mesothelin as a tumor-specific antigen target for a pancreatic cancer vaccine. We first investigated the mesothelin-derived epitope peptide restricted to HLA-A*2402. A total of 19 candidate peptides were synthesized, and we then determined their potential to induce peptide-specific cytotoxic T lymphocytes (CTLs). Peptide-specific CTLs were induced by five peptides derived from mesothelin, and these CTLs successfully exhibited peptide-specific IFN-γ production. After the expansion of each CTL, two CTL lines were established, which were induced by mesothelin-10-5 peptide (AFYPGYLCSL). These CTL lines exhibited peptide-specific cytotoxicity and IFN-γ production. Moreover, we were able to generate mesothelin-10-5 peptide-specific CTL clones. These CTL clones also had specific cytotoxic activity against HLA-A*2402-positive pancreatic cancer cells that endogenously expressed mesothelin. These results indicate that the mesothelin-10-5 peptide is a novel HLA-A*2402 restricted CTL epitope and that it is a promising candidate target for antigen-specific immunotherapy against pancreatic cancers.

Published

2018

50. Non-invasive visualization of tumor infiltrating lymphocytes in patients with metastatic melanoma undergoing immune checkpoint inhibitor therapy: a pilot study

Author

Joseph C. Hung, Svetomir N. Markovic, Vera J. Suman, Andrew Paulsen, Lori A. Erickson, Alberto Signore, Paolo Marchetti, Gregory A. Wiseman, Denise N. Gansen, Wendy K. Nevala, and Filippo Galli

Subjects

Oncology, medicine.medical_specialty, check point inhibitors, medicine.medical_treatment, Ipilimumab, Pembrolizumab, 030218 nuclear medicine & medical imaging, 03 medical and health sciences, 0302 clinical medicine, Immune system, Internal medicine, medicine, melanoma, Colitis, ipilimumab, Tumor-infiltrating lymphocytes, business.industry, Melanoma, Immunotherapy, medicine.disease, 3. Good health, 99mTc-IL2, Tumor progression, 030220 oncology & carcinogenesis, pembrolizumab, business, medicine.drug, Research Paper

Abstract

Early in the course of immunotherapy there is frequently a transient enlargement of tumor masses (pseudo-progression) due to tumor infiltration by TILs. Current clinical imaging modalities are not able to distinguished pseudo-progression from true tumor progression. Thus, patients often remain on treatment 4-8 weeks longer to confirm disease progression. Nuclear medicine offers the possibility to image immune cells and potentially discriminate pseudo-progression and progression. We conducted a pilot study in patients with metastatic melanoma receiving ipilimumab (IPI) or pembrolizumab (PEMBRO) to assess safety and feasibility of SPECT/CT imaging with 99mTc- interleukin-2 (99mTc-HYNIC-IL2) to detect TILs and distinguish between true progression from pseudo- progression. Scans were performed prior to and after 12w treatment. After labelling,99mTc-HYNIC-IL2 was purified and diluted in 10 mL of 5% glucose with 0.1% human serum albumin. Of the 5 patients (2 treated with IPI and 3 with PEMBRO) enrolled, two failed to complete the second scan as they discontinued IPI due grade 3 colitis (1 patient) or patient refusal after developing multiple toxicities attributed to IPI (1 patient). Following the first scan, one patient reported to have a grade 1 pruritus with grade 1 pain. No other toxicities attributed to the radiopharmaceutical infusion were reported. Metastatic lesions could be visualized by 99mTc-IL2 imaging and there was positive correlation between size and 99mTc-HYNIC-IL2 uptake, both before and after 12 weeks of therapy. The results of this pilot study demonstrate the safety and feasibility of 99mTc-IL2 imaging and has led to a number of hypotheses to be tested in future studies.

Published

2018