Your search keyword '"Syngeneic"' showing total 19 results

1. Development and Characterization of a Luciferase Labeled, Syngeneic Murine Model of Ovarian Cancer

Author

Shonagh Russell, Felicia Lim, Pamela N. Peters, Suzanne E. Wardell, Regina Whitaker, Ching-Yi Chang, Rebecca A. Previs, and Donald P. McDonnell

Subjects

ovarian cancer, immune profiling, immunotherapy, intraperitoneal, ovarian intrabursal, murine, high-grade serous, syngeneic, STOSE, Cancer Research, Oncology

Abstract

Despite advances in surgery and targeted therapies, the prognosis for women with high-grade serous ovarian cancer remains poor. Moreover, unlike other cancers, immunotherapy has minimally impacted outcomes in patients with ovarian cancer. Progress in this regard has been hindered by the lack of relevant syngeneic ovarian cancer models to study tumor immunity and evaluate immunotherapies. To address this problem, we developed a luciferase labeled murine model of high-grade serous ovarian cancer, STOSE.M1 luc. We defined its growth characteristics, immune cell repertoire, and response to anti PD-L1 immunotherapy. As with human ovarian cancer, we demonstrated that this model is poorly sensitive to immune checkpoint modulators. By developing the STOSE.M1 luc model, it will be possible to probe the mechanisms underlying resistance to immunotherapies and evaluate new therapeutic approaches to treat ovarian cancer.

Published

2022

2. Experimental animal modeling for immuno-oncology.

Author

Li, Qi-Xiang, Feuer, Gerold, Ouyang, Xuesong, and An, Xiaoyu

Subjects

*ANIMAL models in research, *ONCOLOGY, *IMMUNE response, *ANTINEOPLASTIC agents, *PHARMACEUTICAL industry

Abstract

Immuno-oncology (I/O) research has intensified significantly in recent years due to the breakthrough development and the regulatory approval of several immune checkpoint inhibitors, leading to the rapid expansion of the new discovery of novel I/O therapies, new checkpoint inhibitors and beyond. However, many I/O questions remain unanswered, including why only certain subsets of patients respond to these treatments, who the responders would be, and how to expand patient response (the conversion of non-responders or maximizing response in partial responders). All of these require relevant I/O experimental systems, particularly relevant preclinical animal models. Compared to other oncology drug discovery, e.g . cytotoxic and targeted drugs, a lack of relevant animal models is a major obstacle in I/O drug discovery, and an urgent and unmet need. Despite the obvious importance, and the fact that much I/O research has been performed using many different animal models, there are few comprehensive and introductory reviews on this topic. This article attempts to review the efforts in development of a variety of such models, as well as their applications and limitations for readers new to the field, particularly those in the pharmaceutical industry. [ABSTRACT FROM AUTHOR]

Published

2017

3. A Syngeneic ErbB2 Mammary Cancer Model for Preclinical Immunotherapy Trials

Author

Matthew T. Silvestrini, Clifford G. Tepper, Alexander D. Borowsky, Zsófia Pénzváltó, Jane Qian Chen, Ryan R. Davis, Maxine Umeh-Garcia, and Colleen A Sweeney

Subjects

0301 basic medicine, Cancer Research, Receptor, ErbB-2, animal diseases, medicine.medical_treatment, Drug Screening Assays, Transgenic, B7-H1 Antigen, Mice, Breast cancer, ErbB-2, Antineoplastic Agents, Immunological, 0302 clinical medicine, Immunophenotyping, Antineoplastic Combined Chemotherapy Protocols, Cancer, Tumor, Syngeneic, Immunological, Oncology, 030220 oncology & carcinogenesis, Female, Immunotherapy, Receptor, Biotechnology, PD-L1, Clinical Sciences, Primary Cell Culture, Antineoplastic Agents, Breast Neoplasms, Mice, Transgenic, Biology, Article, Cell Line, Mouse model, Vaccine Related, Experimental, 03 medical and health sciences, Immune system, In vivo, Cell Line, Tumor, medicine, Animals, Humans, Oncology & Carcinogenesis, Transplantation, Mammary Neoplasms, Carcinoma, Mammary Neoplasms, Experimental, Reproducibility of Results, Antitumor, In vitro, 030104 developmental biology, Erbb2, Cell culture, biology.protein, Cancer research, Feasibility Studies, Immunization, Drug Screening Assays, Antitumor

Abstract

In order to develop a practical model of breast cancer, with in vitro and syngeneic,immune-intact, in vivo growth capacity, we established a primary cell line derived from a mammary carcinoma in the transgenic FVB/N-Tg(MMTV-ErbB2*)NDL2-5Mul mouse, referred to as "NDLUCD". The cellline is adapted to standard cell culture and can be transplanted into syngeneic FVB/N mice. The line maintains a stable phenotype over multiple in vitro passages and rounds of in vivo transplantation. NDLUCD tumors in FVB/N mice exhibit high expression of ErbB2 and ErbB3 and signaling molecules downstream of ErbB2. The syngeneic transplant tumors elicit an immune reaction in the adjacent stroma, detected and characterized using histology, immunophenotyping, and gene expression. NDLUCD cells also express PD-L1 in vivo and in vitro, and in vivo transplants are reactive to anti-immune checkpoint therapy with responses conducive to immunotherapy studies. This new NDLUCD cell line model is a practical alternative to the more commonly used 4T1 cells, and our previously described FVB/N-Tg(MMTV-PyVT)634Mul derived Met-1fvb2 and FVB/NTg(MMTV-PyVTY315F/Y322F) derived DB-7fvb2 cell lines. The NDLUCD cells have, so far, remained genetically and phenotypically stable over many generations, with consistent and reproducible results in immune intact preclinical cohorts.

Published

2019

4. Implantable orthotopic bladder cancer model in Wistar rats: A pilot and feasibility study

Author

Mehmet Esad Kosem, Büşra Yaprak Bayrak, Mustafa Yuksekkaya, Yusufhan Yazir, Demir Kursat Yildiz, Kerem Teke, Sema Yusufoğlu, Ozdal Dillioglugil, and Hasan Yilmaz

Subjects

Oncology, bladder cancer model, medicine.medical_specialty, implantable, Bladder cancer, business.industry, wistar rats, medicine.disease, 03 medical and health sciences, 0302 clinical medicine, 030220 oncology & carcinogenesis, Internal medicine, medicine, Medicine, syngeneic, business, orthotopic, 030215 immunology

Abstract

Purpose: The implantable bladder cancer (BC) models allow the researchers to perform rapid and useful experiments for BC. We investigated the implantation success of BC cells obtained from Wistar rats (grown in vitro), into bladders of syngeneic Wistar rats, which are commonly used in the laboratories. Methods: The Nara Bladder Tumor No.2 (NBT-II) BC cells induced with 4-hydroxybutylnitrosamine were grown with passages in Kocaeli University Center for Stem-Cell and Gene-Therapies. After urothelial denudation, 2x106 NBT-II cells were then implanted into bladders of 24 female Wistar rats (aged 7-8 weeks). The rats were randomly divided into four experimental groups; three instillation groups (8 per group) and one sham-operated control group consisting of 6 rats. First, second and third instillation groups were sacrificed at days 7, 14, and 21, respectively, and, bladders were histopathologically evaluated for BC according to WHO / International Society of Urological Pathology. Results: All tumors were pT1 (including 1 rat that prematurely died at 5th day), except one rat that died prematurely at 8th day had pT2 tumor. Implantation rates were 28.58% (2/7) in the first group, and 42.85% (3/7) in the second, for a cumulative rate of 35.71% (5/14) in these two-groups (until 14th day). Interestingly, there was no tumor in the third group, but there was an inflammatory granulation tissue. Conclusion: Seeding NBT-II cells into bladders of Wistar rats was described, successfully tested and demonstrated in this study. This implantable BC model of Wistar rats may be improved to increase the success rate of BC cell implantation in new studies with higher number of animals.

Published

2019

5. Recent Advances in Implantation-Based Genetic Modeling of Biliary Carcinogenesis in Mice

Author

Shingo Kato, Masashi Izumiya, and Yoshitaka Hippo

Subjects

0301 basic medicine, Cancer Research, organoid, Disease, Computational biology, Review, Biology, medicine.disease_cause, 03 medical and health sciences, 0302 clinical medicine, hydrodynamic injection, biliary tract cancer, Genetic model, Organoid, medicine, CRISPR, implantation, syngeneic, RC254-282, genetically engineered mouse, orthotopic model, Cas9, Electroporation, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Genetically Engineered Mouse, Carcinogenesis, nude mouse

Abstract

Simple Summary Biliary tract cancer (BTC) is often refractory to conventional therapeutics and is difficult to diagnose in the early stages. In addition, the pathogenesis of BTC is not fully understood, despite recent advances in cancer genome analysis. To address these issues, the development of fine disease models is critical for BTC. Although still limited in number, there are various platforms for genetic models of BTC owing to newly emerging technology. Among these, implantation-based models have recently drawn attention for their convenience, flexibility, and scalability. To highlight the relevance of this approach, we comprehensively summarize the advantages and disadvantages of BTC models developed using diverse approaches. Currently available research data on intra- and extrahepatic cholangiocarcinoma and gallbladder carcinoma are presented in this review. This information will likely help in selecting the optimal models for various applications and develop novel innovative models based on these technologies. Abstract Epithelial cells in the biliary system can develop refractory types of cancers, which are often associated with inflammation caused by viruses, parasites, stones, and chemicals. Genomic studies have revealed recurrent genetic changes and deregulated signaling pathways in biliary tract cancer (BTC). The causal roles have been at least partly clarified using various genetically engineered mice. Technical advances in Cre-LoxP technology, together with hydrodynamic tail injection, CRISPR/Cas9 technology, in vivo electroporation, and organoid culture have enabled more precise modeling of BTC. Organoid-based genetic modeling, combined with implantation in mice, has recently drawn attention as a means to accelerate the development of BTC models. Although each model may not perfectly mimic the disease, they can complement one another, or two different approaches can be integrated to establish a novel model. In addition, a comparison of the outcomes among these models with the same genotype provides mechanistic insights into the interplay between genetic alterations and the microenvironment in the pathogenesis of BTCs. Here, we review the current status of genetic models of BTCs in mice to provide information that facilitates the wise selection of models and to inform the future development of ideal disease models.

Published

2021

6. DPP4 Inhibitor Sitagliptin Enhances Lymphocyte Recruitment and Prolongs Survival in a Syngeneic Ovarian Cancer Mouse Model

Author

Mark D. Gorrell, Amy L. Wilson, Laura R. Moffitt, Magdalena Plebanski, Andrew N. Stephens, Martin K. Oehler, Kirsty Wilson, Mark D Wright, and Maree Bilandzic

Subjects

0301 basic medicine, Cancer Research, Palliative care, endocrine system diseases, Combination therapy, T cell, Lymphocyte, DPP4, lcsh:RC254-282, Article, sitagliptin, 03 medical and health sciences, 0302 clinical medicine, Immune system, T-cell, medicine, syngeneic, business.industry, FOXP3, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, ID8, 030104 developmental biology, medicine.anatomical_structure, ovarian cancer, Oncology, 030220 oncology & carcinogenesis, Sitagliptin, Cancer research, immune, Ovarian cancer, business, medicine.drug

Abstract

Simple Summary The role of immunity in the development and progression of epithelial ovarian cancer (EOC) is well established. Poor T-cell infiltration is associated with mortality in EOC patients, and recent evidence has suggested that the enzyme DPP4 plays a role in this process. The aim of our study was to evaluate the potential of the clinically-approved DPP4-inhibitor sitagliptin to improve immune responses in mice with EOC. We showed that sitagliptin improved CD8+ T-cell responses in an EOC mouse model, consequently reducing metastatic burden and prolonging survival. These data provide a rationale for the use of DPP4-inhibitors as a second-line treatment for EOC. Abstract Immunity plays a key role in epithelial ovarian cancer (EOC) progression with a well-documented correlation between patient survival and high intratumoral CD8+ to T regulatory cell (Treg) ratios. We previously identified dysregulated DPP4 activity in EOCs as a potentially immune-disruptive influence contributing to a reduction in CXCR3-mediated T-cell infiltration in solid tumours. We therefore hypothesized that inhibition of DPP4 activity by sitagliptin, an FDA-approved inhibitor, would improve T-cell infiltration and function in a syngeneic ID8 mouse model of EOC. Daily oral sitagliptin at 50 mg/kg was provided to mice with established primary EOCs. Sitagliptin treatment decreased metastatic tumour burden and significantly increased overall survival and was associated with significant changes to the immune landscape. Sitagliptin increased overall CXCR3-mediated CD8+ T-cell trafficking to the tumour and enhanced the activation and proliferation of CD8+ T-cells in tumour tissue and the peritoneal cavity. Substantial reductions in suppressive cytokines, including CCL2, CCL17, CCL22 and IL-10, were also noted and were associated with reduced CD4+ CD25+ Foxp3+ Treg recruitment in the tumour. Combination therapy with paclitaxel, however, typical of standard-of-care for patients in palliative care, abolished CXCR3-specific T-cell recruitment stimulated by sitagliptin. Our data suggest that sitagliptin may be suitable as an adjunct therapy for patients between chemotherapy cycles as a novel approach to enhance immunity, optimise T-cell-mediated function and improve overall survival.

Published

2021

7. Mouse Tumor-Bearing Models as Preclinical Study Platforms for Oral Squamous Cell Carcinoma

Author

Qiang Li, Heng Dong, Guangwen Yang, Yuxian Song, Yongbin Mou, and Yanhong Ni

Subjects

0301 basic medicine, Cancer Research, HPV, Review, Bioinformatics, lcsh:RC254-282, chemical carcinogen-induced, 03 medical and health sciences, 0302 clinical medicine, Animal model, genetically engineered models, Medicine, Mouse tumor, Basal cell, mouse models, Cancer biology, xenograft, syngeneic, Clinical treatment, business.industry, High fertility, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, transplanted, stomatognathic diseases, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Genetically Engineered Mouse, OSCC, business

Abstract

Preclinical animal models of oral squamous cell carcinoma (OSCC) have been extensively studied in recent years. Investigating the pathogenesis and potential therapeutic strategies of OSCC is required to further progress in this field, and a suitable research animal model that reflects the intricacies of cancer biology is crucial. Of the animal models established for the study of cancers, mouse tumor-bearing models are among the most popular and widely deployed for their high fertility, low cost, and molecular and physiological similarity to humans, as well as the ease of rearing experimental mice. Currently, the different methods of establishing OSCC mouse models can be divided into three categories: chemical carcinogen-induced, transplanted and genetically engineered mouse models. Each of these methods has unique advantages and limitations, and the appropriate application of these techniques in OSCC research deserves our attention. Therefore, this review comprehensively investigates and summarizes the tumorigenesis mechanisms, characteristics, establishment methods, and current applications of OSCC mouse models in published papers. The objective of this review is to provide foundations and considerations for choosing suitable model establishment methods to study the relevant pathogenesis, early diagnosis, and clinical treatment of OSCC.

Published

2020

8. Myxoma Virus Optimizes Cisplatin for the Treatment of Ovarian Cancer In Vitro and in a Syngeneic Murine Dissemination Model

Author

Jason Liem, Jia Liu, Bernice Nounamo, and Martin J. Cannon

Subjects

0301 basic medicine, Cancer Research, medicine.medical_treatment, MYXV, Myxoma virus, M062R-null MYXV, chemotherapy, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, Immune system, myxoma virus, synergism, Splenocyte, Medicine, Pharmacology (medical), Virotherapy, syngeneic, Cisplatin, biology, business.industry, Immunotherapy, biology.organism_classification, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 3. Good health, Oncolytic virus, 030104 developmental biology, ovarian cancer, Oncology, oncolytic, 030220 oncology & carcinogenesis, Immunology, Cancer research, Molecular Medicine, Original Article, immunotherapy, virotherapy, business, Ovarian cancer, medicine.drug

Abstract

A therapeutic approach to improve treatment outcome of ovarian cancer (OC) in patients is urgently needed. Myxoma virus (MYXV) is a candidate oncolytic virus that infects to eliminate OC cells. We found that in vitro MYXV treatment enhances cisplatin or gemcitabine treatment by allowing lower doses than the corresponding IC 50 calculated for primary OC cells. MYXV also affected OC patient ascites-associated CD14 + myeloid cells, one of the most abundant immunological components of the OC tumor environment; without causing cell death, MYXV infection reduces the ability of these cells to secrete cytokines such as IL-10 that are signatures of the immunosuppressive tumor environment. We found that pretreatment with replication-competent but not replication-defective MYXV-sensitized tumor cells to later cisplatin treatments to drastically improve survival in a murine syngeneic OC dissemination model. We thus conclude that infection with replication-competent MYXV before cisplatin treatment markedly enhances the therapeutic benefit of chemotherapy. Treatment with replication-competent MYXV followed by cisplatin potentiated splenocyte activation and IFNγ expression, possibly by T cells, when splenocytes from treated mice were stimulated with tumor cell antigen ex vivo. The impact on immune responses in the tumor environment may thus contribute to the enhanced antitumor activity of combinatorial MYXV-cisplatin treatment.

Published

2017

9. Intracranial AAV‐IFN‐β gene therapy eliminates invasive xenograft glioblastoma and improves survival in orthotopic syngeneic murine model

Author

Dwijit GuhaSarkar, James Neiswender, Guangping Gao, Miguel Sena-Esteves, and Qin Su

Subjects

0301 basic medicine, Male, Cancer Research, intracranial, Genetic enhancement, viruses, Mice, Nude, medicine.disease_cause, Viral vector, 03 medical and health sciences, Mice, 0302 clinical medicine, Cell Line, Tumor, Genetics, Medicine, interferon‐beta, Animals, Humans, xenograft, syngeneic, Adeno-associated virus, Research Articles, Temozolomide, DNA synthesis, Microglia, business.industry, Brain Neoplasms, Therapeutic effect, adeno‐associated virus, glioblastoma, Promoter, General Medicine, Genetic Therapy, Interferon-beta, Dependovirus, Xenograft Model Antitumor Assays, 3. Good health, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Immunology, Cancer research, Molecular Medicine, business, medicine.drug, Research Article

Abstract

The highly invasive property of glioblastoma (GBM) cells and genetic heterogeneity are largely responsible for tumor recurrence after the current standard-of-care treatment and thus a direct cause of death. Previously, we have shown that intracranial interferon-beta (IFN-β) gene therapy by locally administered adeno-associated viral vectors (AAV) successfully treats noninvasive orthotopic glioblastoma models. Here, we extend these findings by testing this approach in invasive human GBM xenograft and syngeneic mouse models. First, we show that a single intracranial injection of AAV encoding human IFN-β eliminates invasive human GBM8 tumors and promotes long-term survival. Next, we screened five AAV-IFN-β vectors with different promoters to drive safe expression of mouse IFN-β in the brain in the context of syngeneic GL261 tumors. Two AAV-IFN-β vectors were excluded due to safety concerns, but therapeutic studies with the other three vectors showed extensive tumor cell death, activation of microglia surrounding the tumors, and a 56% increase in median survival of the animals treated with AAV/P2-Int-mIFN-β vector. We also assessed the therapeutic effect of combining AAV-IFN-β therapy with temozolomide (TMZ). As TMZ affects DNA replication, an event that is crucial for second-strand DNA synthesis of single-stranded AAV vectors before active transcription, we tested two TMZ treatment regimens. Treatment with TMZ prior to AAV-IFN-β abrogated any benefit from the latter, while the reverse order of treatment doubled the median survival compared to controls. These studies demonstrate the therapeutic potential of intracranial AAV-IFN-β therapy in a highly migratory GBM model as well as in a syngeneic mouse model and that combination with TMZ is likely to enhance its antitumor potency.

Published

2017

10. Longitudinal immune characterization of syngeneic tumor models to enable model selection for immune oncology drug discovery

Author

Lukasz Magiera, Linda Sandin, Anna Staniszewska, Simon T. Barry, Josephine Walton, Amanda Watkins, Larissa S. Carnevalli, Lorraine Mooney, Sigourney Bell, A. Hughes, Anna M. L. Coenen-Stass, Elizabeth Hardaker, and Molly A. Taylor

Subjects

0301 basic medicine, Cancer Research, Syngeneic tumor, medicine.medical_treatment, Immunology, Population, Cancer therapy, Computational biology, lcsh:RC254-282, Immunophenotyping, Immunomodulation, Mice, 03 medical and health sciences, Antineoplastic Agents, Immunological, Lymphocytes, Tumor-Infiltrating, 0302 clinical medicine, Immune system, Neoplasms, Drug Discovery, Biomarkers, Tumor, Tumor Microenvironment, medicine, Animals, Humans, Immunology and Allergy, 4 T1, education, Pharmacology, education.field_of_study, biology, Gene Expression Profiling, Model selection, Drug Synergism, Immunotherapy, Syngeneic, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Disease Models, Animal, CT-26, MC38, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, biology.protein, Molecular Medicine, Oncology drug, Drug Screening Assays, Antitumor, Antibody, Immune checkpoint blockade, Research Article

Abstract

Background The ability to modulate immune-inhibitory pathways using checkpoint blockade antibodies such as αPD-1, αPD-L1, and αCTLA-4 represents a significant breakthrough in cancer therapy in recent years. This has driven interest in identifying small-molecule-immunotherapy combinations to increase the proportion of responses. Murine syngeneic models, which have a functional immune system, represent an essential tool for pre-clinical evaluation of new immunotherapies. However, immune response varies widely between models and the translational relevance of each model is not fully understood, making selection of an appropriate pre-clinical model for drug target validation challenging. Methods Using flow cytometry, O-link protein analysis, RT-PCR, and RNAseq we have characterized kinetic changes in immune-cell populations over the course of tumor development in commonly used syngeneic models. Results This longitudinal profiling of syngeneic models enables pharmacodynamic time point selection within each model, dependent on the immune population of interest. Additionally, we have characterized the changes in immune populations in each of these models after treatment with the combination of α-PD-L1 and α-CTLA-4 antibodies, enabling benchmarking to known immune modulating treatments within each model. Conclusions Taken together, this dataset will provide a framework for characterization and enable the selection of the optimal models for immunotherapy combinations and generate potential biomarkers for clinical evaluation in identifying responders and non-responders to immunotherapy combinations.

Published

2019

11. Mouse-Derived Isograft (MDI) In Vivo Tumor Models II. Carcinogen-Induced cMDI Models: Characterization and Cancer Therapeutic Approaches

Author

Janette Beshay, Peter Jantscheff, Holger Weber, Christoph Schächtele, Cynthia Obodozie, and Thomas Lemarchand

Subjects

0301 basic medicine, immunocompetent animals, Cancer Research, Isograft, Population, Biology, lcsh:RC254-282, Article, Flow cytometry, experimental cancer, immune checkpoint inhibitors, 03 medical and health sciences, Tissue culture, 0302 clinical medicine, Immune system, In vivo, medicine, education, syngeneic, Carcinogen, education.field_of_study, therapy, medicine.diagnostic_test, Cancer, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, mouse tumor models, Cancer research, mouse-derived isografts (MDIs), carcinogen-induced tumors

Abstract

In this second study, we established syngeneic in vivo models named carcinogen-induced mouse-derived isografts (cMDIs). Carcinogen-induced tumors were obtained during short-term observation (3&ndash, 9 months) of CBA/J mice treated with various administration routes with 3-methylcholanthrene (MCA) or N-methyl-N-nitrosourea (MNU) as carcinogens. During necropsy, primary tumors and suspicious tissues were assessed macroscopically and re-transplanted (in PDX-like manner) into sex-matched syngeneic animals. Outgrowing tumors were histologically characterized as either spinocellular carcinoma (1/8) or various differentiated sarcomas (7/8). Growth curves of four sarcomas showed striking heterogeneity. These cMDIs were further characterized by flow cytometry, RNA sequencing, or efficacy studies. A variable invasion of immune cells into the tumors, as well as varying expression of tyrosine kinase receptor, IFN-&gamma, signature, or immune cell population marker genes could be observed. Immune checkpoint inhibitor treatment (anti-mPD-1, anti-mCTLA-4, or a combination thereof) showed different responses in the various cMDI models. In general, cMDI models are carcinogen-induced tumors of low passage number that were propagated as tissue pieces in mice without any tissue culturing. Therefore, the tumors contained conserved tumor characteristics and intratumoral immune cell populations. In contrast to the previously described spontaneous MDI, carcinogen induction resulted in a greater number of individual but histologically related tumors, which were preferentially sarcomas.

Published

2019

12. Mouse-Derived Isograft (MDI) In Vivo Tumor Models I. Spontaneous sMDI Models: Characterization and Cancer Therapeutic Approaches

Author

Janette Beshay, Holger Weber, Peter Jantscheff, Cynthia Obodozie, Thomas Lemarchand, and Christoph Schächtele

Subjects

0301 basic medicine, immunocompetent animals, Cancer Research, Isograft, Population, Biology, lcsh:RC254-282, Article, Flow cytometry, experimental cancer, immune checkpoint inhibitors, 03 medical and health sciences, Tissue culture, 0302 clinical medicine, Immune system, In vivo, medicine, education, syngeneic, education.field_of_study, therapy, medicine.diagnostic_test, Cancer, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 030104 developmental biology, Oncology, spontaneous tumors, 030220 oncology & carcinogenesis, mouse tumor models, Cancer research, mouse-derived isografts (MDIs), Adenocarcinoma, carcinogen-induced tumors

Abstract

Syngeneic in vivo tumor models are valuable for the development and investigation of immune-modulating anti-cancer drugs. In the present study, we established a novel syngeneic in vivo model type named mouse-derived isografts (MDIs). Spontaneous MDIs (sMDIs) were obtained during a long-term observation period (more than one to two years) of na&iuml, ve and untreated animals of various mouse strains (C3H/HeJ, CBA/J, DBA/2N, BALB/c, and C57BL/6N). Primary tumors or suspicious tissues were assessed macroscopically and re-transplanted in a PDX-like manner as small tumor pieces into sex-matched syngeneic animals. Nine outgrowing primary tumors were histologically characterized either as adenocarcinomas, histiocytic carcinomas, or lymphomas. Growth of the tumor pieces after re-transplantation displayed model heterogeneity. The adenocarcinoma sMDI model JA-0009 was further characterized by flow cytometry, RNA-sequencing, and efficacy studies. M2 macrophages were found to be the main tumor infiltrating leukocyte population, whereas only a few T cells were observed. JA-0009 showed limited sensitivity when treated with antibodies against inhibitory checkpoint molecules (anti-mPD-1 and anti-mCTLA-4), but high sensitivity to gemcitabine treatment. The generated sMDI are spontaneously occurring tumors of low passage number, propagated as tissue pieces in mice without any tissue culturing, and thus conserving the original tumor characteristics and intratumoral immune cell populations.

Published

2019

13. Non-Invasive Fluorescent Monitoring of Ovarian Cancer in an Immunocompetent Mouse Model

Author

Maree Bilandzic, Amy L. Wilson, Kirsty Wilson, Martin K. Oehler, Adam Rainczuk, Andrew N. Stephens, Laura R. Moffitt, Ming Makanji, Magdalena Plebanski, and Mark D. Gorrell

Subjects

0301 basic medicine, Cancer Research, T cell, Cell, lcsh:RC254-282, Article, 03 medical and health sciences, 0302 clinical medicine, Immune system, medicine, syngeneic, iRFP, business.industry, Effector, tumour, Dendritic cell, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 3. Good health, ID8, 030104 developmental biology, medicine.anatomical_structure, ovarian cancer, Oncology, iRFP720, 030220 oncology & carcinogenesis, Cancer research, immune, Ovarian cancer, business, Ovarian Implantation, CD8

Abstract

Ovarian cancers (OCs) are the most lethal gynaecological malignancy, with high levels of relapse and acquired chemo-resistance. Whilst the tumour&ndash, immune nexus controls both cancer progression and regression, the lack of an appropriate system to accurately model tumour stage and immune status has hampered the validation of clinically relevant immunotherapies and therapeutic vaccines to date. To address this need, we stably integrated the near-infrared phytochrome iRFP720 at the ROSA26 genomic locus of ID8 mouse OC cells. Intrabursal ovarian implantation into C57BL/6 mice, followed by regular, non-invasive fluorescence imaging, permitted the direct visualization of tumour mass and distribution over the course of progression. Four distinct phases of tumour growth and dissemination were detectable over time that closely mimicked clinical OC progression. Progression-related changes in immune cells also paralleled typical immune profiles observed in human OCs. Specifically, we observed changes in both the CD8+ T cell effector (Teff):regulatory (Treg) ratio, as well as the dendritic cell (DC)-to-myeloid derived suppressor cell (MDSC) ratio over time across multiple immune cell compartments and in peritoneal ascites. Importantly, iRFP720 expression had no detectible influence over immune profiles. This new model permits non-invasive, longitudinal tumour monitoring whilst preserving host&ndash, tumour immune interactions, and allows for the pre-clinical assessment of immune profiles throughout disease progression as well as the direct visualization of therapeutic responses. This simple fluorescence-based approach provides a useful new tool for the validation of novel immuno-therapeutics against OC.

Published

2018

14. Radiosensitisation of Hepatocellular Carcinoma Cells by Vandetanib

Author

Z. A. Bascal, Hassan Shahbakhti, Sami A. Znati, Adam Westhorpe, Jessica Prince, Petra Vlckova, Marcos Duran Vasquez, Chiara De Vellis, Marilena Loizidou, Rebecca Carter, and Ricky A. Sharma

Subjects

0301 basic medicine, vandetanib, Cancer Research, Combination therapy, medicine.drug_class, medicine.medical_treatment, Vandetanib, lcsh:RC254-282, Article, Tyrosine-kinase inhibitor, angiogenesis, 03 medical and health sciences, 0302 clinical medicine, In vivo, medicine, syngeneic, Clonogenic assay, radiotherapy, business.industry, animal model, 3D models, vascular endothelial growth factor receptor-2, Cancer, hepatocellular carcinoma, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, immunocompetent, Radiation therapy, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Hepatocellular carcinoma, Cancer research, radiosensitiser, business, medicine.drug

Abstract

Hepatocellular Carcinoma (HCC) is increasing in incidence worldwide and requires new approaches to therapy. The combination of anti-angiogenic drug therapy and radiotherapy is one promising new approach. The anti-angiogenic drug vandetanib is a tyrosine kinase inhibitor of vascular endothelial growth factor receptor-2 (VEGFR-2) and RET proto-oncogene with radio-enhancement potential. To explore the benefit of combined vandetanib and radiotherapy treatment for HCC, we studied outcomes following combined treatment in pre-clinical models. Methods: Vandetanib and radiation treatment were combined in HCC cell lines grown in vitro and in vivo. In addition to 2D migration and clonogenic assays, the combination was studied in 3D spheroids and a syngeneic mouse model of HCC. Results: Vandetanib IC 50 s were measured in 20 cell lines and the drug was found to significantly enhance radiation cell kill and to inhibit both cell migration and invasion in vitro. In vivo, combination therapy significantly reduced cancer growth and improved overall survival, an effect that persisted for the duration of vandetanib treatment. Conclusion: In 2D and 3D studies in vitro and in a syngeneic model in vivo, the combination of vandetanib plus radiotherapy was more efficacious than either treatment alone. This new combination therapy for HCC merits evaluation in clinical trials.

Published

2020

15. Ovarian Cancer Immunotherapy: Preclinical Models and Emerging Therapeutics

Author

Galpin Kjc, Curtis W McCloskey, Rodriguez Gm, and Barbara C. Vanderhyden

Subjects

0301 basic medicine, Cancer Research, Stromal cell, medicine.medical_treatment, Context (language use), Review, chemotherapy, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, Immune system, Ovarian carcinoma, medicine, tumor microenvironment, hot vs. cold tumors, syngeneic, Tumor microenvironment, immunosuppression, business.industry, immune infiltrating cells, Immunosuppression, Immunotherapy, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 3. Good health, 030104 developmental biology, ovarian cancer, Oncology, 030220 oncology & carcinogenesis, Cancer research, immunotherapy, business, Ovarian cancer, transgenic models

Abstract

Immunotherapy has emerged as one of the most promising approaches for ovarian cancer treatment. The tumor microenvironment (TME) is a key factor to consider when stimulating antitumoral responses as it consists largely of tumor promoting immunosuppressive cell types that attenuate antitumor immunity. As our understanding of the determinants of the TME composition grows, we have begun to appreciate the need to address both inter- and intra-tumor heterogeneity, mutation/neoantigen burden, immune landscape, and stromal cell contributions. The majority of immunotherapy studies in ovarian cancer have been performed using the well-characterized murine ID8 ovarian carcinoma model. Numerous other animal models of ovarian cancer exist, but have been underutilized because of their narrow initial characterizations in this context. Here, we describe animal models that may be untapped resources for the immunotherapy field because of their shared genomic alterations and histopathology with human ovarian cancer. We also shed light on the strengths and limitations of these models, and the knowledge gaps that need to be addressed to enhance the utility of preclinical models for testing novel immunotherapeutic approaches.

Published

2018

16. Establishing 177Lu-PSMA-617 Radioligand Therapy in a Syngeneic Model of Murine Prostate Cancer

Author

Ken Herrmann, Wolfgang P. Fendler, Katharina Lückerath, Caius G. Radu, Matthias Eiber, Jonathan W. Said, Liu Wei, Johannes Czernin, Roger Slavik, Soumya Poddar, Susan Evans-Axelsson, Andreea D. Stuparu, and Woosuk Kim

Subjects

Oncology, Male, Medizin, Pharmacology, Lutetium, Inbred C57BL, 030218 nuclear medicine & medical imaging, Prostate cancer, Mice, Double-Stranded, 0302 clinical medicine, Heterocyclic Compounds, Radioligand, Tissue Distribution, syngeneic, Cancer, 1-Ring, Tumor, Chemistry, Prostate Cancer, Dipeptides, Immunohistochemistry, Tumor Burden, Nuclear Medicine & Medical Imaging, 030220 oncology & carcinogenesis, Toxicity, Urologic Diseases, medicine.medical_specialty, 177Lu-PSMA-617, Clinical Sciences, Cell Line, 03 medical and health sciences, Fluorodeoxyglucose F18, Internal medicine, medicine, PSMA, Animals, Humans, Radiology, Nuclear Medicine and imaging, DNA Breaks, Prostatic Neoplasms, Prostate-Specific Antigen, 177Lu, medicine.disease, specific activity, Positron-Emission Tomography, Specific activity, Histopathology, Radiopharmaceuticals, Lu-177, Ex vivo, Neoplasm Transplantation

Abstract

Clinical 177Lu-PSMA-617 radioligand therapy (RLT) is applied in advanced-stage prostate cancer. However, to the best of our knowledge murine models to study the biologic effects of various activity levels have not been established. The aim of this study was to optimize specific and total activity for 177Lu-PSMA-617 RLT in a syngeneic model of murine prostate cancer. Methods: Murine-reconstituted, oncogene-driven prostate cancer cells (0.1 · 106) (RM1), transduced to express human prostate-specific membrane antigen (PSMA), were injected into the left flank of C57Bl6 immunocompetent mice. RLT was performed by administering a single tail vein injection of 177Lu-PSMA-617 at different formulations for specific (60 MBq at high, 62 MBq/nmol; intermediate, 31 MBq/nmol; or low 15 MBq/nmol specific activity) or total activity (30, 60, or 120 MBq). Organ distribution was determined by ex vivo g-counter measurement. DNA double-strand breaks were measured using anti–gamma-H2A.X (phospho S139) immunohistochemistry. Efficacy was assessed by serial CT tumor volumetry and 18F-FDG PET metabolic volume. Toxicity was evaluated 4 wk after the start of RLT. Results: Mean tumor-to-kidney ratios 6 SEM were 19 6 5, 10 6 5, and 2 6 0 for high, intermediate, and low (each n 5 3) specific activity, respectively. Four of 6 (67%) mice treated with intermediate or high specific activity and none of 6 (0%) mice treated with low specific activity or formulation demonstrated significant DNA double-strand breaks ($5% g-H2A.X–positive cells). High when compared with intermediate or low specific activity resulted in a lower mean 6 SEM tumor load by histopathology (vital tissue, 4 6 2 vs. 8 6 3 mm2; n 5 3 vs. 6), day-4 18F-FDG PET (metabolic volume, 87 6 23 vs. 118 6 14 mm3; n 5 6 vs. 12), and day-7 CT (volume, 323 6 122 vs. 590 6 46 mm3; n 5 3 vs. 6; P 5 0.039). 177Lu-PSMA-617 (120 MBq) with high specific activity induced superior tumor growth inhibition (P 5 0.021, n 5 5/group) without subacute hematologic toxicity (n 5 3/group). Conclusion: 177Lu-PSMA-617 (120 MBq) and high specific activity resulted in the highest efficacy in a syngeneic model of murine prostate cancer. The model will be useful for studying the effects of PSMA-directed RLT combined with potentially synergistic pharmacologic approaches.

Published

2017

17. Longitudinal immune characterization of syngeneic tumor models to enable model selection for immune oncology drug discovery.

Author

Taylor, Molly A., Hughes, Adina M., Walton, Josephine, Coenen-Stass, Anna M. L., Magiera, Lukasz, Mooney, Lorraine, Bell, Sigourney, Staniszewska, Anna D., Sandin, Linda C., Barry, Simon T., Watkins, Amanda, Carnevalli, Larissa S., and Hardaker, Elizabeth L.

Subjects

*PROTEIN analysis, *FLOW cytometry, *CANCER treatment, *ONCOLOGY, *IMMUNE system

Abstract

Background: The ability to modulate immune-inhibitory pathways using checkpoint blockade antibodies such as αPD-1, αPD-L1, and αCTLA-4 represents a significant breakthrough in cancer therapy in recent years. This has driven interest in identifying small-molecule-immunotherapy combinations to increase the proportion of responses. Murine syngeneic models, which have a functional immune system, represent an essential tool for pre-clinical evaluation of new immunotherapies. However, immune response varies widely between models and the translational relevance of each model is not fully understood, making selection of an appropriate pre-clinical model for drug target validation challenging. Methods: Using flow cytometry, O-link protein analysis, RT-PCR, and RNAseq we have characterized kinetic changes in immune-cell populations over the course of tumor development in commonly used syngeneic models. Results: This longitudinal profiling of syngeneic models enables pharmacodynamic time point selection within each model, dependent on the immune population of interest. Additionally, we have characterized the changes in immune populations in each of these models after treatment with the combination of α-PD-L1 and α-CTLA-4 antibodies, enabling benchmarking to known immune modulating treatments within each model. Conclusions: Taken together, this dataset will provide a framework for characterization and enable the selection of the optimal models for immunotherapy combinations and generate potential biomarkers for clinical evaluation in identifying responders and non-responders to immunotherapy combinations. [ABSTRACT FROM AUTHOR]

Published

2019

18. Murine Models of Acute Leukemia: Important Tools in Current Pediatric Leukemia Research

Author

Terry J. Fry, Elad Jacoby, and Christopher D. Chien

Subjects

Cancer Research, acute lymphoblastic leukaemia, medicine.medical_treatment, Review Article, acute lymphoblastic leukemia, Bioinformatics, Immunotherapy, Adoptive, lcsh:RC254-282, adoptive, murine model, medicine, In patient, syngeneic, Pediatric leukemia, Acute leukemia, Chemotherapy, business.industry, Immunotherapy, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, Leukemia, medicine.anatomical_structure, xenografts, Oncology, Immunology, Syngenic, Bone marrow, immunotherapy, business

Abstract

Leukemia remains the most common diagnosis in pediatric oncology and, despite dramatic progress in upfront therapy, is also the most common cause of cancer-related death in children. Much of the initial improvement in outcomes for acute lymphoblastic leukemia (ALL) was due identification of cytotoxic agents that are active against leukemias followed by the recognition that combination of these cytotoxic agents and prolonged therapy are essential for cure. Recent data demonstrating lack of progress in patients for whom standard chemotherapy fails suggests that the ability to improve outcome for these children will not be dramatically impacted through more intensive or newer cytotoxic agents. Thus, much of the recent research focus has been in the area of improving our understanding of the genetics and the biology of leukemias. Although in vitro studies remain critical, given the complexity of a living system and the increasing recognition of the contribution of leukemia extrinsic factors such as the bone marrow microenvironment, in vivo models have provided important insights. The murine systems that are used can be broadly categorized into syngenic models in which a murine leukemia can be studied in an immunologically intact host and xenograft models where human human leukemias are studied in highly immunocompormised murine host. Both of these systems have limitations such that neither can be used exclusively to study all aspects of leukemia biology and therapeutics for humans. This review will describe the various ALL model systems that have been developed as well as discuss the advantages and disadvantages inherent to these systems that make each particularly suitable for specific types of studies.

Published

2014

19. A New Spontaneously Transformed Syngeneic Model of High-Grade Serous Ovarian Cancer with a Tumor-Initiating Cell Population

Author

Curtis W. McCloskey, Reuben L. Goldberg, Lauren E. Carter, Lisa F. Gamwell, Ensaf M. Al-Hujaily, Olga eCollins, Elizabeth A. Macdonald, Kenneth eGarson, Manijeh eDaneshmand, Euridice eCarmona, and Barbara C. Vanderhyden

Subjects

endocrine system, Cancer Research, Pathology, medicine.medical_specialty, Population, lcsh:RC254-282, tumor-initiating cell, CDKN2A, medicine, Doubling time, syngeneic, education, Original Research, education.field_of_study, tumor initiating cells, business.industry, Cancer stem cell, Wnt signaling pathway, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, 3. Good health, stem cell, high-grade serous cancer, ovarian cancer, ovarian surface epithelium, mouse model of ovarian cancer, Oncology, high grade serous cancer, Cell culture, Cancer research, Stem cell, PAX8, Ovarian cancer, business

Abstract

Improving screening and treatment options for patients with epithelial ovarian cancer has been a major challenge in cancer research. Development of novel diagnostic and therapeutic approaches, particularly for the most common subtype, high-grade serous ovarian cancer (HGSC), has been hampered by controversies over the origin of the disease and a lack of spontaneous HGSC models to resolve this controversy. Over long-term culture in our laboratory, an ovarian surface epithelial (OSE) cell line spontaneously transformed OSE (STOSE). The objective of this study was to determine if the STOSE cell line is a good model of HGSC. STOSE cells grow faster than early passage parental M0505 cells with a doubling time of 13 and 48 h, respectively. STOSE cells form colonies in soft agar, an activity for which M0505 cells have negligible capacity. Microarray analysis identified 1755 down-regulated genes and 1203 up-regulated genes in STOSE compared to M0505 cells, many associated with aberrant Wnt/β-catenin and Nf-κB signaling. Upregulation of Ccnd1 and loss of Cdkn2a in STOSE tumors is consistent with changes identified in human ovarian cancers by The Cancer Genome Atlas. Intraperitoneal injection of STOSE cells into severe combined immunodeficient and syngeneic FVB/N mice produced cytokeratin+, WT1+, inhibin−, and PAX8+ tumors, a histotype resembling human HGSC. Based on evidence that a SCA1+ stem cell-like population exists in M0505 cells, we examined a subpopulation of SCA1+ cells that is present in STOSE cells. Compared to SCA1− cells, SCA1+ STOSE cells have increased colony-forming capacity and form palpable tumors 8 days faster after intrabursal injection into FVB/N mice. This study has identified the STOSE cells as the first spontaneous murine model of HGSC and provides evidence for the OSE as a possible origin of HGSC. Furthermore, this model provides a novel opportunity to study how normal stem-like OSE cells may transform into tumor-initiating cells.

Published

2014