Your search keyword '"Syngeneic mouse"' showing total 123 results

1. Potentiated antitumor effects of APS001F/5-FC combined with anti-PD-1 antibody in a CT26 syngeneic mouse model

Author

Koichiro Shioya, Shun'ichiro Taniguchi, Yuji Seki, Takaaki Nakamura, Hitomi Shimizu, and Tomio Matsumura

Subjects

0301 basic medicine, Bifidobacterium longum, Combination therapy, medicine.drug_class, Programmed Cell Death 1 Receptor, Flucytosine, Antineoplastic Agents, CD8-Positive T-Lymphocytes, Pharmacology, Monoclonal antibody, Applied Microbiology and Biotechnology, Biochemistry, Analytical Chemistry, Mice, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, medicine, Animals, Molecular Biology, Survival rate, biology, Chemistry, Organic Chemistry, Cytosine deaminase, Anti pd 1, Antibodies, Monoclonal, General Medicine, biology.organism_classification, 030104 developmental biology, 030220 oncology & carcinogenesis, Syngeneic mouse, Genetic Engineering, CD8, Biotechnology

Abstract

APS001F is a strain of Bifidobacterium longum genetically engineered to express cytosine deaminase that converts 5-fluorocytosine (5-FC) to 5-fluorouracil. In the present study, antitumor effects of APS001F plus 5-FC (APS001F/5-FC) in combination with anti-PD-1 monoclonal antibody were investigated using a CT26 syngeneic mouse model. Both of dosing of APS001F/5-FC before and after anti-PD-1 mAb in the combination dosing exhibited antitumor effects as well as prolonged survival over the nontreated control. The survival rate in the combination therapy significantly increased over the monotherapy with APS001F/5-FC and that with anti-PD-1 mAb. Regulatory T cells among CD4+ T cells in tumor decreased in the combination therapy, while the ratio of CD8+ T cells was maintained in all groups. Taken these results together, APS001F/5-FC not only demonstrates a direct antitumor activity, but also immunomodulatory effects once localized in the hypoxic region of the tumor, which allows anti-PD-1 mAb to exert potentiated antitumor effects.

Published

2021

2. PALM GAMMA-TOCOTRIENOL SUPPLEMENTATION SUPPRESS TUMOUR GROWTH AND METASTASIS IN A SYNGENEIC MOUSE MODEL OF BREAST CANCER

Author

Kanga Rani Selvaduray

Subjects

Renewable Energy, Sustainability and the Environment, business.industry, medicine.disease, Metastasis, Biomaterials, chemistry.chemical_compound, Breast cancer, chemistry, medicine, Cancer research, Syngeneic mouse, Palm, business, Agronomy and Crop Science, gamma-Tocotrienol, Food Science

Published

2021

3. Circulation patterns and seed-soil compatibility factors cooperate to cause cancer organ-specific metastasis

Author

Xiaodong Xie, Lee Jia, Yusheng Lu, Chengbin Fu, Yewei Zhu, Yunlong Cheng, M. Iqbal Parker, Yuying Ye, Chen Zhang, and Shu Lian

Subjects

0301 basic medicine, Organ specific metastasis, Melanoma, Experimental, Biology, Metastasis, law.invention, Carcinoma, Lewis Lung, Mice, 03 medical and health sciences, 0302 clinical medicine, Circulating tumor cell, In vivo, Confocal microscopy, law, Organ specific, Cell Adhesion, Tumor Microenvironment, medicine, In vivo fluorescence, Animals, Humans, Neoplasm Metastasis, Cell Biology, Neoplastic Cells, Circulating, medicine.disease, 030104 developmental biology, Organ Specificity, 030220 oncology & carcinogenesis, Cancer research, Syngeneic mouse, Endothelium, Vascular

Abstract

Despite the recognition of the lethality of cancer metastasis and the importance of developing specific anti-metastasis therapies directed at the cancer metastatic cascade, the dynamics of cancer metastasis remains poorly understood. In this study, we examined the dynamics of circulating tumor cell (CTC) survival in the bloodstream using experimental mouse models. CTCs were arrested in the capillaries by adhesion to vascular endothelium within a few minutes after injection into the bloodstream. The loss of CTCs from the circulation followed a bi-phasic decay pattern, with the number of CTCs in the bloodstream being closely associated with the number of blood circulation cycles. The calculated in vivo Vd (apparent volume of distribution) of the CTC revealed organ specific binding of the CTCs. Moreover, confocal microscopy, in vivo fluorescence imaging in syngeneic mouse metastatic models and analysis of blood circulation patterns support the notion of organ-specific tumor metastasis. The present study suggests that organ-specific tumor metastasis is influenced by cooperation between blood circulation patterns and 'seed-soil' compatibility factors. These new findings provide further insights for optimized cancer metastatic prevention strategies such as by creating a hostile circulation microenvironment and targeting the organ-specific 'seed-soil' compatibility factors.

Published

2019

4. OC-0282 Inhibition of oxidative phosphorylation alters the tumor microenvironment in syngeneic mouse models

Author

R. Van den Bijgaart, Paul N. Span, Sandra Heskamp, Gosse J. Adema, H. Peters, A. Kip, D. Boreel, and Jan Bussink

Subjects

Tumor microenvironment, Oncology, Chemistry, Cancer research, Syngeneic mouse, Radiology, Nuclear Medicine and imaging, Hematology, Oxidative phosphorylation

Published

2021

5. Pre-existing Immunity to Oncolytic Virus Potentiates Its Immunotherapeutic Efficacy

Author

Anton Oseledchyk, Taha Merghoub, Dmitriy Zamarin, Jedd D. Wolchok, Levi Mangarin, Jacob Ricca, Tyler Walther, and Cailian Liu

Subjects

0301 basic medicine, viruses, animal diseases, medicine.medical_treatment, chemical and pharmacologic phenomena, Newcastle disease, Virus, 03 medical and health sciences, Immune system, Cancer immunotherapy, Immunity, Drug Discovery, Genetics, medicine, Molecular Biology, Pharmacology, biology, business.industry, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, 3. Good health, Oncolytic virus, Pre existing immunity, 030104 developmental biology, Immunology, bacteria, Molecular Medicine, Syngeneic mouse, business

Abstract

Anti-viral immunity presents a major hurdle for systemically administered oncolytic viruses (OV). Intratumoral OV therapy has a potential to overcome this problem through activation of anti-tumor immune response, with local and abscopal effects. However, the effects of anti-viral immunity in such a setting are still not well defined. Using Newcastle Disease Virus (NDV) as a model, we explore the effects of pre-existing anti-viral immunity on therapeutic efficacy in syngeneic mouse tumor models. Unexpectedly, we find that while pre-existing immunity to NDV limits its replication in tumors, tumor clearance, abscopal anti-tumor immune effects, and survival are not compromised and, on the contrary, are superior in NDV-immunized mice. These findings demonstrate that pre-existing immunity to NDV may increase its therapeutic efficacy through potentiation of systemic anti-tumor immunity, which provides clinical rationale for repeated therapeutic dosing and prompts investigation of such effects with other OVs.

Published

2018

6. Devimistat in Combination with Bendamustine Potently Inhibits Tumor Growth and Promotes CD8+ T Cell Tumor Infiltration in a Syngeneic Mouse Model of CD30+ T-Cell Lymphoma

Author

Bayard L. Powell, Elizabeth Forbes, Enzo Palma, Timothy S. Pardee, Qianqian Song, Rakhee Vaidya, Wei Zhang, and Ashley Ballard

Subjects

Bendamustine, CD30, Chemistry, Immunology, Cell Biology, Hematology, medicine.disease, Biochemistry, medicine, Cancer research, T-cell lymphoma, Syngeneic mouse, Cytotoxic T cell, Tumor growth, Infiltration (medical), medicine.drug

Abstract

Introduction: Chimeric antigen receptor-based T cell therapy (CAR-T) has shown great promise in B cell malignancies. CD30-targeted therapies like brentuximab vedotin have activity in T cell malignancies expressing CD30. There is interest in developing CD30-targeted CAR-T therapies for the treatment of relapsed T cell malignancies. As the process of generating autologous T cells takes several weeks, there is a need for active bridging therapeutic regimens that can reduce tumor burden to facilitate subsequent treatment with CAR-T cell therapy. We propose the use of devimistat, a TCA cycle inhibitor, in combination with bendamustine as bridging therapy for the treatment of CD30+ T cell lymphoma (TCL) prior to the use of CAR-T cells. We hypothesize that TCA cycle inhibition will increase the sensitivity of TCL cells to bendamustine, negatively impact the function of immunosuppressive cell populations that depend on mitochondrial metabolism, and create a conducive environment for enhanced CAR-T cell efficacy. To test our hypothesis, we developed a model of CD30+ TCL, evaluated the efficacy of the combination, and characterized its effects by transcriptome profiling of immune cell populations in tumors. Methods: Mouse TCL cell line EL4-LUC2 was engineered to express human CD30 by retroviral transduction. Single and combination in vitro efficacy was evaluated by viability assays. Combination indices (CI) were calculated using Compusyn. CD30+ EL4-LUC2 cells (EL4.CD30) were inoculated subcutaneously into the flanks of C57Bl6 mice, tumor volumes were calculated, and CD30 expression in tumors was evaluated by immunohistochemical staining and flow cytometry. Transcriptome profiling was performed on a representative subset of tumors by single cell RNA sequencing (scRNA-seq). Results: EL4.CD30 cells displayed comparable CD30 expression to the human TCL cell line Karpas 299. EC 50 values for Devimistat and bendamustine in EL4.CD30 cells were 64.9 mM (95% CI: 62.4-67.4) and 101.2 mM (96.2-106.4), respectively; in Karpas 299, EC 50 values for Devimistat and bendamustine were substantially higher: 117.2 mM (114.7-119.6) and 188.2 mM (180.0 - 196.8), respectively. When dosed in combination, devimistat and bendamustine (D/B) showed synergy (CI = 0.5-0.8) at effect levels > 0.9 in 8 of the 16 dose combinations tested. D/B synergy at an effect level > 0.9 was less overt in Karpas 299 with only 2 of 16 tested combination levels displaying CI values of 0.5-0.9. Efficacy studies with EL4.CD30 tumor-bearing mice revealed potent D/B anti-tumor activity relative to vehicle and single-agent treatment groups. Six complete regressions and 4 partial regressions were observed in the D/B group (Fig. 1A). Moreover, tumor growth rates and median survival values were significantly different (p Conclusions: Our data demonstrate that D/B has potent pharmacological activity in vitro and in vivo and promotes CTL influx into tumors. This suggests that D/B creates an immunopermissive environment fit for CAR-T cell activity. Subsequent studies will investigate the efficacy of CD30.CAR-T cells following D/B treatment. A Phase II pilot study evaluating the feasibility, safety, and tolerability of D/B in patients with relapsed/refractory T-cell Non-Hodgkin Lymphoma is currently ongoing (NCT04217317). Figure 1 Figure 1. Disclosures Pardee: Rafael Pharmaceuticals: Consultancy, Research Funding; Karyopharm Pharmaceuticals: Research Funding; AbbVie: Membership on an entity's Board of Directors or advisory committees, Speakers Bureau; Genetech: Membership on an entity's Board of Directors or advisory committees; BMS: Speakers Bureau; Pharmacyclics: Speakers Bureau.

Published

2021

7. IMMU-22. THE IMPACT OF MICROGLIA MODULATION ON GBM PROGRESSION IN SYNGENEIC MOUSE MODELS

Author

Gregor Hutter, Tomás A Martins, Tala Shekarian, Marie-Françoise Ritz, and Philip Schmassmann

Subjects

Cancer Research, Platelet-derived growth factor, Microglia, Phagocytosis, Biology, Acquired immune system, chemistry.chemical_compound, medicine.anatomical_structure, Immune system, Oncology, chemistry, Tumor progression, Cancer research, medicine, Syngeneic mouse, Neurology (clinical), Immunocompetence

Abstract

BACKGROUND The tumor immune microenvironment (TME) of Glioblastoma consists of almost myeloid-derived macrophages and microglia called TAMs. We have shown that the disruption of CD47-Sirpα-axis induces an antitumor activity of TAMs against GBM in immune-deficient mice, through increases of phagocytosis of tumor cells by TAMs. We have aimed to study the role of microglia and its activation/depletion on GBM progression, in the syngeneic GBM model in immune-competent mice. We have studied the interplay of innate and adaptive immune response after activation and depletion of microglia and the effect on tumor progression and outcome of the mice. MATERIAL AND METHODS We used different colonies of genetically modified immunocompetent mouse strains to genetically activate/deplete microglia in the tumor context. We generated Sall1 CreERT2/fl mice and Cre-negative littermates. The application of Tamoxifen in this constellation leads to the excision of the transcription factor Sall1 and subsequent enhanced microglia activity. Conversely, we generated Sall1 CreERT2 x Csf1r fl/fl animals and the respective heterozygous and Cre-negative littermates in which Tamoxifen treatment leads to inactivation of microglia through the deletion of Csf1r. Glioblastoma tumors were induced by intracerebral injection of GL261, CT2A, or retrovirus-induced PDGF-Akt in pups and Tamoxifen treatment was started once the tumors were detected. RESULTS We observed a survival advantage in tumor-bearing mice after activation of microglia in Sall1 CreERT/fl animals compared to Cre-negative littermates. Genetic depletion of microglia in this model resulted in a shorter lifespan in microglia-depleted animals compared to Cre-negative littermates. Furthermore, the iTME in these tumors is subjected to scRNAseq analysis to identify mechanistic insights. CONCLUSION Microglia are important players in tumor development and progression of glioblastoma in mouse models. These cells may be targeted in future immunotherapeutic approaches for patients.

Published

2021

8. 559 Preclinical evaluation of pegylated liposomal Doxorubicin or Doxorubicin with mATRC-101 in the EMT6 syngeneic mouse model

Author

Erin Wechsler, Nikhil Vad, and Danhui Zhang

Subjects

Pharmacology, Cancer Research, Oncology, Chemistry, Immunology, medicine, Cancer research, Molecular Medicine, Immunology and Allergy, Syngeneic mouse, Doxorubicin, Pegylated Liposomal Doxorubicin, medicine.drug

Abstract

BackgroundWe previously described ATRC-101, a fully human, engineered IgG1 antibody which is currently under evaluation in the clinic as a monotherapy for solid tumors. A chimeric version of this antibody expressed on a mouse IgG2a (mATRC-101) has shown robust anti-tumor activity as a monotherapy in the EMT6 syngeneic tumor model. In order to assess the potential utility of ATRC-101 in combination with chemotherapeutic agents, non-clinical studies were performed to assess the efficacy of mATRC-101 in combination with chemotherapeutic agents, including Doxorubicin and pegylated liposomal Doxorubicin (PLD), and the impact of these anti-tumor small molecules on mATRC-101 immunoreactivity in mouse tumor and normal tissues.MethodsFemale BALB/c mice with established EMT6 tumors were dosed with mATRC-101 (1 or 3 mg/kg) or vehicle intraperitoneally (IP) twice weekly plus Doxorubicin (2 or 5 mg/Kg) or vehicle (saline) IV once weekly following randomization on Day 6. Statistical analyses of tumor volumes were performed using the normalized area above the curve and the normalized growth rate metrics developed at Atreca. One-sided log-rank (Mantel-Cox) test was used to assess survival advantage relative to the indicated reference group. P-values ≤0.05 were considered significant. In monotherapy studies with Doxorubicin and PLD, EMT6 tumor and non-tumor bearing mice were dosed with vehicle or Doxorubicin (2, 10 mg/kg) or PLD (1, 2, 5,10 mg/kg). Normal mouse tissues were collected at 24 hours and 2 weeks after the last dose. Reactivity for mATRC-101 in EMT6 tumor and normal mouse tissues was evaluated by immunohistochemistryResultsThe combination of 3 mg/kg mATRC-101 and 5 mg/kg Doxorubicin demonstrated significant tumor growth inhibition compared to either monotherapy, or vehicle (pConclusionsThis study provides non-clinical evidence that administration of mATRC-101 in combination with Doxorubicin increases anti-tumor activity in the EMT6 model. Exposure to Doxorubicin or PLD in EMT6 tumor-bearing mice increased mATRC-101 immunoreactivity in the tumor, in a dose-dependent manner Moreover, mATRC-101 immunoreactivity in normal tissues was not influenced by Doxorubicin or PLD. Taken together, these findings support clinical evaluation of the combination of ATRC-101 and doxorubicin.

Published

2021

9. Differential response to exercise in claudin-low breast cancer

Author

Seewaldt, Lee W. Jones, Oliver Glass, Michelle L. Bowie, Jason W. Locasale, Boss K, Fuller J, Christina L. Williams, Xiaojing Liu, David B. Darr, Jerry Usary, Mark W. Dewhirst, Zhen Zhang, and Kingshuk Roy Choudhury

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, Exercise treatment, Digoxin, mouse model, claudin-low, 03 medical and health sciences, breast cancer, 0302 clinical medicine, Breast cancer, Endurance training, Internal medicine, medicine, Treadmill, Cardiac glycoside, exercise, business.industry, medicine.disease, Claudin-Low, 3. Good health, 030104 developmental biology, Hif1-α, 030220 oncology & carcinogenesis, Syngeneic mouse, business, Research Paper, medicine.drug

Abstract

Exposure to exercise following a breast cancer diagnosis is associated with reductions in the risk of recurrence. However, it is not known whether breast cancers within the same molecular-intrinsic subtype respond differently to exercise. Syngeneic mouse models of claudin-low breast cancer (i.e., EO771, 4TO7, and C3(1)SV40Tag-p16-luc) were allocated to a uniform endurance exercise treatment dose (forced treadmill exercise) or sham-exercise (stationary treadmill). Compared to sham-controls, endurance exercise treatment differentially affected tumor growth rate: 1- slowed (EO771), 2- accelerated (C3(1)SV40Tag-p16-luc), or 3- was not affected (4TO7). Differential sensitivity of the three tumor lines to exercise was paralleled by effects on intratumoral Ki-67, Hif1-α, and metabolic programming. Inhibition of Hif1-α synthesis by the cardiac glycoside, digoxin, completely abrogated exercise-accelerated tumor growth in C3(1)SV40Tag-p16-luc. These results suggest that intratumoral Hif1-α expression is an important determinant of claudin-low breast cancer adaptation to exercise treatment.

Published

2017

10. Targeting CD47: the achievements and concerns of current studies on cancer immunotherapy

Author

Yuting Huang, Peng Gao, Zhi Yao, and Yuchi Ma

Subjects

0301 basic medicine, Pulmonary and Respiratory Medicine, medicine.medical_treatment, Bioinformatics, 03 medical and health sciences, 0302 clinical medicine, Cancer immunotherapy, Medicine, neoplasms, Antibody-dependent cell-mediated cytotoxicity, Innate immune system, biology, business.industry, CD47, humanities, respiratory tract diseases, Clinical trial, 030104 developmental biology, Immunology, Cancer cell, biology.protein, Syngeneic mouse, business, Calreticulin, Research Article, 030215 immunology

Abstract

Small-cell lung cancer (SCLC) is a highly aggressive subtype of lung cancer with limited treatment options. CD47 is a cell-surface molecule that promotes immune evasion by engaging signal-regulatory protein alpha (SIRPα), which serves as an inhibitory receptor on macrophages. Here, we found that CD47 is highly expressed on the surface of human SCLC cells; therefore, we investigated CD47-blocking immunotherapies as a potential approach for SCLC treatment. Disruption of the interaction of CD47 with SIRPα using anti-CD47 antibodies induced macrophage-mediated phagocytosis of human SCLC patient cells in culture. In a murine model, administration of CD47-blocking antibodies or targeted inactivation of the Cd47 gene markedly inhibited SCLC tumor growth. Furthermore, using comprehensive antibody arrays, we identified several possible therapeutic targets on the surface of SCLC cells. Antibodies to these targets, including CD56/neural cell adhesion molecule (NCAM), promoted phagocytosis in human SCLC cell lines that was enhanced when combined with CD47-blocking therapies. In light of recent clinical trials for CD47-blocking therapies in cancer treatment, these findings identify disruption of the CD47/SIRPα axis as a potential immunotherapeutic strategy for SCLC. This approach could enable personalized immunotherapeutic regimens in patients with SCLC and other cancers.

Published

2017

11. Deletion of Sirtuin 6 affects tumor-directed innate immune responses in a syngeneic mouse model of hepatocellular carcinoma

Author

D Strand, H Alizor, I Ernst, S Strand, PR Galle, N Zhivkova, and D Gottfried-Brand

Subjects

Innate immune system, biology, Hepatocellular carcinoma, Sirtuin, biology.protein, medicine, Cancer research, Syngeneic mouse, medicine.disease

Published

2020

12. Tankyrase inhibition sensitizes melanoma to PD-1 immune checkpoint blockade in syngeneic mouse models

Author

Elisabeth Dybing, Marte Fauskanger, Nina Therese Solberg, Aleksandra Aizenshtadt, Eivind Hovig, Jo Waaler, Anders Aune Tveita, Martin Frank Strand, Shoshy Alam Brinch, Clara Hammarström, Max Lycke, Karen-Marie Heintz, Alexandre Corthay, Petter Angell Olsen, Vegard Nygaard, Kaja Lund, Sigurd Laeines Boe, Line Mygland, and Stefan Krauss

Subjects

0301 basic medicine, Cytotoxicity, Immunologic, Skin Neoplasms, Programmed Cell Death 1 Receptor, Melanoma, Experimental, Medicine (miscellaneous), Cancer immunotherapy, CD8-Positive T-Lymphocytes, 0302 clinical medicine, Antineoplastic Combined Chemotherapy Protocols, Sulfones, Enzyme Inhibitors, lcsh:QH301-705.5, Immune Checkpoint Inhibitors, Wnt Signaling Pathway, Melanoma, beta Catenin, Tankyrases, Wnt signaling pathway, Drug Synergism, Tumor Burden, Mice, Inbred DBA, 030220 oncology & carcinogenesis, Female, General Agricultural and Biological Sciences, Cancer therapy, Mice, Transgenic, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Interferon-gamma, Immune system, Lymphocytes, Tumor-Infiltrating, Targeted therapies, medicine, Animals, Humans, Adaptor Proteins, Signal Transducing, business.industry, YAP-Signaling Proteins, Triazoles, medicine.disease, Immune checkpoint, Blockade, Mice, Inbred C57BL, 030104 developmental biology, HEK293 Cells, lcsh:Biology (General), Cancer research, Syngeneic mouse, business, CD8

Abstract

The development of immune checkpoint inhibitors represents a major breakthrough in cancer therapy. Nevertheless, a substantial number of patients fail to respond to checkpoint pathway blockade. Evidence for WNT/β-catenin signaling-mediated immune evasion is found in a subset of cancers including melanoma. Currently, there are no therapeutic strategies available for targeting WNT/β-catenin signaling. Here we show that a specific small-molecule tankyrase inhibitor, G007-LK, decreases WNT/β-catenin and YAP signaling in the syngeneic murine B16-F10 and Clone M-3 melanoma models and sensitizes the tumors to anti-PD-1 immune checkpoint therapy. Mechanistically, we demonstrate that the synergistic effect of tankyrase and checkpoint inhibitor treatment is dependent on loss of β-catenin in the tumor cells, anti-PD-1-stimulated infiltration of T cells into the tumor and induction of an IFNγ- and CD8+ T cell-mediated anti-tumor immune response. Our study uncovers a combinatorial therapeutical strategy using tankyrase inhibition to overcome β-catenin-mediated resistance to immune checkpoint blockade in melanoma., Waaler et al. show that a tankyrase inhibitor, G007-LK, decreases WNT/β-catenin and YAP signaling, sensitizing tumors to anti-PD-1 immune checkpoint therapy in mice. This study suggests that a combinatorial therapy using tankyrase inhibition can be used to overcome β-catenin-mediated resistance to immune checkpoint blockade in melanoma.

Published

2020

13. Design and characterization of mouse IgG1 and IgG2a bispecific antibodies for use in syngeneic models

Author

Pavel Strop, Feng Wang, Donata David-brown, Bryant Chau, Christine Bee, Jordan C Tsai, Alexander T. Kozhich, Arvind Rajpal, Jason M. Hogan, Sean M. West, Thomas Cayton, Jia Dong, Tim Sproul, Winse Morishige, Matthew L. Wheeler, Jonathan H Davis, Chengyue Zhang, and Gavin Dollinger

Subjects

Bispecific antibody, CD3 Complex, Protein Conformation, CD3, T-Lymphocytes, inter-chain disulfide bond shifting, Immunology, Mouse bispecific antibodies, electrostatic steering, Computational biology, CHO Cells, Protein Engineering, 03 medical and health sciences, Mice, 0302 clinical medicine, Immune system, Cricetulus, Report, Antibodies, Bispecific, Immunology and Allergy, Animals, Cloning, Molecular, 030304 developmental biology, CD20, 0303 health sciences, biology, Correction, co-expression, Disease Models, Animal, Transplantation, Isogeneic, 030220 oncology & carcinogenesis, Immunoglobulin G, biology.protein, Syngeneic mouse, T-cell engaging bispecific antibody, syngeneic mouse model, Antibody, Rituximab, Protein Binding

Abstract

The development of antibody therapeutics relies on animal models that accurately recapitulate disease biology. Syngeneic mouse models are increasingly used with new molecules to capture the biology of complex cancers and disease states, and to provide insight into the role of the immune system. The establishment of syngeneic mouse models requires the ability to generate surrogate mouse counterparts to antibodies designed for humans. In the field of bispecific antibodies, there remains a dearth of technologies available to generate native IgG-like mouse bispecific antibodies. Thus, we engineered a simple co-expression system for one-step purification of intact mouse IgG1 and IgG2a bispecific antibodies from any antibody pair. We demonstrated proof of concept with CD3/CD20 bispecific antibodies, which highlighted both the quality and efficacy of materials generated by this technology.

Published

2019

14. Natural killer cells impede the engraftment of cardiomyocytes derived from induced pluripotent stem cells in syngeneic mouse model

Author

Shigemi Sasawatari, Shohei Yoshida, Yuki Nakamura, Koichi Toda, Yoshiki Sawa, Toshihiko Toyofuku, and Shigeru Miyagawa

Subjects

0301 basic medicine, Cell Survival, Induced Pluripotent Stem Cells, lcsh:Medicine, Major histocompatibility complex, Article, Mice, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, health services administration, MHC class I, Animals, Myocytes, Cardiac, lcsh:Science, Induced pluripotent stem cell, health care economics and organizations, Immune rejection, Heart Failure, Multidisciplinary, Innate immune system, biology, lcsh:R, Cell Differentiation, Immunity, Innate, Cell biology, Killer Cells, Natural, Innate immune cells, Transplantation, Disease Models, Animal, 030104 developmental biology, biology.protein, Syngeneic mouse, lcsh:Q, Antibody, 030217 neurology & neurosurgery, Stem Cell Transplantation

Abstract

Transplantation of cardiomyocytes derived from induced pluripotent stem cell (iPSC-CMs) is a promising approach for increasing functional CMs during end-stage heart failure. Although major histocompatibility complex (MHC) class I matching between donor cells and recipient could reduce acquired immune rejection, innate immune responses may have negative effects on transplanted iPSC-CMs. Here, we demonstrated that natural killer cells (NKCs) infiltrated in iPSC-CM transplants even in a syngeneic mouse model. The depletion of NKCs using an anti-NKC antibody rescued transplanted iPSC-CMs, suggesting that iPSC-CMs activated NKC-mediated innate immunity. Surprisingly, iPSC-CMs lost inhibitory MHCs but not activating ligands for NKCs. Re-expression of MHC class I induced by IFN-γ as well as suppression of activating ligands by an antibody rescued the transplanted iPSC-CMs. Thus, NKCs impede the engraftment of transplanted iPSC-CMs because of lost MHC class I, and our results provide a basis for an approach to improve iPSC-CM engraftment.

Published

2019

15. Rapid screening of engineered microbial therapies in a 3D multicellular model

Author

Taylor E. Hinchliffe, Samuel Castro, Oscar Velazquez, William H. Mather, Zakary S. Singer, Tal Danino, Tetsuhiro Harimoto, and Joanna Zhang

Subjects

Salmonella typhimurium, High-throughput screening, Computational biology, Biology, 03 medical and health sciences, Synthetic biology, Mice, 0302 clinical medicine, Synthetic gene, Spheroids, Cellular, Diagnosis, Escherichia coli, Animals, Gene Regulatory Networks, Proteus mirabilis, Diagnostic Techniques and Procedures, 030304 developmental biology, 0303 health sciences, Multidisciplinary, Disease progression, Translation (biology), Biological Sciences, Biocontainment, Listeria monocytogenes, In vitro, Coculture Techniques, High-Throughput Screening Assays, Multicellular organism, Disease Models, Animal, 030220 oncology & carcinogenesis, Tumor reduction, Multicellular spheroid, Syngeneic mouse, Synthetic Biology, Drug Screening Assays, Antitumor, Genetic Engineering

Abstract

Synthetic biology is transforming therapeutic paradigms by engineering living cells and microbes to intelligently sense and respond to diseases including inflammation1,2, infections3-5, metabolic disorders6,7, and cancer8,9. However, the ability to rapidly engineer new therapies far outpaces the throughput of animal-based testing regimes, creating a major bottleneck for clinical translation10,11. In vitro approaches to address this challenge have been limited in scalability and broad-applicability. Here, we present a bacteria-in-spheroid co-culture (BSCC) platform that simultaneously tests host species, therapeutic payloads and synthetic gene circuits of engineered bacteria within multicellular spheroids over a timescale of weeks. Long-term monitoring of bacterial dynamics and disease progression enables quantitative comparison of critical therapeutic parameters such as efficacy and biocontainment. Specifically, we screen S. typhimurium strains expressing and delivering a library of antitumor therapeutic molecules via several synthetic gene circuits. We identify novel candidates exhibiting significant tumor reduction and demonstrate high similarity in their efficacies using a syngeneic mouse model. Lastly, we show that our platform can be expanded to dynamically profile diverse microbial species including L. monocytogenes, P. mirabilis, and E. coli in various host cell types. This high-throughput framework may serve to accelerate synthetic biology for clinical applications and understanding the host-microbe interactions in disease sites.

Published

2019

16. Abstract 1796: PD-L1 photoimmunotherapy kills immunosuppressive myeloid cells to activate local and systemic antitumor immunity in syngeneic mouse models

Author

Jason Lapetoda, Amy H. Thorne, Daniel Mendoza, Christopher M. Parry, Michelle H. Hsu, Miguel Garcia-Guzman, and Jerry Fong

Subjects

Cancer Research, Oncology, biology, Antitumor immunity, business.industry, PD-L1, Myeloid cells, biology.protein, Cancer research, Medicine, Syngeneic mouse, Photoimmunotherapy, business

Abstract

Introduction: Photoimmunotherapy is an investigational anticancer treatment platform that combines the cell surface binding of an antibody conjugated to a light activatable dye (IRDye® 700DX, IR700) with non-thermal red light illumination for selective cell killing. PD-L1, the target of anti-PD-L1 inhibitors, is a suppressive checkpoint marker expressed on tumor cells and immunosuppressive myeloid cells in the tumor microenvironment. Here we examined the anticancer activity and immune activation elicited by anti-PD-L1-IR700 photoimmunotherapy (PD-L1 photoimmunotherapy). Methods: CT26 or LL/2 tumors were used to assess antitumor immune response following PD-L1 photoimmunotherapy. CT26PD-L1-/- tumors were generated by CRISPR/Cas9. Tumor volume was determined by caliper measurements in illuminated and non-illuminated tumors. Intratumoral immune responses were assessed by flow cytometry. Complete responder (CR) mice were challenged with either CT26 or 4T1 tumors to evaluate immune memory. Results: Mice bearing CT26 or LL/2 tumors treated with PD-L1 photoimmunotherapy exhibited a notable reduction of tumor growth compared to mice that received control treatments (saline, anti-PD-L1-IR700 conjugate alone without illumination, or multi-dosing with anti-PD-L1 antibody). Pre-treatment depletion of CD8+ T cells in the mice abrogated the antitumor activity of PD-L1 photoimmunotherapy, demonstrating a key role of CD8+ T-cell effector activity in the responses. PD-L1 photoimmunotherapy induced CRs in 7/15 mice, and all CR mice rejected CT26 tumor growth after re-challenge, indicating the generation of immunological memory. Furthermore, 6/8 mice rejected inoculation of 4T1 tumors, suggesting an enhanced ability to prime new T cells with tumor neoantigens. Intratumoral immune cell analysis showed a reduction of myeloid cells 2 hours following illumination, an increase of CD103+ dendritic cells 2 days following illumination, and an increase of non-exhausted PD-1-CD8+ T effector cells 8 days after illumination. In a bilateral tumor model, PD-L1 photoimmunotherapy resulted in tumor reduction in the non-illuminated tumor. Mice bearing CT26PD-L1-/- tumor cells similarly exhibited tumor reduction after PD-L1 photoimmunotherapy, suggesting that antitumor activity resulted from the elimination of PD-L1+ non-tumor cells. Conclusions: PD-L1photoimmunotherapy induces anticancer responses by killing PD-L1+ myeloid cells and possibly PD-L1+ cancer cells within the tumor, resulting in augmentation of local and systemic antitumor immunity. These results indicate that PD-L1 photoimmunotherapy can elicit anticancer immune responses in target and distal tumors, including syngeneic mouse models refractory to checkpoint inhibition. Citation Format: Amy H. Thorne, Michelle H. Hsu, Daniel Mendoza, Jason Lapetoda, Christopher M. Parry, Jerry J. Fong, Miguel Garcia-Guzman. PD-L1 photoimmunotherapy kills immunosuppressive myeloid cells to activate local and systemic antitumor immunity in syngeneic mouse models [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2021; 2021 Apr 10-15 and May 17-21. Philadelphia (PA): AACR; Cancer Res 2021;81(13_Suppl):Abstract nr 1796.

Published

2021

17. Abstract 265: Evaluating variation in drug efficacy endpoints in a syngeneic mouse model (CT26.WT) under immune checkpoint blockade

Author

Binchen Mao, Henry Li, Davy Ouyang, and Sheng Guo

Subjects

Efficacy, Cancer Research, Oncology, Cancer research, Syngeneic mouse, Biology, Immune checkpoint, Blockade

Abstract

INTRODUCTION: Preclinical research into immune checkpoint blockade (ICB) requires in vivo models with fully functional immunity. Syngeneic mouse models are homografts derived by transplanting immortalized mouse cancer cell lines or tumor tissues into strain-matched mouse hosts, and are well suited for evaluating the efficacy of new immunotherapies due to retaining an intact mouse immune system. Tumor growth inhibition (TGI) is widely used to characterize drug efficacy, however, a considerable amount of heterogeneity among TGI is often observed for a given ICB treatment in the same syngeneic mouse model. It is of vital importance to understand the source of such variation. The present study sets out to systematically investigate the variation of TGI for ICB treatment in syngeneic mouse models, using tumor growth data of anti-PD-1 treatment in the CT26.WT syngeneic mouse model for 27 independent studies. METHODS: For each study, we calculated TGI and median area under curve (AUC) ratio on the corresponding study day when tumor volume data was collected. We utilized standard deviation and inter quantile range to quantify the variation. We evaluated the relationship between TGI and the corresponding day, and also compared the variation between TGI and median AUC ratio. Furthermore, to better understand the source of drug efficacy variation, we utilized a Bayesian multilevel model to quantify the amount of tumor growth variation at both the study and mouse level. RESULTS: We found that TGI variation was much higher at earlier stages of studies. In contrast, the median AUC ratio showed smaller variation across the duration of each study than TGI for the majority of studies. Additionally, we found neither TGI nor median AUC ratio had significant correlation with the number of mice used in the study. Based on a Bayesian multilevel model, we observed that drug efficacy had larger variation on the mouse level (i.e. within a study), than variation on the study level (i.e. observed between studies), which could indicate heterogeneity of the tumor microenvironment (e.g. TILs) among mice play a major role in the variation of ICB treatment efficacy among studies. CONCLUSIONS: Response to ICB treatment among mice of the same syngeneic model is inherently heterogeneous. TGI of later time points should be favored to reduce variation, and generally median AUC Ratio is more stable than TGI. Citation Format: Binchen Mao, Sheng Guo, Davy Ouyang, Henry Li. Evaluating variation in drug efficacy endpoints in a syngeneic mouse model (CT26.WT) under immune checkpoint blockade [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2021; 2021 Apr 10-15 and May 17-21. Philadelphia (PA): AACR; Cancer Res 2021;81(13_Suppl):Abstract nr 265.

Published

2021

18. Defining the optimal murine models to investigate immune checkpoint blockers and their combination with other immunotherapies

Author

Miguel F. Sanmamed, Ignacio Melero, Holbrook E Kohrt, and Cariad Chester

Subjects

0301 basic medicine, Cell cycle checkpoint, medicine.medical_treatment, Cell Cycle Proteins, Mice, 03 medical and health sciences, Immune system, Neoplasms, Tumor Microenvironment, medicine, Animals, Humans, Tumor microenvironment, business.industry, Antibodies, Monoclonal, Cancer, Hematology, Immunotherapy, medicine.disease, Immune checkpoint, Human tumor, Disease Models, Animal, 030104 developmental biology, Oncology, Immunology, Cancer research, Syngeneic mouse, business

Abstract

The recent success of checkpoint blockers to treat cancer has demonstrated that the immune system is a critical player in the war against cancer. Historically, anticancer therapeutics have been tested in syngeneic mouse models (with a fully murine immune system) or in immunodeficient mice that allow the engraftment of human xenografts. Animal models with functioning human immune systems are critically needed to more accurately recapitulate the complexity of the human tumor microenvironment. Such models are integral to better predict tumor responses to both immunomodulatory agents and directly antineoplastic therapies. In this regard, the development of humanized models is a promising, novel strategy that offers the possibility of testing checkpoint blockers' capacity and their combination with other antitumor drugs. In this review, we discuss the strengths and weaknesses of the available animal models regarding their capacity to evaluate checkpoint blockers and checkpoint blocker-based combination immunotherapy.

Published

2016

19. TMOD-11. APPLICATION OF A NOVEL TRANSGENIC AND SYNGENEIC MOUSE MODELS OF HUMAN CLASSICAL GLIOBLASTOMA FOR DRUG SCREENING AND PRE-CLINICAL TRIALS

Author

Qingxia Wei, Kenneth Aldape, Hafsah Ali, Kanwalpreet Walia, Gelareh Zadeh, Mira Li, Farshad Nassiri, Olivia Singh, Mathew Voisin, Suganth Suppiah, and Shirin Karimi

Subjects

Drug, Cancer Research, business.industry, media_common.quotation_subject, Transgene, Clinical trial, Oncology, Tumor Models, Cancer research, Syngeneic mouse, Medicine, Classical Glioblastoma, Neurology (clinical), business, media_common

Abstract

Glioblastoma multiforme (GBM) is the most common malignant brain tumor in adults with 1 year median survival. The classical subtype of GBM occurs in about 10% of GBM cases and has the worst clinical outcome. The most frequent genetic alteration associated with classical GBM is amplification in the epidermal growth factor receptor (EGFR) and homozygous deletion in CDKN2A (Cyclin Dependent Kinase Inhibitor 2A). We generated a transgenic mouse harboring EGFRvIII, a constitutively active mutant of EGFR, knock in and homozygous deletion in p19 ARF, an alternative spliced form of the CDKN2a gene, restricted to glial cells. Transgenic mice develop tumors as early as 1 month and 73% of mice die by 6 months of age. MRIs reveal that mice develop infiltrative tumor cells throughout the brain and craniospinal junction with some infiltration within the leptomeninges that can result in hydrocephalus. Histology shows that 72% of tumors are high grade gliomas and some tumors demonstrate classical histological features of human GBM such as pseudopallisading necrosis, hyper vascularity and cellular atypia. We generated primary cell lines from transgenic mice that retained EGFRVIII expression and P19 ARF deletion and formed allografts in syngeneic mouse brains. Epigenetic modifications are considered a key mechanism in GBM development. We have therefore evaluated the efficacy of a panel of 42 compounds that target various epigenetic proteins including the readers, writers, and editors of several histone marks available from the Structural Genomics Consortium in primary cell lines derived from our mouse model. The primary cell lines were exposed to epigenetic drugs showing different responses to the same epigenetic modifiers. Key candidate drugs will further be tested pre-clinically in our syngeneic mouse model. In summary, we developed a novel transgenic and syngeneic mouse model for human classical GBM that can be used for drug screening and pre-clinical trials.

Published

2020

20. Targeting one-carbon metabolism in syngeneic mouse model of BRCA-mutated high-grade serous ovarian cancer

Author

Adrianne Wallace-Povirk, Larry H. Matherly, R.T. Morris, Carrie O'Connor, Zhanjun Hou, Aleem Gangjee, and Lisa Rubinsak

Subjects

One-carbon metabolism, Oncology, business.industry, Cancer research, Serous ovarian cancer, Obstetrics and Gynecology, Medicine, Syngeneic mouse, business

Published

2020

21. Abstract 2781: Diffusion weighted MRI evaluation of response to immunotherapy and radiotherapy in CT26 and 4T1 syngeneic mouse models of cancer

Author

Isabel Peset Martin, Denis G. Alferez, Susan Cheung, Muhammad Babur, Damien J. McHugh, Michael Berks, Yvonne Watson, James P B O'Connor, Ross A. Little, Kaye J. Williams, Jamie Honeychurch, and Grazyna Lipowska-Bhalla

Subjects

Radiation therapy, Cancer Research, Oncology, business.industry, medicine.medical_treatment, medicine, Cancer research, Cancer, Syngeneic mouse, Immunotherapy, medicine.disease, business, Diffusion MRI

Abstract

Immunotherapy has potential to improve outcome for cancer patients. The MRI biomarker apparent diffusion co-efficient (ADC) can map response to radiotherapy (RT) through its sensitivity to changes in tumor fluid and cellularity. The role of ADC in evaluating immunotherapy agents is unknown, despite investigators using ADC change as an exploratory endpoint in early phase clinical trials. Our study sought to evaluate and validate ADC changes induced by both RT and immunotherapy agents in syngeneic mouse tumor models. Three experiments were performed in BALB/c mice bearing CT26 colorectal cancers: (1) single 10Gy fraction RT versus control (sham); (2) TLR 7/8 agonist R848 versus control (saline); (3) anti-PD-L1 antibody versus control (saline). We acquired MRI data at 7T Bruker system at days 0, 3, 7, +/- 10 after therapy start, with tumors measuring between 250-300 mm3 at day 0. Median ADC and the inter-quartile range (IQR; a measure of tumor heterogeneity) were derived. Three further equivalent experiments were performed in BALB/c mice bearing triple negative 4T1 breast tumors. All CT26 and 4T1 tumors were bisected at cull for immunohistochemistry and FACS analysis. For CT26 model, RT-induced tumor growth inhibition (p In conclusion, our data are the first to evaluate ADC changes induced by RT and immunotherapy agents in syngeneic mouse models of cancer. RT, R848 and anti-PD-L1 induced different ADC responses, each with varied relationships to immune cells. This highlights the need for extensive validation before diffusion weighted MRI biomarkers can be used in clinical trials to monitor response to immunotherapies alone or in combination with RT. Citation Format: Grazyna Lipowska-Bhalla, Damien J. McHugh, Muhammad Babur, Isabel Peset Martin, Michael Berks, Ross A. Little, Susan Cheung, Yvonne Watson, Denis G. Alferez, Kaye J. Williams, Jamie Honeychurch, James P. O'Connor. Diffusion weighted MRI evaluation of response to immunotherapy and radiotherapy in CT26 and 4T1 syngeneic mouse models of cancer [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr 2781.

Published

2020

22. Tankyrase inhibition sensitizes melanoma to PD-1 immune checkpoint blockade in syngeneic mouse models

Author

Alexandre Corthay, Alam Brinch S, Kaja Lund, Sigurd Laeines Boe, Jo Waaler, Martin Frank Strand, Nina Therese Solberg, Line Mygland, Anders Aune Tveita, Angell Olsen P, Nygaard, Clara Hammarström, Max Lycke, Karen-Marie Heintz, Elisabeth Dybing, Stefan Krauss, and Eivind Hovig

Subjects

business.industry, Melanoma, Cancer research, Medicine, Syngeneic mouse, business, medicine.disease, Immune checkpoint, Blockade

Abstract

The development of immune checkpoint inhibitors represents a major breakthrough in cancer therapy. Nevertheless, a substantial number of patients fail to respond to checkpoint pathway blockade. β-catenin is the key transcriptional regulator of WNT/β-catenin signaling. Evidence for β-catenin-mediated immune evasion is found in 13% of all cancers, 42% of primary cutaneous melanoma and a mouse melanoma model. Currently, there are no therapeutic strategies available for targeting WNT/β-catenin signaling to counteract checkpoint inhibitor resistance in melanoma. Here we report that a specific small-molecule tankyrase inhibitor, G007-LK, attenuates WNT/β-catenin and YAP signaling pathways in the syngeneic murine B16-F10 melanoma model enabling sensitivity to anti-PD-1 immune checkpoint therapy. RNA sequencing of 18 tankyrase inhibitor-treated human melanoma cell lines and B16-F10 cells revealed a transcriptional response profile for a subpopulation. This cell line sub-group displayed elevated baseline YAP signaling activity and was susceptible to reduce melanocyte inducing transcription factor (MITF) expression upon tankyrase inhibition.

Published

2019

23. Evaluation of Breast Cancer and Melanoma Metastasis in Syngeneic Mouse Models

Author

Andreas Lundqvist and Kristina Witt

Subjects

business.industry, Melanoma, Tumor cells, medicine.disease, Metastasis, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Immune system, 030220 oncology & carcinogenesis, medicine, Cancer research, Syngeneic mouse, 030211 gastroenterology & hepatology, Tumor growth, business, B16 melanoma

Abstract

Syngeneic mouse models enable us to study the interaction of the immune system with tumor cells during tumor development and metastasis. It further allows us to evaluate the efficacy of immunotherapies on the different stages of tumor growth and the metastatic process. Here we describe two syngeneic mouse models, a murine mammary carcinoma and a murine melanoma model, that are used to study metastasis. Metastases occur spontaneously in the murine mammary carcinoma. The presence and number of foci are evaluated by culturing the lung tissue in a colony formation assay. For the murine melanoma model, tumor cells are injected intravenously, and metastatic burden is analyzed by counting of metastatic lesions.

Published

2019

24. Sirtuin 6 regulates innate immune responses in a syngeneic mouse model of hepatocellular carcinoma

Author

PR Galle, I Ernst, D Gottfried-Brand, Dennis Strand, Susanne Strand, N Zhivkova, J Schäfer, H Alizor, and H Janssen

Subjects

Innate immune system, biology, Hepatocellular carcinoma, Sirtuin, biology.protein, medicine, Cancer research, Syngeneic mouse, medicine.disease

Published

2019

25. Abstract B94: Targeted ablation of FoxP3+ T cells activates peripheral and tumor-infiltrating cytotoxic CD8+ T cells in multiple syngeneic mouse tumor models

Author

Sascha Rutz, Jill M. Schartner, Teresita Delfino, and Yingyun Wang

Subjects

Cancer Research, Chemistry, medicine.medical_treatment, Immunology, Cancer research, medicine, Cytotoxic T cell, Syngeneic mouse, FOXP3, Ablation, Peripheral

Abstract

FoxP3+ regulatory T cells (Treg) are essential to prevent autoimmunity but have also been implicated in suppressing antitumor immune responses. We assessed the impact of depletion of Treg cells in 8 different syngeneic tumor models, including cancer immunotherapy-sensitive and -resistant models. Robust, rapid tumor control or regression was observed in all models tested. Analysis of both peripheral and tumor-infiltrating T cells revealed that Treg cell depletion resulted in robust proliferation and cytokine production by CD8+ T cells in lymph nodes, spleen and tumor tissue. Tumor regression was CD8+ T cell-dependent, as antibody-mediated depletion of these cells abrogated tumor regression in a representative model. Interestingly, studies using FTY720 to pharmacologically block T-cell egress from the lymph nodes suggest that following Treg depletion cancer immunotherapy-sensitive models may not require new T-cell infiltration into tumor for tumor regression. This is in contrast to an immunotherapy-resistant model, which failed to regress following Treg depletion when lymph node egress was concurrently blocked. These data suggest that Treg cells play a critical role in suppressing both priming of novel anti-tumor CD8+ T-cell responses as well as limiting effector functionality of tumor-infiltrating CD8+ T cells within the tumor microenvironment. Citation Format: Yingyun Wang, Teresita Delfino, Jill M. Schartner, Sascha Rutz. Targeted ablation of FoxP3+ T cells activates peripheral and tumor-infiltrating cytotoxic CD8+ T cells in multiple syngeneic mouse tumor models [abstract]. In: Proceedings of the AACR Special Conference on Tumor Immunology and Immunotherapy; 2018 Nov 27-30; Miami Beach, FL. Philadelphia (PA): AACR; Cancer Immunol Res 2020;8(4 Suppl):Abstract nr B94.

Published

2020

26. Multimodality cellular and molecular imaging of concomitant tumour enhancement in a syngeneic mouse model of breast cancer metastasis

Author

Ashley V. Makela, Veronica P. Dubois, John A. Ronald, Katie M. Parkins, Amanda M. Hamilton, and Paula J. Foster

Subjects

0301 basic medicine, Green Fluorescent Proteins, lcsh:Medicine, Breast Neoplasms, Multimodal Imaging, Metastasis, 03 medical and health sciences, 0302 clinical medicine, Text mining, In vivo, Cell Line, Tumor, Animals, Humans, Medicine, Bioluminescence imaging, lcsh:Science, Mice, Inbred BALB C, Multidisciplinary, medicine.diagnostic_test, Brain Neoplasms, business.industry, lcsh:R, Magnetic resonance imaging, medicine.disease, Magnetic Resonance Imaging, Molecular Imaging, Disease Models, Animal, 030104 developmental biology, 030220 oncology & carcinogenesis, Concomitant, Luminescent Measurements, Cancer research, Syngeneic mouse, lcsh:Q, Female, Molecular imaging, business, Spleen

Abstract

The mechanisms that influence metastatic growth rates are poorly understood. One mechanism of interest known as concomitant tumour resistance (CTR) can be defined as the inhibition of metastasis by existing tumour mass. Conversely, the presence of a primary tumour has also been shown to increase metastatic outgrowth, termed concomitant tumour enhancement (CTE). The majority of studies evaluating CTR/CTE in preclinical models have relied on endpoint histological evaluation of tumour burden. The goal of this research was to use conventional magnetic resonance imaging (MRI), cellular MRI, and bioluminescence imaging to study the impact of a primary tumour on the development of brain metastases in a syngeneic mouse model. Here, we report that the presence of a 4T1 primary tumour significantly enhances total brain tumour burden in Balb/C mice. Using in vivo BLI/MRI we could determine this was not related to differences in initial arrest or clearance of viable cells in the brain, which suggests that the presence of a primary tumour can increase the proliferative growth of brain metastases in this model. The continued application of our longitudinal cellular and molecular imaging tools will yield a better understanding of the mechanism(s) by which this physiological inhibition (CTR) and/or enhancement (CTE) occurs.

Published

2018

27. A Syngeneic Pancreatic Cancer Mouse Model to Study the Effects of Irreversible Electroporation

Author

Jayanth S. Shankara Narayanan, Rebekah R. White, Ibtehaj A. Naqvi, and Partha Ray

Subjects

Male, 0301 basic medicine, Cancer Research, Necrosis, General Chemical Engineering, medicine.medical_treatment, Adenocarcinoma, General Biochemistry, Genetics and Molecular Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, Pancreatic cancer, Carcinoma, medicine, Animals, Humans, Tumor growth, Tumor microenvironment, General Immunology and Microbiology, business.industry, General Neuroscience, fungi, Irreversible electroporation, medicine.disease, Ablation, Mice, Inbred C57BL, Disease Models, Animal, Electroporation, 030104 developmental biology, 030220 oncology & carcinogenesis, Cancer research, Syngeneic mouse, medicine.symptom, business, Carcinoma, Pancreatic Ductal

Abstract

Pancreatic cancer (PC), a disease which kills approximately 40,000 patients each year in the US, has successfully evaded several therapeutic approaches including the promising immunotherapeutic strategies. Irreversible electroporation (IRE) is a non-thermal ablation technique that induces tumor cell death without destruction of adjacent collagenous structures, thus enabling the procedure to be performed in tumors very close to blood vessels. Unlike thermal ablation techniques, IRE results in gradual apoptotic cell death, along with immediate ablation induced necrosis, and is currently in clinical use for selected patients with locally advanced PC. An ablative, non-target specific procedure like IRE can induce a myriad of responses in the tumor microenvironment. A few studies have addressed the effects of IRE on tumor growth in other tumor types, but none have focused on PC. We have developed a syngeneic mouse model of PC in which subcutaneous (SQ) and orthotopic tumors can be successfully treated with IRE in a highly controlled setting, facilitating various longitudinal studies post procedure. This animal model serves as a robust system to study the effects of IRE and ways to improve the clinical efficacy of IRE.

Published

2018

28. Survival and Metabolic Function of Syngeneic Mouse Islet Grafts Transplanted Into the Hepatic Sinus Tract

Author

Ning Sun, Chengshuo Zhang, Xiaohang Li, Ao Jiao, Feng Li, and Jialin Zhang

Subjects

Blood Glucose, Male, endocrine system, Pathology, medicine.medical_specialty, Time Factors, endocrine system diseases, medicine.medical_treatment, Islets of Langerhans Transplantation, 030209 endocrinology & metabolism, Glucagon, Infusion Site, Article, 03 medical and health sciences, Islets of Langerhans, 0302 clinical medicine, Medicine, Animals, Insulin, Sinus (anatomy), Transplantation, geography, geography.geographical_feature_category, Metabolic function, business.industry, Graft Survival, Islet, Mice, Inbred C57BL, Transplantation, Isogeneic, surgical procedures, operative, medicine.anatomical_structure, Liver, Syngeneic mouse, 030211 gastroenterology & hepatology, business

Abstract

Background Islet grafts are transplanted into the liver via a portal vein in 90% of the clinical islet transplantations. However, the portal vein is far from being the ideal infusion site due to its unique drawbacks. These issues necessitated the exploration of an alternatively optimized site for clinical islet transplantation. With the widespread clinical application of percutaneous transhepatic puncture technique, we envisioned the possibility of islet transplantation into the hepatic sinus tract (HST). Methods The HST was created by temporarily placing a medically approved material into the hepatic parenchyma of C57BL/6 mice. The syngeneic islets were transplanted into the HST, after which, the nonfasting blood glucose, intraperitoneal glucose tolerance, and morphology were evaluated. Results A collagen-lined HST was formed by the 28-day implantation of a cylindrical nylon rod. Transplantation of ~300 syngeneic islets into the HST routinely reversed the hyperglycemia of the recipient mice and maintained normoglycemia for longer than 100 days until the graft was removed. The islet grafts within the HST stained positively for insulin, glucagon, and abundant microvessels and achieved comparable results to the islet grafts under the kidney capsule with respect to glycemic control and glucose tolerance. Conclusions These results suggested that an HST can be constructed for islet transplantation by temporarily placing a nylon material in the liver parenchyma. The HST is a promising site for clinical islet transplantation, thereby providing a satisfactory environment for the survival and metabolic function of islet grafts.

Published

2018

29. Pre-Existing Immunity to Oncolytic Virus Potentiates Its Immunotherapeutic Efficacy

Author

Anton Oseledchyk, Jedd D. Wolchok, Levi Mangarin, Jacob Ricca, Dmitriy Zamarin, and Taha Merghoub

Subjects

biology, business.industry, viruses, animal diseases, chemical and pharmacologic phenomena, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, Newcastle disease, Virus, Blockade, Oncolytic virus, Pre existing immunity, Immune system, Immunity, Immunology, bacteria, Syngeneic mouse, Medicine, business

Abstract

Anti-viral immunity presents a major hurdle for systemically-administered oncolytic viruses (OV). Intratumoral OV therapy has a potential to overcome this problem through activation of anti-tumor immune response, with local and abscopal effects. However, the effects of anti-viral immunity in such a setting are still not well defined. Using Newcastle Disease Virus (NDV) as a model, we explore the effects of pre-existing anti-viral immunity on therapeutic efficacy in syngeneic mouse tumor models. Unexpectedly, we find that while pre-existing immunity to NDV limits its replication in tumors, tumor clearance, abscopal effects and survival are not compromised and, on the contrary, are superior in NDV-immunized mice, both in a setting of NDV monotherapy and in combination with systemic CTLA-4 blockade. These findings demonstrate that pre-existing immunity to NDV may increase its therapeutic efficacy through potentiation of systemic anti-tumor immunity, which provides clinical rationale for repeated therapeutic dosing and prompts investigation of such effects with other OVs.

Published

2018

30. A personalised approach for anti-GITR-based immunotherapy in pre-clinical models of pancreatic ductal adenocarcinoma

Author

J.M.J. Larkin, Krisha Desai, Stephan Wullschleger, Chanthirika Ragulan, Douglas Hanahan, Kate Young, Elisa Fontana, Gary Box, Naureen Starling, Anguraj Sadanandam, David Cunningham, Patrick Varun Lawrence, and M.L. Tichet

Subjects

Oncology, medicine.medical_specialty, Pancreatic ductal adenocarcinoma, Response to therapy, business.industry, medicine.medical_treatment, Hematology, Immunotherapy, Fluorescence-Activated Cell Sorting, Internal medicine, Cancer genome, medicine, Syngeneic mouse, In patient, business, Tumor necrosis factor receptor, health care economics and organizations

Abstract

Background Patient outcomes with pancreatic ductal adenocarcinoma (PDA) remain dismal, despite the introduction of combination chemotherapies. Response to therapy is hampered by tumour stroma, which is highly heterogeneous but poorly characterised. The clinical success of immunotherapy in certain cancer types justifies investigation in PDA using a personalised approach of selecting pre-clinical models. Methods Patient PDA samples (n = 70; International Cancer Genome Consortium) were subjected to hierarchical clustering using a gene set representing CD8 and regulatory T cells to identify sub-groups. Syngeneic mouse models recapitulating these sub-groups (cross-species analysis) were developed using cell lines from genetically engineered mouse (GEM) models. Models bearing subcutaneous tumours were treated with anti-GITR agonist (DTA-1; 10mg/kg) or isotype (IgG2b) and tissues were collected for 12-color fluorescence activated cell sorting (FACS), NanoString and immunohistochemistry (IHC). Results Using clustering analysis, we identified four distinct patient PDA immune sub-groups with differential expression of T cell genes. These sub-groups showed differential expression of glucocorticoid-induced TNF receptor (GITR) and its associated genes. Hence, we hypothesised that these groups may respond differently to anti-GITR therapy in vivo. As expected, the three syngeneic models showed differential response to anti-GITR treatment. Model with increased GITR expression (>2-fold; NanoString and immunoblot) showed a significant (p = 0.02) survival benefit and a modest decrease in tumour burden upon anti-GITR treatment (n = 10) compared to the isotype control (n = 7) and the other two models. We observed anti-GITR mediated increase in GITR+ CD8+ cells and no change in GITR+ FOXP3+ cells (FACS, NanoString and IHC) along with increased gene expression of Pdcd1, Lag3, Spn and Itk. Conclusion Our models recapitulate the immunological gene expression profiles observed in patient PDA samples making them a highly useful resource to study personalized immunotherapies. This integrated study highlights the importance of patient selection to maximize therapy benefit and spare immune related adverse events. Legal entity responsible for the study The authors. Funding Bristol-Myers Squibb. Disclosure D. Cunningham: Research grant / Funding (self): Amgen; Research grant / Funding (self): Sanofi; Research grant / Funding (self): Merrimack; Research grant / Funding (self): AstraZeneca; Research grant / Funding (self): Celgene; Research grant / Funding (self): MedImmune; Research grant / Funding (self): Bayer; Research grant / Funding (self): 4SC; Research grant / Funding (self): Clovis; Research grant / Funding (self): Eli Lilly; Research grant / Funding (self): Janssen; Research grant / Funding (self): Merck. N. Starling: Research grant / Funding (self): AstraZeneca; Research grant / Funding (self): Bristol-Myers Squibb; Research grant / Funding (self): Pfizer; Travel / Accommodation / Expenses: AstraZeneca; Travel / Accommodation / Expenses: Bristol-Myers Squibb; Travel / Accommodation / Expenses: Eli Lilly; Travel / Accommodation / Expenses: Merck; Travel / Accommodation / Expenses: Roche; Honoraria (self): Eli Lilly; Honoraria (self): Merck Serono; Honoraria (self): MSD Oncology; Honoraria (self): Pierre Fabre; Advisory / Consultancy: Pfizer; Advisory / Consultancy: AstraZeneca; Advisory / Consultancy: Servier. A. Sadanandam: Research grant / Funding (self): Bristol-Myers Squibb; Research grant / Funding (self): Merck KGaa; Research grant / Funding (self): Pierre Fabre. All other authors have declared no conflicts of interest.

Published

2019

31. N-Myristoyltransferase Inhibition Decreases Tumor Growth in a Syngeneic Mouse Model of Lung Cancer

Author

Natalie C. McClintock, Stacy Behare, Kathryn T. Chen, and Begoña Díaz

Subjects

business.industry, Cancer research, Medicine, Syngeneic mouse, N-myristoyltransferase, Surgery, Tumor growth, business, Lung cancer, medicine.disease

Published

2019

32. P12.04 Synergistic effects of combination therapy of CAR-NK cells and anti-PD-1 antibody result in high efficacy against advanced stage orthotopic glioblastoma grafts in a syngeneic mouse model and induce protective anti-tumor immunity in vivo

Author

Joachim P. Steinbach, M I Strecker, Patrick N. Harter, Congcong Zhang, F Strassheimer, Winfried S. Wels, Michael C. Burger, Iris C. Mildenberger, and Torsten Tonn

Subjects

Cancer Research, Antitumor immunity, Combination therapy, business.industry, Advanced stage, Anti pd 1, medicine.disease, Poster Presentations, Oncology, In vivo, Cancer research, medicine, Syngeneic mouse, Neurology (clinical), business, Glioblastoma

Abstract

BACKGROUND Checkpoint inhibitors as well as adoptive cell therapy hold great promise for cancer treatment and encouraging treatment responses have already been demonstrated in different cancer indications. Glioblastoma (GB) is the most common and aggressive primary brain tumor. Standard therapy has very limited efficacy in the majority of patients. Analysis of the GB tumor microenvironment (TME) has shown prominent immunosuppressive features including expression of PD-L1 on tumor cells and increased frequency of FOX-P3 positive regulatory T cells. While the surrounding brain is HER2-negative, GB tumors are frequently HER2-positive, suggesting HER2 as a promising target for adoptive immunotherapy. MATERIALS AND METHODS The murine glioma cell line GL261 was transfected with HER2. Tumor cells were orthotopically implanted into C57BL/6 mice and treated either with HER2-specific NK-92/5.28.z cells alone or in combination with an anti-PD-1 antibody. Effects on tumor growth and survival were determined, lymphocyte infiltration and immunosuppressive TME were characterized. RESULTS Combined treatment with NK-92/5.28.z cells and anti-PD-1 antibody resulted in synergistic tumor regression and long-term survival of advanced-stage tumor bearing mice. Analysis of TME showed enhanced cytotoxic lymphocyte infiltration and altered profiles of exhaustion markers in tumor and immune cells. CONCLUSION These data demonstrate that efficacy of NK-92/5.28.z cells can be enhanced by co-therapy with checkpoint inhibitors, resulting in successful treatment of advanced tumors refractory to mono-therapy. Furthermore, this combination therapy induces a cytotoxic rather than immunosuppressive TME, leading to a primed immune system. To address this question in a clinical setting, we are planning a phase I clinical study (CAR2BRAIN-CHECK).

Published

2019

33. Abstract 3197: BI-907828, a novel and potent MDM2-p53 antagonist, acts synergistically in a triple combination with anti-PD-1 and anti-LAG-3 antibodies in syngeneic mouse models of cancer

Author

Martina Sykora, Dorothea Rudolph, Ulrike Weyer-Czernilofsky, Gabriela Gremel, Andreas Wernitznig, Sophia Blake, Markus Reschke, Jörg Rinnenthal, Andreas Gollner, Norbert Kraut, and Jürgen Moll

Subjects

0301 basic medicine, Cancer Research, biology, business.industry, Antagonist, Cancer, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Immune system, Oncology, biology.protein, Triple combination, Cancer research, Syngeneic mouse, Mdm2, Medicine, Antibody, business, CD8, 030215 immunology

Abstract

MDM2-p53 antagonists block the interaction between the Tumor Protein p53 and MDM2, its key negative regulator, and represent a new therapeutic concept for cancer therapy. MDM2-p53 antagonists are designed to restore p53 activity in TP53 wild-type tumors. Several MDM2-p53 antagonists are currently being evaluated in early clinical development. BI-907828 is a novel and potent MDM2-p53 antagonist with optimized drug-like properties that has shown efficacy in human tumor xenograft models at daily low oral dose as well as intermittent high dose schedules. Recent preclinical studies in syngeneic mouse models of cancer have demonstrated that BI-907828, apart from its direct tumor-targeting activity, also has immunomodulatory activity shown to contribute to efficacy. Single-agent BI-907828 induced anti-tumor immunological memory that controlled tumor growth in a re-challenge study. Moreover, a dual combination with an anti-mouse PD-1 checkpoint inhibitor resulted in synergistic efficacy in a syngeneic mouse model of cancer (AACR 2018, abstract 4866). Here we present data for the triple combination of BI-907828 with two checkpoint inhibitors. In syngeneic mouse tumor models (Colon-26 and B16-F10), the combination of BI-907828 with tool antibodies against mouse PD-1 and mouse LAG-3 shows high response rates of 50-90% with tumor regressions observed for even very large tumors. Moreover, efficacy of the triple combination is superior to each single agent and all dual combinations. An antibody-mediated depletion study suggests a contribution of CD8+ T cells but not of CD4+ T cells to full efficacy of the triple combination. FACS analysis of tumors isolated from Colon-26 tumor-bearing mice indicates that treatment with the triple combination leads to expansion of tumor-infiltrating CD8+ T cells. In summary, BI-907828 is a novel, potent, orally bioavailable MDM2-p53 antagonist that shows synergistic efficacy in a triple combination with antibodies targeting the immune checkpoints PD-1 and LAG-3 in syngeneic mouse models of cancer. BI-907828 is currently under evaluation in a Phase I clinical study (NCT03449381). Citation Format: Dorothea Rudolph, Ulrike Weyer-Czernilofsky, Markus Reschke, Martina Sykora, Jörg Rinnenthal, Sophia Blake, Gabriela Gremel, Andreas Wernitznig, Andreas Gollner, Norbert Kraut, Jürgen Moll. BI-907828, a novel and potent MDM2-p53 antagonist, acts synergistically in a triple combination with anti-PD-1 and anti-LAG-3 antibodies in syngeneic mouse models of cancer [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2019; 2019 Mar 29-Apr 3; Atlanta, GA. Philadelphia (PA): AACR; Cancer Res 2019;79(13 Suppl):Abstract nr 3197.

Published

2019

34. Slowdown intracranial glioma progression by optical hyperthermia therapy: study on a CT-2A mouse astrocytoma model

Author

Oscar Casanova-Carvajal, José Javier Serrano-Olmedo, Ricardo Martínez-Murillo, Ana Lorena Urbano-Bojorge, Milagros Ramos, Universidad Nacional Experimental del Táchira, Centro de Investigación Biomédica en Red Bioingeniería, Biomateriales y Nanomedicina (España), Universidad Politécnica de Madrid, and Ministerio de Ciencia e Innovación (España)

Subjects

medicine.medical_treatment, 02 engineering and technology, syngeneic mouse, Injections, Intralesional, 01 natural sciences, Stereotaxic Techniques, Mice, General Materials Science, AC133 Antigen, Telecomunicaciones, Nanotubes, medicine.diagnostic_test, Brain Neoplasms, Astrocytoma, hyperthermia, 021001 nanoscience & nanotechnology, Hyperthermia therapy, Tumor Burden, 3. Good health, Mechanics of Materials, Disease Progression, Laser Therapy, 0210 nano-technology, Hyperthermia, Materials science, Medicina, Bioengineering, 010402 general chemistry, In vivo, Cell Line, Tumor, medicine, Animals, Humans, Electrical and Electronic Engineering, Lasers, Mechanical Engineering, glioblastoma, Magnetic resonance imaging, Hyperthermia, Induced, General Chemistry, Surface Plasmon Resonance, CT-2A cells, medicine.disease, gold nanorods, Antibodies, Neutralizing, 0104 chemical sciences, Mice, Inbred C57BL, Transplantation, Disease Models, Animal, Tumor progression, Stereotaxic technique, Cancer research, Gold, Neoplasm Transplantation

Abstract

Metallic nanorods are promising agents for a wide range of biomedical applications. We report an optical hyperthermia method capable of inducing slowdown tumor progression of an experimental in vivo CT-2A glioblastoma tumor. The tumor model used in this research is based on the transplantation of mouse astrocytoma CT-2A cells in the striatum of mice by intracranial stereotaxic surgery. Two weeks after cell implant, the resulting tumor is treated by irradiating intratumoral injected gold nanorods, biofunctionalized with CD133 antibody (B-GNRs), using a continuous wave laser. Nanoparticles convert the absorbed light into localized heat (reaching up to 44 °C) due to the effect of surface plasmon resonance. A significant slowdown in CT-2A tumor progression is evident, by histology and magnetic resonance imaging, at one (p = 0.03) and two weeks (p = 0.008) after irradiation treatment. A notable deceleration in tumor size (15%-75%) as compared to the control untreated groups, it is observed. Thus, laser irradiation of B-GNRs is found to be effective for the treatment of CT-2A tumor progression. Similarities between the pre-clinical CT-2A tumor model and the human astrocytoma disease, in terms of anatomy, metastatic behavior and histopathology, suggest that hyperthermic treatment by laser irradiation of B-GNRs administered into high-grade human astrocytoma might constitute a promising alternative treatment to limit the progression of this deadly disease., We thank Ms Soledad Martinez (cell culture experiments), Centre for Biomedical Technology (CTB) for technical help. Also, PhD Teresa López de Mora for critical reading of the manuscript. The authors are thankful to their grant supporters, Universidad Nacional Experimental del Táchira (UNET)— Venezuela to Oscar Casanova-Carvajal. This study was also financially supported in part by CIBER-BBN (Spain) and NEUROCENTRO-CM (B2017/BMD-3760) consortium. Characterization of the MNPs has been performed by the ICTS 'NANBIOSIS', Unit 15 (Functional Characterization of Magnetic Nanoparticles) of the CIBER in Bioengineering, Biomaterials & Nanomedicine (CIBER-BBN) at the Center for Biomedical Technology (CTB) of the 'Universidad Politécnica de Madrid' (UPM). This work was carried out as part of Project PGC2018-097531-B-I00, funded by the Ministry of Science of Spain.

Published

2019

35. The effects of Wnt inhibition on tumor progression and the tumor microenvironment in a syngeneic mouse model of ovarian cancer

Author

Troy D. Randall, Selene Meza-Perez, Lyse A. Norian, Whitney N. Goldsberry, Ashwini A. Katre, David W. Doo, and Rebecca C. Arend

Subjects

Cancer Research, Tumor microenvironment, business.industry, Wnt signaling pathway, medicine.disease, Gene expression profiling, 03 medical and health sciences, 0302 clinical medicine, Oncology, Tumor progression, 030220 oncology & carcinogenesis, Cancer research, Medicine, Syngeneic mouse, business, Ovarian cancer, 030215 immunology

Abstract

e17078 Background: Alterations in the Wnt/β-catenin pathway have been associated with tumor progression in multiple cancers. Gene expression profiling in ovarian cancer has correlated Wnt upregulation to patterns of immune evasion in the tumor microenvironment (TME). We investigated effects of in vitro Wnt inhibition in a murine ovarian cancer cell line with p53 knocked out as a model to mimic human ovarian carcinoma. Methods: We used a small molecule inhibitor, CGX-1321, in C57Bl6 mice, an immunocompetent mouse model, injected intraperitoneally with either ID8 cells, a murine ovarian cancer cell line, or ID8-p53-/- cells. Mouse omentums were collected and weighed for evaluation of tumor growth. Representative histology slides were stained for H&E. Western blots for β-catenin baseline levels were performed on the cell lines. TopFlash Assays with WNT3A stimulation were used for analysis of cell line nuclear β-catenin levels. Flow cytometry was performed on mouse omentums for TME evaluation. Results: Treatment with CGX-1321 decreased tumor size via omentum weight with both cell lines, p = 0.0098 with ID8 cells and p = 0.0855 with ID8-p53-/- cells. H&E slides revealed a decreased tumor progression. Western blots confirmed a difference in baseline β-catenin levels between these two cell lines. However, TopFlash assays showed a response to stimulation. Changes in the TME between treated samples with ID8-p53-/- cells did now show significant differences via flow cytometry. Conclusions: In the syngeneic mouse model with a murine ovarian cancer cell line, with p53 knocked out, tumor size and proliferation were decreased with treatment with Wnt inhibition. Surprisingly, the TME changes were inconclusive via flow cytometry. Perhaps these cells do not rely upon the Wnt/ β-catenin pathway as heavily, as seen in changes to baseline β-catenin levels, or perhaps tumors progress quicker and the critical time point of TME change is being overlooked. More investigation needs to be performed to further elucidate these differences.

Published

2019

36. MR Imaging by Using Very Short Echo–Time Sequences after Syngeneic Lung Transplantation in Mice

Author

Natalie Chuck, Walter Weder, Wolfgang Jungraithmayr, Thomas Frauenfelder, and Andreas Boss

Subjects

Pathology, medicine.medical_specialty, medicine.medical_treatment, Ischemia, Signal-To-Noise Ratio, Mice, Imaging, Three-Dimensional, Parenchyma, medicine, Animals, Lung transplantation, Radiology, Nuclear Medicine and imaging, business.industry, respiratory system, medicine.disease, Magnetic Resonance Imaging, Mr imaging, respiratory tract diseases, Mice, Inbred C57BL, Transplantation, Isogeneic, Normal lung, Reperfusion Injury, Syngeneic mouse, business, Reperfusion injury, Lung Transplantation, Short echo time

Abstract

To test the in vivo feasibility of magnetic resonance (MR) imaging of ischemia reperfusion injury after syngeneic lung transplantation in mice and to characterize tissue relaxation properties by using very short echo-time (TE) sequences at 4.7 T.The experimental protocol was approved by the institutional animal committee. MR imaging was performed in six C57BL/6 mice 24 hours after the animals underwent syngeneic orthotopic left lung transplantation. A small-animal MR imager was equipped with a linear polarized hydrogen birdcage mouse coil. In addition to conventional T1-weighted spoiled gradient-echo and T2-weighted fast spin-echo sequences, three-dimensional very short TE sequences (50-5000 μsec) were performed. Color-encoded parametric maps of T2* transverse relaxation times were calculated on a pixel-by-pixel basis. Quantitative T2* values of the parenchyma of the transplanted lungs and relative spin density were compared by using region-of-interest analysis with the two-sided paired Student t test. After MR imaging, transplanted lungs were processed for histologic examination.Transplanted ventilated lungs in all the mice showed similar low signal intensity with the conventional T1- and T2-weighted sequences. The very short TE sequence exhibited signal yield in the lungs that was higher than that of the noise level. Increased spin density (50.8% ± 26.9 [standard deviation], P = .006) and longer T2* relaxation time (1041 μsec ± 424, P = .016) were found in the transplanted lungs. Best visualization was possible using color-encoded log-transformed parametric T2* maps. Conventional T2-weighted sequences revealed small pleural effusions. Histologic examination demonstrated ischemia reperfusion injury with a predominance of either cell influx or edema.Ischemia reperfusion injury after syngeneic lung transplantation can be visualized and characterized using very short TE sequences showing different MR imaging relaxation properties when compared with normal lung parenchyma.

Published

2012

37. P3.07-001 Overcoming Resistance to Anti-PD Immunotherapy in a Syngeneic Mouse Lung Cancer Model Using Adenovirus-Mediated Gene Therapy

Author

Bingliang Fang and X. Yan

Subjects

Pulmonary and Respiratory Medicine, Oncology, business.industry, Genetic enhancement, medicine.medical_treatment, Immunology, Medicine, Syngeneic mouse, Immunotherapy, business, Lung cancer, medicine.disease

Published

2017

38. Comparison of exendin-4 on beta-cell replication in mouse and human islet grafts

Author

Guangbin Weng, H Yi, Z. Guo, Jie Gao, Bole Tian, Timothy O'Brien, and L. Tian

Subjects

endocrine system, Transplantation, geography, medicine.medical_specialty, geography.geographical_feature_category, Insulin, medicine.medical_treatment, Diabetic mouse, Biology, Islet, medicine.disease, Staining, chemistry.chemical_compound, Endocrinology, chemistry, Internal medicine, Diabetes mellitus, medicine, Syngeneic mouse, Beta cell, Bromodeoxyuridine

Abstract

Exendin-4 can stimulate β-cell replication in mice. Whether it can stimulate β-cell replication in human islet grafts remains unknown. Therefore, we compared the effects of exendin-4 on β-cell replication in mouse and human islet grafts. Islets, isolated from mouse and human donors at different ages, were transplanted into diabetic mice and/or diabetic nude mice that were given bromodeoxyuridine (BrdU) with or without exendin-4. At 4 weeks post-transplantation, islet grafts were removed for insulin and BrdU staining and quantification of insulin(+)/BrdU(+) cells. Although diabetes was reversed in all mice transplanting syngeneic mouse islets from young or old donors, normoglycemia was achieved significantly faster in exendin-4 treated mice. Mouse islet grafts in exendin-4 treated mice had significantly more insulin(+)/BrdU(+) β cells than in untreated mice (P < 0.01). Human islet grafts from ≤22-year-old donors had more insulin(+)/BrdU(+) β cells in exendin-4 treated mice than that in untreated mice (P < 0.01). However, human islet grafts from ≥35-year-old donors contained few insulin(+)/BrdU(+) β cells in exendin-4 treated or untreated mice. Our data demonstrated that the capacity for β-cell replication in mouse and human islet grafts is different with and without exendin-4 treatment and indicated that GLP-1 agonists can stimulate β-cell replication in human islets from young donors.

Published

2011

39. Evaluation of an Intraperitoneal Ovarian Cancer Syngeneic Mouse Model Using18F-FDG MicroPET Imaging

Author

Todd E. Peterson, Ronald R. Price, Ki Taek Nam, Mohammed N. Tantawy, Hye Jeong Lee, and Inyeong Choi

Subjects

Standardized uptake value, Mice, Ovarian tumor, Peritoneal cavity, Fluorodeoxyglucose F18, Ovarian carcinoma, medicine, Animals, Tumor growth, Ovarian Neoplasms, Gastrointestinal tract, business.industry, Carcinoma, Obstetrics and Gynecology, medicine.disease, Mice, Inbred C57BL, medicine.anatomical_structure, Oncology, Positron-Emission Tomography, Models, Animal, Syngeneic mouse, Female, Radiopharmaceuticals, Nuclear medicine, business, Ovarian cancer, Injections, Intraperitoneal

Abstract

Objectives:The objective of this study was to evaluate the syngeneic immunocompetent mouse model by using the micro-positron emission tomography with 2-[fluorine-18]-fluoro-2-deoxy-d-glucose (18F-FDG microPET) imaging of ovarian tumor growth.Methods:ID8 ovarian carcinoma cells derived from C57BL/6 mice were intraperitoneally injected into female C57BL/6 mice. Mice were injected with18F-FDG (7.4 MBq, intravenous injection), and microPET images were obtained 40 minutes later. Micro-computed tomographic images were also obtained immediately after microPET images for anatomical reference.18F-FDG microPET images were acquired at baseline and at 4, 8, 10, and 11 weeks after tumor cell injection. The maximum standardized uptake value (SUVmax) in each time point was obtained from the images and compared to follow the tumor growth.Results:Physiological uptake of18F-FDG was intensely found in the bladder and heart and frequently in the gastrointestinal tract. Diffused uptake of18F-FDG was observed in the peritoneal cavity of all tumor-bearing mice at 4 weeks, and high focal uptakes were developed in the peritoneal cavity at 8 to 11 weeks. High focal uptakes increased over time, correlating with a progressive increase in the SUVmaxof18F-FDG. At 11 weeks, the SUVmaxvalue was significantly increased (1.49 ± 0.10 at 11 weeks vs 0.29 ± 0.03 at baseline,P< 0.01). Tumors in the gut and peritoneum were confirmed by anatomical and histopathological examination.Conclusions:Our results demonstrate that the peritoneal tumor growth in the syngeneic ovarian cancer model can be detected by the18F-FDG microPET imaging.

Published

2011

40. Immunotherapy with dendritic cells derived from bone marrow hematopoietic stems cells inhibited tumor growth on a TRAMP-C1 syngeneic mouse model of prostate cancer

Author

Choung Soo Kim, Hyunyong Kim, Hyunna Lee, Sungyoul Choi, Bong Min Kim, and Yunlim Kim

Subjects

business.industry, medicine.medical_treatment, Hematology, Immunotherapy, medicine.disease, Prostate cancer, Haematopoiesis, medicine.anatomical_structure, Oncology, Cancer research, Medicine, Syngeneic mouse, Tumor growth, Bone marrow, business, Tramp

Published

2018

41. The role of blood in early endometrial-peritoneal interactions in a syngeneic mouse model of endometriosis

Author

Minoru Irahara, Natsuyo Ugumori, Hiroyuki Furumoto, Akira Kuwahara, Toshiyuki Yasui, Hirokazu Uemura, Masaharu Kamada, Anna Tani, Masahiko Maegawa, Ayako Kobayashi, Toshiya Matsuzaki, Satoshi Yamamoto, and Yuka Kasai

Subjects

Pathology, medicine.medical_specialty, business.industry, medicine.medical_treatment, Endometriosis, Cell Biology, medicine.disease, Reproductive Medicine, Murine model, Fibrinolysis, medicine, Syngeneic transplantation, Syngeneic mouse, Original Article, Stage (cooking), business

Abstract

The aim of this study was to clarify the role of blood in the early stage of development of endometriotic lesions by developing a syngeneic transplantation model using immunocompetent mice.Endometriotic lesions were induced in C57BL/6 mice by an intraperitoneal injection of endometrial fragments plus saline or endometrial fragments plus blood. Some endometrial fragments plus blood were injected with heparin, hirudin or tissue plasminogen activator (tPA). Endometriotic lesions on days 1, 3 and 5 were evaluated by gross and microscopic findings.The areas of endometriotic lesions in the blood group (6.4 ± 1.7 mmBlood accelerates the early stage of development of endometriotic lesions when endometrial fragments plus blood are injected. Blood property might be involved in early endometrial-peritoneal interactions.

Published

2010

42. Abstract 1411: Proteogenomic analysis of the syngeneic mouse gastric stem cell-like cancer cell line

Author

Hanna Yang and Hark Kyun Kim

Subjects

Proteogenomic Analysis, Cancer Research, Oncology, Cancer research, Syngeneic mouse, Cancer cell lines, Stem cell, Biology

Abstract

Gastric cancer is the third main cause of cancer deaths worldwide. To understand molecular mechanism of gastric cancer incidence and metastasis, we generated NCC-S1M lacking Smad4, Trp53 and Cdh1, which is the unique syngeneic gastric cancer cell line transplant model in the scientific society. NCC-S1M showed cancer stem cell-like features and strong tumor-initiating potential. Using proteogenomic analysis of NCC-S1M, we elucidated the specific signaling pathways that control gastric cancer stem cell-like properties and immune checkpoint. Cd274, Ccne1 and Il1rl1 were overexpressed and their protein levels were higher than normal gastric tissues. Cd274 encodes PD-L1, which is one of the important immune checkpoint proteins. The growth rate of NCC-S1M allograft was reduced after treatment with anti-PD-1. When Smad4 was ectopically expressed in NCC-S1M, Cd274 expression was decreased. In addition, TGF-β treatment induced reduction in Cd274 expression of Smad4 overexpressed NCC-S1M cells even more comparing with normal Smad4 overexpressed NCC-S1M. The knockdown of Il1rl1 in NCC-S1M reduced tumorigenicity and in vivo chemoresistance. We demonstrated that NCC-S1M focally amplified Ccne1 gene through array comparative genomic hybridization. Ccne1 knocked down NCC-S1M showed reduced metastatic potential. The proteogenomic characterization of NCC-S1M explains that Smad4 is important for PD-L1 immune evasion and that Il1rl1 has a significant role in cancer stem cell-like properties. Furthermore, it could imply that Ccne1 regulates metastasis. Citation Format: Hanna Yang, Hark Kyun Kim. Proteogenomic analysis of the syngeneic mouse gastric stem cell-like cancer cell line [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 1411.

Published

2018

43. Abstract 4866: BI 907828: A novel, potent MDM2 inhibitor that induces antitumor immunologic memory and acts synergistically with an anti-PD-1 antibody in syngeneic mouse models of cancer

Author

Ulrike Weyer-Czernilofsky, Pilar Garin-Chesa, Christian Haslinger, Sophia Blake, Jens Quant, Andreas Gollner, Dorothea Rudolph, Jürgen Moll, Jörg Rinnenthal, Darryl B. McConnell, Kraut Norbert, Andreas Wernitznig, and Markus Reschke

Subjects

0301 basic medicine, Cancer Research, biology, business.industry, Cancer, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Oncology, Oral administration, Immunity, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Mdm2, Medicine, Syngeneic mouse, Antibody, business, Immunologic memory, CD8

Abstract

MDM2 inhibitors block the interaction between the Tumor Protein p53 (TP53) and MDM2, its key negative regulator, and represent a new therapeutic concept in cancer therapy. MDM2 inhibitors are designed to restore p53 activity in TP53 wild-type tumors. Several MDM2 inhibitors are currently being evaluated in early clinical development. While the tumor targeting activity of MDM2 inhibitors has been well documented, recent preclinical data with the tool compound Nutlin-3 have shown that p53 activation by local, intra-tumoral injections induces anti-tumor immunity (Cancer Res 2017, 77(9) 2292-2305). Here we present data on BI 907828, a novel and potent MDM2 inhibitor with optimized drug-like properties that is suitable for intermittent dose schedules in syngeneic mouse models of cancer. Our data show that immune modulation contributes to efficacy of BI 907828 after oral administration in a Colon-26 syngeneic mouse model. Responding mice develop anti-tumor immunity that can control the tumor growth of a secondary tumor without any further treatment in a re-challenge study. A T cell depletion study shows a contribution of CD8+ T cells but not of CD4+ T cells to single-agent efficacy with BI 907828. Moreover, preclinical data in a Colon-26 syngeneic mouse model of cancer show synergistic efficacy for the combination of a PD-1 checkpoint inhibitor with BI 907828. In summary, BI 907828 is a novel, potent, orally bioavailable MDM2 inhibitor that shows synergistic efficacy in combination with a PD-1 checkpoint inhibitor in syngeneic mouse models of cancer. Citation Format: Dorothea Rudolph, Markus Reschke, Sophia Blake, Jörg Rinnenthal, Andreas Wernitznig, Ulrike Weyer-Czernilofsky, Andreas Gollner, Christian Haslinger, Pilar Garin-Chesa, Jens Quant, Darryl B. McConnell, Kraut Norbert, Jürgen Moll. BI 907828: A novel, potent MDM2 inhibitor that induces antitumor immunologic memory and acts synergistically with an anti-PD-1 antibody in syngeneic mouse models of cancer [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 4866.

Published

2018

44. Abstract 1723: CD4+ and CD8a+ PET imaging in syngeneic mouse models for prediction of immuno-therapeutic response

Author

Carsten H. Nielsen, Thomas Tuxen Poulsen, Johan Lantto, Gunther R. Galler, Andreas Kjaer, Maria C. Melander, Ivan Horak, Camilla L. Christensen, Camilla Fröhlich, Lotte K. Kristensen, and Michael Kragh

Subjects

Cancer Research, Oncology, business.industry, Cancer research, Medicine, Syngeneic mouse, Pet imaging, business, CD8A

Abstract

Introduction: The clinical success of immune-checkpoint inhibitors in oncology has stimulated development of immune-based agents and revolutionized treatment for many types of cancer. With only a subpopulation of patients benefiting from immuno-therapeutic agents, the development of a predictive in vivo biomarker of response is critical to enhance the therapeutic efficacy of such agents. The level of immune infiltration in tumors seems to reflect the outcome of immuno-therapy, and treatment failure is usually attributed to the so-called “cold” tumors that do not attract T-cell infiltration. Thus, we sought to develop specific PET radiotracers for non-invasive in vivo detection, tracking and quantification of CD4+ and CD8a+ tumor-infiltrating lymphocytes (TILs). Experimental procedures: A panel of syngeneic mouse tumor models was analyzed for the level of TILs using flow cytometry and immunohistochemistry (IHC), and for response to Sym021, a humanized anti-PD1 antibody cross-reactive with mouse PD1. Radiotracers were generated from F(ab)'2 fragments of rat-anti-mouse CD4 and CD8a antibodies conjugated to the p-SCN-Bn-Deferoxamine (p-SCN-Bn-DFO) chelator and radiolabeled with 89Zr. Immuno-reactivity of 89Zr-DFO-CD4-F(ab)'2 and 89Zr-DFO-CD8a-F(ab)'2 was assessed with murine T-cells. Tracers were assessed in vivo in a panel of syngeneic mouse models following optimization of dose and imaging time-points. Results: Based on flow cytometry and IHC analysis, the syngeneic tumor models were characterized as “hot” or “cold” by the level of TILs. The “hot” tumor phenotype clearly correlated with response to Sym021 treatment. 89Zr-labeled CD4- and CD8a-targeting radiotracers were successfully generated with a radiochemical purity >99% and an immuno-reactivity >85%. The optimal imaging parameters were 24 hours post-injection of 1 MBq of tracer. Co-injection with 30 μg unlabeled CD4/CD8a-F(ab)'2 significantly decreased spleen and lymph node uptake, whereas tumor uptake was increased. PET imaging in syngeneic mouse models revealed differential uptake of 89Zr-DFO-CD4-F(ab)'2 and 89Zr-DFO-CD8a-F(ab)'2, with an increased uptake primarily seen in “hot” tumors. In addition, an increase in CD8a+ TILs after fractionated external radiation therapy (XRT) was successfully detected by 89Zr-DFO-CD8a-F(ab)'2 PET imaging. Conclusions: We have developed 89Zr-DFO-CD4-F(ab)'2 and 89Zr-DFO-CD8a-F(ab)'2 PET imaging radiotracers for whole-body detection and assessment of CD4+ and CD8a+ status. These radiotracers can be used as tools to predict efficacy of immuno-therapeutic treatment in preclinical drug development. In addition, they may be used to develop non-invasive in vivo biomarkers for identifying patients responding to immuno-therapeutic agents, such as Sym021. Citation Format: Lotte K. Kristensen, Camilla Fröhlich, Camilla Christensen, Maria C. Melander, Thomas T. Poulsen, Gunther R. Galler, Johan Lantto, Ivan D. Horak, Michael Kragh, Carsten H. Nielsen, Andreas Kjaer. CD4+ and CD8a+ PET imaging in syngeneic mouse models for prediction of immuno-therapeutic response [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 1723.

Published

2018

45. Abstract 3834: Antibodies targeting Resokine, a soluble immune modulator, inhibit tumor growth in syngeneic mouse models

Author

Leslie A. Nangle, Jeanette Ampudia, Joon Chang, John D. Mendlein, Cherie Ng, David J. King, Andrea Cubitt, and Kathy Ogilvie

Subjects

Immune modulator, Cancer Research, Oncology, biology, Chemistry, biology.protein, Cancer research, Syngeneic mouse, Tumor growth, Antibody

Abstract

A number of non-canonical functions have been established for proteins generated from the tRNA synthetase gene family. One of these, termed Resokine, is derived from histidyl tRNA synthetase and plays an important role in controlling immune cell activation. Circulating levels are sufficient to down-regulate the extent of T cell activation that can be achieved in vitro. A panel of specific monoclonal antibodies have been generated and tested for their anti-tumor activity in mouse syngeneic tumor models. Antibodies to Resokine demonstrated anti-tumor activity across three different tumor models. Treatment of subcutaneous CT26 tumors resulted in improved efficacy compared to treatment with antibodies that block the PD-1/PD-L1 interaction. Significant efficacy was also observed in the difficult to treat subcutaneous B16F10 melanoma and 4T1 breast tumor models. In addition anti-Resokine demonstrated significant activity in a tumor seeding model using B16F10 melanoma which resulted in inhibition of tumor nodules in the lung, and was more efficacious than a combination of antibodies to PD-L1 and CTLA-4. Combinations of anti-Resokine antibody with either anti-PD-1 or anti-PD-L1 demonstrated at least additive, and potentially synergistic activity in these models. Animals with long-term tumor regressions were re-implanted with viable tumor cells, and demonstrated long-term immune memory with rejection of the newly implanted tumors. To understand the mechanism of anti-Resokine antibody therapy, cell depletion studies were carried out in the B16F10 tumor model. In these experiments activity of anti-Resokine antibodies was demonstrated to be dependent upon the presence of CD8 T cells and also NK cells, but independent of CD4 T cells. The immune based mechanism of antibodies to Resokine was further demonstrated by re-challenge of mice that had regressed tumors upon treatment. Tumor re-growth was not observed even in the absence of further treatment whereas control mice grew tumors at the normal rate, suggesting that immune memory had been induced. Antibodies to Resokine offer an exciting new potential option for immunotherapy of cancer, which has significant activity as monotherapy and is compatible with more established modalities. Anti-Resokine antibodies are currently being developed to initiate clinical evaluation. Citation Format: Kathy Ogilvie, Cherie Ng, Leslie Nangle, Jeanette Ampudia, Joon Chang, Andrea Cubitt, David J. King, John Mendlein. Antibodies targeting Resokine, a soluble immune modulator, inhibit tumor growth in syngeneic mouse models [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 3834.

Published

2018

46. Abstract 4735: Role of myeloid derived suppressor cells in promoting ovarian cancer

Author

Sharif Sakr, Thomas E. Buekers, Robert T. Morris, Adnan R. Munkarah, Shailendra Giri, Ramandeep Rattan, and Raymond Quiles

Subjects

Cancer Research, Poor prognosis, Angiogenesis, business.industry, medicine.medical_treatment, Cancer, Immunotherapy, medicine.disease, Metastasis, Oncology, medicine, Cancer research, Myeloid-derived Suppressor Cell, Syngeneic mouse, Ovarian cancer, business

Abstract

Myeloid Derived Suppressor Cells (MDSCs) are a heterogeneous population of immature myeloid cells that are increased in tumors and create an immunosuppressive environment by inhibiting the T-cell function. In addition, MDSCs promote angiogenesis, tumor invasion, and metastasis. Increased MDSC accumulation in epithelial ovarian cancer (EOC) has been associated with poor prognosis. Our study investigated whether depletion of MDSCs will influence EOC progression and enhance the therapeutic response of programmed death-1 (PD1) immunotherapy. The intraperitoneal ID8-luciferase syngeneic mouse epithelial ovarian cancer cell model in B6 mice was used for the study ID8 bearing mice exhibited significantly higher levels of MDSCs (CD11bGr1+) (p Citation Format: Ramandeep Rattan, Sharif Sakr, Raymond Quiles, Robert Morris, Thomas Buekers, Adnan Munkarah, Shailendra Giri. Role of myeloid derived suppressor cells in promoting ovarian cancer [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 4735.

Published

2018

47. Optimizing Orthotopic Bladder Tumor Implantation in a Syngeneic Mouse Model

Author

Warren D. Heston, Eddie Shu-Yin Chan, William A. Larchian, Amit R. Patel, John B. Klein, Anil A. Thomas, and Armine K. Smith

Subjects

Nephrology, medicine.medical_specialty, Pathology, Ratón, Urology, Urinary system, urologic and male genital diseases, Mice, Internal medicine, medicine, Bladder tumor, Animals, Mice, Inbred C3H, Bladder cancer, Urinary bladder, business.industry, medicine.disease, Trypsin, female genital diseases and pregnancy complications, Disease Models, Animal, medicine.anatomical_structure, Urinary Bladder Neoplasms, Syngeneic mouse, Female, business, Neoplasm Transplantation, medicine.drug

Abstract

We established a reliable technique for orthotopically implanting bladder tumor cells in a syngeneic mouse model.MBT-2 murine bladder cancer cells were transurethrally implanted in the bladder of syngeneic C3H/He mice (Jackson Laboratory, Bar Harbor, Maine). Different chemical pretreatments were used before tumor implantation, including phosphate buffered saline (control), HCl, trypsin and poly-L-lysine. MBT-2 cells (1 x 10(6) or 2 x 10(6)) were instilled into the intravesical space after chemical pretreatment. Tumor take and bladder tumor volume were determined by micro ultrasound. Bladders were harvested at the end of the study to measure bladder weight and for histopathological examination.Bladder pretreatment with HCl in 5 preparations was discontinued due to significant adverse reactions, resulting in death in 1 mouse, and severe bladder inflammation and hematuria 3 days after pretreatment in 2. Pretreatment with phosphate buffered saline, trypsin and poly-L-lysine in 6 animals each was tolerated well without significant adverse reactions or mortality. The tumor take rate in the control, trypsin and poly-L-lysine pretreatment groups was 33%, 83% and 83%, respectively. The take rate was higher in mice instilled with 2 x 10(6) cells than in those with 1 x 10(6) cells (93% vs 73%, p0.05).We report a reliable, feasible method of orthotopically implanting bladder tumor cells into a syngeneic mouse model. Poly-L-lysine and trypsin are useful adjunctive pretreatment agents to improve bladder tumor uptake. This model may be suitable to evaluate treatment paradigms for bladder cancer.

Published

2009

48. American Society of Pediatric Hematology/Oncology 22nd Annual Meeting: Abstracts

Author

Gregor S. D. Reid, Valerie I. Brown, David A. Barrett, Alix E. Seif, and Stephan A. Grupp

Subjects

CpG Oligodeoxynucleotide, business.industry, Lymphoblastic Leukemia, Cancer, hemic and immune systems, Hematology, medicine.disease, Immune system, Oncology, hemic and lymphatic diseases, Pediatrics, Perinatology and Child Health, medicine, Cancer research, Syngeneic mouse, business

Abstract

DURABLE IMMUNE-MEDIATED PROTECTION FROM ACUTE LYMPHOBLASTIC LEUKEMIA (ALL) IS INDUCED BY CPG OLIGODEOXYNUCLEOTIDES (CPG ODN) IN A SYNGENEIC MOUSE MODEL Alix Seif;David Barrett;Valerie Brown;Stephan Grupp;Gregor Reid; Pediatric Blood & Cancer

Published

2009

49. Deformability of Tumor Cells versus Blood Cells

Author

Sangwon Byun, Josephine Shaw Bagnall, Shannon L. Stott, Richard O. Hynes, Vivian C. Hecht, David T. Miyamoto, Mehmet Toner, Shahinoor Begum, Shyamala Maheswaran, Scott R. Manalis, Massachusetts Institute of Technology. Department of Biological Engineering, Massachusetts Institute of Technology. Department of Biology, Massachusetts Institute of Technology. Department of Mechanical Engineering, Koch Institute for Integrative Cancer Research at MIT, Bagnall, Josephine, Byun, Sangwon, Begum, Shahinoor, Hecht, Vivian Chaya, Hynes, Richard O., and Manalis, Scott R.

Subjects

Pathology, medicine.medical_specialty, Cancer metastasis, Tumor cells, Article, Mice, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Circulating tumor cell, Cell Line, Tumor, Leukocytes, medicine, Animals, Cluster Analysis, Humans, In patient, 030304 developmental biology, Mice, Inbred BALB C, 0303 health sciences, Multidisciplinary, business.industry, Microfluidic Analytical Techniques, Neoplastic Cells, Circulating, medicine.disease, Phenotype, 3. Good health, Microscopy, Fluorescence, Cell culture, 030220 oncology & carcinogenesis, Models, Animal, Leukocytes, Mononuclear, Syngeneic mouse, business

Abstract

The potential for circulating tumor cells (CTCs) to elucidate the process of cancer metastasis and inform clinical decision-making has made their isolation of great importance. However, CTCs are rare in the blood, and universal properties with which to identify them remain elusive. As technological advancements have made single-cell deformability measurements increasingly routine, the assessment of physical distinctions between tumor cells and blood cells may provide insight into the feasibility of deformability-based methods for identifying CTCs in patient blood. To this end, we present an initial study assessing deformability differences between tumor cells and blood cells, indicated by the length of time required for them to pass through a microfluidic constriction. Here, we demonstrate that deformability changes in tumor cells that have undergone phenotypic shifts are small compared to differences between tumor cell lines and blood cells. Additionally, in a syngeneic mouse tumor model, cells that are able to exit a tumor and enter circulation are not required to be more deformable than the cells that were first injected into the mouse. However, a limited study of metastatic prostate cancer patients provides evidence that some CTCs may be more mechanically similar to blood cells than to typical tumor cell lines., Janssen Pharmaceutical Ltd., National Cancer Institute (U.S.). Physical Sciences Oncology Center (U54CA143874), MIT-Harvard Center of Cancer Nanotechnology Excellence (Grant 26697290-47281-A), Stand Up To Cancer, National Institutes of Health (U.S.). P41 Biotechnology Resource Center, National Cancer Institute (U.S.) (Koch Institute Support Grant P30-CA14051)

Published

2015

50. Expression of genes and pathways associated with colorectal liver metastases in an orthotopic and syngeneic mouse model

Author

T Beißbarth, S König, D Bocuk, A Wolff, and Petra Krause

Subjects

Pathology, medicine.medical_specialty, business.industry, Gastroenterology, Medicine, Syngeneic mouse, business, Gene

Published

2015