Your search keyword '"G. Yancey Gillespie"' showing total 20 results

1. Synergistic Antivascular and Antitumor Efficacy with Combined Cediranib and SC6889 in Intracranial Mouse Glioma

Author

Ayaka Kukino, Marjorie R. Grafe, Huong Tran, Matthias C. Schabel, Randall L. Woltjer, G. Yancey Gillespie, Merryl R. Lobo, Charles S. Springer, and Martin M. Pike

Subjects

lcsh:Medicine, Vascular permeability, Pharmacology, Cediranib, Mice, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Glioma, Antineoplastic Combined Chemotherapy Protocols, medicine, Animals, lcsh:Science, 030304 developmental biology, Semicarbazones, 0303 health sciences, Multidisciplinary, Brain Neoplasms, business.industry, lcsh:R, medicine.disease, Extravasation, 3. Good health, Cerebral blood flow, 030220 oncology & carcinogenesis, Concomitant, Quinazolines, Proteasome inhibitor, lcsh:Q, business, Perfusion, Research Article, medicine.drug

Abstract

Prognosis remains extremely poor for malignant glioma. Targeted therapeutic approaches, including single agent anti-angiogenic and proteasome inhibition strategies, have not resulted in sustained anti-glioma clinical efficacy. We tested the anti-glioma efficacy of the anti-angiogenic receptor tyrosine kinase inhibitor cediranib and the novel proteasome inhibitor SC68896, in combination and as single agents. To assess anti-angiogenic effects and evaluate efficacy we employed 4C8 intracranial mouse glioma and a dual-bolus perfusion MRI approach to measure Ktrans, relative cerebral blood flow and volume (rCBF, rCBV), and relative mean transit time (rMTT) in combination with anatomical MRI measurements of tumor growth. While single agent cediranib or SC68896 treatment did not alter tumor growth or survival, combined cediranib/SC68896 significantly delayed tumor growth and increased median survival by 2-fold, compared to untreated. This was accompanied by substantially increased tumor necrosis in the cediranib/SC68896 group (p

Published

2015

2. ROCK Inhibition Facilitates In Vitro Expansion of Glioblastoma Stem-Like Cells

Author

Samantha G. Tilson, Ursula L. Triantafillu, Catherine P. Langford, David A. Dozier, G. Yancey Gillespie, Yonghyun Kim, and Elizabeth M. Haley

Subjects

Cell, lcsh:Medicine, Apoptosis, In Vitro Techniques, Biology, Stem cell marker, 03 medical and health sciences, 0302 clinical medicine, Cancer stem cell, Cell Line, Tumor, medicine, Humans, lcsh:Science, Protein Kinase Inhibitors, 030304 developmental biology, rho-Associated Kinases, 0303 health sciences, Multidisciplinary, Brain Neoplasms, lcsh:R, In vitro, Cell biology, medicine.anatomical_structure, Cell culture, 030220 oncology & carcinogenesis, Cancer cell, Neoplastic Stem Cells, lcsh:Q, Stem cell, Glioblastoma, Research Article

Abstract

Due to their stem-like characteristics and their resistance to existing chemo- and radiation therapies, there is a growing appreciation that cancer stem cells (CSCs) are the root cause behind cancer metastasis and recurrence. However, these cells represent a small subpopulation of cancer cells and are difficult to propagate in vitro. Glioblastoma is an extremely deadly form of brain cancer that is hypothesized to have a subpopulation of CSCs called glioblastoma stem cells (GSCs; also called brain tumor initiating cells, BTICs). We propose the use of selective Rho-kinase (ROCK) inhibitors, Y-27632 and fasudil, to promote GSC/BTIC-like cell survival and propagation in vitro. ROCK inhibitors have been implicated in suppressing apoptosis, and it was hypothesized that they would increase the number of GSC/BTIC-like cells grown in vitro and improve cloning efficiencies. Indeed, our data demonstrate that transient and continuous supplementation of non-toxic concentrations of Y-27632 and fasudil inhibited apoptosis, enhanced the cells’ ability to form spheres, and increased stem cell marker expressing GSC/BTIC-like cell subpopulation. Our data indicated that pharmacological and genetic (siRNA) inhibitions of the ROCK pathway facilitates in vitro expansion of GSC/BTIC-like cells. Thus, ROCK pathway inhibition shows promise for future optimization of CSC culture media.

Published

2015

3. Combined efficacy of cediranib and quinacrine in glioma is enhanced by hypoxia and causally linked to autophagic vacuole accumulation

Author

Xiaoyan Wang, Merryl R. Lobo, Martin M. Pike, Randall L. Woltjer, and G. Yancey Gillespie

Subjects

Cell signaling, Kinase Inhibitors, Cancer Treatment, lcsh:Medicine, Apoptosis, Vacuole, Pharmacology, Signal transduction, Biochemistry, Mice, Antineoplastic Combined Chemotherapy Protocols, Medicine and Health Sciences, Blastomas, Enzyme Inhibitors, AKT signaling cascade, lcsh:Science, Hypoxia, Neurological Tumors, Cultured Tumor Cells, Multidisciplinary, Cell Death, Brain Neoplasms, Signaling cascades, Glioma, Cell Hypoxia, 3. Good health, Neurology, Oncology, Quinacrine, Cell Processes, Biological Cultures, medicine.symptom, medicine.drug, Research Article, Cell biology, Autophagic Cell Death, Glioblastoma Cells, Antineoplastic Agents, Tyrosine Kinase Inhibitors, Biology, Research and Analysis Methods, Cediranib, Cell Line, Tumor, medicine, Autophagy, Animals, Viability assay, Protein kinase B, Biology and life sciences, lcsh:R, Cancers and Neoplasms, Hypoxia (medical), Cell Cultures, medicine.disease, Enzyme Activation, Vacuoles, Quinazolines, Enzymology, lcsh:Q, Proto-Oncogene Proteins c-akt, Glioblastoma Multiforme

Abstract

We have previously reported that the in vivo anti-glioma efficacy of the anti-angiogenic receptor tyrosine kinase inhibitor cediranib is substantially enhanced via combination with the late-stage autophagy inhibitor quinacrine. The current study investigates the role of hypoxia and autophagy in combined cediranib/quinacrine efficacy. EF5 immunostaining revealed a prevalence of hypoxia in mouse intracranial 4C8 glioma, consistent with high-grade glioma. MTS cell viability assays using 4C8 glioma cells revealed that hypoxia potentiated the efficacy of combined cediranib/quinacrine: cell viability reductions induced by 1 µM cediranib +2.5 µM quinacrine were 78±7% (hypoxia) vs. 31±3% (normoxia), p

Published

2014

4. Preclinical evaluation of engineered oncolytic herpes simplex virus for the treatment of pediatric solid tumors

Author

Elizabeth A. Beierle, Hugh C. Nabers, Jerry E. Stewart, Elizabeth Mroczek-Musulman, James M. Markert, G. Yancey Gillespie, Michael L. Megison, Jennifer M. Coleman, Virginia M. Kelly, Alicia M. Waters, Lauren A. Gillory, and Gregory K. Friedman

Subjects

Pathology, Cancer Treatment, lcsh:Medicine, Virus Replication, medicine.disease_cause, Pediatrics, 0302 clinical medicine, Renal cell carcinoma, Basic Cancer Research, Simplexvirus, lcsh:Science, Oncolytic Virotherapy, 0303 health sciences, Multidisciplinary, Liver Neoplasms, Kidney Neoplasms, Tumor Burden, 3. Good health, Oncolytic Viruses, Oncology, Renal Cancer, 030220 oncology & carcinogenesis, Hepatocellular carcinoma, Medicine, Female, Sarcoma, Viral Vectors, Research Article, Hepatoblastoma, medicine.medical_specialty, Cell Survival, Clinical Research Design, Preclinical Models, Urology, Nectins, Mice, Nude, Sarcoma, Ewing, Microbiology, Vector Biology, 03 medical and health sciences, Cell Line, Tumor, medicine, Animals, Humans, Biology, Rhabdoid Tumor, 030304 developmental biology, business.industry, lcsh:R, medicine.disease, Oncolytic virus, Herpes simplex virus, Viral replication, Pediatric Oncology, Cell culture, Cancer research, Surgery, lcsh:Q, business, Cell Adhesion Molecules, Neoplasm Transplantation

Abstract

Recently, investigators showed that mice with syngeneic murine gliomas that were treated with a neuroattenuated oncolytic herpes simplex virus-1 (oHSV), M002, had a significant increase in survival. M002 has deletions in both copies of the γ134.5 gene, enabling replication in tumor cells but precluding infection of normal cells. Previous studies have shown antitumor effects of other oHSV against a number of adult tumors including hepatocellular carcinoma and renal cell carcinoma. The purpose of the current study was to investigate the oncolytic potential of M002 against difficult to treat pediatric liver and kidney tumors. We showed that the oHSV, M002, infected, replicated, and decreased cell survival in hepatoblastoma, malignant rhabdoid kidney tumor, and renal sarcoma cell lines. In addition, we showed that in murine xenografts, treatment with M002 significantly increased survival and decreased tumor growth. Finally, these studies showed that the primary entry protein for oHSV, CD111 (nectin-1) was present in human hepatoblastoma and malignant rhabdoid kidney tumor specimens. We concluded that M002 effectively targeted these rare aggressive tumor types and that M002 may have potential for use in children with unresponsive or relapsed pediatric solid tumors.

Published

2014

5. Engineered drug resistant γδ T cells kill glioblastoma cell lines during a chemotherapy challenge: a strategy for combining chemo- and immunotherapy

Author

G. Yancey Gillespie, Anindya Dasgupta, Austin Johnson, H. Trent Spencer, Lawrence S. Lamb, Joscelyn Bowersock, and Yun Su

Subjects

Cytotoxicity, Immunologic, medicine.medical_treatment, T-Lymphocytes, lcsh:Medicine, Zoledronic Acid, Basic Cancer Research, Cytotoxic T cell, lcsh:Science, Neurological Tumors, Cells, Cultured, Multidisciplinary, Diphosphonates, T Cells, Brain Neoplasms, Imidazoles, Receptors, Antigen, T-Cell, gamma-delta, Flow Cytometry, Dacarbazine, medicine.anatomical_structure, Oncology, Medicine, Intercellular Signaling Peptides and Proteins, Genetic Engineering, medicine.drug, Research Article, Biotechnology, Interleukin 2, Cell Survival, T cell, Immune Cells, Immunology, Genetic Vectors, Biomedical Engineering, Bioengineering, Biology, GPI-Linked Proteins, Immunomodulation, O(6)-Methylguanine-DNA Methyltransferase, Antigen, Glioma, Cell Line, Tumor, medicine, Temozolomide, Humans, Antineoplastic Agents, Alkylating, Lentivirus, lcsh:R, O-6-methylguanine-DNA methyltransferase, Cancers and Neoplasms, Immunotherapy, medicine.disease, Drug Resistance, Neoplasm, Cancer research, Interleukin-2, Clinical Immunology, lcsh:Q, Glioblastoma, Glioblastoma Multiforme

Abstract

Classical approaches to immunotherapy that show promise in some malignancies have generally been disappointing when applied to high-grade brain tumors such as glioblastoma multiforme (GBM). We recently showed that ex vivo expanded/activated γδ T cells recognize NKG2D ligands expressed on malignant glioma and are cytotoxic to glioma cell lines and primary GBM explants. In addition, γδ T cells extend survival and slow tumor progression when administered to immunodeficient mice with intracranial human glioma xenografts. We now show that temozolomide (TMZ), a principal chemotherapeutic agent used to treat GBM, increases the expression of stress-associated NKG2D ligands on TMZ-resistant glioma cells, potentially rendering them vulnerable to γδ T cell recognition and lysis. TMZ is also highly toxic to γδ T cells, however, and to overcome this cytotoxic effect γδ T cells were genetically modified using a lentiviral vector encoding the DNA repair enzyme O(6)-alkylguanine DNA alkyltransferase (AGT) from the O(6)-methylguanine methyltransferase (MGMT) cDNA, which confers resistance to TMZ. Genetic modification of γδ T cells did not alter their phenotype or their cytotoxicity against GBM target cells. Importantly, gene modified γδ T cells showed greater cytotoxicity to two TMZ resistant GBM cell lines, U373(TMZ-R) and SNB-19(TMZ-R) cells, in the presence of TMZ than unmodified cells, suggesting that TMZ exposed more receptors for γδ T cell-targeted lysis. Therefore, TMZ resistant γδ T cells can be generated without impairing their anti-tumor functions in the presence of high concentrations of TMZ. These results provide a mechanistic basis for combining chemotherapy and γδ T cell-based drug resistant cellular immunotherapy to treat GBM.

Published

2013

6. Preclinical evaluation of engineered oncolytic herpes simplex virus for the treatment of neuroblastoma

Author

Gregory K. Friedman, G. Yancey Gillespie, Lauren A. Gillory, Alicia M. Waters, James M. Markert, Hugh C. Nabers, Michael L. Megison, Elizabeth A. Beierle, Elizabeth Mroczek-Musulman, Virginia M. Kelly, Jerry E. Stewart, and Jennifer M. Coleman

Subjects

medicine.medical_treatment, Mice, Nude, lcsh:Medicine, Biology, Virus Replication, medicine.disease_cause, p38 Mitogen-Activated Protein Kinases, Virus, Mice, Neuroblastoma, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Chlorocebus aethiops, medicine, Animals, Humans, Simplexvirus, Phosphorylation, lcsh:Science, Vero Cells, 030304 developmental biology, Oncolytic Virotherapy, 0303 health sciences, Multidisciplinary, Brain Neoplasms, CD11 Antigens, lcsh:R, medicine.disease, Pediatric cancer, 3. Good health, Oncolytic virus, Radiation therapy, STAT1 Transcription Factor, Herpes simplex virus, Viral replication, Cell culture, 030220 oncology & carcinogenesis, Immunology, Cancer research, Female, lcsh:Q, Genetic Engineering, Research Article

Abstract

Despite intensive research efforts and therapeutic advances over the last few decades, the pediatric neural crest tumor, neuroblastoma, continues to be responsible for over 15% of pediatric cancer deaths. Novel therapeutic options are needed for this tumor. Recently, investigators have shown that mice with syngeneic murine gliomas treated with an engineered, neuroattenuated oncolytic herpes simplex virus-1 (oHSV), M002, had a significant increase in survival. M002 has deletions in both copies of the γ 1 34.5 gene, enabling replication in tumor cells but precluding infection of normal neural cells. We hypothesized that M002 would also be effective in the neural crest tumor, neuroblastoma. We showed that M002 infected, replicated, and decreased survival in neuroblastoma cell lines. In addition, we showed that in murine xenografts, treatment with M002 significantly decreased tumor growth, and that this effect was augmented with the addition of ionizing radiation. Importantly, survival could be increased by subsequent doses of radiation without re-dosing of the virus. Finally, these studies showed that the primary entry protein for oHSV, CD111 was expressed by numerous neuroblastoma cell lines and was also present in human neuroblastoma specimens. We concluded that M002 effectively targeted neuroblastoma and that this oHSV may have potential for use in children with unresponsive or relapsed neuroblastoma.

Published

2013

7. Acquisition of chemoresistance in gliomas is associated with increased mitochondrial coupling and decreased ROS production

Author

Claudia R. Oliva, G. Yancey Gillespie, Douglas R. Moellering, and Corinne E. Griguer

Subjects

Mitochondrial ROS, Cancer Treatment, lcsh:Medicine, Apoptosis, Mitochondrion, medicine.disease_cause, Biochemistry, Oxidative Damage, 0302 clinical medicine, Basic Cancer Research, lcsh:Science, Neurological Tumors, chemistry.chemical_classification, 0303 health sciences, Multidisciplinary, biology, Glutathione Disulfide, Glioma, Glutathione, Dacarbazine, Neurology, Oncology, 030220 oncology & carcinogenesis, Medicine, Research Article, Bioenergetics, DNA, Mitochondrial, Electron Transport Complex IV, 03 medical and health sciences, Cell Line, Tumor, medicine, Temozolomide, Cytochrome c oxidase, Humans, Antineoplastic Agents, Alkylating, Biology, 030304 developmental biology, Reactive oxygen species, lcsh:R, Cancers and Neoplasms, Chemotherapy and Drug Treatment, medicine.disease, Metabolism, chemistry, Cell culture, Drug Resistance, Neoplasm, Cancer research, biology.protein, lcsh:Q, Reactive Oxygen Species, Oxidative stress, Neuroscience

Abstract

Temozolomide (TMZ) is an alkylating agent used for treating gliomas. Chemoresistance is a severe limitation to TMZ therapy; there is a critical need to understand the underlying mechanisms that determine tumor response to TMZ. We recently reported that chemoresistance to TMZ is related to a remodeling of the entire electron transport chain, with significant increases in the activity of complexes II/III and cytochrome c oxidase (CcO). Moreover, pharmacologic and genetic manipulation of CcO reverses chemoresistance. Therefore, to test the hypothesis that TMZ-resistance arises from tighter mitochondrial coupling and decreased production of reactive oxygen species (ROS), we have assessed mitochondrial function in TMZ-sensitive and -resistant glioma cells, and in TMZ-resistant glioblastoma multiform (GBM) xenograft lines (xenolines). Maximum ADP-stimulated (state 3) rates of mitochondrial oxygen consumption were greater in TMZ-resistant cells and xenolines, and basal respiration (state 2), proton leak (state 4), and mitochondrial ROS production were significantly lower in TMZ-resistant cells. Furthermore, TMZ-resistant cells consumed less glucose and produced less lactic acid. Chemoresistant cells were insensitive to the oxidative stress induced by TMZ and hydrogen peroxide challenges, but treatment with the oxidant L-buthionine-S,R-sulfoximine increased TMZ-dependent ROS generation and reversed chemoresistance. Importantly, treatment with the antioxidant N-acetyl-cysteine inhibited TMZ-dependent ROS generation in chemosensitive cells, preventing TMZ toxicity. Finally, we found that mitochondrial DNA-depleted cells (ρ°) were resistant to TMZ and had lower intracellular ROS levels after TMZ exposure compared with parental cells. Repopulation of ρ° cells with mitochondria restored ROS production and sensitivity to TMZ. Taken together, our results indicate that chemoresistance to TMZ is linked to tighter mitochondrial coupling and low ROS production, and suggest a novel mitochondrial ROS-dependent mechanism underlying TMZ-chemoresistance in glioma. Thus, perturbation of mitochondrial functions and changes in redox status might constitute a novel strategy for sensitizing glioma cells to therapeutic approaches.

Published

2011

8. Expression signature of IFN/STAT1 signaling genes predicts poor survival outcome in glioblastoma multiforme in a subtype-specific manner

Author

Laura Vaughan, Raymond O. McCubrey, Nikolai N. Khodarev, Degui Zhi, Christopher D. Willey, Christine W. Duarte, Jacqueline J. Harris, Tapan Mehta, Ralph R. Weichselbaum, Xiangqin Cui, and G. Yancey Gillespie

Subjects

Time Factors, Epidemiology, Gene regulatory network, lcsh:Medicine, Bioinformatics, 0302 clinical medicine, Databases, Genetic, Gene Regulatory Networks, lcsh:Science, Regulation of gene expression, 0303 health sciences, Multidisciplinary, Systems Biology, Statistics, Genomics, Phenotype, 3. Good health, Gene Expression Regulation, Neoplastic, STAT1 Transcription Factor, Treatment Outcome, Oncology, 030220 oncology & carcinogenesis, Medicine, Signal Transduction, Research Article, Biology, Molecular Genetics, 03 medical and health sciences, Genetics, Humans, Gene, Survival analysis, 030304 developmental biology, Proportional Hazards Models, Clinical Genetics, Models, Genetic, Population Biology, Gene Expression Profiling, lcsh:R, Reproducibility of Results, Computational Biology, Bayes Theorem, Human Genetics, Gene signature, Survival Analysis, Gene expression profiling, Tumor progression, Cancer research, lcsh:Q, Interferons, Glioblastoma, Mathematics, Genes, Neoplasm

Abstract

Previous reports have implicated an induction of genes in IFN/STAT1 (Interferon/STAT1) signaling in radiation resistant and prosurvival tumor phenotypes in a number of cancer cell lines, and we have hypothesized that upregulation of these genes may be predictive of poor survival outcome and/or treatment response in Glioblastoma Multiforme (GBM) patients. We have developed a list of 8 genes related to IFN/STAT1 that we hypothesize to be predictive of poor survival in GBM patients. Our working hypothesis that over-expression of this gene signature predicts poor survival outcome in GBM patients was confirmed, and in addition, it was demonstrated that the survival model was highly subtype-dependent, with strong dependence in the Proneural subtype and no detected dependence in the Classical and Mesenchymal subtypes. We developed a specific multi-gene survival model for the Proneural subtype in the TCGA (the Cancer Genome Atlas) discovery set which we have validated in the TCGA validation set. In addition, we have performed network analysis in the form of Bayesian Network discovery and Ingenuity Pathway Analysis to further dissect the underlying biology of this gene signature in the etiology of GBM. We theorize that the strong predictive value of the IFN/STAT1 gene signature in the Proneural subtype may be due to chemotherapy and/or radiation resistance induced through prolonged constitutive signaling of these genes during the course of the illness. The results of this study have implications both for better prediction models for survival outcome in GBM and for improved understanding of the underlying subtype-specific molecular mechanisms for GBM tumor progression and treatment response.

Published

2011

9. CD133 is a marker of bioenergetic stress in human glioma

Author

Corinne E. Griguer, Jack R. Lancaster, Dale J. Benos, Claudia R. Oliva, G. Yancey Gillespie, Eric Gobin, and Pascale Marcorelles

Subjects

Cell, lcsh:Medicine, Mitochondrion, Biology, DNA, Mitochondrial, Models, Biological, 03 medical and health sciences, 0302 clinical medicine, Antigens, CD, Stress, Physiological, Rotenone, Glioma, Biomarkers, Tumor, Tumor Cells, Cultured, medicine, Humans, AC133 Antigen, Progenitor cell, lcsh:Science, neoplasms, Glycoproteins, Oncology/Neuro-Oncology, 030304 developmental biology, Regulation of gene expression, 0303 health sciences, Multidisciplinary, Brain Neoplasms, Uncoupling Agents, lcsh:R, Cell Biology/Cellular Death and Stress Responses, medicine.disease, Cell Hypoxia, Neural stem cell, Cell biology, Gene Expression Regulation, Neoplastic, carbohydrates (lipids), medicine.anatomical_structure, 030220 oncology & carcinogenesis, Cell Biology/Neuronal and Glial Cell Biology, Cancer cell, embryonic structures, Neoplastic Stem Cells, lcsh:Q, Stem cell, Energy Metabolism, Peptides, Research Article

Abstract

Mitochondria dysfunction and hypoxic microenvironment are hallmarks of cancer cell biology. Recently, many studies have focused on isolation of brain cancer stem cells using CD133 expression. In this study, we investigated whether CD133 expression is regulated by bioenergetic stresses affecting mitochondrial functions in human glioma cells. First, we determined that hypoxia induced a reversible up-regulation of CD133 expression. Second, mitochondrial dysfunction through pharmacological inhibition of the Electron Transport Chain (ETC) produced an up-regulation of CD133 expression that was inversely correlated with changes in mitochondrial membrane potential. Third, generation of stable glioma cells depleted of mitochondrial DNA showed significant and stable increases in CD133 expression. These glioma cells, termed rho(0) or rho(0), are characterized by an exaggerated, uncoupled glycolytic phenotype and by constitutive and stable up-regulation of CD133 through many cell passages. Moreover, these rho(0) cells display the ability to form "tumor spheroids" in serumless medium and are positive for CD133 and the neural progenitor cell marker, nestin. Under differentiating conditions, rho(0) cells expressed multi-lineage properties. Reversibility of CD133 expression was demonstrated by transfering parental mitochondria to rho(0) cells resulting in stable trans-mitochondrial "cybrid" clones. This study provides a novel mechanistic insight about the regulation of CD133 by environmental conditions (hypoxia) and mitochondrial dysfunction (genetic and chemical). Considering these new findings, the concept that CD133 is a marker of brain tumor stem cells may need to be revised.

Published

2008

10. A Multi Targeting Conditionally Replicating Adenovirus Displays Enhanced Oncolysis while Maintaining Expression of Immunotherapeutic Agents

Author

Hideyo Ugai, David T. Curiel, G. Yancey Gillespie, and G. Clement Dobbins

Subjects

viruses, medicine.medical_treatment, lcsh:Medicine, Biology, Virus Replication, medicine.disease_cause, Virus, Adenoviridae, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Neoplasms, medicine, Humans, lcsh:Science, Cytotoxicity, Sequence Deletion, 030304 developmental biology, Cytopathic effect, Oncolytic Virotherapy, 0303 health sciences, Multidisciplinary, Base Sequence, lcsh:R, Immunotherapy, Virology, 3. Good health, Oncolytic virus, Oncolytic Viruses, Viral replication, Cell culture, 030220 oncology & carcinogenesis, lcsh:Q, Adenovirus E1A Proteins, Oligopeptides, Research Article

Abstract

Studies have demonstrated that oncolytic adenoviruses based on a 24 base pair deletion in the viral E1A gene (D24) may be promising therapeutics for treating a number of cancer types. In order to increase the therapeutic potential of these oncolytic viruses, a novel conditionally replicating adenovirus targeting multiple receptors upregulated on tumors was generated by incorporating an Ad5/3 fiber with a carboxyl terminus RGD ligand. The virus displayed full cytopathic effect in all tumor lines assayed at low titers with improved cytotoxicity over Ad5-RGD D24, Ad5/3 D24 and an HSV oncolytic virus. The virus was then engineered to deliver immunotherapeutic agents such as GM-CSF while maintaining enhanced heterogenic oncolysis.

Published

2015

11. Dynamics of Circulating γδ T Cell Activity in an Immunocompetent Mouse Model of High-Grade Glioma

Author

Rebecca L. O'Brien, Neil Hoa, Benjamin H. Beck, Gretchen A. Cloud, Lawrence S. Lamb, Catherine P. Langford, Martin R. Jadus, Hyunggoon Kim, Lualhati Harkins, G. Yancey Gillespie, and Richard D. Lopez

Subjects

T cell, Population, lcsh:Medicine, Biology, Flow cytometry, 03 medical and health sciences, 0302 clinical medicine, Immune system, T-Lymphocyte Subsets, Cell Line, Tumor, Glioma, medicine, Animals, Humans, Cytotoxic T cell, lcsh:Science, education, 030304 developmental biology, 0303 health sciences, education.field_of_study, Multidisciplinary, medicine.diagnostic_test, Brain Neoplasms, lcsh:R, Interleukin-17, T-cell receptor, Brain, Receptors, Antigen, T-Cell, gamma-delta, medicine.disease, 3. Good health, Mice, Inbred C57BL, Disease Models, Animal, medicine.anatomical_structure, Tumor progression, 030220 oncology & carcinogenesis, Immunology, Cancer research, lcsh:Q, Interleukin-4, Research Article

Abstract

Human γδ T cells are potent effectors against glioma cell lines in vitro and in human/mouse xenograft models of glioblastoma, however, this effect has not been investigated in an immunocompetent mouse model. In this report, we established GL261 intracranial gliomas in syngeneic WT C57BL/6 mice and measured circulating γδ T cell count, phenotype, Vγ/Vδ repertoire, tumor histopathology, NKG2D ligands expression, and T cell invasion at day 10-12 post-injection and at end stage. Circulating γδ T cells transiently increased and upregulated Annexin V expression at post-tumor day 10-12 followed by a dramatic decline in γδ T cell count at end stage. T cell receptor repertoire showed no changes in Vγ1, Vγ4, Vγ7 or Vδ1 subsets from controls at post-tumor day 10-12 or at end stage except for an end-stage increase in the Vδ4 population. Approximately 12% of γδ T cells produced IFN-γ. IL-17 and IL-4 producing γδ T cells were not detected. Tumor progression was the same in TCRδ-/- C57BL/6 mice as that observed in WT mice, suggesting that γδ T cells exerted neither a regulatory nor a sustainable cytotoxic effect on the tumor. WT mice that received an intracranial injection of γδ T cells 15m following tumor placement showed evidence of local tumor growth inhibition but this was insufficient to confer a survival advantage over untreated controls. Taken together, our findings suggest that an early nonspecific proliferation of γδ T cells followed by their depletion occurs in mice implanted with syngeneic GL261 gliomas. The mechanism by which γδ T cell expansion occurs remains a subject for further investigation of the mechanisms responsible for this immune response in the setting of high-grade glioma.

Published

2015

12. CMV-Independent Lysis of Glioblastoma by Ex Vivo Expanded/Activated Vδ1+ γδ T Cells

Author

Lawrence S. Lamb, Yun Su, Andrea Knight, Mark W. Lowdell, Lualhati Harkins, William J. Britt, Hilal Arnouk, G. Yancey Gillespie, and Gretchen A. Cloud

Subjects

Cytotoxicity, Immunologic, Cytomegalovirus Infection, Viral Diseases, T-Lymphocytes, Cancer Treatment, lcsh:Medicine, Cytomegalovirus, Lymphocyte Activation, 0302 clinical medicine, Tumor Cells, Cultured, Cytotoxic T cell, lcsh:Science, Cytotoxicity, Immune Response, Neurological Tumors, In Situ Hybridization, Bone Marrow Transplantation, 0303 health sciences, Multidisciplinary, medicine.diagnostic_test, T Cells, virus diseases, Receptors, Antigen, T-Cell, gamma-delta, Flow Cytometry, 3. Good health, Infectious Diseases, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Cytomegalovirus Infections, Intercellular Signaling Peptides and Proteins, Medicine, Immunotherapy, Research Article, Tumor Immunology, Immune Cells, T cell, Immunology, Biology, GPI-Linked Proteins, Cell Line, Flow cytometry, 03 medical and health sciences, Antigen, Cell Line, Tumor, Glioma, medicine, Humans, 030304 developmental biology, lcsh:R, Immunity, Cancers and Neoplasms, Immunologic Subspecialties, medicine.disease, Virology, Cell culture, lcsh:Q, Clinical Immunology, Glioblastoma, Glioblastoma Multiforme, Ex vivo

Abstract

Vδ2(neg) γδ T cells, of which Vδ1+ γδ T cells are by far the largest subset, are important effectors against CMV infection. Malignant gliomas often contain CMV genetic material and proteins, and evidence exists that CMV infection may be associated with initiation and/or progression of glioblastoma multiforme (GBM). We sought to determine if Vδ1+ γδ T cells were cytotoxic to GBM and the extent to which their cytotoxicity was CMV dependent. We examined the cytotoxic effect of ex vivo expanded/activated Vδ1+ γδ T cells from healthy CMV seropositive and CMV seronegative donors on unmanipulated and CMV-infected established GBM cell lines and cell lines developed from short- term culture of primary tumors. Expanded/activated Vδ1+ T cells killed CMV-negative U251, U87, and U373 GBM cell lines and two primary tumor explants regardless of the serologic status of the donor. Experimental CMV infection did not increase Vδ1+ T cell--mediated cytotoxicity and in some cases the cell lines were more resistant to lysis when infected with CMV. Flow cytometry analysis of CMV-infected cell lines revealed down-regulation of the NKG2D ligands ULBP-2, and ULBP-3 as well as MICA/B in CMV-infected cells. These studies show that ex vivo expanded/activated Vδ1+ γδ T cells readily recognize and kill established GBM cell lines and primary tumor-derived GBM cells regardless of whether CMV infection is present, however, CMV may enhance the resistance GBM cell lines to innate recognition possibly contributing to the poor immunogenicity of GBM.

Published

2013

13. Prognostic Relevance of Cytochrome c Oxidase in Primary Glioblastoma Multiforme

Author

Corinne E. Griguer, Alan B. Cantor, Hassan M. Fathallah-Shaykh, Claudia R. Oliva, Ivan Radovanovic, Amber S. Gordon, Virginie Clément-Schatlo, G. Yancey Gillespie, James M. Markert, and Chevis N. Shannon

Subjects

Oncology, Pathology, Tumor Physiology, medicine.medical_treatment, Enzyme Metabolism, lcsh:Medicine, Biochemistry, Polymerase Chain Reaction, Targeted therapy, 0302 clinical medicine, Basic Cancer Research, Medicine, lcsh:Science, Neurological Tumors, Energy-Producing Organelles, 0303 health sciences, Multidisciplinary, biology, Brain Neoplasms, Hazard ratio, Glioma, Prognosis, Oxygen Metabolism, Enzymes, 3. Good health, 030220 oncology & carcinogenesis, Research Article, medicine.medical_specialty, macromolecular substances, Bioenergetics, Electron Transport Complex IV, 03 medical and health sciences, Diagnostic Medicine, Internal medicine, Humans, Cytochrome c oxidase, Biology, Survival analysis, DNA Primers, Retrospective Studies, 030304 developmental biology, Base Sequence, business.industry, Proportional hazards model, lcsh:R, Cancers and Neoplasms, Cancer, DNA Methylation, medicine.disease, Survival Analysis, Metabolism, Tumor progression, biology.protein, lcsh:Q, Glioblastoma, business, Biomarkers, Glioblastoma Multiforme, General Pathology

Abstract

Patients with primary glioblastoma multiforme (GBM) have one of the lowest overall survival rates among cancer patients, and reliable biomarkers are necessary to predict patient outcome. Cytochrome c oxidase (CcO) promotes the switch from glycolytic to OXPHOS metabolism, and increased CcO activity in tumors has been associated with tumor progression after chemotherapy failure. Thus, we investigated the relationship between tumor CcO activity and the survival of patients diagnosed with primary GBM. A total of 84 patients with grade IV glioma were evaluated in this retrospective cohort study. Cumulative survival was calculated by the Kaplan-Meier method and analyzed by the log-rank test, and univariate and multivariate analyses were performed with the Cox regression model. Mitochondrial CcO activity was determined by spectrophotometrically measuring the oxidation of cytochrome c. High CcO activity was detected in a subset of glioma tumors (∼30%), and was an independent prognostic factor for shorter progression-free survival and overall survival [P = 0.0087 by the log-rank test, hazard ratio = 3.57 for progression-free survival; P

Published

2013

14. Downregulation of FIP200 Induces Apoptosis of Glioblastoma Cells and Microvascular Endothelial Cells by Enhancing Pyk2 Activity

Author

Russell O. Pieper, G. Yancey Gillespie, Robert J. Weil, Jeongwu Lee, Jun-Lin Guan, Dongyan Wang, Russell Tipps, Paul W. Sanders, Mitchell A. Olman, Richard A. Prayson, Jerry E. Stewart, Ping Huang, Cheryl A. Palmer, Wei Michael Liu, Candece L. Gladson, and Eric C. Toline

Subjects

Small interfering RNA, Gene Expression, Autophagy-Related Proteins, Apoptosis, 0302 clinical medicine, Molecular Cell Biology, Basic Cancer Research, Tumor Cells, Cultured, Signaling in Cellular Processes, RNA, Small Interfering, Neurological Tumors, Apoptotic Signaling Cascade, Apoptotic Signaling, Neurons, 0303 health sciences, Multidisciplinary, Brain, Glioma, Human brain, Protein-Tyrosine Kinases, Signaling Cascades, Cell biology, medicine.anatomical_structure, Neurology, Oncology, Tyrosine kinase 2, 030220 oncology & carcinogenesis, Medicine, Cellular Types, Research Article, Signal Transduction, Protein Binding, Cell type, Science, Down-Regulation, Biology, Focal adhesion, 03 medical and health sciences, Downregulation and upregulation, medicine, Humans, 030304 developmental biology, Microcirculation, Endothelial Cells, Cancers and Neoplasms, Focal Adhesion Kinase 2, Glioblastoma, Glioblastoma Multiforme

Abstract

The expression of focal adhesion kinase family interacting protein of 200-kDa (FIP200) in normal brain is limited to some neurons and glial cells. On immunohistochemical analysis of biopsies of glioblastoma tumors, we detected FIP200 in the tumor cells, tumor-associated endothelial cells, and occasional glial cells. Human glioblastoma tumor cell lines and immortalized human astrocytes cultured in complete media also expressed FIP200 as did primary human brain microvessel endothelial cells (MvEC), which proliferate in culture and resemble reactive endothelial cells. Downregulation of endogenous expression of FIP200 using small interfering RNA resulted in induction of apoptosis in the human glioblastoma tumor cells, immortalized human astrocytes, and primary human brain MvEC. It has been shown by other investigators using cells from other tissues that FIP200 can interact directly with, and inhibit, proline-rich tyrosine kinase 2 (Pyk2) and focal adhesion kinase (FAK). In the human glioblastoma tumor cells, immortalized human astrocytes, and primary human brain MvEC, we found that downregulation of FIP200 increased the activity of Pyk2 without increasing its expression, but did not affect the activity or expression of FAK. Coimmunoprecipitation and colocalization studies indicated that the endogenous FIP200 was largely associated with Pyk2, rather than FAK, in the glioblastoma tumor cells and brain MvEC. Moreover, the pro-apoptotic effect of FIP200 downregulation was inhibited significantly by a TAT-Pyk2-fusion protein containing the Pyk2 autophosphorylation site in these cells. In summary, downregulation of endogenous FIP200 protein in glioblastoma tumor cells, astrocytes, and brain MvECs promotes apoptosis, most likely due to the removal of a direct interaction of FIP200 with Pyk2 that inhibits Pyk2 activation, suggesting that FIP200 expression may be required for the survival of all three cell types found in glioblastoma tumors.

Published

2011

15. Synergistic Antivascular and Antitumor Efficacy with Combined Cediranib and SC6889 in Intracranial Mouse Glioma.

Author

Merryl R Lobo, Ayaka Kukino, Huong Tran, Matthias C Schabel, Charles S Springer, G Yancey Gillespie, Marjorie R Grafe, Randall L Woltjer, and Martin M Pike

Subjects

Medicine, Science

Abstract

Prognosis remains extremely poor for malignant glioma. Targeted therapeutic approaches, including single agent anti-angiogenic and proteasome inhibition strategies, have not resulted in sustained anti-glioma clinical efficacy. We tested the anti-glioma efficacy of the anti-angiogenic receptor tyrosine kinase inhibitor cediranib and the novel proteasome inhibitor SC68896, in combination and as single agents. To assess anti-angiogenic effects and evaluate efficacy we employed 4C8 intracranial mouse glioma and a dual-bolus perfusion MRI approach to measure Ktrans, relative cerebral blood flow and volume (rCBF, rCBV), and relative mean transit time (rMTT) in combination with anatomical MRI measurements of tumor growth. While single agent cediranib or SC68896 treatment did not alter tumor growth or survival, combined cediranib/SC68896 significantly delayed tumor growth and increased median survival by 2-fold, compared to untreated. This was accompanied by substantially increased tumor necrosis in the cediranib/SC68896 group (p

Published

2015

16. Combined efficacy of cediranib and quinacrine in glioma is enhanced by hypoxia and causally linked to autophagic vacuole accumulation.

Author

Merryl R Lobo, Xiaoyan Wang, G Yancey Gillespie, Randall L Woltjer, and Martin M Pike

Subjects

Medicine, Science

Abstract

We have previously reported that the in vivo anti-glioma efficacy of the anti-angiogenic receptor tyrosine kinase inhibitor cediranib is substantially enhanced via combination with the late-stage autophagy inhibitor quinacrine. The current study investigates the role of hypoxia and autophagy in combined cediranib/quinacrine efficacy. EF5 immunostaining revealed a prevalence of hypoxia in mouse intracranial 4C8 glioma, consistent with high-grade glioma. MTS cell viability assays using 4C8 glioma cells revealed that hypoxia potentiated the efficacy of combined cediranib/quinacrine: cell viability reductions induced by 1 µM cediranib +2.5 µM quinacrine were 78±7% (hypoxia) vs. 31±3% (normoxia), p

Published

2014

17. Preclinical evaluation of engineered oncolytic herpes simplex virus for the treatment of pediatric solid tumors.

Author

Michael L Megison, Lauren A Gillory, Jerry E Stewart, Hugh C Nabers, Elizabeth Mroczek-Musulman, Alicia M Waters, Jennifer M Coleman, Virginia Kelly, James M Markert, G Yancey Gillespie, Gregory K Friedman, and Elizabeth A Beierle

Subjects

Medicine, Science

Abstract

Recently, investigators showed that mice with syngeneic murine gliomas that were treated with a neuroattenuated oncolytic herpes simplex virus-1 (oHSV), M002, had a significant increase in survival. M002 has deletions in both copies of the γ134.5 gene, enabling replication in tumor cells but precluding infection of normal cells. Previous studies have shown antitumor effects of other oHSV against a number of adult tumors including hepatocellular carcinoma and renal cell carcinoma. The purpose of the current study was to investigate the oncolytic potential of M002 against difficult to treat pediatric liver and kidney tumors. We showed that the oHSV, M002, infected, replicated, and decreased cell survival in hepatoblastoma, malignant rhabdoid kidney tumor, and renal sarcoma cell lines. In addition, we showed that in murine xenografts, treatment with M002 significantly increased survival and decreased tumor growth. Finally, these studies showed that the primary entry protein for oHSV, CD111 (nectin-1) was present in human hepatoblastoma and malignant rhabdoid kidney tumor specimens. We concluded that M002 effectively targeted these rare aggressive tumor types and that M002 may have potential for use in children with unresponsive or relapsed pediatric solid tumors.

Published

2014

18. Engineered drug resistant γδ T cells kill glioblastoma cell lines during a chemotherapy challenge: a strategy for combining chemo- and immunotherapy.

Author

Lawrence S Lamb, Joscelyn Bowersock, Anindya Dasgupta, G Yancey Gillespie, Yun Su, Austin Johnson, and H Trent Spencer

Subjects

Medicine, Science

Abstract

Classical approaches to immunotherapy that show promise in some malignancies have generally been disappointing when applied to high-grade brain tumors such as glioblastoma multiforme (GBM). We recently showed that ex vivo expanded/activated γδ T cells recognize NKG2D ligands expressed on malignant glioma and are cytotoxic to glioma cell lines and primary GBM explants. In addition, γδ T cells extend survival and slow tumor progression when administered to immunodeficient mice with intracranial human glioma xenografts. We now show that temozolomide (TMZ), a principal chemotherapeutic agent used to treat GBM, increases the expression of stress-associated NKG2D ligands on TMZ-resistant glioma cells, potentially rendering them vulnerable to γδ T cell recognition and lysis. TMZ is also highly toxic to γδ T cells, however, and to overcome this cytotoxic effect γδ T cells were genetically modified using a lentiviral vector encoding the DNA repair enzyme O(6)-alkylguanine DNA alkyltransferase (AGT) from the O(6)-methylguanine methyltransferase (MGMT) cDNA, which confers resistance to TMZ. Genetic modification of γδ T cells did not alter their phenotype or their cytotoxicity against GBM target cells. Importantly, gene modified γδ T cells showed greater cytotoxicity to two TMZ resistant GBM cell lines, U373(TMZ-R) and SNB-19(TMZ-R) cells, in the presence of TMZ than unmodified cells, suggesting that TMZ exposed more receptors for γδ T cell-targeted lysis. Therefore, TMZ resistant γδ T cells can be generated without impairing their anti-tumor functions in the presence of high concentrations of TMZ. These results provide a mechanistic basis for combining chemotherapy and γδ T cell-based drug resistant cellular immunotherapy to treat GBM.

Published

2013

19. Preclinical evaluation of engineered oncolytic herpes simplex virus for the treatment of neuroblastoma.

Author

Lauren A Gillory, Michael L Megison, Jerry E Stewart, Elizabeth Mroczek-Musulman, Hugh C Nabers, Alicia M Waters, Virginia Kelly, Jennifer M Coleman, James M Markert, G Yancey Gillespie, Gregory K Friedman, and Elizabeth A Beierle

Subjects

Medicine, Science

Abstract

Despite intensive research efforts and therapeutic advances over the last few decades, the pediatric neural crest tumor, neuroblastoma, continues to be responsible for over 15% of pediatric cancer deaths. Novel therapeutic options are needed for this tumor. Recently, investigators have shown that mice with syngeneic murine gliomas treated with an engineered, neuroattenuated oncolytic herpes simplex virus-1 (oHSV), M002, had a significant increase in survival. M002 has deletions in both copies of the γ 1 34.5 gene, enabling replication in tumor cells but precluding infection of normal neural cells. We hypothesized that M002 would also be effective in the neural crest tumor, neuroblastoma. We showed that M002 infected, replicated, and decreased survival in neuroblastoma cell lines. In addition, we showed that in murine xenografts, treatment with M002 significantly decreased tumor growth, and that this effect was augmented with the addition of ionizing radiation. Importantly, survival could be increased by subsequent doses of radiation without re-dosing of the virus. Finally, these studies showed that the primary entry protein for oHSV, CD111 was expressed by numerous neuroblastoma cell lines and was also present in human neuroblastoma specimens. We concluded that M002 effectively targeted neuroblastoma and that this oHSV may have potential for use in children with unresponsive or relapsed neuroblastoma.

Published

2013

20. Expression signature of IFN/STAT1 signaling genes predicts poor survival outcome in glioblastoma multiforme in a subtype-specific manner.

Author

Christine W Duarte, Christopher D Willey, Degui Zhi, Xiangqin Cui, Jacqueline J Harris, Laura Kelly Vaughan, Tapan Mehta, Raymond O McCubrey, Nikolai N Khodarev, Ralph R Weichselbaum, and G Yancey Gillespie

Subjects

Medicine, Science

Abstract

Previous reports have implicated an induction of genes in IFN/STAT1 (Interferon/STAT1) signaling in radiation resistant and prosurvival tumor phenotypes in a number of cancer cell lines, and we have hypothesized that upregulation of these genes may be predictive of poor survival outcome and/or treatment response in Glioblastoma Multiforme (GBM) patients. We have developed a list of 8 genes related to IFN/STAT1 that we hypothesize to be predictive of poor survival in GBM patients. Our working hypothesis that over-expression of this gene signature predicts poor survival outcome in GBM patients was confirmed, and in addition, it was demonstrated that the survival model was highly subtype-dependent, with strong dependence in the Proneural subtype and no detected dependence in the Classical and Mesenchymal subtypes. We developed a specific multi-gene survival model for the Proneural subtype in the TCGA (the Cancer Genome Atlas) discovery set which we have validated in the TCGA validation set. In addition, we have performed network analysis in the form of Bayesian Network discovery and Ingenuity Pathway Analysis to further dissect the underlying biology of this gene signature in the etiology of GBM. We theorize that the strong predictive value of the IFN/STAT1 gene signature in the Proneural subtype may be due to chemotherapy and/or radiation resistance induced through prolonged constitutive signaling of these genes during the course of the illness. The results of this study have implications both for better prediction models for survival outcome in GBM and for improved understanding of the underlying subtype-specific molecular mechanisms for GBM tumor progression and treatment response.

Published

2012