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151. Abstract LB175: MicroRNA-138 suppresses glioblastoma proliferation through downregulation of CD44 and sensitizes to temozolomide

Author

Tae Jin Lee, Ji Young Yoo, Deokhwa Nam, Ji Seon Shim, Alberto Bueso-Perez, and Balveen Kaur

Subjects
Cancer Research, Oncology
Abstract

Tumor suppressive microRNAs (miRNAs) are increasingly implicated in the development of anti-tumor therapy by reprogramming gene network that are aberrantly regulated in cancer cells. This study aimed to pinpoint tumor suppressive miRNAs with therapeutic potential against GBM, one of the most deadly cancers. Whole transcriptome and miRNA expression profiling analyses were performed on human GBM patient tissues. Transient transfection of miRNA mimics was used to investigate the tumor suppressive role of a miRNA (miR-138) in cell proliferation, cell cycle, migration, would healing, and chemosensitivity to temozolomide (TMZ). Orthotopic xenograft mice model using human patient-derived primary GBM cells was used for the survival studies. miR-138 was found as one of the most significantly downregulated miRNAs with an inverse correlation with CD44 expression. Functional studies unveiled that miR-138 negatively regulates the expression of CD44 at protein level by directly binding to the 3’ UTR of CD44. CD44 inhibition by miR-138 overexpression resulted in an inhibition of glioblastoma cell proliferation in vitro through cell cycle arrest as evidenced by a significant induction of p27 and its translocation into nucleus. Ectopic expression of miR-138 also increased survival rates in mice that had an intracranial xenograft tumor derived from human patient-derived primary GBM cells. In addition, miR-138 sensitized GBM tumor to TMZ in mice. We demonstrated a therapeutic potential of tumor suppressive miR-138 through direct downregulation of CD44 and sensitization to chemotherapy for the treatment of primary and even chemoresistant GBM Citation Format: Tae Jin Lee, Ji Young Yoo, Deokhwa Nam, Ji Seon Shim, Alberto Bueso-Perez, Balveen Kaur. MicroRNA-138 suppresses glioblastoma proliferation through downregulation of CD44 and sensitizes to temozolomide [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2022; 2022 Apr 8-13. Philadelphia (PA): AACR; Cancer Res 2022;82(12_Suppl):Abstract nr LB175.

Published
2022

152. DDRE-26. INHIBITION OF PRMT5 SENSITIZES GLIOBLASTOMA MODELS TO TRAMETINIB TREATMENT

Author

Ashis Chowdhury, Shilpa Thammegowda, Toshihiko Shimizu, Hannah Sur, Yoshihiro Otani, Tae Jin Lee, Sriya Namagiri, John D. Heiss, Yesh Banasavadi, Ji Young Yoo, Jean-Paul Bryant, Dragan Maric, Cole T. Lewis, Sarah R. Rivas, Balveen Kaur, and Stuart Walbridge

Subjects
Trametinib, Cancer Research, Oncology, Chemistry, Tumor progression, Proto-Oncogene Proteins c-akt, Apoptosis, Protein arginine methyltransferase 5, Cancer research, Protein-Arginine N-Methyltransferases, Neurology (clinical), Cell cycle, Survival rate
Abstract

With limited effective therapeutic strategies, the prognosis for glioblastoma (GBM) is very poor. Our previous study shows that the expression of Protein Arginine Methyltransferase 5 (PRMT5) is upregulated in GBM; its inhibition promotes apoptosis and senescence in differentiated and stem-like tumor cells, respectively. MEK inhibitors, including trametinib, are currently under investigation for GBM therapy. In this study, we tested whether inhibition of PRMT5 can enhance the anti-GBM efficacy of trametinib. Patient-derived primary GBM neurospheres (GBMNS) with transient PRMT5 knockdown were treated with trametinib and cell viability, proliferation, cell cycle progression, ELISA, and western blot analysis were conducted. In vivo, PRMT5-intact and -depleted GBMNS were intracranially implanted in NSG mice and treated with trametinib by daily oral gavage, and tumor progression and mice survival rate were analyzed by MRI and Kaplan-Meier survival curve, respectively. Depletion of PRMT5 increased the cytotoxic effect of trametinib in GBMNS. Trametinib treatment increased the activity of ERBB3 and AKT; With PRMT5 knockdown, the activity of both AKT and ERBB3 decreased significantly. But, inhibition of ERBB3 alone failed to block the trametinib-induced AKT activity suggesting that even though PRMT5 regulates the activity of both ERBB3 and AKT, the enhanced antitumor effect imparted by PRMT5 knockdown in trametinib treated GBMNS is because of AKT inhibition alone. In vivo, PRMT5-depletion extended the survival of the tumor-bearing mice that further increased in combination with trametinib treatment. Interestingly, trametinib treatment alone had no survival benefit.

Published
2021

153. Rodent Brain Tumor Models for Neuro-Oncology Research

Author

Balveen Kaur, Yoshihiro Otani, and Ryan M McCormack

Subjects
Immune system, Rodent, biology, Tumor biology, biology.animal, Glioma, Neuro oncology, Humanized mouse, Cancer research, medicine, Brain tumor, Tumor-Derived, medicine.disease
Abstract

Neuro-Oncology research has dictated the need for animal models and since early 1970s rodent glioma models have been the choice model for investigators. These initial models were developed by exposing adult rodents to carcinogens to induce brain tumors. A panel of rodent tumor derived cells which form tumors upon reimplantation were then used to study tumor biology and response to therapeutics. The advent of immune compromised mouse models led to the expansion of these efforts to include human patient derived tumor cells. While these tumors captured the molecular background of GBM, they were poor models to understand immune micro-environment of brain tumors. Molecular biology advances further led to the development of murine models that generated spontaneous tumors. These models exquisitely recapitulate GBM molecular alterations in an immune competent environment. However the murine origin of these models often limits their utility for investigations of biological therapeutics that are inherently species specific. The advent of humanized mouse models heralds a new phase providing mice repopulated with human immune cells that bear human tumors. While these models are rarely isogenic, they are now considered the gold standard for research. However these models are cumbersome to use, and extremely expensive. Here we summarize the utility and challenges of the different rodent models frequently used in Neuro-Oncology research.

Published
2021

154. Strategies to Modulate MicroRNA Functions for the Treatment of Cancer or Organ Injury

Author

Keith Kerr, Holger K. Eltzschig, Tae Jin Lee, Ji Young Yoo, Balveen Kaur, Dong H. Kim, and Xiaoyi Yuan

Subjects
0301 basic medicine, Lung injury, Bioinformatics, 03 medical and health sciences, 0302 clinical medicine, Neoplasms, microRNA, medicine, Biomarkers, Tumor, Animals, Humans, Myocardial infarction, Review Articles, Pharmacology, Regulation of gene expression, Medical treatment, business.industry, Cancer, Perioperative, medicine.disease, Clinical trial, MicroRNAs, 030104 developmental biology, Molecular Medicine, Wounds and Injuries, business, 030217 neurology & neurosurgery
Abstract

Cancer and organ injury-such as that occurring in the perioperative period, including acute lung injury, myocardial infarction, and acute gut injury-are among the leading causes of death in the United States and impose a significant impact on quality of life. MicroRNAs (miRNAs) have been studied extensively during the last two decades for their role as regulators of gene expression, their translational application as diagnostic markers, and their potential as therapeutic targets for disease treatment. Despite promising preclinical outcomes implicating miRNA targets in disease treatment, only a few miRNAs have reached clinical trials. This likely relates to difficulties in the delivery of miRNA drugs to their targets to achieve efficient inhibition or overexpression. Therefore, understanding how to efficiently deliver miRNAs into diseased tissues and specific cell types in patients is critical. This review summarizes current knowledge on various approaches to deliver therapeutic miRNAs or miRNA inhibitors and highlights current progress in miRNA-based disease therapy that has reached clinical trials. Based on ongoing advances in miRNA delivery, we believe that additional therapeutic approaches to modulate miRNA function will soon enter routine medical treatment of human disease, particularly for cancer or perioperative organ injury. SIGNIFICANCE STATEMENT: MicroRNAs have been studied extensively during the last two decades in cancer and organ injury, including acute lung injury, myocardial infarction, and acute gut injury, for their regulation of gene expression, application as diagnostic markers, and therapeutic potentials. In this review, we specifically emphasize the pros and cons of different delivery approaches to modulate microRNAs, as well as the most recent exciting progress in the field of therapeutic targeting of microRNAs for disease treatment in patients.

Published
2020

155. Glioma induced alterations in fecal short-chain fatty acids and neurotransmitters

Author

Nagireddy Putluri, Bhanu P. Ganesh, Louise D. McCullough, Ryan M McCormack, Anthony Patrizz, Yoshua Esquenazi, Leomar Y. Ballester, Balveen Kaur, and Antonio Dono

Subjects
Adult, Male, medicine.medical_specialty, Adolescent, Metabolite, microbiome, temozolomide, norepinephrine, Feces, Young Adult, chemistry.chemical_compound, Norepinephrine, glioma, Internal medicine, Glioma, Biomarkers, Tumor, medicine, Animals, Humans, Prospective Studies, Microbiome, Neurotransmitter, neoplasms, Aged, Neurotransmitter Agents, Temozolomide, Brain Neoplasms, 5-Hydroxyindoleacetic acid, business.industry, 5-HIAA, glioblastoma, General Medicine, Preliminary Communication, Middle Aged, Fatty Acids, Volatile, Prognosis, medicine.disease, nervous system diseases, serotonin, Mice, Inbred C57BL, Endocrinology, chemistry, Female, Serotonin, 5-hydroxyindoleacetic acid, business, fecal metabolites, Follow-Up Studies, medicine.drug
Abstract

Aim: To explore fecal short-chain fatty acids and neurotransmitter alterations in a mouse–glioma model and glioma patients. Methods: Liquid chromatography–mass spectrometry and 16S rRNA-sequencing from fecal samples were performed to measure metabolite levels and taxa abundance in mice/humans. Mice underwent GL261 implantation with/without temozolomide. Glioma patients were compared with healthy controls. Results: Glioma altered several short-chain fatty acids and neurotransmitter levels. Reduced 5-hydroxyindoleaceic acid and norepinephrine levels were seen in mice and humans. Interestingly, temozolomide treatment abrogates the effects of glioma on fecal metabolites. Conclusion: Our findings demonstrate the interplay between glioma and the gut–brain axis. Further work is required to identify pathways within the gut–brain axis by which glioma influences and promotes the modulation of fecal metabolites and microbiome.

Published
2020

156. Glioma and temozolomide induced alterations in gut microbiome

Author

Gabriella Hines, Antonio Dono, Nitin Tandon, Takeshi Takayasu, Bhanu P. Ganesh, Yoshihiro Otani, Nuruddin Husein, Louise D. McCullough, Octavio Arevalo, Balveen Kaur, Yoshua Esquenazi, Soheil Zorofchian, Leomar Y. Ballester, Jude P.J. Savarraj, H. Alex Choi, and Anthony Patrizz

Subjects
Adult, Male, Adolescent, Firmicutes, Biology, Article, Mice, Glioma, medicine, Temozolomide, Animals, Humans, Microbiome, Antineoplastic Agents, Alkylating, Multidisciplinary, Brain Neoplasms, Gastrointestinal Microbiome, Verrucomicrobia, Akkermansia, Middle Aged, biology.organism_classification, medicine.disease, Mice, Inbred C57BL, CNS cancer, Cancer research, Dysbiosis, Female, Bacteroides, Cancer in the nervous system, medicine.drug
Abstract

The gut microbiome is fundamental in neurogenesis processes. Alterations in microbial constituents promote inflammation and immunosuppression. Recently, in immune-oncology, specific microbial taxa have been described to enhance the effects of therapeutic modalities. However, the effects of microbial dysbiosis on glioma are still unknown. The aim of this study was to explore the effects of glioma development and Temozolomide (TMZ) on fecal microbiome in mice and humans. C57BL/6 mice were implanted with GL261/Sham and given TMZ/Saline. Fecal samples were collected longitudinally and analyzed by 16S rRNA sequencing. Fecal samples were collected from healthy controls as well as glioma patients at diagnosis, before and after chemoradiation. Compared to healthy controls, mice and glioma patients demonstrated significant differences in beta diversity, Firmicutes/Bacteroides (F/B) ratio, and increase of Verrucomicrobia phylum and Akkermansia genus. These changes were not observed following TMZ in mice. TMZ treatment in the non-tumor bearing mouse-model diminished the F/B ratio, increase Muribaculaceae family and decrease Ruminococcaceae family. Nevertheless, there were no changes in Verrucomicrobia/Akkermansia. Glioma development leads to gut dysbiosis in a mouse-model, which was not observed in the setting of TMZ. These findings seem translational to humans and warrant further study.

Published
2020

157. Enhancing Antitumor Efficacy of Heavily Vascularized Tumors by RAMBO Virus through Decreased Tumor Endothelial Cell Activation

Author

Mitra Nair, Matthew O. Old, Chelsea Bolyard, Jun-Ge Yu, Raphael E. Pollock, Gonzalo Lopez, Yoshihiro Otani, Yeshavanth Kumar Banasavadi-Siddegowda, Balveen Kaur, Ji Young Yoo, Tae Jin Lee, Maninder Khosla, Jin Muk Kang, Margaret Yeh, Toshihiko Shimizu, and Flora Park

Subjects
0301 basic medicine, Cancer Research, Angiogenesis, lcsh:RC254-282, Virus, Article, 03 medical and health sciences, angiogenesis, 0302 clinical medicine, soft tissue sarcoma (STS), vasculostatin (Vstat120), In vivo, medicine, tumor microenvironment (TME), Cytotoxicity, business.industry, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, rapid antiangiogenesis mediated by oncolytic virus (RAMBO), Oncolytic virus, Endothelial stem cell, 030104 developmental biology, Oncology, Viral replication, 030220 oncology & carcinogenesis, Cancer research, Sarcoma, oncolytic herpes simplex virus-1 (oHSV), business
Abstract

Vascularization is a common pathology for many solid tumors, and therefore anti-angiogenic strategies are being investigated as a therapeutic target for treatment. Numerous studies are also being conducted regarding the effects of oncolytic viruses, including ImlygicTM, an FDA approved oncolytic herpes simplex virus-1 (oHSV) for the treatment of highly vascularized tumors such as Kaposi sarcoma (NCT04065152), and brain tumors. To our knowledge, the effects of combining oncolytic HSV with angiogenesis inhibition on endothelial cell activation has not been previously described. Here, we tested the effects of Rapid Antiangiogenesis Mediated By Oncolytic Virus (RAMBO), an oHSV which expresses a potent anti-angiogenic gene Vasculostatin on endothelial cell activation in heavily vascularized solid tumors. oHSV treatment induces endothelial cell activation, which inhibits virus propagation and oncolysis in adjacent tumor cells in vitro. Consistently, this was also observed in intravital imaging of intracranial tumor-bearing mice in vivo where infected tumor endothelial cells could efficiently clear the virus without cell lysis. Quantitative real-time PCR (Q-PCR), leukocyte adhesion assay, and fluorescent microscopy imaging data, however, revealed that RAMBO virus significantly decreased expression of endothelial cell activation markers and leukocyte adhesion, which in turn increased virus replication and cytotoxicity in endothelial cells. In vivo RAMBO treatment of subcutaneously implanted sarcoma tumors significantly reduced tumor growth in mice bearing sarcoma compared to rHSVQ. In addition, histological analysis of RAMBO-treated tumor tissues revealed large areas of necrosis and a statistically significant reduction in microvessel density (MVD). This study provides strong preclinical evidence of the therapeutic benefit for the use of RAMBO virus as a treatment option for highly vascularized tumors.

Published
2020

158. Oncolytic HSV Vectors and Anti-Tumor Immunity

Author

Joseph C. Glorioso, Justus B. Cohen, William F. Goins, Bonnie Hall, Joseph W. Jackson, Gary Kohanbash, Nduka Amankulor, Balveen Kaur, Michael A. Caligiuri, E. Antonio Chiocca, Eric C. Holland, and Christophe Quéva

Published
2020

159. An oncolytic herpesvirus expressing E-cadherin improves survival in mouse models of glioblastoma

Author

Ping Yi, Jianying Zhang, Luke Russell, Hiroshi Nakashima, Ji Young Yoo, Jianhua Yu, Jianfeng Han, Rui Ma, Michael A. Caligiuri, Balveen Kaur, Hanwei Cui, E. Antonio Chiocca, Bo Xu, and Hongsheng Dai

Subjects
0303 health sciences, Innate immune system, Effector, viruses, Biomedical Engineering, Bioengineering, Biology, medicine.disease_cause, Applied Microbiology and Biotechnology, Virus, 3. Good health, Oncolytic virus, 03 medical and health sciences, 0302 clinical medicine, Cell killing, Herpes simplex virus, Viral entry, Cancer research, medicine, Molecular Medicine, Virotherapy, 030217 neurology & neurosurgery, 030304 developmental biology, Biotechnology
Abstract

The efficacy of oncolytic herpes simplex virus (oHSV) is limited by rapid viral clearance by innate immune effector cells and poor intratumoral viral spread. We combine two approaches to overcome these barriers: inhibition of natural killer (NK) cells and enhancement of intratumoral viral spread. We engineered an oHSV to express CDH1, encoding E-cadherin, an adherent molecule and a ligand for KLRG1, an inhibitory receptor expressed on NK cells. In vitro, infection with this engineered virus, named OV-CDH1, induced high surface E-cadherin expression on infected glioblastoma (GBM) cells, which typically lack endogenous E-cadherin. Ectopically expressed E-cadherin enhanced the spread of OV-CDH1 by facilitating cell-to-cell infection and viral entry and reduced viral clearance by selectively protecting OV-CDH1-infected cells from KLRG1+ NK cell killing. In vivo, OV-CDH1 treatment substantially prolonged the survival in GBM-bearing mouse models, primarily because of improved viral spread rather than inhibition of NK cell activity. Thus, virus-induced overexpression of E-cadherin may be a generalizable strategy for improving cancer virotherapy.

Published
2018

160. PTEN expression by an oncolytic herpesvirus directs T-cell mediated tumor clearance

Author

Yeshavanth Kumar Banasavadi-Siddegowda, Alena Cristina Jaime-Ramirez, Michael C. Ostrowski, Alex Sprague, Raleigh D. Kladney, Balveen Kaur, Jianying Zhang, Gina M. Sizemore, Yufeng Wang, Michael A. Caligiuri, Bangxing Hong, Jessica Swanner, Luke Russell, Norman L. Lehman, Ji Young Yoo, and Jianhua Yu

Subjects
0301 basic medicine, T cell, animal diseases, T-Lymphocytes, viruses, Science, General Physics and Astronomy, Biology, Models, Biological, General Biochemistry, Genetics and Molecular Biology, Article, B7-H1 Antigen, 03 medical and health sciences, Mice, 0302 clinical medicine, Immune system, Cell Line, Tumor, medicine, Tensin, PTEN, Animals, Humans, lcsh:Science, PI3K/AKT/mTOR pathway, Herpesviridae, Multidisciplinary, Brain Neoplasms, Immunity, PTEN Phosphohydrolase, Mammary Neoplasms, Experimental, General Chemistry, Acquired immune system, 3. Good health, Oncolytic virus, Kinetics, Oncolytic Viruses, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Protein kinase B signaling, Cancer research, biology.protein, lcsh:Q, Female, Proto-Oncogene Proteins c-akt
Abstract

Engineered oncolytic viruses are used clinically to destroy cancer cells and have the ability to boost anticancer immunity. Phosphatase and tensin homolog deleted on chromosome 10 loss is common across a broad range of malignancies, and is implicated in immune escape. The N-terminally extended isoform, phosphatase and tensin homolog deleted on chromosome 10 alpha (PTENα), regulates cellular functions including protein kinase B signaling and mitochondrial adenosine triphosphate production. Here we constructed HSV-P10, a replicating, PTENα expressing oncolytic herpesvirus, and demonstrate that it inhibits PI3K/AKT signaling, increases cellular adenosine triphosphate secretion, and reduces programmed death-ligand 1 expression in infected tumor cells, thus priming an adaptive immune response and overcoming tumor immune escape. A single dose of HSV-P10 resulted in long term survivors in mice bearing intracranial tumors, priming anticancer T-cell immunity leading to tumor rejection. This implicates HSV-P10 as an oncolytic and immune stimulating therapeutic for anticancer therapy., Oncolytic viruses are a promising therapeutic approach for cancer treatment. The authors demonstrate the efficacy of an engineered HSV-1 expressing PTENα as an oncolytic and immune stimulating therapy against brain cancer metastases.

Published
2018

161. White paper on microbial anti-cancer therapy and prevention

Author

Ke Liu, Steve H. Thorne, Daniel A. Saltzman, Peter Tattersall, Grant McFadden, Liang Deng, Balveen Kaur, Laura Evgin, Steve Fiering, Richard G. Vile, Sheryl Ruppel, Herbert Kim Lyerly, Robert M. Hoffman, James L. Gulley, Robert Coffin, Matthew Giacalone, Claudia Gravekamp, Ariel E. Marciscano, Halle Huihong Zhang, Neil S. Forbes, Eddie Moradian, Shibin Zhou, and Hal Gunn

Subjects
0301 basic medicine, Cancer Research, medicine.medical_specialty, Genetic Vectors, Immunology, Treatment outcome, Drug Evaluation, Preclinical, Cancer therapy, Cancer Vaccines, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, White paper, Neoplasms, medicine, Animals, Humans, Immunology and Allergy, Combined Modality Therapy, Viral therapy, Intensive care medicine, Oncolytic Virotherapy, Pharmacology, Immune Stimulation, Bacteria, business.industry, Clinical Studies as Topic, Neoplasms therapy, Cancer, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Biological Therapy, Treatment Outcome, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Viruses, Molecular Medicine, Genetic Engineering, business, Research Article
Abstract

In this White Paper, we discuss the current state of microbial cancer therapy. This paper resulted from a meeting (‘Microbial Based Cancer Therapy’) at the US National Cancer Institute in the summer of 2017. Here, we define ‘Microbial Therapy’ to include both oncolytic viral therapy and bacterial anticancer therapy. Both of these fields exploit tumor-specific infectious microbes to treat cancer, have similar mechanisms of action, and are facing similar challenges to commercialization. We designed this paper to nucleate this growing field of microbial therapeutics and increase interactions between researchers in it and related fields. The authors of this paper include many primary researchers in this field. In this paper, we discuss the potential, status and opportunities for microbial therapy as well as strategies attempted to date and important questions that need to be addressed. The main areas that we think will have the greatest impact are immune stimulation, control of efficacy, control of delivery, and safety. There is much excitement about the potential of this field to treat currently intractable cancer. Much of the potential exists because these therapies utilize unique mechanisms of action, difficult to achieve with other biological or small molecule drugs. By better understanding and controlling these mechanisms, we will create new therapies that will become integral components of cancer care.

Published
2018

162. Abstract PD9-11: Platelet derived growth factor receptor-β signaling: A novel therapeutic target for breast cancer associated brain metastasis

Author

Michael C. Ostrowski, Lynn Schoenfield, Gina M. Sizemore, Sarah A. Steck, Chelsea Bolyard, Manjusri Das, Arnab Chakravarti, Luke Russell, Anthony J. Trimboli, Balveen Kaur, Anisha M. Hammer, Jose Otero, Raleigh D. Kladney, Gustavo Leone, Robert Pilarski, Steven T. Sizemore, Matthew D. Ringel, Blake E. Hildreth, and Katie A. Thies

Subjects
Cancer Research, PDGFB, business.industry, Brain tumor, Cancer, medicine.disease, Primary tumor, Metastasis, chemistry.chemical_compound, Oncology, chemistry, Cancer research, medicine, business, Triple-negative breast cancer, Crenolanib, Brain metastasis
Abstract

PDGFRβ is a receptor tyrosine kinase found in cells of mesenchymal origin such as fibroblasts and pericytes. Activation of this receptor is dependent on paracrine ligand induction, and its preferred ligand, PDGFB, is released by neighboring epithelial and endothelial cells. While expression of both PDGFRβ and PDGFB has been noted in patient breast tumors for decades, how PDGFB-to-PDGFRβ tumor-stromal signaling mediates breast cancer initiation, progression, and metastasis remains unclear. To test this important research question, we developed a mouse model of mesenchymal-specific PDGFRβ hyper-activation. PDGFRβ mutant mammary glands exhibit increased tertiary side-branching and epithelial proliferation confirming a stromal-specific PDGFRβ effect on neighboring epithelium during normal development. To test the effect of hyper-active mesenchymal PDGFRβ on disease progression, experimental tail vein metastasis assays were performed where we observed prominent brain metastases in 50% of the PDGFRβ mutantmice (n=5/10) with no brain lesions seen in controls (n=0/19). There was no difference in the incidence of lung or liver metastases in the mutant mice suggesting a pro-metastatic function for PDGFRβ in the brain metastatic niche. To rule out dysfunction of the blood brain barrier contributing to the observed metastatic spread, we then intracranially injected mammary tumor cells, and as expected based on our metastasis assay, found that larger tumors formed in the brains of PDGFRβ mutant mice versus controls. To our knowledge, these combined findings are the first example where genetic manipulation of the stroma increases breast cancer associated brain metastases (BCBM). Given that these pre-clinical data suggest that primary breast tumors expressing high PDGFB could preferentially metastasize to the brain, we analyzed PDGFB protein expression in a tissue microarray comprised of HER2-positive and triple negative breast cancer (TNBC) primary tumors (total n=425). While high PDGFB did not correlate with site-independent metastatic recurrence, it was prognostic of brain metastasis, mirroring our mouse data. Evaluation of PDGFB in a small cohort of matched primary breast tumors with associated brain (n=5) and lung metastases (n=2) revealed intense PDGFB staining in 100% of the brain metastases, but only 50% of the lung metastases. These findings further suggest that high primary tumor PDGFBexpression defines a subset of breast cancer patients predisposed to brain metastases and that these patients may benefit from therapeutic inhibition of PDGFRβ signaling. To test this pre-clinically, we treated mice harboring intracranial tumors with the PDGFR specific inhibitor crenolanib. Excitingly, crenolanib treatment significantly inhibited the brain tumor burden in these mice. Combined, our findings to date (1) advocate that primary tumor expression of PDGFB is a novel prognostic biomarker for the development of BCBM and (2) support clinical trial evaluation of PDGFR inhibitors for the prevention and treatment of BCBM. Ongoing studies are evaluating how the PDGFRβ-expressing mesenchymal cells within the brain promote a pro-metastatic niche. Citation Format: Sizemore GM, Hammer AM, Thies KA, Hildreth BE, Russell LO, Sizemore ST, Trimboli AJ, Kladney RD, Steck SA, Das M, Bolyard CM, Pilarski R, Schoenfield L, Otero J, Chakravarti A, Ringel M, Kaur B, Leone G, Ostrowski MC. Platelet derived growth factor receptor-β signaling: A novel therapeutic target for breast cancer associated brain metastasis [abstract]. In: Proceedings of the 2018 San Antonio Breast Cancer Symposium; 2018 Dec 4-8; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2019;79(4 Suppl):Abstract nr PD9-11.

Published
2019

163. IM-4 Impact of oHSV activated NOTCH signaling in tumor microenvironment and its impact on anti-tumor immunity

Author

Otani Yoshihiro, Ji Young Yoo, Sean E Lawler, Antonio E Chiocca, and Balveen Kaur

Subjects
Oncolytic HSV, Tumor microenvironment, AcademicSubjects/MED00300, Immunology (IM), AcademicSubjects/MED00310, Immunotherapy, Supplement Abstracts
Abstract

Oncolytic herpes simplex virus-1 (oHSV) is novel FDA-approved immunotherapy for advanced melanoma patients in US. Also, oHSV is recently approved for the treatment of recurrent GBM in Japan. We have shown that oHSV treatment of GBM cells induces NICD cleavage and NOTCH activation in adjacent uninfected glioma cells via HSV-1 microRNA-H16 (Otani Y and Yoo JY, Clin Cancer Res, 2020), however, the consequences of NOTCH on immunotherapy in GBM is unknow. Here we have investigated the impact of oHSV-induced NOTCH signaling on the tumor microenvironment (TME). Analysis of TCGA GBM data and experimental murine models revealed NOTCH induced immunosuppressive myeloid cell recruitment and limited anti-tumor immunity. In oHSV treated tissue, viral infection educated tumor associated macrophages to secrete CCL2 which recruited monocytic myeloid derived suppressor cell (MDSC) that attenuated anti-tumor immunity. Consistent with this, CCL2 induction was also observed in serum of recurrent GBM patients treated with oHSV (NCT03152318). Importantly, blockade of NOTCH signaling reduced the oHSV induced immunosuppressive environment and activated a CD8 dependent anti-tumor memory response. These findings present the opportunities for combination therapies that can help improve therapeutic benefit and anti-tumor immunity in GBM.

Published
2021

164. PRMT5 as a druggable target for glioblastoma therapy

Author

Mitch A. Phelps, Guqin Shi, Chenglong Li, Yeshavanth Kumar Banasavadi-Siddegowda, Jianying Zhang, Balveen Kaur, Jiang Wang, Min An, Christine E. Beattie, Robert A. Baiocchi, Wei Zhou, Alessandra M. Welker, Xiaozhi Yang, Sigmund Hsu, and Jaime Imitola

Subjects
0301 basic medicine, Protein-Arginine N-Methyltransferases, Cancer Research, Cellular differentiation, Apoptosis, Gene Expression Regulation, Enzymologic, Small Molecule Libraries, Mice, 03 medical and health sciences, In vivo, Spheroids, Cellular, Neurosphere, Glioma, Animals, Humans, Medicine, Protein Kinase Inhibitors, Zebrafish, Cell Proliferation, Brain Neoplasms, business.industry, Cell growth, Protein arginine methyltransferase 5, Cell Cycle, Cell Differentiation, Cell cycle, medicine.disease, Xenograft Model Antitumor Assays, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Oncology, Basic and Translational Investigations, Cancer research, Neurology (clinical), Stem cell, Glioblastoma, business, Signal Transduction
Abstract

Background In spite of standard multimodal therapy consisting of surgical resection followed by radiation and concurrent chemotherapy, prognosis for glioblastoma (GBM) patients remains poor. The identification of both differentiated and undifferentiated "stem cell like" populations in the tumor highlights the significance of finding novel targets that affect the heterogeneous tumor cell population. Protein arginine methyltransferase 5 (PRMT5) is one such candidate gene whose nuclear expression correlates with poor survival and has been reported to be required for survival of differentiated GBM cells and self-renewal of undifferentiated GBM cells. In the current study we screened the specificity and efficacy of 4 novel PRMT5 inhibitors in the treatment of GBM. Methods Efficacies of these inhibitors were screened using an in vitro GBM neurosphere model and an in vivo intracranial zebrafish model of glioma. Standard molecular biology methods were employed to investigate changes in cell cycle, growth, and senescence. Results In vitro and in vivo studies revealed that among the 4 PRMT5 inhibitors, treatment of GBM cells with compound 5 (CMP5) mirrored the effects of PRMT5 knockdown wherein it led to apoptosis of differentiated GBM cells and drove undifferentiated primary patient derived GBM cells into a nonreplicative senescent state. Conclusion In vivo antitumor efficacy combined with the specificity of CMP5 underscores the importance of developing it for translation.

Published
2017

165. Efficacy of Onalespib, a Long-Acting Second-Generation HSP90 Inhibitor, as a Single Agent and in Combination with Temozolomide against Malignant Gliomas

Author

Erik P. Sulman, Metin N. Gurcan, Jihong Xu, Deepa Sampath, Divya Kesanakurti, Joseph Liu, Alessandro Canella, Christine E. Beattie, Joy Gumin, Balveen Kaur, Vinay K. Puduvalli, Alessandra M. Welker, Prabhakaran Nagarajan, Fazly Salleh Abas, Ji Young Yoo, and Frederick F. Lang

Subjects
0301 basic medicine, Cancer Research, Angiogenesis, Gene Expression, Antineoplastic Agents, Isoindoles, Pharmacology, Biology, Hsp90 inhibitor, Mice, 03 medical and health sciences, Cell Movement, In vivo, Cell Line, Tumor, Glioma, Temozolomide, medicine, Animals, Humans, HSP90 Heat-Shock Proteins, Extracellular Signal-Regulated MAP Kinases, Protein kinase B, Zebrafish, Cell Proliferation, Cell growth, Ribosomal Protein S6 Kinases, Drug Synergism, medicine.disease, Xenograft Model Antitumor Assays, In vitro, Dacarbazine, ErbB Receptors, Survival Rate, Disease Models, Animal, Protein Transport, 030104 developmental biology, Oncology, Blood-Brain Barrier, Benzamides, Neoplastic Stem Cells, Cancer research, Drug Therapy, Combination, Female, Proto-Oncogene Proteins c-akt, Signal Transduction, medicine.drug
Abstract

Purpose: HSP90, a highly conserved molecular chaperone that regulates the function of several oncogenic client proteins, is altered in glioblastoma. However, HSP90 inhibitors currently in clinical trials are short-acting, have unacceptable toxicities, or are unable to cross the blood–brain barrier (BBB). We examined the efficacy of onalespib, a potent, long-acting novel HSP90 inhibitor as a single agent and in combination with temozolomide (TMZ) against gliomas in vitro and in vivo. Experimental Design: The effect of onalespib on HSP90, its client proteins, and on the biology of glioma cell lines and patient-derived glioma-initiating cells (GSC) was determined. Brain and plasma pharmacokinetics of onalespib and its ability to inhibit HSP90 in vivo were assessed in non–tumor-bearing mice. Its efficacy as a single agent or in combination with TMZ was assessed in vitro and in vivo using zebrafish and patient-derived GSC xenograft mouse glioma models. Results: Onalespib-mediated HSP90 inhibition depleted several survival-promoting client proteins such as EGFR, EGFRvIII, and AKT, disrupted their downstream signaling, and decreased the proliferation, migration, angiogenesis, and survival of glioma cell lines and GSCs. Onalespib effectively crossed the BBB to inhibit HSP90 in vivo and extended survival as a single agent in zebrafish xenografts and in combination with TMZ in both zebrafish and GSC mouse xenografts. Conclusions: Our results demonstrate the long-acting effects of onalespib against gliomas in vitro and in vivo, which combined with its ability to cross the BBB support its development as a potential therapeutic agent in combination with TMZ against gliomas. Clin Cancer Res; 23(20); 6215–26. ©2017 AACR.

Published
2017

166. RNA Nanoparticle-Based Targeted Therapy for Glioblastoma through Inhibition of Oncogenic miR-21

Author

Dan Shu, Jun Ge Yu, Hui-Lung Sun, Matthew O. Old, Carlo M. Croce, Ri Cui, Tae Jin Lee, Peixuan Guo, Jianying Zhang, Mario Acunzo, Hui Li, Balveen Kaur, Zhenghua Luo, Ji Young Yoo, Alena Cristina Jaime-Ramirez, and Giulia Romano

Subjects
0301 basic medicine, Biodistribution, medicine.medical_treatment, Genetic enhancement, Oligonucleotides, Mice, Nude, law.invention, Targeted therapy, Mice, 03 medical and health sciences, Folic Acid, law, Cell Line, Tumor, Drug Discovery, microRNA, Genetics, medicine, Animals, Humans, PTEN, Molecular Biology, Pharmacology, Drug Carriers, biology, Brain Neoplasms, Folate Receptors, GPI-Anchored, PTEN Phosphohydrolase, Antagomirs, RNA-Binding Proteins, RNA, Survival Analysis, Xenograft Model Antitumor Assays, Gene Expression Regulation, Neoplastic, MicroRNAs, 030104 developmental biology, Apoptosis, biology.protein, Cancer research, Nanoparticles, Molecular Medicine, Suppressor, Female, Original Article, Apoptosis Regulatory Proteins, Glioblastoma
Abstract

Targeted inhibition of oncogenic miRNA-21 has been proposed to treat glioblastoma by rescuing tumor suppressors, PTEN and PDCD4. However, systemic delivery of anti-miR-21 sequences requires a robust and efficient delivery platform to successfully inhibit this druggable target. Three-way-junction (3WJ)-based RNA nanoparticles (RNP), artificially derived from pRNA of bacteriophage phi29 DNA packaging motor, was recently shown to target glioblastoma. Here, we report that multi-valent folate (FA)-conjugated 3WJ RNP constructed to harbor anti-miR-21 LNA sequences (FA-3WJ-LNA-miR21) specifically targeted and delivered anti-miR-21 LNA and knocked down miR-21 expression in glioblastoma cells in vitro and in vivo with favorable biodistribution. Systemically injected FA-3WJ-LNA-miR21 RNP efficiently rescued PTEN and PDCD4, resulting in glioblastoma cell apoptosis and tumor growth regression. Overall survival rate was also significantly improved by FA-3WJ-LNA-miR21 RNP. These results are indicative of the clinical benefit of FA-3WJ RNP-based gene therapy for the successful targeted therapy of developing and even recurring glioblastoma.

Published
2017

167. CBMT-40. THE RELATIONSHIP BETWEEN GLIOMA AND THE GUT-BRAIN AXIS

Author

Jessica Swanner, Nitin Tandon, Yoshihiro Otani, Gabriella Hines, Vasanta Putluri, Yoshua Esquenazi, Pedram Honarpisheh, Takeshi Takayasu, Balveen Kaur, Bhanu P. Ganesh, Anthony Patrizz, Nagireddy Putluri, Louise D. McCullough, Soheil Zorofchain, and Leomar Y. Ballester

Subjects
Cancer Research, Natural immunosuppression, Pathology, medicine.medical_specialty, Temozolomide, business.industry, Gut–brain axis, Tumor cells, Stool specimen, medicine.disease, Cell Biology and Metabolism, Therapeutic immunosuppression, Oncology, Glioma, Medicine, Neurology (clinical), business, Balance impairment, medicine.drug
Abstract

Recent studies demonstrate the potential role of the microbiome in immune-oncology, revealing specific microbial taxa can augment the effects of various therapeutic modalities against tumors. Gut dysbiosis, a disequilibrium in the host’s bacterial ecosystem, can potentially lead to overrepresentation of some bacteria and favor chronic inflammation and immunosuppression. However, the effects of microbial dysbiosis on non-gastrointestinal cancers in particular gliomas are unknown. Here, we explored the effects of glioma and Temozolomide (TMZ) on the fecal microbiome (FM) in mice (n=24) and FM and metabolome in humans (n=40). Aged C57/B6 mice were implanted with Gl261 tumor cells or vehicle and were assigned to one of the following treatment (oral) groups: vehicle, 5mg/kg TMZ or 25mg/kg TMZ beginning 14 days after surgery for 3-weeks following a 5 day on/2 day off treatment. Fecal samples were collected prior to surgery, at treatment initiation and weekly thereafter until sacrifice and sequenced for 16s RNA. Fecal samples were collected from humans with newly diagnosed glioma before resection, chemoradiation, and after chemoradiation (16s RNA, metabolomic, neurotransmitter analysis). In mice, FM beta diversity was significantly altered with glioma (p=0.003) while the alpha diversity remained unchanged. At a genus and family level analysis the relative abundance of Bacteroides (p=0.01) and Bacteroidaceae (p=0.02) was increased. Beta diversity of mice receiving 5mg/kg TMZ changed from baseline (p=0.02). Collectively, this suggests that glioma alters the FM, to what consequence remains to be explored. Alpha (Observed OTUs, p=0.029) and beta diversity (p=0.034) differences in mice correlated with survival (< 25 - >25 days). In humans, norepinephrine and 5-hydroxyindoleacetic acid were significantly lower in glioma patients at diagnosis compared to controls. Our findings demonstrate for the first time the relationship between glioma and the gut-brain axis. Understanding alterations in the FM in glioma patients may allow novel interventions and should be further investigated.

Published
2019

168. STEM-16. DUAL INHIBITION OF PROTEIN ARGININE METHYLTRANSFERASE 5 AND PROTEIN PHOSPHATASE 2A ENHANCES THE ANTI-TUMOR EFFICACY IN PRIMARY GLIOBLASTOMA NEUROSPHERES

Author

Zhengping Zhuang, John D. Heiss, Abhik Ray-Chaudhury, Arunakumar Gangaplara, Sachin Kumar, Ji Young Yoo, Balveen Kaur, Yeshavanth Kumar Banasavadi-Siddegowda, Hannah Sur, and Xiang Wang

Subjects
Cancer Research, Arginine, biology, Chemistry, Protein arginine methyltransferase 5, Stem Cells, Phosphatase, Retinoblastoma protein, Protein phosphatase 2, Methylation, Cell cycle, Oncology, Neurosphere, Cancer research, biology.protein, Neurology (clinical)
Abstract

INTRODUCTION Glioblastoma (GBM) is the most common malignant primary brain tumor and has a heterogeneous tumor cell population. The median survival of GBM patients is less than two years with current multi-model therapy of maximal surgical resection followed by chemotherapy, radiation and tumor treating fields. Protein Arginine Methyltransferase 5 (PRMT5) regulates cellular functions through symmetric di-methylation of arginine residues of histone and non-histone proteins. Our recent findings show that PRMT5 is overexpressed in GBM; its inhibition causes apoptosis and senescence of mature and immature GBM tumor cells respectively. Protein Phosphatase 2A (PP2A), a serine-threonine phosphatase, is associated with senescent tumor cells that contribute to therapy resistance; LB100 is a first-in-class small molecule inhibitor of PP2A that can sensitize tumor cells that are chemo- and radiation-therapy resistant. In this study, using patient-derived primary GBM neurospheres (GBMNS), we tested the anti-GBM effect of concurrent PRMT5 and PP2A inhibition. METHODS Patient-derived primary GBM neurospheres transfected with PRMT5 target-specific siRNA were treated with LB100 and subjected to in vitro assays such as proliferation assay, cell cycle analysis, cytotoxicity assay, PP2A activity and western blot. RESULTS LB100 treatment significantly reduced the viability of PRMT5-depleted GBM cells as compared to PRMT5 intact cells. LB100 caused G1 cell cycle arrest through inactivation of Rb protein; this effect is further enhanced in combination with PRMT5-depletion. Combination therapy also increased the expression of phospho-MLKL; Necrostatin-1 rescued PRMT5-depleted cells from the cytotoxic effects of LB100 indicating that necroptosis caused the enhanced cytotoxicity in combination therapy. We also found that PRMT5-depletion increased the PP2A activity in GBM neurospheres. CONCLUSION Combining the PRMT5 inhibition and PP2A inhibition produced greater antitumor effects than with PRMT5 inhibition alone.

Published
2019

169. Oncolytic HSV-Infected Glioma Cells Activate NOTCH in Adjacent Tumor Cells Sensitizing Tumors to Gamma Secretase Inhibition

Author

Ji Young Yoo, Jianhua Yu, Joseph C. Glorioso, Tae Jin Lee, Yuanqing Yan, Michael A. Caligiuri, Joseph N. Liu, Brian Hurwitz, Alena Cristina Jaime-Ramirez, Balveen Kaur, Samantha Chao, Yoshihiro Otani, and Hongsheng Dai

Subjects
0301 basic medicine, Male, Cancer Research, Ubiquitin-Protein Ligases, Notch signaling pathway, Mice, Nude, Herpesvirus 1, Human, Diamines, medicine.disease_cause, Article, Mixed Function Oxygenases, 03 medical and health sciences, Mice, Random Allocation, 0302 clinical medicine, Downregulation and upregulation, Glioma, Cell Line, Tumor, medicine, Bioluminescence imaging, Animals, Humans, Gamma secretase, Oncolytic Virotherapy, Receptors, Notch, Chemistry, Brain Neoplasms, Benzazepines, medicine.disease, Xenograft Model Antitumor Assays, Oncolytic virus, Repressor Proteins, MicroRNAs, Thiazoles, 030104 developmental biology, Herpes simplex virus, Oncology, 030220 oncology & carcinogenesis, Cancer research, Female, Signal transduction, Amyloid Precursor Protein Secretases, Glioblastoma, Signal Transduction
Abstract

Purpose: To examine the effect of oncolytic herpes simplex virus (oHSV) on NOTCH signaling in central nervous system tumors. Experimental Design: Bioluminescence imaging, reverse phase protein array proteomics, fluorescence microscopy, reporter assays, and molecular biology approaches were used to evaluate NOTCH signaling. Orthotopic glioma-mouse models were utilized to evaluate effects in vivo. Results: We have identified that herpes simplex virus-1 (HSV-1; oncolytic and wild-type)-infected glioma cells induce NOTCH signaling, from inside of infected cells into adjacent tumor cells (inside out signaling). This was canonical NOTCH signaling, which resulted in activation of RBPJ-dependent transcriptional activity that could be rescued with dnMAML. High-throughput screening of HSV-1–encoded cDNA and miRNA libraries further uncovered that HSV-1 miR-H16 induced NOTCH signaling. We further identified that factor inhibiting HIF-1 (FIH-1) is a direct target of miR-H16, and that FIH-1 downregulation by virus encoded miR-H16 induces NOTCH activity. FIH-1 binding to Mib1 has been reported, but this is the first report that shows FIH-1 sequester Mib1 to suppress NOTCH activation. We observed that FIH-1 degradation induced NOTCH ligand ubiquitination and NOTCH activity. REMBRANDT and The Cancer Genome Atlas data analysis also uncovered a significant negative regulation between FIH-1 and NOTCH. Furthermore, combination of oHSV with NOTCH-blocking gamma secretase inhibitor (GSI) had a therapeutic advantage in two different intracranial glioma models treated with oncolytic HSV, without affecting safety profile of the virus in vivo. Conclusions: To our knowledge this is the first report to identify impact of HSV-1 on NOTCH signaling and highlights the significance of combining oHSV and GSI for glioblastoma therapy.

Published
2019

170. Immune therapy, a double-edged sword for oncolytic viruses

Author

Ryan M McCormack and Balveen Kaur

Subjects
Pharmacology, Tumor microenvironment, Genetically engineered, viruses, Clinical Biochemistry, technology, industry, and agriculture, Biology, Virology, Article, Viral vector, Targeted immunotherapy, Immune therapy, Oncolytic virus, Immunity, Drug Discovery
Abstract

In recent years, oncolytic viruses (OVs) have emerged as a powerful, targeted immunotherapy with the identification of new viral vectors as well as genetically engineered viral payloads. Owing to t...

Published
2019

171. Oncolytic HSV therapy increases trametinib access to brain tumors and sensitizes them in vivo

Author

Flora Park, Bangxing Hong, Mitch Phelphs, Joseph N. Liu, Balveen Kaur, Alena Cristina Jaime-Ramirez, Tae Jin Lee, Feng Geng, Deliang Guo, Yeshavanth Kumar Banasavadi-Siddegowda, Haroon Quadri, Yoshihiro Otani, Mitra Nair, Ji Young Yoo, Jessica Swanner, and Darlene M. Bystry

Subjects
Cancer Research, Pyridones, Herpesvirus 1, Human, Pyrimidinones, CD8-Positive T-Lymphocytes, Mice, Immune system, In vivo, Glioma, Cell Line, Tumor, Medicine, Animals, Humans, Protein Kinase Inhibitors, Trametinib, Mitogen-Activated Protein Kinase Kinases, Oncolytic Virotherapy, Microglia, business.industry, Brain Neoplasms, Tumor Necrosis Factor-alpha, Macrophages, Editorials, medicine.disease, Xenograft Model Antitumor Assays, Oncolytic virus, Survival Rate, Disease Models, Animal, medicine.anatomical_structure, RAW 264.7 Cells, Oncology, Apoptosis, Blood-Brain Barrier, Cancer research, Tumor necrosis factor alpha, Neurology (clinical), business, Glioblastoma, Immunocompetence
Abstract

BackgroundHyperactivation of the RAS-RAF-MEK-ERK signaling pathway is exploited by glioma cells to promote their growth and evade apoptosis. MEK activation in tumor cells can increase replication of ICP34.5-deleted herpes simplex virus type 1 (HSV-1), but paradoxically its activation in tumor-associated macrophages promotes a pro-inflammatory signaling that can inhibit virus replication and propagation. Here we investigated the effect of blocking MEK signaling in conjunction with oncolytic HSV-1 (oHSV) for brain tumors.MethodsInfected glioma cells co-cultured with microglia or macrophages treated with or without trametinib were used to test trametinib effect on macrophages/microglia. Enzyme-linked immunosorbent assay, western blotting, and flow cytometry were utilized to evaluate the effect of the combination therapy. Pharmacokinetic (PK) analysis of mouse plasma and brain tissue was used to evaluate trametinib delivery to the CNS. Intracranial human and mouse glioma-bearing immune deficient and immune competent mice were used to evaluate the antitumor efficacy.ResultOncolytic HSV treatment rescued trametinib-mediated feedback reactivation of the mitogen-activated protein kinase signaling pathway in glioma. In vivo, PK analysis revealed enhanced blood–brain barrier penetration of trametinib after oHSV treatment. Treatment by trametinib, a MEK kinase inhibitor, led to a significant reduction in microglia- and macrophage-derived tumor necrosis factor alpha (TNFα) secretion in response to oHSV treatment and increased survival of glioma-bearing mice. Despite the reduced TNFα production observed in vivo, the combination treatment activated CD8+ T-cell mediated immunity and increased survival in a glioma-bearing immune-competent mouse model.ConclusionThis study provides a rationale for combining oHSV with trametinib for the treatment of brain tumors.

Published
2019

172. Amendments: Publisher Correction: An oncolytic herpesvirus expressing E-cadherin improves survival in mouse models of glioblastoma

Author

Hanwei Cui, Bo Xu, Hiroshi Nakashima, Rui Ma, Ji Young Yoo, Jianfeng Han, Jianhua Yu, Michael A. Caligiuri, Balveen Kaur, Hongsheng Dai, Ping Yi, E. Antonio Chiocca, Luke Russell, and Jianying Zhang

Subjects
0303 health sciences, Phrase, Cadherin, media_common.quotation_subject, Biomedical Engineering, Bioengineering, Art, Legend, medicine.disease, Applied Microbiology and Biotechnology, Linguistics, Oncolytic virus, 03 medical and health sciences, 0302 clinical medicine, Reading (process), medicine, Molecular Medicine, 030217 neurology & neurosurgery, 030304 developmental biology, Biotechnology, media_common, Glioblastoma
Abstract

Nat. Biotechnol.; 10.1038/nbt.4302; corrected online 19 December 2018 In the HTML and PDF versions of this article initially published online, KLRG1− should have read KLRG1+ in the first instance of the phrase in the Figure 1e legend reading “For KLRG1− NK cells, uninfected vs. OV-Q1.” In the HTML version, KLRG1− should have read KLRG1+ in the following locations: the first instance in the Figure 1b legend, the first instance in the Figure 1c legend, and the first instance in the Figure 1e legend.

Published
2019

173. Current Challenges and Applications of Oncolytic Viruses in Overcoming the Development of Resistance to Therapies in Cancer

Author

Bangxing Hong, Balveen Kaur, W. Hans Meisen, Ryan M McCormack, Jessica Swanner, and Cole T. Lewis

Subjects
Oncolytic adenovirus, Combination therapy, business.industry, medicine.medical_treatment, Cancer, Immunotherapy, medicine.disease, Oncolytic virus, Clinical trial, Immune system, Cancer research, Medicine, Stem cell, business
Abstract

Oncolytic viruses (OVs) are designed to ablate cancerous cells while sparing non-malignant cells and tissues. In the wake of an active tumor infection, OVs can activate an anti-tumor immune response. Currently, an oncolytic Herpes simplex 1 (HSV-1) derived virus encoding for granulocyte-macrophage colony stimulating factor (GM-CSF) is approved in the US and Europe as a treatment for metastatic melanoma, and an oncolytic adenovirus (oAd) is approved in China for head and neck cancer therapy. Despite the approved use for these indications, this promising biological therapy is currently under-used. However, a multitude of viruses are actively being explored in preclinical animal models and clinically in patients with different malignancies for safety and efficacy. Several ongoing clinical trials evaluate OV utility in combination with other therapies, such as chemotherapeutics and immune checkpoint inhibitors. In this chapter, we highlight some of the barriers faced by OVs and discuss methods used to convert these challenges into opportunities for improvement. Major advancements in this field include engineering OVs to deliver payloads with anti-angiogenic, immune modulatory, or extracellular matrix degrading proteins, as well as in combination with immunotherapies, DNA damaging agents, and stem cells to enhance the therapeutic efficacy of OVs. Despite facing some challenges, there is continued enthusiasm for this innovative and promising biological arsenal in treating cancer.

Published
2019

174. Medroxyprogesterone acetate and levonorgestrel increase genital mucosal permeability and enhance susceptibility to genital herpes simplex virus type 2 infection

Author

N.E. Quispe Calla, Wayne Trout, Balveen Kaur, Stephen D. Pavelko, Prosper N. Boyaka, Thomas L. Cherpes, Luanne Hall-Stoodley, and R.D. Vicetti Miguel

Subjects
0301 basic medicine, medicine.drug_class, Herpesvirus 2, Human, Immunology, Medroxyprogesterone Acetate, Biology, Article, Permeability, Mice, 03 medical and health sciences, 0302 clinical medicine, estrogen, Contraceptive Agents, Female, medicine, genital mucosal barrier protection, Animals, Immunology and Allergy, Medroxyprogesterone acetate, Levonorgestrel, Barrier function, Herpes Genitalis, Mucous Membrane, 030219 obstetrics & reproductive medicine, levonorgestrel, Mucous membrane, Estrogens, 3. Good health, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Mucosal immunology, Hormonal contraception, medroxyprogesterone, Vagina, Female, Disease Susceptibility, Progestin, medicine.drug
Abstract

Depot-medroxyprogesterone acetate (DMPA) is a hormonal contraceptive especially popular in areas with high prevalence of HIV and other sexually transmitted infections (STI). Although observational studies identify DMPA as an important STI risk factor, mechanisms underlying this connection are undefined. Levonorgestrel (LNG) is another progestin used for hormonal contraception, but its effect on STI susceptibility is much less explored. Using a mouse model of genital herpes simplex virus type 2 (HSV-2) infection, we herein found that DMPA and LNG similarly reduced genital expression of the desmosomal cadherin desmoglein-1α (DSG1α), enhanced access of inflammatory cells to genital tissue by increasing mucosal epithelial permeability, and increased susceptibility to viral infection. Additional studies with uninfected mice revealed that DMPA-mediated increases in mucosal permeability promoted tissue inflammation by facilitating endogenous vaginal microbiota invasion. Conversely, concomitant treatment of mice with DMPA and intravaginal estrogen restored mucosal barrier function and prevented HSV-2 infection. Evaluating ectocervical biopsy tissue from women before and 1 month after initiating DMPA remarkably revealed that inflammation and barrier protection were altered by treatment identically to changes seen in progestin-treated mice. Together, our work reveals DMPA and LNG diminish the genital mucosal barrier; a first-line defense against all STI, but may offer foundation for new contraceptive strategies less compromising of barrier protection.

Published
2016

175. Elevated STAT3 expression in ovarian cancer ascites promotes invasion and metastasis: a potential therapeutic target

Author

Shan Naidu, Periannan Kuppusamy, John J. Wallbillich, Adam C. ElNaggar, Karuppaiyah Selvendiran, David E. Cohn, Hemant K. Bid, Kristin Bixel, Balveen Kaur, Uksha Saini, Adrian A. Suarez, Chelsea Bolyard, Paul J. Goodfellow, and John L. Hays

Subjects
STAT3 Transcription Factor, 0301 basic medicine, Cancer Research, Angiogenesis, Biology, Article, Metastasis, Gene Knockout Techniques, Mice, 03 medical and health sciences, Ovarian tumor, 0302 clinical medicine, Cell Movement, Genetics, medicine, Animals, Humans, Neoplasm Invasiveness, Neoplasm Metastasis, Molecular Biology, Piperidones, Ovarian Neoplasms, Ascites, Cancer, medicine.disease, Xenograft Model Antitumor Assays, Primary tumor, Up-Regulation, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Tumor progression, 030220 oncology & carcinogenesis, Cancer research, Female, Ovarian cancer, Ex vivo, Signal Transduction
Abstract

Although activation of the STAT3 pathway has been associated with tumor progression in a wide variety of cancer types (including ovarian cancer), the precise mechanism of invasion and metastasis due to STAT3 are not fully delineated in ovarian cancer. We found that pSTAT3 Tyr705 is constitutively activated in patient ascites and ascites-derived ovarian cancer cells (ADOCCs), and the range of STAT3 expression could be very high to low. In vivo transplantation of ADOCCs with high pSTAT3 expression into the ovarian bursa of mice resulted in a large primary tumor and widespread peritoneal metastases as well liver. In contrast, ADOCCs with low STAT3 expression or ADOCCs with STAT3 expression knocked down led to reduced tumor growth and an absence of metastases in vivo. Cytokines derived from the ADOCC culture medium activate the IL-6/STAT pathway in the STAT3 knockout (Ko) cells, compensating for the absence of inherent STAT3 in the cells. Treatment with HO-3867 (a novel STAT3 inhibitor at 100 ppm in an orthotopic murine model) significantly suppressed ovarian tumor growth, angiogenesis, and metastasis by targeting STAT3 and its downstream proteins. HO-3867 was found to have cytotoxic effects in ex-vivo cultures of freshly-collected human ovarian cancers, including those resistant to platinum-based chemotherapy. Our results show that STAT3 is necessary for ovarian tumor progression/metastasis and highlight the potential for targeting STAT3 by HO-3867 as a therapeutic strategy for ovarian cancer.

Published
2016

176. TGFβ Treatment Enhances Glioblastoma Virotherapy by Inhibiting the Innate Immune Response

Author

Jianfeng Han, Jianhong Chu, Qi-En Wang, Jianying Zhang, Lingling Zhang, Jianhua Yu, Xiaoming He, Xilin Chen, Lichao Chen, Michael A. Caligiuri, Bo Xu, Walter Hans Meisen, E. Antonio Chiocca, and Balveen Kaur

Subjects
Cancer Research, medicine.medical_treatment, Biology, Real-Time Polymerase Chain Reaction, Article, Flow cytometry, Mice, Mice, Inbred NOD, Transforming Growth Factor beta, Immunity, medicine, Animals, Humans, Simplexvirus, Virotherapy, Oncolytic Virotherapy, Innate immune system, Microglia, medicine.diagnostic_test, Brain Neoplasms, Reverse Transcriptase Polymerase Chain Reaction, Transforming growth factor beta, Flow Cytometry, Xenograft Model Antitumor Assays, Immunity, Innate, Oncolytic virus, Disease Models, Animal, Oncolytic Viruses, medicine.anatomical_structure, Cytokine, Oncology, Immunology, biology.protein, Glioblastoma, Immunosuppressive Agents
Abstract

Oncolytic viruses, including oncolytic herpes simplex virus (oHSV), have produced provocative therapeutic responses in patients with glioblastoma, the most aggressive brain tumor. Paradoxically, innate immune responses mediated by natural killer (NK) cells and macrophages/microglia appear to limit oHSV efficacy. Therefore, we investigated whether pretreatment with an immunosuppressive cytokine, TGFβ, might reverse these effects and thereby potentiate oHSV efficacy. TGFβ treatment of NK cells rendered them less cytolytic against oHSV-infected glioblastoma cells and stem-like cells in vitro. Furthermore, TGFβ treatment of NK cells, macrophages, or microglia increased viral titers of oHSV in cocultures with glioblastoma cells. In a syngeneic mouse model of glioblastoma, administering TGFβ prior to oHSV injection inhibited intracranial infiltration and activation of NK cells and macrophages. Notably, a single administration of TGFβ prior to oHSV therapy was sufficient to phenocopy NK-cell depletion and suppress tumor growth and prolong survival in both xenograft and syngeneic models of glioblastoma. Collectively, our findings show how administering a single dose of TGFβ prior to oncolytic virus treatment of glioblastoma can transiently inhibit innate immune cells that limit efficacy, thereby improving therapeutic responses and survival outcomes. Cancer Res; 75(24); 5273–82. ©2015 AACR.

Published
2015

177. CSIG-17. PRMT5 INHIBITION SENSITIZES GLIOBLASTOMA MODELS TO TRAMETINIB TREATMENT

Author

Hannah Sur, Ji Young Yoo, Shilpa Thammegowda, Toshihiko Shimizu, Balveen Kaur, John D. Heiss, Yeshavanth Kumar Banasavadi-Siddegowda, Dragan Maric, Yoshihiro Otani, Sriya Namagiri, Ashis Chowdhury, Tae Jin Lee, and Cole T. Lewis

Subjects
Trametinib, Cancer Research, Proto-Oncogene Proteins c-akt, Chemistry, Protein arginine methyltransferase 5, Cell Signaling and Signaling Pathways, Cell cycle, Oncology, Apoptosis, Tumor progression, Cancer research, Neurology (clinical), Signal transduction, Survival rate
Abstract

INTRODUCTION Glioblastoma (GBM) is the most common malignant primary brain tumor. With limited effective therapeutic strategies, prognosis for GBM is very poor. Our previous study shows that the expression of Protein Arginine Methyltransferase 5 (PRMT5) is upregulated in GBM; its inhibition promotes anti-GBM effect through apoptosis and senescence of mature and immature tumor cells, respectively. In GBM, RAS-RAF- MEK-ERK signaling is aberrantly activated and promotes tumor growth. Therefore, MEK inhibitors, including trametinib are currently under investigation for GBM therapy. In this study, we tested whether inhibition of PRMT5 can enhance the anti-tumor efficacy of trametinib in GBM. METHODS Patient-derived primary GBM neurospheres (GBMNS) with transient PRMT5 knockdown were treated with trametinib and cell viability, proliferation, cell cycle progression, and western blot analysis were conducted. In vivo, PRMT5-intact and -depleted GBMNS were intracranially implanted in NSG mice and treated with trametinib by daily oral gavage, and tumor progression and mice survival rate were analyzed by MRI and Kaplan-Meier survival curve, respectively. RESULTS Trametinib treatment upregulated the expression of PRMT5 in GBMNS. Depletion of PRMT5 increased the cytotoxic effect of trametinib in GBMNS. In concurrence with the trametinib-induced PRMT5 upregulation, trametinib treatment increased the activity of AKT that was blocked with PRMT5 knockdown. In vivo, PRMT5-depletion extended the survival of the tumor bearing mice that further increased in combination with trametinib treatment. Interestingly, trametinib treatment alone had no survival benefit. CONCLUSION Trametinib treatment induces PRMT5 expression. Depletion of trametinib-induced PRMT5 expression sensitizes GBMNS for trametinib by inhibiting AKT activity.

Published
2020

178. TAMI-11. IMPACT OF oHSV ACTIVATED NOTCH SIGNALING IN TUMOR MICROENVIRONMENT, AND ITS IMPACT ON ANTI-TUMOR IMMUNITY

Author

Yeshavanth Kumar Banasavadi-Siddegowda, Yoshihiro Otani, Bangxing Hong, Josue Pineda, Zhongming Zhao, Scott D. Olson, Ji Young Yoo, Yuanqing Yan, Balveen Kaur, Guangsheng Pei, Kimberly Rivera Caraballo, Samantha Chao, Sara A. Murphy, Toshihiko Shimizu, John D. Heiss, and Cole T. Lewis

Subjects
Cancer Research, Tumor microenvironment, Oncology, Antitumor immunity, Cancer research, Notch signaling pathway, Tumor Microenvironment/Angiogenesis/Metabolism/Invasion, Neurology (clinical), Biology
Abstract

NOTCH signaling is a method of cell-cell communication where membrane bound NOTCH ligands on signal-sending cells can bind to and initiate cleavage of the NOTCH receptor, releasing NICD which can initiate signal transduction in adjacent “signal-receiving” cells. We have recently shown that oHSV treatment of GBM cells induces NICD cleavage and NOTCH activation in adjacent uninfected glioma cells. RNA sequencing of GBM cells post-infection also uncovered Gene Ontology NOTCH signaling pathway to be significantly upregulated. This activation was induced by viral miRNA-H16, which represses FIH-1 expression. FIH-1 was found to be a negative regulator of Mib1, a ubiquitin ligase, which activates NOTCH ligand-mediated activation of adjacent signal-receiving cells bearing the NOTCH receptor (Otani et al Clin. Can. Res. 2020). Here we have investigated the impact of oHSV-induced NOTCH signaling on the tumor microenvironment. Treatment of brain tumors in immune competent mice with oHSV and NOTCH blocking gamma secretase inhibitor (GSI) induced an anti-tumor memory immune response. Long term survivors in mice treated with the combination also completely rejected subsequent tumor re-challenge in the other hemisphere. UMAP of flow cytometry of tumor-bearing hemispheres and functional analysis of isolated cellular fractions from treated mice showed a significant influx of MDSC cells after oHSV treatment that was rescued in mice treated with oHSV and GSI. Ongoing mechanistic studies are uncovering a significant induction of NOTCH in tumor associated macrophages that aids in recruitment of MDSC cells. Overall these studies have uncovered a significant impact of oHSV therapy on GBM tumor microenvironment and presents opportunities for combination therapies that can help improve therapeutic benefit and anti-tumor immunity.

Published
2020

179. CSIG-33. ONCOLYTIC HERPES VIRUS TREATMENT INDUCED NOTCH SIGNALING VIA HSV-1 microRNA H16 AND IT INVOLVED IN TREATMENT RESISTANCE

Author

Alena Cristina Jaime-Ramirez, Balveen Kaur, Joseph N. Liu, Tae Jin Lee, Ji Young Yoo, and Yoshihiro Otani

Subjects
Cancer Research, Abstracts, Oncology, business.industry, microRNA, Cancer research, Notch signaling pathway, Medicine, Neurology (clinical), HSL and HSV, Treatment resistance, business, Oncolytic herpes virus
Abstract

INTRODUCTION: Glioblastomas (GBMs) are resistant to traditional therapies. Thus, the development of novel treatment strategies is urgently needed. NOTCH signaling is activated in GBM and important for mediating proliferation, angiogenesis, and resistance to therapy. In this study, we uncovered the mechanism by which oncolytic herpes simplex viruse-1 (oHSV) therapy induced NOTCH activation in the tumor microenvironment (TME). We also investigated the therapeutic benefit of combining oHSV therapy with Gamma-secretase inhibitor (GSI), a NOTCH inhibitor. METHODS: Real time Q-PCR, NOTCH reporter assay, and bioluminescence mice imaging were used to test oHSV-induced NOTCH activation. Screening of HSV-1-encoded microRNAs (HSVmiRs) and genes were performed to identify the mechanism which regulates the NOTCH signaling. Intracranial glioma-bearing xenografts were used to evaluate the anti-tumor efficacy of combination of GSI and oHSV. RESULTS: oHSV infection induced gene expression of NOTCH ligands resulting in activation of NOTCH signaling in adjacent cells in primary GBM derived cells. This was mediated by HSV encoded miRH16. HSVmiRH16 targets and suppresses Factor Inhibitor Hif1-1 (FIH-1) expression which is known to inhibit NOTCH activation. Consistent with this both overexpression of HSVmiRH16 and knockdown of FIH-1 significantly induced NOTCH signaling. Treatment of mice bearing intracranial glioma with GSI and oHSV therapy significantly enhanced survival compared to that with monotherapy. CONCLUSION: We identified oHSV-induced NOTCH signaling activation, via HSV encoded miRH16. We further find that GSI treatment in combination with oHSV therapy demonstrated improved efficacy. To our knowledge this is the first report investigating NOTCH signaling in conjunction with oHSV therapy.

Published
2018

180. Pyruvate kinase M2 regulates homologous recombination-mediated DNA double-strand break repair

Author

Pierre A. Robe, Brian Hurwitz, Weili Miao, Balveen Kaur, Michael C. Ostrowski, Yinsheng Wang, Ju Hwan Cho, Manchao Zhang, Arnab Chakravarti, Gina M. Sizemore, Fen Xia, Norman L. Lehman, and Steven T. Sizemore

Subjects
0301 basic medicine, Thyroid Hormones, DNA Repair, Cell Survival, DNA damage, Nude, Clinical Sciences, Mice, Nude, Biology, PKM2, Article, Cell Line, Double-Stranded, Mice, 03 medical and health sciences, chemistry.chemical_compound, Rare Diseases, PARP1, Cell Line, Tumor, Genetics, medicine, 2.1 Biological and endogenous factors, Animals, Humans, DNA Breaks, Double-Stranded, Aetiology, Molecular Biology, Cancer, Tumor, DNA Breaks, Membrane Proteins, Cell Biology, medicine.disease, Double Strand Break Repair, 3. Good health, Cell biology, 030104 developmental biology, chemistry, Cancer cell, Female, Biochemistry and Cell Biology, Carrier Proteins, Homologous recombination, DNA, Developmental Biology
Abstract

Resistance to genotoxic therapies is a primary cause of treatment failure and tumor recurrence. The underlying mechanisms that activate the DNA damage response (DDR) and allow cancer cells to escape the lethal effects of genotoxic therapies remain unclear. Here, we uncover an unexpected mechanism through which pyruvate kinase M2 (PKM2), the highly expressed PK isoform in cancer cells and a master regulator of cancer metabolic reprogramming, integrates with the DDR to directly promote DNA double-strand break (DSB) repair. In response to ionizing radiation and oxidative stress, ATM phosphorylates PKM2 at T328 resulting in its nuclear accumulation. pT328-PKM2 is required and sufficient to promote homologous recombination (HR)-mediated DNA DSB repair through phosphorylation of CtBP-interacting protein (CtIP) on T126 to increase CtIP's recruitment at DSBs and resection of DNA ends. Disruption of the ATM-PKM2-CtIP axis sensitizes cancer cells to a variety of DNA-damaging agents and PARP1 inhibition. Furthermore, increased nuclear pT328-PKM2 level is associated with significantly worse survival in glioblastoma patients. Combined, these data advocate the use of PKM2-targeting strategies as a means to not only disrupt cancer metabolism but also inhibit an important mechanism of resistance to genotoxic therapies.

Published
2018

181. Oncolytic Herpes Virus Armed with Vasculostatin in Combination with Bevacizumab Abrogates Glioma Invasion via the CCN1 and AKT Signaling Pathways

Author

Tetsuo Oka, Atsuhito Uneda, Toshihiko Shimizu, Tomotsugu Ichikawa, Yasuhiko Hattori, Balveen Kaur, Yusuke Tomita, Isao Date, Yoshihiro Otani, Kazuhiko Kurozumi, Kentaro Fujii, Yuji Matsumoto, and Ji Young Yoo

Subjects
0301 basic medicine, Cancer Research, genetic structures, Bevacizumab, Oncolytic herpes virus, Hepevirus, Neovascularization, 03 medical and health sciences, Mice, 0302 clinical medicine, In vivo, Cell Movement, Glioma, Cell Line, Tumor, Medicine, Animals, Humans, Cytotoxicity, Protein kinase B, Oncolytic Virotherapy, Neovascularization, Pathologic, business.industry, medicine.disease, Combined Modality Therapy, Xenograft Model Antitumor Assays, eye diseases, Oncolytic virus, ErbB Receptors, Disease Models, Animal, Oncolytic Viruses, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, sense organs, medicine.symptom, business, Proto-Oncogene Proteins c-akt, medicine.drug, Cysteine-Rich Protein 61, Signal Transduction
Abstract

Anti-VEGF treatments such as bevacizumab have demonstrated convincing therapeutic advantage in patients with glioblastoma. However, bevacizumab has also been reported to induce invasiveness of glioma. In this study, we examined the effects of rapid antiangiogenesis mediated by oncolytic virus (RAMBO), an oncolytic herpes simplex virus-1 expressing vasculostatin, on bevacizumab-induced glioma invasion. The effect of the combination of RAMBO and bevacizumab in vitro was assessed by cytotoxicity, migration, and invasion assays. For in vivo experiments, glioma cells were stereotactically inoculated into the brain of mice. RAMBO was intratumorally injected 7 days after tumor inoculation, and bevacizumab was administered intraperitoneally twice a week. RAMBO significantly decreased both the migration and invasion of glioma cells treated with bevacizumab. In mice treated with bevacizumab and RAMBO combination, the survival time was significantly longer and the depth of tumor invasion was significantly smaller than those treated with bevacizumab monotherapy. Interestingly, RAMBO decreased the expression of cysteine-rich protein 61 and phosphorylation of AKT, which were increased by bevacizumab. These results suggest that RAMBO suppresses bevacizumab-induced glioma invasion, which could be a promising approach to glioma therapy.

Published
2018

182. Complex role of NK cells in regulation of oncolytic virus–bortezomib therapy

Author

Yangjin Kim, Ji Young Yoo, Joseph N. Liu, Jianhua Yu, Tae Jin Lee, Avner Friedman, Michael A. Caligiuri, and Balveen Kaur

Subjects
0301 basic medicine, Combination therapy, Bortezomib, 03 medical and health sciences, 0302 clinical medicine, In vivo, Immunity, Cell Line, Tumor, Chlorocebus aethiops, medicine, Tumor Microenvironment, Animals, Humans, Vero Cells, Oncolytic Virotherapy, Tumor microenvironment, Multidisciplinary, business.industry, Models, Immunological, Biological Sciences, In vitro, Oncolytic virus, Killer Cells, Natural, 030104 developmental biology, 030220 oncology & carcinogenesis, Hematologic Neoplasms, Cancer research, Proteasome inhibitor, business, medicine.drug
Abstract

Significance The present work considers the effect of NK cell treatment in a combination therapy with oncolytic virus (OV) and bortezomib. It demonstrates by cross-disciplinary analysis of a complex biological process that the standard strategies, wherein “more is better,” do not necessarily apply when multiple drugs of different classes and interactions are being used in the combination. While many combination clinical trials are being conducted with little forethought as to the interactions that may be expected between diverse agents, this work provides a basis for the generation of mathematical models and simulations that address the complexity of the interactions among the diverse agents and could play an important role in the future development of clinical trials.

Published
2018

183. Contributors

Author

Rolla Abu-Arja, Ana Aguilar-Bonilla, Manmeet S. Ahluwalia, Sheikh C. Ali, Deborah H. Allen, Iyad Alnahhas, Gregory D. Arnone, Pascal Auquier, Nicholas G. Avgeropoulos, Kristen A. Batich, Karine Baumstarck, Susan D. Bell, Viviana Benitez, Deborah T. Blumenthal, Miriam Bornhorst, Laurent Boyer, Alexa N. Bramall, Sarah Braun, Henry Brem, William C. Broaddus, Alberto Broniscer, Nicholas Butowski, Soonmee Cha, Marc C. Chamberlain, Susan Chang, Alain Charest, Zhi-Jian Chen, Sajeel Chowdhary, Jennifer L. Clarke, Adam L. Cohen, Howard Colman, Michael Cooper, Jennifer Cotter, Sunit Das, Kuntal De, Macarena I. De la Fuente, Anand K. Deo, Annick Desjardins, Girish Dhall, Nancy D. Doolittle, Kira M. Downey, Gavin P. Dunn, Herbert H. Engelhard, Emilie Ernoult, Richard G. Everson, Robert A. Fenstermaker, Isabelle Ferry, Sheila Figel, Karen L. Fink, Jonathan L. Finlay, Joanna E. Gernsback, Pierre Giglio, Noah Gorelick, Daphne Haas-Kogan, Jan T. Hachmann, Hasan Hashem, John W. Henson, Sherri Y. Huang, Mai Anh Huynh, Eugene I. Hwang, Eric Jackson, Tanner M. Johanns, Liron Kahlon, Deepak Kanojia, Matthias A. Karajannis, Balveen Kaur, Santosh Kesari, Lindsay B. Kilburn, Julius W. Kim, Cassie Kline, John Paul G. Kolcun, Ricardo J. Komotar, Matthew Koshy, Claudia M. Kuzan-Fischer, Sajani S. Lakka, Autumn Lanoye, George P. Lee, Eudocia Q. Lee, Maciej S. Lesniak, Linda M. Liau, Ashlee R. Loughan, Mark G. Malkin, Brendan J. McCullough, John M. McGregor, Ankit I. Mehta, Julie J. Miller, Nimish Mohile, Paul L. Moots, Sabine Mueller, Joydeep Mukherjee, Tulio P. Murillo, Megan E. Muroski, Edward A. Neuwelt, Herbert B. Newton, Martin K. Nicholas, Nancyann Oberheim Bush, Hideho Okada, Antonio M. Omuro, Roger J. Packer, Nina A. Paleologos, Wojciech K. Panek, Sebastian P. Pernal, Emily Owens Pickle, Katarzyna C. Pituch, Ian F. Pollack, Jeffrey Raizer, Aida Rashidi, David A. Reardon, Alyssa T. Reddy, J. Robert Kane, James T. Rutka, John H. Sampson, Mithun Sattur, Adrienne C. Scheck, Brian J. Scott, Wendy L. See, Nawal Shaikh, Mayur Sharma, Tolou Shokuhfar, Seema Shroff, Amy A. Smith, Subanandhini Subramaniam, Carter M. Suryadevara, Kenneth D. Swanson, Benita Tamrazi, Shervin Taslimi, Beverly Teicher, Hung N. Tran, Betty Tyler, Santhosh A. Upadhyaya, Rafael A. Vega, Monica Venere, Michael Vogelbaum, Diane Von Ah, Barliz Waissengrin, Emily S. Waite, Eric T. Wong, Annie Xiao, Jer-Yen Yang, Jacob S. Young, Ji Young Yoo, and Wafik Zaky

Published
2018

184. The Impact of Macrophage- and Microglia-Secreted TNFα on Oncolytic HSV-1 Therapy in the Glioblastoma Tumor Microenvironment

Author

Luke Russell, Kamaldeen A. Muili, W. Hans Meisen, Eric S. Wohleb, Michael A. Caligiuri, Samuel Dubin, Jonathan P. Godbout, Alena Cristina Jaime-Ramirez, Balveen Kaur, Ji Young Yoo, Jianhua Yu, Chelsea Bolyard, and Jayson Hardcastle

Subjects
Cancer Research, Blotting, Western, Mice, Nude, Antineoplastic Agents, Herpesvirus 1, Human, Biology, Article, Virus, Mice, Glioma, Tumor Microenvironment, medicine, Animals, Cells, Cultured, Mice, Knockout, Oncolytic Virotherapy, Tumor microenvironment, Microglia, Brain Neoplasms, Tumor Necrosis Factor-alpha, Macrophages, Flow Cytometry, medicine.disease, Xenograft Model Antitumor Assays, Coculture Techniques, Oncolytic virus, Disease Models, Animal, Oncolytic Viruses, medicine.anatomical_structure, Oncology, Viral replication, Immunology, Oncolytic Virus Therapy, Female, Tumor necrosis factor alpha, Glioblastoma
Abstract

Purpose: Oncolytic herpes simplex viruses (oHSV) represent a promising therapy for glioblastoma (GBM), but their clinical success has been limited. Early innate immune responses to viral infection reduce oHSV replication, tumor destruction, and efficacy. Here, we characterized the antiviral effects of macrophages and microglia on viral therapy for GBM. Experimental Design: Quantitative flow cytometry of mice with intracranial gliomas (±oHSV) was used to examine macrophage/microglia infiltration and activation. In vitro coculture assays of infected glioma cells with microglia/macrophages were used to test their impact on oHSV replication. Macrophages from TNFα-knockout mice and blocking antibodies were used to evaluate the biologic effects of TNFα on virus replication. TNFα blocking antibodies were used to evaluate the impact of TNFα on oHSV therapy in vivo. Results: Flow-cytometry analysis revealed a 7.9-fold increase in macrophage infiltration after virus treatment. Tumor-infiltrating macrophages/microglia were polarized toward a M1, proinflammatory phenotype, and they expressed high levels of CD86, MHCII, and Ly6C. Macrophages/microglia produced significant amounts of TNFα in response to infected glioma cells in vitro and in vivo. Using TNFα-blocking antibodies and macrophages derived from TNFα-knockout mice, we discovered TNFα-induced apoptosis in infected tumor cells and inhibited virus replication. Finally, we demonstrated the transient blockade of TNFα from the tumor microenvironment with TNFα-blocking antibodies significantly enhanced virus replication and survival in GBM intracranial tumors. Conclusions: The results of these studies suggest that FDA approved TNFα inhibitors may significantly improve the efficacy of oncolytic virus therapy. Clin Cancer Res; 21(14); 3274–85. ©2015 AACR.

Published
2015

185. Changes in BAI1 and Nestin Expression Are Prognostic Indicators for Survival and Metastases in Breast Cancer and Provide Opportunities for Dual Targeted Therapies

Author

Kimerly A. Powell, Samuel Dubin, Balveen Kaur, Norman L. Lehman, Michael C. Ostrowski, Alena Cristina Jaime-Ramirez, J. Bradley Elder, Arnab Chakravarti, Steven T. Sizemore, Walter Hans Meisen, Haritha Mathsyaraja, Katie A. Thies, and Peter Boyer

Subjects
Cancer Research, Breast Neoplasms, Disease, Article, Receptors, G-Protein-Coupled, Nestin, Mice, Immune system, Breast cancer, Cell Line, Tumor, Chlorocebus aethiops, Biomarkers, Tumor, medicine, Animals, Humans, Angiogenic Proteins, Neoplasm Metastasis, Intermediate filament, Vero Cells, Survival rate, Oncolytic Virotherapy, business.industry, Prognosis, medicine.disease, Oncolytic virus, Angiogenesis inhibitor, Gene Expression Regulation, Neoplastic, Oncolytic Viruses, Oncology, Immunology, MCF-7 Cells, Cancer research, Female, business
Abstract

The 2-year survival rate of patients with breast cancer brain metastases is less than 2%. Treatment options for breast cancer brain metastases are limited, and there is an unmet need to identify novel therapies for this disease. Brain angiogenesis inhibitor 1 (BAI1) is a GPCR involved in tumor angiogenesis, invasion, phagocytosis, and synaptogenesis. For the first time, we identify that BAI1 expression is significantly reduced in breast cancer and higher expression is associated with better patient survival. Nestin is an intermediate filament whose expression is upregulated in several cancers. We found that higher Nestin expression significantly correlated with breast cancer lung and brain metastases, suggesting both BAI1 and Nestin can be therapeutic targets for this disease. Here, we demonstrate the ability of an oncolytic virus, 34.5ENVE, to target and kill high Nestin-expressing cells and deliver Vstat120 (extracellular fragment of BAI1). Finally, we created two orthotopic immune-competent murine models of breast cancer brain metastases and demonstrated 34.5ENVE extended the survival of immune-competent mice bearing intracranial breast cancer tumors. Mol Cancer Ther; 14(1); 307–14. ©2014 AACR.

Published
2015

186. Use of miRNA Response Sequences to Block Off-target Replication and Increase the Safety of an Unattenuated, Glioblastoma-targeted Oncolytic HSV

Author

Michael A. Caligiuri, Justus B. Cohen, Hiroaki Uchida, Balveen Kaur, Yoshitaka Miyagawa, Joseph C. Glorioso, Timothy P. Cripe, Lucia Mazzacurati, Nduka Amankulor, Bonnie Reinhart, Aofei Li, Paola Grandi, Marco Marzulli, Nino Chiocca, and William F. Goins

Subjects
Pharmacology, HEK 293 cells, Biology, Virology, Immediate early protein, Virus, Oncolytic virus, Viral replication, Lytic cycle, Drug Discovery, microRNA, Genetics, Molecular Medicine, Original Article, Vector (molecular biology), Molecular Biology
Abstract

Glioblastoma multiforme (GBM) is an aggressive brain cancer for which there is no effective treatment. Oncolytic HSV vectors (oHSVs) are attenuated lytic viruses that have shown promise in the treatment of human GBM models in animals, but their efficacy in early phase patient trials has been limited. Instead of attenuating the virus with mutations in virulence genes, we engineered four copies of the recognition sequence for miR-124 into the 3′UTR of the essential ICP4 gene to protect healthy tissue against lytic virus replication; miR-124 is expressed in neurons but not in glioblastoma cells. Following intracranial inoculation into nude mice, the miR-124-sensitive vector failed to replicate or show overt signs of pathogenesis. To address the concern that this safety feature may reduce oncolytic activity, we inserted the miR-124 response elements into an unattenuated, human receptor (EGFR/EGFRvIII)-specific HSV vector. We found that miR-124 sensitivity did not cause a loss of treatment efficiency in an orthotopic model of primary human GBM in nude mice. These results demonstrate that engineered miR-124 responsiveness can eliminate off-target replication by unattenuated oHSV without compromising oncolytic activity, thereby providing increased safety.

Published
2015

187. Doxorubicin Synergizes with 34.5ENVE to Enhance Antitumor Efficacy against Metastatic Ovarian Cancer

Author

Pin-Yi Wang, Jianying Zhang, Kellie S. Rath, Timothy P. Cripe, Ji Young Yoo, Balveen Kaur, Karuppaiyah Selvendiran, Uksha Saini, and Chelsea Bolyard

Subjects
Cancer Research, Cell Survival, Receptor expression, Genetic Vectors, Population, Biology, Virus Replication, Article, Nestin, Mice, Ovarian tumor, Cytopathogenic Effect, Viral, Cell Line, Tumor, Gene Order, medicine, Animals, Humans, Cytotoxic T cell, Doxorubicin, Viability assay, Neoplasm Metastasis, education, Caspase 7, Oncolytic Virotherapy, Ovarian Neoplasms, education.field_of_study, Antibiotics, Antineoplastic, Caspase 3, Ascites, Drug Synergism, medicine.disease, Xenograft Model Antitumor Assays, Tumor Burden, Oncolytic virus, Disease Models, Animal, Oncolytic Viruses, Oncology, Cancer research, Female, Ovarian cancer, medicine.drug
Abstract

Purpose: Novel therapeutic regimens are needed to improve dismal outcomes associated with late-stage ovarian cancer. Oncolytic viruses are currently being tested in patients with ovarian cancer. Here, we tested the therapeutic efficacy of combining doxorubicin with 34.5ENVE, an oncolytic herpes simplex virus transcriptionally driven by a modified stem cell–specific nestin promoter, and encoding for antiangiogenic Vasculostatin-120 (VStat120) for use against progressive ovarian cancer. Experimental Design: Antitumor efficacy of 34.5ENVE was assessed in ovarian cancer cell lines, mouse ascites–derived tumor cells, and primary patient ascites–derived tumor cells by standard MTT assay. The ability of conditioned medium derived from 34.5ENVE-infected ovarian cancer cells to inhibit endothelial cell migration was measured by a Transwell chamber assay. Scope of cytotoxic interactions between 34.5ENVE and doxorubicin were evaluated using Chou–Talalay synergy analysis. Viral replication, herpes simplex virus receptor expression, and apoptosis were evaluated. Efficacy of oncolytic viral therapy in combination with doxorubicin was evaluated in vivo in the murine xenograft model of human ovarian cancer. Results: Treatment with 34.5ENVE reduced cell viability of ovarian cancer cell lines, and mouse ascites–derived and patient ascites–derived ovarian tumor cells. Conditioned media from tumor cells infected with 34.5ENVE reduced endothelial cell migration. When combined with doxorubicin, 34.5ENVE killed synergistically with a significant increase in caspase-3/7 activation, and an increase in sub-G1 population of cells. The combination of doxorubicin and 34.5ENVE significantly prolonged survival in nude mice bearing intraperitoneal ovarian cancer tumors. Conclusions: This study indicates significant antitumor efficacy of 34.5ENVE alone, and in combination with doxorubicin against disseminated peritoneal ovarian cancer. Clin Cancer Res; 20(24); 6479–94. ©2014 AACR.

Published
2014

188. EXTH-83. TARGETING DNA REPAIR AND SURVIVAL PATHWAYS THROUGH HEAT SHOCK PROTEIN INHIBITION USING AT13387 TO SENSITIZE GLIOMA TO CHEMORADIATION THERAPY

Author

Balveen Kaur, Nadella, Christine E. Beattie, Deepa Sampath, Lai T, Alessandra M. Welker, Naduparambil K. Jacob, Jun Xu, Jaclyn Wu, Timmers C, Alessandro Canella, and Puduvalli

Subjects
Oncology, Cancer Research, medicine.medical_specialty, business.industry, DNA repair, medicine.disease, Survival pathways, Abstracts, Text mining, Internal medicine, Glioma, Heat shock protein, medicine, Cancer research, Neurology (clinical), business
Published
2017

189. Humanized Chondroitinase ABC Sensitizes Glioblastoma Cells to Temozolomide

Author

Alena Cristina Jaime-Ramirez, Nina Dmitrieva, Jeffrey Wojton, Ji Young Yoo, Balveen Kaur, Yeshavanth Kumar Banasavadi-Siddegowda, Theresa Relation, Jianying Zhang, and Chelsea Bolyard

Subjects
0301 basic medicine, Gene Expression, Apoptosis, Herpesvirus 1, Human, Pharmacology, Chondroitin ABC Lyase, chemistry.chemical_compound, Mice, 0302 clinical medicine, Transduction, Genetic, Drug Discovery, Chlorocebus aethiops, Tumor Cells, Cultured, Genetics (clinical), Oncolytic Virotherapy, Tumor Burden, Dacarbazine, Treatment Outcome, 030220 oncology & carcinogenesis, Molecular Medicine, medicine.drug, Cell Survival, Genetic Vectors, Gene delivery, Article, 03 medical and health sciences, Glioma, Neurosphere, Cell Line, Tumor, Genetics, medicine, Temozolomide, Animals, Humans, Chondroitin sulfate, Molecular Biology, Protein kinase B, Antineoplastic Agents, Alkylating, Vero Cells, Alleles, medicine.disease, Xenograft Model Antitumor Assays, In vitro, Oncolytic virus, Enzyme Activation, Disease Models, Animal, 030104 developmental biology, chemistry, Amino Acid Substitution, Drug Resistance, Neoplasm, Mutation, Cancer research, Glioblastoma
Abstract

BACKGROUND Malignant gliomas (glioblastomas; GBMs) are extremely aggressive and have a median survival of approximately 15 months. Current treatment modalities, which include surgical resection, radiation and chemotherapy, have done little to prolong the lives of GBM patients. Chondroitin sulfate proteoglycans (CSPG) are critical for cell-cell and cell-extracellular matrix (ECM) interactions and are implicated in glioma growth and invasion. Chondroitinase (Chase) ABC is a bacterial enzyme that cleaves chondroitin sulfate disaccharide chains from CSPGs in the tumor ECM. Wild-type Chase ABC has limited stability and/or activity in mammalian cells; therefore, we created a mutant humanized version (Chase M) with enhanced function in mammalian cells. METHODS We hypothesized that disruption of cell-cell and cell-ECM interactions by ChaseM and temozolomide (TMZ) will enhance the chemotherapeutic availability and sensitivity of glioma cells. RESULTS Utilizing primary patient-derived neurospheres, we found that ChaseM decreases glioma neurosphere aggregation in vitro. Furthermore, an oncolytic HSV-1 virus expressing secreted ChaseM (OV-ChaseM) enhanced viral spread and glioma cell killing compared to OV-Control, in vitro. OV-ChaseM plus TMZ combinatorial treatment resulted in a significant synergistic enhancement of glioma cell killing accompanied by an increase in apoptotic cell death. Intracellular flow cytometric analysis revealed a significant reduction in the phosphorylation of the pro-survival AKT protein following OV-ChaseM plus TMZ treatment. Lastly, in nude mice bearing intracranial GBM30 glioma xenografts, intratumoral OV-ChaseM plus TMZ (10 mg/kg by oral gavage) combination therapy resulted in a significant (p

Published
2017

190. Reolysin and Histone Deacetylase Inhibition in the Treatment of Head and Neck Squamous Cell Carcinoma

Author

Quintin Pan, John H. Lee, Alena Cristina Jaime-Ramirez, Theodoros N. Teknos, Bhavna Kumar, Enrico Caserta, Flavia Pichiorri, Robert A. Baiocchi, Jianying Zhang, Tae Jin Lee, Pawan Kumar, Jun Ge Yu, Ji Young Yoo, Craig C. Hofmeister, Balveen Kaur, and Matthew O. Old

Subjects
0301 basic medicine, Cancer Research, Combination therapy, Cell, oncolytics, Biology, reovirus, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, Reolysin, medicine, Pharmacology (medical), Vorinostat, Head and neck cancer, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, Head and neck squamous-cell carcinoma, Virology, immune impact, 3. Good health, Oncolytic virus, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Cancer research, Molecular Medicine, Original Article, head and neck cancer, Histone deacetylase, medicine.drug
Abstract

Oncolytic viruses (OVs) are emerging as powerful anti-cancer agents and are currently being tested for their safety and efficacy in patients. Reovirus (Reolysin), a naturally occurring non-pathogenic, double-stranded RNA virus, has natural oncolytic activity and is being tested in phase I–III clinical trials in a variety of tumor types. With its recent US Food and Drug Administration (FDA) orphan drug designation for several tumor types, Reolysin is a potential therapeutic agent for various cancers, including head and neck squamous cell carcinomas (HNSCCs), which have a 5-year survival of ∼55%. Histone deacetylase inhibitors (HDACis) comprise a structurally diverse class of compounds with targeted anti-cancer effects. The first FDA-approved HDACi, vorinostat (suberoylanilide hydroxamic acid [SAHA]), is currently being tested in patients with head and neck cancer. Recent findings indicate that HDAC inhibition in myeloma cells results in the upregulation of the Reolysin entry receptor, junctional adhesion molecule 1 (JAM-1), facilitating reovirus infection and tumor cell killing both in vitro and in vivo. In this study, we tested the anti-tumor efficacy of HDAC inhibitors AR-42 or SAHA in conjunction with Reolysin in HNSCCs. While HDAC inhibition increased JAM-1 and reovirus entry, the impact of this combination therapy was tested on the development of anti-tumor immune responses.

Published
2017

191. Role of Cysteine-rich 61 Protein (CCN1) in Macrophage-mediated Oncolytic Herpes Simplex Virus Clearance

Author

Amy Haseley Thorne, Luke Russell, Justin D. Lathia, Chelsea Bolyard, Ji Young Yoo, Jianhua Yu, Walter Hans Meisen, Jeremy N. Rich, Balveen Kaur, Hsiaoyin Mao, Vinay K. Puduvalli, Michael A. Caligiuri, and Susheela Tridandapani

Subjects
Genetic Vectors, Herpesvirus 1, Human, medicine.disease_cause, Virus, Proinflammatory cytokine, Mice, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Drug Discovery, Genetics, medicine, Animals, Humans, Macrophage, Molecular Biology, Chemokine CCL2, 030304 developmental biology, Pharmacology, 0303 health sciences, biology, Macrophages, Antibodies, Monoclonal, Macrophage Activation, Virology, 3. Good health, Oncolytic virus, Oncolytic Viruses, Herpes simplex virus, Viral replication, Cell culture, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Molecular Medicine, Female, Original Article, Antibody, Glioblastoma, Neoplasm Transplantation, Cysteine-Rich Protein 61
Abstract

Glioblastoma is a devastating disease, and there is an urgent need to develop novel therapies, such as oncolytic HSV1 (OV) to effectively target tumor cells. OV therapy depends on tumor-specific replication leading to destruction of neoplastic tissues. Host responses that curtail virus replication limit its efficacy in vivo. We have previously shown that cysteine-rich 61 protein (CCN1) activates a type 1 IFN antiviral defense response in glioblastoma cells. Incorporating TCGA data, we found CCN1 expression to be a negative prognostic factor for glioblastoma patients. Based on this, we used neutralizing antibodies against CCN1 to investigate its effect on OV therapy. Use of an anti-CCN1 antibody in mice bearing glioblastomas treated with OV led to enhanced virus expression along with reduced immune cell infiltration. OV-induced CCN1 increases macrophage migration toward infected glioblastoma cells by directly binding macrophages and also by enhancing the proinflammatory activation of macrophages inducing MCP-1 expression in glioblastoma cells. Activation of macrophages by CCN1 also increases viral clearance. Neutralization of integrin αMβ2 reversed CCN1-induced macrophage activation and migration, and reduced MCP-1 expression by glioblastoma cells. Our findings reveal that CCN1 plays a novel role in pathogen clearance; increasing macrophage infiltration and activation resulting in increased virus clearance in tumors.

Published
2014

192. Piperlongumine treatment inactivates peroxiredoxin 4, exacerbates endoplasmic reticulum stress, and preferentially kills high-grade glioma cells

Author

Tae Hyong Kim, Arav Krishnavadan Parikh, Ichiro Nakano, Xiaokui Mo, Sung Hak Kim, Jianhua Yu, Chang-Hyuk Kwon, Balveen Kaur, Jieun Song, Sung Ok Yoon, and Kamalakannan Palanichamy

Subjects
Cancer Research, Databases, Factual, Antineoplastic Agents, Apoptosis, Biology, Mice, chemistry.chemical_compound, Tumor Cells, Cultured, Animals, Humans, Piperlongumine, Brain Neoplasms, Cell growth, Endoplasmic reticulum, Dioxolanes, Glioma, Peroxiredoxins, Endoplasmic Reticulum Stress, Survival Analysis, Neural stem cell, Cell biology, Oncology, chemistry, Basic and Translational Investigations, Unfolded protein response, Neurology (clinical), Signal transduction, Reactive Oxygen Species, Intracellular
Abstract

Piperlongumine, a natural plant product, kills multiple cancer types with little effect on normal cells. Piperlongumine raises intracellular levels of reactive oxygen species (ROS), a phenomenon that may underlie the cancer-cell killing. Although these findings suggest that piperlongumine could be useful for treating cancers, the mechanism by which the drug selectively kills cancer cells remains unknown.We treated multiple high-grade glioma (HGG) sphere cultures with piperlongumine and assessed its effects on ROS and cell-growth levels as well as changes in downstream signaling. We also examined the levels of putative piperlongumine targets and their roles in HGG cell growth.Piperlongumine treatment increased ROS levels and preferentially killed HGG cells with little effect in normal brain cells. Piperlongumine reportedly increases ROS levels after interactions with several redox regulators. We found that HGG cells expressed higher levels of the putative piperlongumine targets than did normal neural stem cells (NSCs). Furthermore, piperlongumine treatment in HGG cells, but not in normal NSCs, increased oxidative inactivation of peroxiredoxin 4 (PRDX4), an ROS-reducing enzyme that is overexpressed in HGGs and facilitates proper protein folding in the endoplasmic reticulum (ER). Moreover, piperlongumine exacerbated intracellular ER stress, an effect that was mimicked by suppressing PRDX4 expression.Our results reveal that the mechanism by which piperlongumine preferentially kills HGG cells involves PRDX4 inactivation, thereby inducing ER stress. Therefore, piperlongumine treatment could be considered as a novel therapeutic option for HGG treatment.

Published
2014

193. EXTH-05. MicroRNA-138 SUPPRESSES GLIOBLASTOMA PROLIFERATION AND SENSITIZES CHEMOTHERAPY THROUGH FOCAL ADHESION KINASE INACTIVATION

Author

Margaret Yeh, Tae Jin Lee, Balveen Kaur, and Ji Young Yoo

Subjects
Cancer Research, Chemotherapy, Chemistry, medicine.medical_treatment, medicine.disease, Focal adhesion, Abstracts, Oncology, microRNA, Cancer research, medicine, Neurology (clinical), neoplasms, Glioblastoma
Abstract

Glioblastoma is one of the most deadly cancers and limited to only a few therapeutic options that are available in clinical settings, mainly due to the resistance to many chemotherapies. MicroRNAs are increasingly implicated in the tumor survival from chemotherapies, which may lead to a better therapeutic option by overcoming the resistance. Here, we found that miR-138 is significantly downregulated in human glioblastoma patient tissues compared to normal brain tissues. MiR-138 has been known to play as a tumor suppressor in many types of cancer, which may imply that miR-138 can benefit in the development of anti-glioblastoma therapy. Global proteomic analysis revealed that ectopic expression of miR-138 in patient derived glioblastoma primary cells suppressed FAK pathway, which has been known to be highly activated in many cancers including glioblastoma. FAK inactivation by miR-138 resulted inhibition of glioblastoma cell proliferation in vitro and improved tumor free survival in vivo. We also found that miR-138 induced FAK inhibition sensitizes glioblastoma cells to tyrosine kinase inhibitors, such as Imatinib. The studies are indicative of the clinical benefit of miR-138 based therapy of primary and even recurrent glioblastoma.

Published
2018

194. CSIG-23. NOTCH ACTIVATION INDUCED BY HSV-1 ENCODED miRNA-H16 SENSITIZES oHSV-TREATED TUMORS TO NOTCH INHIBITOR

Author

Ji Young Yoo, Jianhua Yu, Alena Cristina Jaime-Ramirez, Balveen Kaur, Joseph C. Glorioso, Brian Hurwitz, Tae Jin Lee, Yuanqing Yan, Hongsheng Dai, Joseph Liu, Michael A. Caligiuri, Samantha Chao, and Yoshihiro Otani

Subjects
Cancer Research, Oncology, microRNA, Cell Signaling and Signaling Pathways, Cancer research, Neurology (clinical)
Abstract

INTRODUCTION Glioblastomas (GBMs) are resistant to traditional therapies, and new treatment is urgently needed. NOTCH signaling is highly activated in glioma and activated NOTCH signaling is associated with increased tumor growth and therapeutic resistance. Effect of oncolytic virus therapy on NOTCH signaling activation has not been reported to our knowledge. METHODS Western blotting, real time Q-PCR, reporter assay, and bioluminescence mice imaging were used to evaluate oHSV-mediated activation of NOTCH signaling. High throughput analysis of HSV-1-encoded microRNAs and genes were performed to identify the activator of NOTCH signaling, and in silico analysis, 3’ untranslated region (3’UTR) assay, and immunoprecipitation were used to uncover the down-stream signaling. Anti-tumor efficacy of NOTCH inhibitor, gamma-secretase inhibitor (GSI) combined with oHSV was evaluated using intracranial glioma-bearing mouse xenografts. RESULTS oHSV infection induced NOTCH activity in glioma PDX cells. High throughput analysis uncovered this to be due to HSV-1-encoded miR-H16 (miR-H16). 3’UTR analysis of Factor Inhibiting HIF-1 (FIH-1) indicated miR-H16 directly target FIH-1 and repress its protein expression. Immunoprecipitation analysis also uncovered that FIH-1 reduction liberated Mild bomb 1 (Mib1) from FIH-1 mediated sequestration, permitting it to activate NOTCH signaling by ubiquitination of NOTCH ligands. Forced expression of either antago-miR-H16 or FIH-1 attenuated the oHSV-induced NOTCH activation. Furthermore, oHSV therapy-induced activation of NOTCH signaling sensitized tumors to GSI, resulting in significantly improved therapeutic response to oHSV therapy and prolonged the survival in several intracranial GBM xenografts. CONCLUSION In this study, we identified the mechanism of oHSV therapy-mediated activation of NOTCH signaling, and showed the therapeutic benefit of combining oHSV with GSI.

Published
2019

195. BSCI-11. STROMAL PLATELET DERIVED GROWTH FACTOR RECEPTOR-β (PDGFRβ) PROMOTES BREAST CANCER BRAIN METASTASIS

Author

Arnab Chakravarti, Gustavo Leone, Maria C. Cuitiño, Manjusri Das, Gina M. Sizemore, Steven T. Sizemore, Raleigh D. Kladney, Luke Russell, Zaibo Li, Michael C. Ostrowski, Lynn Schoenfield, Anisha M. Hammer, Sarah A. Steck, Jose Otero, Robert Pilarski, Christopher Koivisto, Balveen Kaur, Matthew D. Ringel, Anthony J. Trimboli, Chelsea Bolyard, Blake E. Hildreth, and Katie A. Thies

Subjects
Platelet-derived growth factor, Tissue microarray, Stromal cell, biology, Receptor Protein-Tyrosine Kinases, Epithelium, Abstracts, chemistry.chemical_compound, medicine.anatomical_structure, Basic Science, chemistry, Proto-Oncogene Proteins c-sis, Cancer research, biology.protein, medicine, Signal transduction, Platelet-derived growth factor receptor
Abstract

Stromal platelet-derived growth factor receptor-beta (PDGFRβ) has emerged as an actionable mediator of breast tumor-stromal communication. As a receptor tyrosine kinase, PDGFRβ is activated by its ligand, PDGFB, which is released by neighboring tumor epithelium and endothelium. However, how PDGF signaling mediates breast cancer (BC) initiation, progression, and metastasis remains unclear. To evaluate PDGFRβ in this disease, we developed a mouse model of stromal-specific PDGFRβ activation using the Fsp-cre transgene previously published by our group. Mesenchymal-specific activation of PDGFRβ promotes preferential experimental brain metastasis of PDGFB-expressing mammary tumor cells when injected intravenously and accelerates intracranial tumor growth of these cells. Mammary tumor cells expressing low levels of PDGFB do not exhibit a similar increase in brain metastases in PDGFRβ mutant mice. To our knowledge, this is the first example where genetic manipulation of the stroma leads to an increased incidence of BCBM. Our pre-clinical data suggests that primary breast tumors that express high PDGFB could preferentially metastasize to the brain. To test this in patients, we analyzed PDGFB protein expression in a tissue microarray comprised of HER2-positive and triple negative BC primary tumors. While high PDGFB did not correlate with site-independent metastatic recurrence, it was prognostic of brain metastasis, mirroring our mouse data. Our findings suggest that high primary tumor PDGFB expression defines a subset of BC patients predisposed to brain metastases. These patients may benefit from therapeutic intervention of PDGFRβ signaling. To test this pre-clinically, we treated mice harboring intracranial tumors with the PDGFR-specific inhibitor, crenolanib. Excitingly, crenolanib treatment significantly inhibited the brain tumor burden in these mice. Combined, our findings (1) advocate that primary tumor expression of PDGFB is a novel prognostic biomarker for the development of BCBM and (2) support clinical trial evaluation of PDGFR inhibitors for the prevention and treatment of BCBM.

Published
2019

196. Abstract 5215: Targeting of HOX-PBX binding in glioblastoma multiforme as a novel therapeutic treatment

Author

Richard Morgan, Monika Primon, Steven Shnyder, Susan Short, Balveen Kaur, Bangxing Hong, Izhar Bagwan, William Rogers, and Hardev S. Pandha

Subjects
Cancer Research, Oncology
Abstract

The HOX genes encode a family of transcription factors that play an essential role in embryonic patterning. They are also aberrantly expressed in numerous cancers, including glioblastoma (GBM). Three Amino Acid Loop Extension Homeobox (TALE) proteins act as important co-factors for HOX proteins, modulating their binding affinities to genomic targets. TALE proteins include the Pre-B-cell leukemia homeobox (PBX) proteins 1-4, which bind anterior HOX proteins, facilitating their nuclear entry and limiting their degradation. HTL00-1 is a 2nd generation hexapeptide drug that inhibits HOX-PBX dimer formation, and has been shown to induce rapid apoptosis in cancer cells, but not normal cells, through the rapid upregulation of genes including cFos, DUSP1, and EGR1. We have found that both HOX and TALE genes are markedly dysregulated in primary GBM tumors as well as in murine (GL261), adult (LN18, U87-MG, U251-MG) and pediatric (KNS42, SF188) GBM cell lines, all of which are sensitive to HTL-001. These genes were even more highly expressed in experimentally induced GBM cancer stem cells (CSCs) compared with parental lines, with a corresponding increase in sensitivity to HTL-001. We also investigated the in vivo activity of HTL-001 in Black 6 mice carrying GL-261 subcutaneous and orthotropic tumors with twice weekly intraperitoneal delivery. HTL-001 was shown to cross the blood brain barrier using Alexa660 labelled peptide, and significant anti-tumor activity was observed in both subcutaneous and orthotropic models with increased survival (p Citation Format: Richard Morgan, Monika Primon, Steven Shnyder, Susan Short, Balveen Kaur, Bangxing Hong, Izhar Bagwan, William Rogers, Hardev S. Pandha. Targeting of HOX-PBX binding in glioblastoma multiforme as a novel therapeutic treatment [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 5215.

Published
2019

197. Systemic Delivery of SapC-DOPS Has Antiangiogenic and Antitumor Effects Against Glioblastoma

Author

Sherry Thornton, Balveen Kaur, Haritha Mathsyaraja, Zhengtao Chu, Tristan Bourdeau, Mary B. Palascak, Nicholas L Denton, Michael C. Ostrowski, Chang-Hyuk Kwon, Jeffrey Wojton, Lionel M.L. Chow, Walter Hans Meisen, Robert S. Franco, and Xiaoyang Qi

Subjects
Male, Cell, Brain tumor, Neovascularization, Physiologic, Angiogenesis Inhibitors, Antineoplastic Agents, Phosphatidylserines, Pharmacology, Biology, Blood–brain barrier, Saposins, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, In vivo, Cell Line, Tumor, Drug Discovery, Genetics, medicine, Animals, Humans, Molecular Biology, 030304 developmental biology, 0303 health sciences, Brain Neoplasms, Cell Membrane, Phosphatidylserine, medicine.disease, Xenograft Model Antitumor Assays, Cell Hypoxia, Recombinant Proteins, In vitro, 3. Good health, Disease Models, Animal, medicine.anatomical_structure, chemistry, Blood-Brain Barrier, Cell culture, 030220 oncology & carcinogenesis, Cancer cell, Nanoparticles, Molecular Medicine, Female, Original Article, Glioblastoma
Abstract

Saposin C-dioleoylphosphatidylserine (SapC-DOPS) nanovesicles are a nanotherapeutic which effectively target and destroy cancer cells. Here, we explore the systemic use of SapC-DOPS in several models of brain cancer, including glioblastoma multiforme (GBM), and the molecular mechanism behind its tumor-selective targeting specificity. Using two validated spontaneous brain tumor models, we demonstrate the ability of SapC-DOPS to selectively and effectively cross the blood–brain tumor barrier (BBTB) to target brain tumors in vivo and reveal the targeting to be contingent on the exposure of the anionic phospholipid phosphatidylserine (PtdSer). Increased cell surface expression of PtdSer levels was found to correlate with SapC-DOPS–induced killing efficacy, and tumor targeting in vivo was inhibited by blocking PtdSer exposed on cells. Apart from cancer cell killing, SapC-DOPS also exerted a strong antiangiogenic activity in vitro and in vivo. Interestingly, unlike traditional chemotherapy, hypoxic cells were sensitized to SapC-DOPS–mediated killing. This study emphasizes the importance of PtdSer exposure for SapC-DOPS targeting and supports the further development of SapC-DOPS as a novel antitumor and antiangiogenic agent for brain tumors.

Published
2013

198. The integrin inhibitor cilengitide enhances the anti-glioma efficacy of vasculostatin-expressing oncolytic virus

Author

Manabu Onishi, Kazuhiko Kurozumi, Ennio Antonio Chiocca, Joji Ishida, Tomotsugu Ichikawa, Balveen Kaur, Yosuke Shimazu, K. Fujii, and Isao Date

Subjects
Cancer Research, Combination therapy, Angiogenesis, Integrin, Mice, Nude, Cilengitide, Pharmacology, Article, Receptors, G-Protein-Coupled, Mice, chemistry.chemical_compound, Cell Movement, In vivo, Cell Line, Tumor, glioma, Glioma, Chlorocebus aethiops, Animals, Humans, Medicine, Angiogenic Proteins, Vero Cells, Molecular Biology, Oncolytic Virotherapy, Tube formation, Mice, Inbred BALB C, biology, Brain Neoplasms, business.industry, oncolytic viral therapy, medicine.disease, Combined Modality Therapy, Immunohistochemistry, Xenograft Model Antitumor Assays, Peptide Fragments, Oncolytic virus, Oncolytic Viruses, chemistry, cilengitide, biology.protein, Molecular Medicine, business, Snake Venoms
Abstract

Oncolytic viral (OV) therapy has been considered as a promising treatment modality for brain tumors. Vasculostatin, the fragment of brain-specific angiogenesis inhibitor-1, shows anti-angiogenic activity against malignant gliomas. Previously, a vasculostatin-expressing oncolytic herpes simplex virus-1, Rapid Antiangiogenesis Mediated By Oncolytic virus (RAMBO), was reported to have a potent antitumor effect. Here, we investigated the therapeutic efficacy of RAMBO and cilengitide, an integrin inhibitor, combination therapy for malignant glioma. In vitro, tube formation was significantly decreased in RAMBO and cilengitide combination treatment compared with RAMBO or cilengitide monotherapy. Moreover, combination treatment induced a synergistic suppressive effect on endothelial cell migration compared with the control virus. RAMBO, combined with cilengitide, induced synergistic cytotoxicity on glioma cells. In the caspase-8 and -9 assays, the relative absorption of U87 Delta EGFR cell clusters treated with cilengitide and with RAMBO was significantly higher than that of those treated with control. In addition, the activity of caspase 3/7 was significantly increased with combination therapy. In vivo, there was a significant increase in the survival of mice treated with combination therapy compared with RAMBO or cilengitide monotherapy. These results indicate that cilengitide enhanced vasculostatin-expressing OV therapy for malignant glioma and provide a rationale for designing future clinical trials combining these two agents.

Published
2013

199. VEGF Blockade Enables Oncolytic Cancer Virotherapy in Part by Modulating Intratumoral Myeloid Cells

Author

David A. Hildeman, Francis Eshun, Keri A. Streby, Margaret H. Collins, Timothy P. Cripe, Louis Boon, William F. Goins, Jason S. Frischer, Amy Haseley, Allyson Sholl, Pin Yi Wang, Senad Divanovic, Brett W. Hendrickson, Mark A. Currier, Artur Chernoguz, Balveen Kaur, Jennifer L. Leddon, Rolf A. Brekken, Kelly M. Crawford, and William H. Baird

Subjects
Vascular Endothelial Growth Factor A, Myeloid, Angiogenesis, Cell Culture Techniques, Virus Replication, medicine.disease_cause, Mice, chemistry.chemical_compound, 0302 clinical medicine, Neoplasms, Drug Discovery, Simplexvirus, Myeloid Cells, Cytotoxicity, Oncolytic Virotherapy, 0303 health sciences, CD11b Antigen, Neovascularization, Pathologic, Sarcoma, 3. Good health, Bevacizumab, Vascular endothelial growth factor, Oncolytic Viruses, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Molecular Medicine, Female, Original Article, Genetic Vectors, Biology, Antibodies, Monoclonal, Humanized, Virus, 03 medical and health sciences, Cell Line, Tumor, medicine, Genetics, Animals, Humans, Virotherapy, Molecular Biology, 030304 developmental biology, Pharmacology, Macrophages, Xenograft Model Antitumor Assays, Oncolytic virus, Disease Models, Animal, Herpes simplex virus, chemistry, Immunology, Cancer research, Stromal Cells
Abstract

Understanding the host response to oncolytic viruses is important to maximize their antitumor efficacy. Despite robust cytotoxicity and high virus production of an oncolytic herpes simplex virus (oHSV) in cultured human sarcoma cells, intratumoral (ITu) virus injection resulted in only mild antitumor effects in some xenograft models, prompting us to characterize the host inflammatory response. Virotherapy induced an acute neutrophilic infiltrate, a relative decrease of ITu macrophages, and a myeloid cell-dependent upregulation of host-derived vascular endothelial growth factor (VEGF). Anti-VEGF antibodies, bevacizumab and r84, the latter of which binds VEGF and selectively inhibits binding to VEGF receptor-2 (VEGFR2) but not VEGFR1, enhanced the antitumor effects of virotherapy, in part due to decreased angiogenesis but not increased virus production. Neither antibody affected neutrophilic infiltration but both partially mitigated virus-induced depletion of macrophages. Enhancement of virotherapy-mediated antitumor effects by anti-VEGF antibodies could largely be recapitulated by systemic depletion of CD11b(+) cells. These data suggest the combined effect of oHSV virotherapy and anti-VEGF antibodies is in part due to modulation of a host inflammatory reaction to virus. Our data provide strong preclinical support for combined oHSV and anti-VEGF antibody therapy and suggest that understanding and counteracting the innate host response may help enable the full antitumor potential of oncolytic virotherapy.

Published
2013
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200. BAI1 Orchestrates Macrophage Inflammatory Response to HSV Infection-Implications for Oncolytic Viral Therapy

Author

Balveen Kaur, Christopher Alvarez-Breckenridge, Jianying Zhang, W. Hans Meisen, Jeffrey Wojton, Eric S. Wohleb, Matthew O. Old, Jonathan C. Smith, Michael A. Caligiuri, Samuel Dubin, Erwin G. Van Meir, Yeshavanth Kumar Banasavadi-Siddegowda, Jun Ge Yu, Ji Young Yoo, Maninder Khosla, Bo Xu, Jianhua Yu, Jonathan P. Godbout, Flavia Pichiorri, Dan Zhu, Jayson Hardcastle, Pete Pow-anpongkul, and Chelsea Bolyard

Subjects
0301 basic medicine, Cancer Research, medicine.medical_treatment, Phagocytosis, Inflammation, Biology, medicine.disease_cause, Virus, Article, Receptors, G-Protein-Coupled, 03 medical and health sciences, Mice, Cell Line, Tumor, medicine, Animals, Humans, Simplexvirus, Angiogenic Proteins, Oncolytic Virotherapy, Microglia, Macrophages, Brain, Glioma, Xenograft Model Antitumor Assays, Oncolytic virus, Oncolytic Viruses, 030104 developmental biology, medicine.anatomical_structure, Cytokine, Herpes simplex virus, Oncology, Immunology, Tumor necrosis factor alpha, medicine.symptom
Abstract

Purpose: Brain angiogenesis inhibitor (BAI1) facilitates phagocytosis and bacterial pathogen clearance by macrophages; however, its role in viral infections is unknown. Here, we examined the role of BAI1, and its N-terminal cleavage fragment (Vstat120) in antiviral macrophage responses to oncolytic herpes simplex virus (oHSV). Experimental Design: Changes in infiltration and activation of monocytic and microglial cells after treatment of glioma-bearing mice brains with a control (rHSVQ1) or Vstat120-expressing (RAMBO) oHSV was analyzed using flow cytometry. Co-culture of infected glioma cells with macrophages or microglia was used to examine antiviral signaling. Cytokine array gene expression and Ingenuity Pathway Analysis (IPA) helped evaluate changes in macrophage signaling in response to viral infection. TNFα-blocking antibodies and macrophages derived from Bai1−/− mice were used. Results: RAMBO treatment of mice reduced recruitment and activation of macrophages/microglia in mice with brain tumors, and showed increased virus replication compared with rHSVQ1. Cytokine gene expression array revealed that RAMBO significantly altered the macrophage inflammatory response to infected glioma cells via altered secretion of TNFα. Furthermore, we showed that BAI1 mediated macrophage TNFα induction in response to oHSV therapy. Intracranial inoculation of wild-type/RAMBO virus in Bai1−/− or wild-type non–tumor-bearing mice revealed the safety of this approach. Conclusions: We have uncovered a new role for BAI1 in facilitating macrophage anti-viral responses. We show that arming oHSV with antiangiogenic Vstat120 also shields them from inflammatory macrophage antiviral response, without reducing safety. Clin Cancer Res; 23(7); 1809–19. ©2016 AACR.

Published
2016

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