Your search keyword '"Betty Tyler"' showing total 248 results

1. CCR2 and CCR5 co-inhibition modulates immunosuppressive myeloid milieu in glioma and synergizes with anti-PD-1 therapy

Author

Ayush Pant, Brandon Hwa-Lin Bergsneider, Siddhartha Srivastava, Timothy Kim, Aanchal Jain, Sadhana Bom, Pavan Shah, Nivedha Kannapadi, Kisha Patel, John Choi, Kwang Bog Cho, Rohit Verma, Caren Yu-Ju Wu, Henry Brem, Betty Tyler, Drew M. Pardoll, Christina Jackson, and Michael Lim

Subjects

Immunotherapy, MDSC, Glioma, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

ABSTRACTImmunotherapy has revolutionized the treatment of cancers. Reinvigorating lymphocytes with checkpoint blockade has become a cornerstone of immunotherapy for multiple tumor types, but the treatment of glioblastoma has not yet shown clinical efficacy. A major hurdle to treat GBM with checkpoint blockade is the high degree of myeloid-mediated immunosuppression in brain tumors that limits CD8 T-cell activity. A potential strategy to improve anti-tumor efficacy against glioma is to use myeloid-modulating agents to target immunosuppressive cells, such as myeloid-derived suppressor cells (MDSCs) in the tumor microenvironment. We found that the co-inhibition of the chemokine receptors CCR2 and CCR5 in murine model of glioma improves the survival and synergizes robustly with anti-PD-1 therapy. Moreover, the treatment specifically reduced the infiltration of monocytic-MDSCs (M-MDSCs) into brain tumors and increased lymphocyte abundance and cytokine secretion by tumor-infiltrating CD8 T cells. The depletion of T-cell subsets and myeloid cells abrogated the effects of CCR2 and CCR5 blockade, indicating that while broad depletion of myeloid cells does not improve survival, specific reduction in the infiltration of immunosuppressive myeloid cells, such as M-MDSCs, can boost the anti-tumor immune response of lymphocytes. Our study highlights the potential of CCR2/CCR5 co-inhibition in reducing myeloid-mediated immunosuppression in GBM patients.

Published

2024

2. Ultrasound inhibits tumor growth and selectively eliminates malignant brain tumor in vivo

Author

Nitsa Buaron, Antonella Mangraviti, Yuan Wang, Ann Liu, Mariangela Pedone, Eric Sankey, Itay Adar, Abraham Nyska, Riki Goldbart, Tamar Traitel, Henry Brem, Betty Tyler, and Joseph Kost

Subjects

brain tumor, cavitation, glioma, low frequency ultrasound, reactive gliosis, Chemical engineering, TP155-156, Biotechnology, TP248.13-248.65, Therapeutics. Pharmacology, RM1-950

Abstract

Abstract Glioma is one of the most common primary malignant brain tumors. Despite progress in therapeutic approaches, the median survival of patients with glioma remains less than 2 years, generating the need for new therapeutic approaches. Ultrasound (US) is widely used in medical fields and is used as a therapeutic tool mainly for improving the performance of therapeutic entities. In this study, we examined a novel approach using low frequency US (20 kHz) (LFUS) as an independent treatment tool for malignant glioma, since primary studies showed that cancer cells are more susceptible to LFUS than healthy cells. LFUS safety and efficacy were examined in a 9L gliosarcoma‐bearing female Fischer 344 rats. Two LFUS protocols were examined: a one‐time treatment (US1X), and two treatments 24 h apart (US2X). For safety evaluation, rats were monitored for weight change and pain measurements. For efficacy, tumor volume was measured as a function of time and the tumor structural chances were examined histopathologically. LFUS treatment showed rapid inhibition of tumor growth, seen as soon as 12 h after US application. In addition, LFUS was found to affect the tumor structure, which was more extensive (>60% of tumor area) in smaller tumors. In US2X, the tumor tissue was completely destroyed, and an extensive immune response was observed. Importantly, the treatment was highly selective, keeping the healthy tissue surrounding the tumor unharmed. We developed a highly efficient and selective therapeutic protocol for treating malignant glioma with minimal side effects based solely on LFUS.

Published

2024

3. GPR68-ATF4 signaling is a novel prosurvival pathway in glioblastoma activated by acidic extracellular microenvironment

Author

Charles H. Williams, Leif R. Neitzel, Jessica Cornell, Samantha Rea, Ian Mills, Maya S. Silver, Jovanni D. Ahmad, Konstantin G. Birukov, Anna Birukova, Henry Brem, Betty Tyler, Eli E. Bar, and Charles C. Hong

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Glioblastoma multiforme (GBM) stands as a formidable challenge in oncology because of its aggressive nature and severely limited treatment options. Despite decades of research, the survival rates for GBM remain effectively stagnant. A defining hallmark of GBM is a highly acidic tumor microenvironment, which is thought to activate pro-tumorigenic pathways. This acidification is the result of altered tumor metabolism favoring aerobic glycolysis, a phenomenon known as the Warburg effect. Low extracellular pH confers radioresistant tumors to glial cells. Notably GPR68, an acid sensing GPCR, is upregulated in radioresistant GBM. Usage of Lorazepam, which has off target agonism of GPR68, is linked to worse clinical outcomes for a variety of cancers. However, the role of tumor microenvironment acidification in GPR68 activation has not been assessed in cancer. Here we interrogate the role of GPR68 specifically in GBM cells using a novel highly specific small molecule inhibitor of GPR68 named Ogremorphin (OGM) to induce the iron mediated cell death pathway: ferroptosis. Method OGM was identified in a non-biased zebrafish embryonic development screen and validated with Morpholino and CRISPR based approaches. Next, A GPI-anchored pH reporter, pHluorin2, was stably expressed in U87 glioblastoma cells to probe extracellular acidification. Cell survival assays, via nuclei counting and cell titer glo, were used to demonstrate sensitivity to GPR68 inhibition in twelve immortalized and PDX GBM lines. To determine GPR68 inhibition’s mechanism of cell death we use DAVID pathway analysis of RNAseq. Our major indication, ferroptosis, was then confirmed by western blotting and qRT-PCR of reporter genes including TFRC. This finding was further validated by transmission electron microscopy and liperfluo staining to assess lipid peroxidation. Lastly, we use siRNA and CRISPRi to demonstrate the critical role of ATF4 suppression via GPR68 for GBM survival. Results We used a pHLourin2 probe to demonstrate how glioblastoma cells acidify their microenvironment to activate the commonly over expressed acid sensing GPCR, GPR68. Using our small molecule inhibitor OGM and genetic means, we show that blocking GPR68 signaling results in robust cell death in all thirteen glioblastoma cell lines tested, irrespective of genetic and phenotypic heterogeneity, or resistance to the mainstay GBM chemotherapeutic temozolomide. We use U87 and U138 glioblastoma cell lines to show how selective induction of ferroptosis occurs in an ATF4-dependent manner. Importantly, OGM was not-acutely toxic to zebrafish and its inhibitory effects were found to spare non-malignant neural cells. Conclusion These results indicate GPR68 emerges as a critical sensor for an autocrine pro-tumorigenic signaling cascade triggered by extracellular acidification in glioblastoma cells. In this context, GPR68 suppresses ATF4, inhibition of GPR68 increases expression of ATF4 which leads to ferroptotic cell death. These findings provide a promising therapeutic approach to selectively induce ferroptosis in glioblastoma cells while sparing healthy neural tissue.

Published

2024

4. Metabolic Reprogramming in Glioblastoma Multiforme: A Review of Pathways and Therapeutic Targets

Author

Ashley Irin Cortes Ballen, Maryam Amosu, Surya Ravinder, Joey Chan, Emre Derin, Hasan Slika, and Betty Tyler

Subjects

glioblastoma multiforme, metabolic reprogramming, tumor microenvironment, Warburg effect, glycolysis, therapeutic drugs, Cytology, QH573-671

Abstract

Glioblastoma (GBM) is an aggressive and highly malignant primary brain tumor characterized by rapid growth and a poor prognosis for patients. Despite advancements in treatment, the median survival time for GBM patients remains low. One of the crucial challenges in understanding and treating GBMs involves its remarkable cellular heterogeneity and adaptability. Central to the survival and proliferation of GBM cells is their ability to undergo metabolic reprogramming. Metabolic reprogramming is a process that allows cancer cells to alter their metabolism to meet the increased demands of rapid growth and to survive in the often oxygen- and nutrient-deficient tumor microenvironment. These changes in metabolism include the Warburg effect, alterations in several key metabolic pathways including glutamine metabolism, fatty acid synthesis, and the tricarboxylic acid (TCA) cycle, increased uptake and utilization of glutamine, and more. Despite the complexity and adaptability of GBM metabolism, a deeper understanding of its metabolic reprogramming offers hope for developing more effective therapeutic interventions against GBMs.

Published

2024

5. Towards standardization of the parameters for opening the blood–brain barrier with focused ultrasound to treat glioblastoma multiforme: A systematic review of the devices, animal models, and therapeutic compounds used in rodent tumor models

Author

Rasika Thombre, Griffin Mess, Kelley M. Kempski Leadingham, Shivani Kapoor, Andrew Hersh, Molly Acord, Tarana Kaovasia, Nicholas Theodore, Betty Tyler, and Amir Manbachi

Subjects

blood-brain barrier, chemotherapy, focused ultrasound, glioblastoma multiforme, immunotherapy, microbubble, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Glioblastoma multiforme (GBM) is a deadly and aggressive malignant brain cancer that is highly resistant to treatments. A particular challenge of treatment is caused by the blood–brain barrier (BBB), the relatively impermeable vasculature of the brain. The BBB prevents large molecules from entering the brain parenchyma. This protective characteristic of the BBB, however, also limits the delivery of therapeutic drugs for the treatment of brain tumors. To address this limitation, focused ultrasound (FUS) has been safely utilized to create transient openings in the BBB, allowing various high molecular weight drugs access to the brain. We performed a systematic review summarizing current research on treatment of GBMs using FUS-mediated BBB openings in in vivo mouse and rat models. The studies gathered here highlight how the treatment paradigm can allow for increased brain and tumor perfusion of drugs including chemotherapeutics, immunotherapeutics, gene therapeutics, nanoparticles, and more. Given the promising results detailed here, the aim of this review is to detail the commonly used parameters for FUS to open the BBB in rodent GBM models.

Published

2023

6. Disulfiram and copper combination therapy targets NPL4, cancer stem cells and extends survival in a medulloblastoma model

Author

Riccardo Serra, Tianna Zhao, Sakibul Huq, Noah Leviton Gorelick, Joshua Casaos, Arba Cecia, Antonella Mangraviti, Charles Eberhart, Renyuan Bai, Alessandro Olivi, Henry Brem, Eric M. Jackson, and Betty Tyler

Subjects

Medicine, Science

Abstract

Background Medulloblastoma (MB) is the most common brain malignancy in children, and is still responsible for significant mortality and morbidity. The aim of this study was to assess the safety and efficacy of Disulfiram (DSF), an FDA-approved inhibitor of Aldehyde-Dehydrogenase (ALDH), and Copper (Cu++) in human SSH-driven and Group 3 MB. The molecular mechanisms, effect on cancer-stem-cells (CSC) and DNA damage were investigated in xenograft models. Methods The cytotoxic and anti-CSC effects of DSF/Cu++ were evaluated with clonogenic assays, flow-cytometry, immunofluorescence, western-blotting. ONS76, UW228 (SHH-driven with Tp53m), D425med, D283 and D341 (Group 3) cell-lines were used. In vivo survival and nuclear protein localization protein-4 (NPL4), Ki67, Cleaved-Caspase-3, GFAP and NeuN expression were assessed in two Group 3 MB xenografts with immunohistochemistry and western-blotting. Results Significant in vitro cytotoxicity was demonstrated at nanomolar concentrations. DSF/Cu++ induced cell-death through NPL4 accumulation in cell-nucleus and buildup of poly-ubiquitylated proteins. Flow-cytometry demonstrated a significant decrease in ALDH+, Nestin+ and CD133+ following treatment, anti-CSC effect was confirmed in vitro and in vivo. DSF/Cu++ prolonged survival, and increased nuclear NPL4 expression in vivo. Conclusions Our data suggest that this combination may serve as a novel treatment, as monotherapy or in combination with existing therapies, for aggressive subtypes of pediatric MB.

Published

2021

7. Dendrimer size effects on the selective brain tumor targeting in orthotopic tumor models upon systemic administration

Author

Kevin Liaw, Fan Zhang, Antonella Mangraviti, Sujatha Kannan, Betty Tyler, and Rangaramanujam M. Kannan

Subjects

brain tumor targeting, dendrimer, glioblastoma, immunotherapies, tumor‐associated macrophages, Chemical engineering, TP155-156, Biotechnology, TP248.13-248.65, Therapeutics. Pharmacology, RM1-950

Abstract

Abstract Malignant gliomas are the most common and aggressive form of primary brain tumors, with a median survival of 15–20 months for patients receiving maximal interventions. Advances in nanomedicine have provided tumor‐specific delivery of chemotherapeutics to potentially overcome their off‐target toxicities. Recent advances in dendrimer‐based nanomedicines have established that hydroxyl‐terminated poly(amidoamine) dendrimers can intrinsically target neuroinflammation and brain tumors from systemic administration without the need for targeting moieties. The size of nanocarriers is a critical parameter that determines their tumor‐targeting efficiency, intratumor distribution, and clearance mechanism. In this study, we explore the dendrimer size effects on brain tumor targeting capability in two clinically relevant orthotopic brain tumor models, the 9L rat and GL261 mouse models, which capture differing aspects of gliomas. We show that increasing dendrimers from Generation 4 to Generation 6 significantly enhances their tumor accumulation (~10‐fold greater at 24 hr), tumor specificity (~2–3 fold higher), and tumor retention. The superior tumor targeting effect of G6 dendrimers is associated with its reduced renal clearance rate, resulting in longer circulation time compared to G4 dendrimers. Additionally, the increase in dendrimer generation does not compromise its homogeneous tumor distribution and intrinsic targeting of tumor‐associated macrophages. These results validate the potential for these dendrimers as an effective, clinically translatable platform for effectively targeting tumor‐associated macrophages in malignant gliomas.

Published

2020

8. Drug Repurposing for Glioblastoma and Current Advances in Drug Delivery—A Comprehensive Review of the Literature

Author

Safwan Alomari, Irma Zhang, Adrian Hernandez, Caitlin Y. Kraft, Divyaansh Raj, Jayanidhi Kedda, and Betty Tyler

Subjects

brain tumor, drug delivery, glioma, repurposed drugs, Microbiology, QR1-502

Abstract

Glioblastoma (GBM) is the most common primary malignant brain tumor in adults with an extremely poor prognosis. There is a dire need to develop effective therapeutics to overcome the intrinsic and acquired resistance of GBM to current therapies. The process of developing novel anti-neoplastic drugs from bench to bedside can incur significant time and cost implications. Drug repurposing may help overcome that obstacle. A wide range of drugs that are already approved for clinical use for the treatment of other diseases have been found to target GBM-associated signaling pathways and are being repurposed for the treatment of GBM. While many of these drugs are undergoing pre-clinical testing, others are in the clinical trial phase. Since GBM stem cells (GSCs) have been found to be a main source of tumor recurrence after surgery, recent studies have also investigated whether repurposed drugs that target these pathways can be used to counteract tumor recurrence. While several repurposed drugs have shown significant efficacy against GBM cell lines, the blood–brain barrier (BBB) can limit the ability of many of these drugs to reach intratumoral therapeutic concentrations. Localized intracranial delivery may help to achieve therapeutic drug concentration at the site of tumor resection while simultaneously minimizing toxicity and side effects. These strategies can be considered while repurposing drugs for GBM.

Published

2021

9. TIGIT and PD-1 dual checkpoint blockade enhances antitumor immunity and survival in GBM

Author

Alice L. Hung, Russell Maxwell, Debebe Theodros, Zineb Belcaid, Dimitrios Mathios, Andrew S. Luksik, Eileen Kim, Adela Wu, Yuanxuan Xia, Tomas Garzon-Muvdi, Christopher Jackson, Xiaobu Ye, Betty Tyler, Mark Selby, Alan Korman, Bryan Barnhart, Su-Myeong Park, Je-In Youn, Tamrin Chowdhury, Chul-Kee Park, Henry Brem, Drew M. Pardoll, and Michael Lim

Subjects

tigit, pvr, cd155, pd-1, dendritic cell, glioma, checkpoint inhibitor, immunotherapy, gbm, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

The use of inhibitory checkpoint blockade in the management of glioblastoma has been studied in both preclinical and clinical settings. TIGIT is a novel checkpoint inhibitor recently discovered to play a role in cancer immunity. In this study, we sought to determine the effect of anti-PD-1 and anti-TIGIT combination therapy on survival in a murine glioblastoma (GBM) model, and to elucidate the underlying immune mechanisms. Using mice with intracranial GL261-luc+ tumors, we found that TIGIT expression was upregulated on CD8+ and regulatory T cells (Tregs) in the brain compared to draining cervical lymph nodes (CLN) and spleen. We then demonstrated that treatment using anti-PD-1 and anti-TIGIT dual therapy significantly improved survival compared to control and monotherapy groups. The therapeutic effect was correlated with both increased effector T cell function and downregulation of suppressive Tregs and tumor-infiltrating dendritic cells (TIDCs). Clinically, TIGIT expression on tumor-infiltrating lymphocytes was shown to be elevated in patient GBM samples, suggesting that the TIGIT pathway may be a valuable therapeutic target. Expression of the TIGIT ligand, PVR, further portended a poor survival outcome in patients with low-grade glioma. We conclude that anti-TIGIT is an effective treatment strategy against murine GBM when used in combination with anti-PD-1, improving overall survival via modifications of both the T cell and myeloid compartments. Given evidence of PVR expression on human GBM cells, TIGIT presents as a promising immune therapeutic target in the management of these patients.

Published

2018

10. Erratum to: Agonist anti-GITR monoclonal antibody and stereotactic radiation induce immune-mediated survival advantage in murine intracranial glioma

Author

Christina Jackson, Ada Tam, Sarah Harris-Bookman, Brian Francica, Charles G. Drake, Drew M. Pardoll, Debebe Theodros, Esteban Velarde, Betty Tyler, Xiaobu Ye, Henry Brem, Mark Selby, Dimitrios Mathios, Mira A. Patel, Jennifer E. Kim, Christina M. Kochel, Thomas R. Nirschl, Ali Ghasemzadeh, Christopher C. Jackson, Phuoc T. Tran, Vladimir Coric, and Michael Lim

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Published

2016

11. Agonist anti-GITR monoclonal antibody and stereotactic radiation induce immune-mediated survival advantage in murine intracranial glioma

Author

Christina Jackson, Ada Tam, Sarah Harris-Bookman, Brian Francica, Charles G. Drake, Drew M. Pardoll, Debebe Theodros, Esteban Velarde, Betty Tyler, Xiaobu Ye, Henry Brem, Mark Selby, Dimitrios Mathios, Mira A. Patel, Jennifer E. Kim, Christina M. Kochel, Thomas R. Nirschl, Ali Ghasemzadeh, Christopher C. Jackson, Phuoc T. Tran, Vladimir Coric, and Michael Lim

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Background Glioblastoma (GBM) is a poorly immunogenic neoplasm treated with focused radiation. Immunotherapy has demonstrated synergistic survival effects with stereotactic radiosurgery (SRS) in murine GBM. GITR is a co-stimulatory molecule expressed constitutively on regulatory T-cells and by effector T-cells upon activation. We tested the hypothesis that anti-GITR monoclonal antibody (mAb) and SRS together would confer an immune-mediated survival benefit in glioma using the orthotopic GL261 glioma model.Methods Mice received SRS and anti-GITR 10 days after implantation. The anti-GITR mAbs tested were formatted as mouse IgG1 D265A (anti-GITR (1)) and IgG2a (anti-GITR (2a)) isotypes. Mice were randomized to four treatment groups: (1) control; (2) SRS; (3) anti-GITR; (4) anti-GITR/SRS. SRS was delivered to the tumor in one fraction, and mice were treated with mAb thrice. Mice were euthanized on day 21 to analyze the immunologic profile of tumor, spleen, and tumor draining lymph nodes.Results Anti-GITR (1)/SRS significantly improved survival over either treatment alone (p

Published

2016

12. Focal radiation therapy combined with 4-1BB activation and CTLA-4 blockade yields long-term survival and a protective antigen-specific memory response in a murine glioma model.

Author

Zineb Belcaid, Jillian A Phallen, Jing Zeng, Alfred P See, Dimitrios Mathios, Chelsea Gottschalk, Sarah Nicholas, Meghan Kellett, Jacob Ruzevick, Christopher Jackson, Emilia Albesiano, Nicholas M Durham, Xiaobu Ye, Phuoc T Tran, Betty Tyler, John W Wong, Henry Brem, Drew M Pardoll, Charles G Drake, and Michael Lim

Subjects

Medicine, Science

Abstract

Glioblastoma (GBM) is the most common malignant brain tumor in adults and is associated with a poor prognosis. Cytotoxic T lymphocyte antigen -4 (CTLA-4) blocking antibodies have demonstrated an ability to generate robust antitumor immune responses against a variety of solid tumors. 4-1BB (CD137) is expressed by activated T lymphocytes and served as a co-stimulatory signal, which promotes cytotoxic function. Here, we evaluate a combination immunotherapy regimen involving 4-1BB activation, CTLA-4 blockade, and focal radiation therapy in an immune-competent intracranial GBM model.GL261-luciferace cells were stereotactically implanted in the striatum of C57BL/6 mice. Mice were treated with a triple therapy regimen consisted of 4-1BB agonist antibodies, CTLA-4 blocking antibodies, and focal radiation therapy using a small animal radiation research platform and mice were followed for survival. Numbers of brain-infiltrating lymphocytes were analyzed by FACS analysis. CD4 or CD8 depleting antibodies were administered to determine the relative contribution of T helper and cytotoxic T cells in this regimen. To evaluate the ability of this immunotherapy to generate an antigen-specific memory response, long-term survivors were re-challenged with GL261 glioma en B16 melanoma flank tumors.Mice treated with triple therapy had increased survival compared to mice treated with focal radiation therapy and immunotherapy with 4-1BB activation and CTLA-4 blockade. Animals treated with triple therapy exhibited at least 50% long-term tumor free survival. Treatment with triple therapy resulted in a higher density of CD4+ and CD8+ tumor infiltrating lymphocytes. Mechanistically, depletion of CD4+ T cells abrogated the antitumor efficacy of triple therapy, while depletion of CD8+ T cells had no effect on the treatment response.Combination therapy with 4-1BB activation and CTLA-4 blockade in the setting of focal radiation therapy improves survival in an orthotopic mouse model of glioma by a CD4+ T cell dependent mechanism and generates antigen-specific memory.

Published

2014

13. Evaluation of tyrosine kinase inhibitor combinations for glioblastoma therapy.

Author

Avadhut D Joshi, Watcharin Loilome, I-Mei Siu, Betty Tyler, Gary L Gallia, and Gregory J Riggins

Subjects

Medicine, Science

Abstract

Glioblastoma multiforme (GBM) is the most common intracranial cancer but despite recent advances in therapy the overall survival remains about 20 months. Whole genome exon sequencing studies implicate mutations in the receptor tyrosine kinase pathways (RTK) for driving tumor growth in over 80% of GBMs. In spite of various RTKs being mutated or altered in the majority of GBMs, clinical studies have not been able to demonstrate efficacy of molecular targeted therapies using tyrosine kinase inhibitors in GBMs. Activation of multiple downstream signaling pathways has been implicated as a possible means by which inhibition of a single RTK has been ineffective in GBM. In this study, we sought a combination of approved drugs that would inhibit in vitro and in vivo growth of GBM oncospheres. A combination consisting of gefitinib and sunitinib acted synergistically in inhibiting growth of GBM oncospheres in vitro. Sunitinib was the only RTK inhibitor that could induce apoptosis in GBM cells. However, the in vivo efficacy testing of the gefitinib and sunitinib combination in an EGFR amplified/PTEN wild type GBM xenograft model revealed that gefitinib alone could significantly improve survival in animals whereas sunitinib did not show any survival benefit. Subsequent testing of the same drug combination in a different syngeneic glioma model that lacked EGFR amplification but was more susceptible to sunitinib in vitro demonstrated no survival benefit when treated with gefitinib or sunitinib or the gefitinib and sunitinib combination. Although a modest survival benefit was obtained in one of two animal models with EGFR amplification due to gefitinib alone, the addition of sunitinib, to test our best in vitro combination therapy, did not translate to any additional in vivo benefit. Improved targeted therapies, with drug properties favorable to intracranial tumors, are likely required to form effective drug combinations for GBM.

Published

2012

14. Self-assembling paclitaxel-mediated stimulation of tumor-associated macrophages for postoperative treatment of glioblastoma

Author

Feihu Wang, Qian Huang, Hao Su, Mingjiao Sun, Zeyu Wang, Ziqi Chen, Mengzhen Zheng, Rami W. Chakroun, Maya K. Monroe, Daiqing Chen, Zongyuan Wang, Noah Gorelick, Riccardo Serra, Han Wang, Yun Guan, Jung Soo Suk, Betty Tyler, Henry Brem, Justin Hanes, and Honggang Cui

Subjects

Multidisciplinary

Abstract

The unique cancer-associated immunosuppression in brain, combined with a paucity of infiltrating T cells, contributes to the low response rate and poor treatment outcomes of T cell-based immunotherapy for patients diagnosed with glioblastoma multiforme (GBM). Here, we report on a self-assembling paclitaxel (PTX) filament (PF) hydrogel that stimulates macrophage-mediated immune response for local treatment of recurrent glioblastoma. Our results suggest that aqueous PF solutions containing aCD47 can be directly deposited into the tumor resection cavity, enabling seamless hydrogel filling of the cavity and long-term release of both therapeutics. The PTX PFs elicit an immune-stimulating tumor microenvironment (TME) and thus sensitizes tumor to the aCD47-mediated blockade of the antiphagocytic “don’t eat me” signal, which subsequently promotes tumor cell phagocytosis by macrophages and also triggers an antitumor T cell response. As adjuvant therapy after surgery, this aCD47/PF supramolecular hydrogel effectively suppresses primary brain tumor recurrence and prolongs overall survivals with minimal off-target side effects.

Published

2023

15. Data from Repurposing the FDA-Approved Antiviral Drug Ribavirin as Targeted Therapy for Nasopharyngeal Carcinoma

Author

Betty Tyler, Nicolas Skuli, Henry Brem, Mariana Brait, David Sidransky, Ian Suk, Chenchen Ji, Arba Cecia, Alexander Perdomo-Pantoja, Wataru Ishida, Tianna Zhao, Noah L. Gorelick, Manuel Morales, Jayanidhi N. Kedda, Jeff Ehresman, Andy S. Ding, Yuanxuan Xia, Michael Peters, Riccardo Serra, Joshua Casaos, and Sakibul Huq

Abstract

Nasopharyngeal carcinoma (NPC) is a squamous cell carcinoma with a proclivity for systemic dissemination, leading many patients to present with advanced stage disease and fail available treatments. There is a notable lack of targeted therapies for NPC, despite working knowledge of multiple proteins with integral roles in NPC cancer biology. These proteins include EZH2, Snail, eIF4E, and IMPDH, which are all overexpressed in NPC and correlated with poor prognosis. These proteins are known to be modulated by ribavirin, an FDA-approved hepatitis C antiviral that has recently been repurposed as a promising therapeutic in several solid and hematologic malignancies. Here, we investigated the potential of ribavirin as a targeted anticancer agent in five human NPC cell lines. Using cellular growth assays, flow cytometry, BrdU cell proliferation assays, scratch wound assays, and invasion assays, we show in vitro that ribavirin decreases NPC cellular proliferation, migration, and invasion and promotes cell-cycle arrest and cell death. Modulation of EZH2, Snail, eIF4E, IMPDH, mTOR, and cyclin D1 were observed in Western blots and enzymatic activity assays in response to ribavirin treatment. As monotherapy, ribavirin reduced flank tumor growth in multiple NPC xenograft models in vivo. Most importantly, we demonstrate that ribavirin enhanced the effects of radiotherapy, a central component of NPC treatment, both in vitro and in vivo. Our work suggests that NPC responds to ribavirin-mediated EZH2, Snail, eIF4E, IMPDH, and mTOR changes and positions ribavirin for clinical evaluation as a potential addition to our NPC treatment armamentarium.

Published

2023

16. Supplementary Data from Repurposing the FDA-Approved Antiviral Drug Ribavirin as Targeted Therapy for Nasopharyngeal Carcinoma

Author

Betty Tyler, Nicolas Skuli, Henry Brem, Mariana Brait, David Sidransky, Ian Suk, Chenchen Ji, Arba Cecia, Alexander Perdomo-Pantoja, Wataru Ishida, Tianna Zhao, Noah L. Gorelick, Manuel Morales, Jayanidhi N. Kedda, Jeff Ehresman, Andy S. Ding, Yuanxuan Xia, Michael Peters, Riccardo Serra, Joshua Casaos, and Sakibul Huq

Abstract

Supplementary Figures 1-6

Published

2023

17. Synergy between glutamate modulation and anti–programmed cell death protein 1 immunotherapy for glioblastoma

Author

Christopher M. Jackson, Laura Saleh, Ayush Pant, Denis Routkevitch, Michael Lim, Sakibul Huq, Henry Brem, Betty Tyler, Christina Jackson, Zach Pennington, Ravi Medikonda, Timothy Kim, Kisha K. Patel, Siddhartha Srivastava, Yuanxuan Xia, Dimitrios Mathios, John Choi, Young Hoon Kim, Luqing Tong, Zineb Belcaid, Jeff Ehresman, and Pavan P. Shah

Subjects

Tumor microenvironment, Brain Neoplasms, business.industry, Melanoma, medicine.medical_treatment, Glutamate receptor, Glutamic Acid, FOXP3, General Medicine, Immunotherapy, medicine.disease, Mice, Inbred C57BL, Mice, Immune system, Cell Line, Tumor, Glioma, Tumor Microenvironment, Cancer research, medicine, Animals, Humans, Glioblastoma, business, CD8

Abstract

OBJECTIVE Immune checkpoint inhibitors such as anti–programmed cell death protein 1 (anti-PD-1) have shown promise for the treatment of cancers such as melanoma, but results for glioblastoma (GBM) have been disappointing thus far. It has been suggested that GBM has multiple mechanisms of immunosuppression, indicating a need for combinatorial treatment strategies. It is well understood that GBM increases glutamate in the tumor microenvironment (TME); however, the significance of this is not well understood. The authors posit that glutamate upregulation in the GBM TME is immunosuppressive. The authors utilized a novel glutamate modulator, BHV-4157, to determine synergy between glutamate modulation and the well-established anti-PD-1 immunotherapy for GBM. METHODS C57BL/6J mice were intracranially implanted with luciferase-tagged GL261 glioma cells. Mice were randomly assigned to the control, anti-PD-1, BHV-4157, or combination anti-PD-1 plus BHV-4157 treatment arms, and median overall survival was assessed. In vivo microdialysis was performed at the tumor site with administration of BHV-4157. Intratumoral immune cell populations were characterized with immunofluorescence and flow cytometry. RESULTS The BHV-4157 treatment arm demonstrated improved survival compared with the control arm (p < 0.0001). Microdialysis demonstrated that glutamate concentration in TME significantly decreased after BHV-4157 administration. Immunofluorescence and flow cytometry demonstrated increased CD4+ T cells and decreased Foxp3+ T cells in mice that received BHV-4157 treatment. No survival benefit was observed when CD4+ or CD8+ T cells were depleted in mice prior to BHV-4157 administration (p < 0.05). CONCLUSIONS In this study, the authors showed synergy between anti-PD-1 immunotherapy and glutamate modulation. The authors provide a possible mechanism for this synergistic benefit by showing that BHV-4157 relies on CD4+ and CD8+ T cells. This study sheds light on the role of excess glutamate in GBM and provides a basis for further exploring combinatorial approaches for the treatment of this disease.

Published

2022

18. Impact of international research fellows in neurosurgery: results from a single academic center

Author

Gary L. Gallia, Betty Tyler, George I. Jallo, Wuyang Yang, Gregory J. Riggins, Henry Brem, Timothy F. Witham, Debraj Mukherjee, Judy Huang, Alfredo Quiñones-Hinojosa, Sheng Fu L. Lo, Ali Bydon, Alan R. Cohen, Adham M. Khalafallah, Alban Latremoliere, James Feghali, Rafael J. Tamargo, Daniel M. Sciubba, William S. Anderson, Mark Luciano, Alexander Perdomo-Pantoja, Daniele Rigamonti, Wataru Ishida, Michael Lim, Lintao Qu, Alessandro Olivi, Ziya L. Gokaslan, and Jordina Rincon-Torroella

Subjects

Adult, Male, medicine.medical_specialty, Students, Medical, International Cooperation, Neurosurgery, Language differences, Scientific productivity, Mentorship, Surveys and Questionnaires, medicine, Undergraduate student, Humans, Fellowships and Scholarships, Language, International research, Academic Medical Centers, business.industry, Mentors, Publications, Significant difference, Cultural Diversity, General Medicine, United States, Country of origin, Neurosurgeons, Family medicine, Female, business

Abstract

OBJECTIVE International research fellows have been historically involved in academic neurosurgery in the United States (US). To date, the contribution of international research fellows has been underreported. Herein, the authors aimed to quantify the academic output of international research fellows in the Department of Neurosurgery at The Johns Hopkins University School of Medicine. METHODS Research fellows with Doctor of Medicine (MD), Doctor of Philosophy (PhD), or MD/PhD degrees from a non-US institution who worked in the Hopkins Department of Neurosurgery for at least 6 months over the past decade (2010–2020) were included in this study. Publications produced during fellowship, number of citations, and journal impact factors (IFs) were analyzed using ANOVA. A survey was sent to collect information on personal background, demographics, and academic activities. RESULTS Sixty-four international research fellows were included, with 42 (65.6%) having MD degrees, 17 (26.6%) having PhD degrees, and 5 (7.8%) having MD/PhD degrees. During an average 27.9 months of fellowship, 460 publications were produced in 136 unique journals, with 8628 citations and a cumulative journal IF of 1665.73. There was no significant difference in total number of publications, first-author publications, and total citations per person among the different degree holders. Persons holding MD/PhDs had a higher number of citations per publication per person (p = 0.027), whereas those with MDs had higher total IFs per person (p = 0.048). Among the 43 (67.2%) survey responders, 34 (79.1%) had nonimmigrant visas at the start of the fellowship, 16 (37.2%) were self-paid or funded by their country of origin, and 35 (81.4%) had mentored at least one US medical student, nonmedical graduate student, or undergraduate student. CONCLUSIONS International research fellows at the authors’ institution have contributed significantly to academic neurosurgery. Although they have faced major challenges like maintaining nonimmigrant visas, negotiating cultural/language differences, and managing self-sustainability, their scientific productivity has been substantial. Additionally, the majority of fellows have provided reciprocal mentorship to US students.

Published

2022

19. Data from Suppression of Human Glioma Xenografts with Second-Generation IL13R-Specific Chimeric Antigen Receptor–Modified T Cells

Author

Prakash Sampath, Richard P. Junghans, Henry Brem, Bob S. Carter, Ayguen Sahin, Jinyuan Zhou, Saryn Doucette, Qiangzhong Ma, Anthony J. Bais, Betty Tyler, Sadhak Sengupta, and Seogkyoung Kong

Abstract

Purpose: Glioblastoma multiforme (GBM) remains highly incurable, with frequent recurrences after standard therapies of maximal surgical resection, radiation, and chemotherapy. To address the need for new treatments, we have undertaken a chimeric antigen receptor (CAR) “designer T cell” (dTc) immunotherapeutic strategy by exploiting interleukin (IL)13 receptor α-2 (IL13Rα2) as a GBM-selective target.Experimental Design: We tested a second-generation IL13 “zetakine” CAR composed of a mutated IL13 extracellular domain linked to intracellular signaling elements of the CD28 costimulatory molecule and CD3ζ. The aim of the mutation (IL13.E13K.R109K) was to enhance selectivity of the CAR for recognition and killing of IL13Rα2+ GBMs while sparing normal cells bearing the composite IL13Rα1/IL4Rα receptor.Results: Our aim was partially realized with improved recognition of tumor and reduced but persisting activity against normal tissue IL13Rα1+ cells by the IL13.E13K.R109K CAR. We show that these IL13 dTcs were efficient in killing IL13Rα2+ glioma cell targets with abundant secretion of cytokines IL2 and IFNγ, and they displayed enhanced tumor-induced expansion versus control unmodified T cells in vitro. In an in vivo test with a human glioma xenograft model, single intracranial injections of IL13 dTc into tumor sites resulted in marked increases in animal survivals.Conclusions: These data raise the possibility of immune targeting of diffusely invasive GBM cells either via dTc infusion into resection cavities to prevent GBM recurrence or via direct stereotactic injection of dTcs to suppress inoperable or recurrent tumors. Systemic administration of these IL13 dTc could be complicated by reaction against normal tissues expressing IL13Ra1. Clin Cancer Res; 18(21); 5949–60. ©2012 AACR.

Published

2023

20. Supplementary Figure 1 from Suppression of Human Glioma Xenografts with Second-Generation IL13R-Specific Chimeric Antigen Receptor–Modified T Cells

Author

Prakash Sampath, Richard P. Junghans, Henry Brem, Bob S. Carter, Ayguen Sahin, Jinyuan Zhou, Saryn Doucette, Qiangzhong Ma, Anthony J. Bais, Betty Tyler, Sadhak Sengupta, and Seogkyoung Kong

Abstract

PDF file, 136K, Bar graph representing IL2 secretion by untransduced or IL13-CAR transduced T cells upon co-culturing.

Published

2023

21. CCR Translation for This Article from Suppression of Human Glioma Xenografts with Second-Generation IL13R-Specific Chimeric Antigen Receptor–Modified T Cells

Author

Prakash Sampath, Richard P. Junghans, Henry Brem, Bob S. Carter, Ayguen Sahin, Jinyuan Zhou, Saryn Doucette, Qiangzhong Ma, Anthony J. Bais, Betty Tyler, Sadhak Sengupta, and Seogkyoung Kong

Abstract

CCR Translation for This Article from Suppression of Human Glioma Xenografts with Second-Generation IL13R-Specific Chimeric Antigen Receptor–Modified T Cells

Published

2023

22. Disruption of the Blood-Spinal Cord Barrier using Low-Intensity Focused Ultrasound in a Rat Model

Author

Amir Manbachi, Nicholas Theodore, Betty Tyler, Joshua C. Doloff, Kelley M. Kempski Leadingham, Joshua Punnoose, A. Daniel Davidar, Carly Weber-Levine, Kelly Jiang, Arjun K. Menta, Ali Mohammadabadi, Andrew M. Hersh, Denis Routkevitch, and Meghana Bhimreddy

Subjects

General Immunology and Microbiology, General Chemical Engineering, General Neuroscience, General Biochemistry, Genetics and Molecular Biology

Published

2023

23. Sonodynamic Therapy for the Treatment of Glioblastoma Multiforme in a Mouse Model Using a Portable Benchtop Focused Ultrasound System

Author

Amir Manbachi, Betty Tyler, Santosh K. Yadav, Kelley M. Kempski-Leadingham, Emre Derin, Ruixing Liang, Rasika Thombre, Shivani Kapoor, Taylor Anderson, and Griffin Mess

Subjects

General Immunology and Microbiology, General Chemical Engineering, General Neuroscience, General Biochemistry, Genetics and Molecular Biology

Published

2023

24. A Highly Translatable Dual‐arm Local Delivery Strategy To Achieve Widespread Therapeutic Coverage in Healthy and Tumor‐bearing Brain Tissues

Author

Karina Negron, Gijung Kwak, Heng Wang, Haolin Li, Yi‐Ting Huang, Shun‐Wen Chen, Betty Tyler, Charles G. Eberhart, Justin Hanes, and Jung Soo Suk

Subjects

Biomaterials, General Materials Science, General Chemistry, Biotechnology

Published

2023

25. Targeting of cyclin-dependent kinases in atypical teratoid rhabdoid tumors with multikinase inhibitor TG02

Author

Andy S. Ding, Sakibul Huq, Henry Brem, Riccardo Serra, Joshua Casaos, Timothy Kim, Noah Gorelick, Ayush Pant, Betty Tyler, Divyaansh Raj, Siddhartha Srivastava, Manuel Morales, and Tianna Zhao

Subjects

Cisplatin, Radiosensitizer, medicine.diagnostic_test, biology, Cell growth, business.industry, General Medicine, medicine.disease, Flow cytometry, Cyclin D1, Cyclin-dependent kinase, Atypical teratoid rhabdoid tumor, medicine, Cancer research, biology.protein, Clonogenic assay, business, medicine.drug

Abstract

OBJECTIVE Atypical teratoid rhabdoid tumors (ATRTs) are aggressive pediatric brain tumors with no current standard of care and an estimated median patient survival of 12 to 18 months. Previous genetic analyses have implicated cyclin D1 and enhancer of zeste homolog 2 (EZH2), a histone methyltransferase that is implicated in many cancers, as key drivers of tumorigenicity in ATRTs. Since the effects of EZH2 and cyclin D1 are facilitated by a host of cyclin-dependent kinases (CDKs), the authors sought to investigate the potential therapeutic effects of targeting CDKs in ATRTs with the multi–CDK inhibitor, TG02. METHODS Human ATRT cell lines BT12, BT37, CHLA05, and CHLA06 were selected for investigation. The effects of TG02 on cell viability, proliferation, clonogenicity, and apoptosis were assessed via Cell Counting Kit-8 assays, cell counting, clonogenic assays, and flow cytometry, respectively. Similar methods were used to determine the effects of TG02 combined with radiation therapy (RT) or cisplatin. Synergism indices for TG02-cisplatin combination therapy were calculated using CompuSyn software. RESULTS TG02 was observed to significantly impair ATRT cell growth in vitro by limiting cell proliferation and clonogenicity, and by inducing apoptosis. TG02 inhibited ATRT cell proliferation and decreased cell viability in a dose-dependent manner with nanomolar half maximal effective concentration (EC50) values (BT12, 207.0 nM; BT37, 127.8 nM; CHLA05, 29.7 nM; CHLA06, 18.7 nM). TG02 (150 nM) dramatically increased the proportion of apoptotic ATRT cells 72 hours posttreatment (TG02 8.50% vs control 1.52% apoptotic cells in BT12, p < 0.0001; TG02 70.07% vs control 15.36%, p < 0.0001). Combination therapy studies revealed that TG02 acted as a potent radiosensitizer in ATRT cells (BT12 surviving fraction, RT 51.2% vs RT + TG02 21.7%). Finally, CompuSyn analysis demonstrated that TG02 acted synergistically with cisplatin against ATRT cells at virtually all therapeutic doses. These findings were consistent in cell lines that cover all three molecular subgroups of ATRTs. CONCLUSIONS The results of this investigation have established that TG02 is an effective therapeutic against ATRTs in vitro. Given the lack of standard therapy for ATRTs, these findings help fill an unmet need and support further study of TG02 as a potential therapeutic option for patients with this deadly disease.

Published

2021

26. Pharmacological strategies for improving the prognosis of glioblastoma

Author

Pranjal Agrawal, Hallie Gaitsch, Elizabeth C. Wicks, Divyaansh Raj, and Betty Tyler

Subjects

Central Nervous System, Oncology, medicine.medical_specialty, Combination therapy, medicine.medical_treatment, Article, Internal medicine, Temozolomide, Humans, Medicine, Pharmacology (medical), Pharmacology, Chemotherapy, Brain Neoplasms, business.industry, General Medicine, Immunotherapy, Prognosis, medicine.disease, United States, Clinical trial, Cns malignancy, Drug delivery, Glioblastoma, business, medicine.drug

Abstract

INTRODUCTION: Treatments for brain cancer have radically evolved in the past decade due to a better understanding of the interplay between the immune system and tumors of the central nervous system (CNS). However, glioblastoma multiforme (GBM) remains the most common and lethal CNS malignancy affecting adults. AREAS COVERED: The authors review the literature on glioblastoma pharmacologic therapies with a focus on trials of combination chemo-/immunotherapies and drug delivery platforms from 2015 to 2021. EXPERT OPINION: Few therapeutic advances in GBM treatment have been made since the Food and Drug Administration (FDA) approval of the BCNU-eluting wafer, Gliadel, in 1996 and oral temozolomide (TMZ) in 2005. Recent advances in our understanding of GBM have promoted a wide assortment of new therapeutic approaches including combination therapy, immunotherapy, vaccines, and Car T-cell therapy along with developments in drug delivery. Given promising preclinical data, these novel pharmacotherapies for the treatment of GBM are currently being evaluated in various stages of clinical trials.

Published

2021

27. Preclinical efficacy of ribavirin in SHH and group 3 medulloblastoma

Author

Henry Brem, Joshua Casaos, Nivedha V. Kannapadi, Ravi Medikonda, Raphael Felder, Noah Gorelick, Andy S. Ding, Arba Cecia, Miguel A. Ruiz-Cardozo, Betty Tyler, Nicolas Skuli, Tarik Lott, Jeff Ehresman, Riccardo Serra, and Sakibul Huq

Subjects

medicine.medical_treatment, Flow cytometry, Targeted therapy, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cell Movement, In vivo, Cell Line, Tumor, Ribavirin, medicine, Animals, Humans, Enhancer of Zeste Homolog 2 Protein, Hedgehog Proteins, Cerebellar Neoplasms, Cell Proliferation, Medulloblastoma, medicine.diagnostic_test, business.industry, Cell growth, EZH2, Cell migration, General Medicine, medicine.disease, Xenograft Model Antitumor Assays, Eukaryotic Initiation Factor-4E, chemistry, 030220 oncology & carcinogenesis, Cancer research, business, 030217 neurology & neurosurgery

Abstract

OBJECTIVE Medulloblastoma, the most common pediatric brain malignancy, has Sonic Hedgehog (SHH) and group 3 (Myc driven) subtypes that are associated with the activity of eukaryotic initiation factor 4E (eIF4E), a critical mediator of translation, and enhancer of zeste homolog 2 (EZH2), a histone methyltransferase and master regulator of transcription. Recent drug repurposing efforts in multiple solid and hematologic malignancies have demonstrated that eIF4E and EZH2 are both pharmacologically inhibited by the FDA-approved antiviral drug ribavirin. Given the molecular overlap between medulloblastoma biology and known ribavirin activity, the authors investigated the preclinical efficacy of repurposing ribavirin as a targeted therapeutic in cell and animal models of medulloblastoma. METHODS Multiple in vitro assays were performed using human ONS-76 (a primitive SHH model) and D425 (an aggressive group 3 model) cells. The impacts of ribavirin on cellular growth, death, migration, and invasion were quantified using proliferation and Cell Counting Kit-8 (CCK-8) assays, flow cytometry with annexin V (AnnV) staining, scratch wound assays, and Matrigel invasion chambers, respectively. Survival following daily ribavirin treatment (100 mg/kg) was assessed in vivo in immunodeficient mice intracranially implanted with D425 cells. RESULTS Compared to controls, ribavirin treatment led to a significant reduction in medulloblastoma cell growth (ONS-76 proliferation assay, p = 0.0001; D425 CCK-8 assay, p < 0.0001) and a significant increase in cell death (flow cytometry for AnnV, ONS-76, p = 0.0010; D425, p = 0.0284). In ONS-76 cells, compared to controls, ribavirin significantly decreased cell migration and invasion (Matrigel invasion chamber assay, p = 0.0012). In vivo, ribavirin significantly extended survival in an aggressive group 3 medulloblastoma mouse model compared to vehicle-treated controls (p = 0.0004). CONCLUSIONS The authors demonstrate that ribavirin, a clinically used drug known to inhibit eIF4E and EZH2, has significant antitumor effects in multiple preclinical models of medulloblastoma, including an aggressive group 3 animal model. Ribavirin may represent a promising targeted therapeutic in medulloblastoma.

Published

2021

28. Abstract 443: Therapeutic targeting of GPR68 activated by acidic extracellular microenvironment induces ferroptosis in glioblastoma cells

Author

Charles H. Williams, Leif R. Neitzel, Jessica Cornell, Samantha Rea, Ian Mills, Maya Silver-Isenstadt, Jovanni D. Ahmad, Henry Brem, Betty Tyler, Eli E. Bar, and Charles C. Hong

Subjects

Cancer Research, Oncology

Abstract

The Warburg Effect is a common feature of cancer cells characterized by increased glucose uptake and fermentation of glucose to lactate even in the presence of oxygen. While it is commonly accepted that Warburg Effect promotes the growth, survival, proliferation, and long-term maintenance of cancers, its precise function and its downstream mediators remain unclear. A key physiological consequence of the Warburg effect is lactate secretion, which acidifies the tumor milieu, thought to promote oncogenesis and confer tumor resistance to chemotherapy and radiotherapy. Glioblastoma multiforme (GBM) is one of the most aggressive and deadly cancers, characterized by cellular heterogeneity and plasticity, which are thought to drive extreme therapeutic resistance. Despite their heterogeneity, common hallmarks of GBM tumors are high levels of aerobic glycolysis (“Warburg Effect”) and a resultant acidic tumor microenvironment (TME), which promotes tumor progression. In an in vivo zebrafish developmental screen, we identified ogremorphin (OGM), a small molecule inhibitor of GPR68/OGR-1, a G-protein coupled receptor (GPCR) which is activated by extracellular protons. Using ogremorphin and pHluorin2-GPI, a novel sensor of extracellular acidification, we demonstrate that glioblastoma cells acidify their own environment in vitro and activate GPR68, and visualize, for the first time, the establishment of the acidic extracellular microenvironment during the formation of GBM spheroids in vitro. Selective inhibition of GPR68 causes robust cell death in all 12 glioblastoma cell lines tested to date, despite genetic and molecular heterogeneity, without toxicity on healthy cells in whole animals. Mechanistically, GPR68 inhibition activates ferroptosis, a programmed cell death characterized by lipid peroxidation, in an ATF4 (activating transcription factor 4)-dependent manner. Finally, in GBM cells, ogremorphin treatment demonstrates strong synergistic effects with the frontline therapeutics temozolomide and ionizing radiation. Our results indicate that GPR68 activation by extracellular acidification is a key cancer survival pathway downstream of the Warburg Effect, and that GPR68 inhibition, either alone or in combination with temozolomide and radiation therapy, is a promising therapeutic approach to selectively induce ferroptosis in GBM tumors. Citation Format: Charles H. Williams, Leif R. Neitzel, Jessica Cornell, Samantha Rea, Ian Mills, Maya Silver-Isenstadt, Jovanni D. Ahmad, Henry Brem, Betty Tyler, Eli E. Bar, Charles C. Hong. Therapeutic targeting of GPR68 activated by acidic extracellular microenvironment induces ferroptosis in glioblastoma cells [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2023; Part 1 (Regular and Invited Abstracts); 2023 Apr 14-19; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2023;83(7_Suppl):Abstract nr 443.

Published

2023

29. Implementation of Minimally Invasive Brain Tumor Resection in Rodents for High Viability Tissue Collection

Author

Betty Tyler, Graeme F. Woodworth, Henry Brem, Heather M. Ames, Netanel Ben-Shalom, Jordina Rincon-Torroella, Bruno Gallo, Lilia Sukhon, Emylee McFarland, Su Xu, Pavlos Anastasiadis, Victor Pacis, Adarsha P. Malla, Jayanidhi Kedda, and Safwan Alomari

Subjects

Stereotaxic Techniques, Microsurgery, General Immunology and Microbiology, Brain Neoplasms, General Chemical Engineering, General Neuroscience, Animals, Brain, Humans, Minimally Invasive Surgical Procedures, Rodentia, General Biochemistry, Genetics and Molecular Biology

Abstract

The present protocol describes a standardized paradigm for rodent brain tumor resection and tissue preservation. In clinical practice, maximal tumor resection is the standard-of-care treatment for most brain tumors. However, most currently available preclinical brain tumor models either do not include resection, or utilize surgical resection models that are time-consuming and lead to significant postoperative morbidity, mortality, or experimental variability. In addition, performing resection in rodents can be daunting for several reasons, including a lack of clinically comparable surgical tools or protocols and the absence of an established platform for standardized tissue collection. This protocol highlights the use of a multi-functional, non-ablative resection device and an integrated tissue preservation system adapted from the clinical version of the device. The device applied in the present study combines tunable suction and a cylindrical blade at the aperture to precisely probe, cut, and suction tissue. The minimally invasive resection device performs its functions via the same burr hole used for the initial tumor implantation. This approach minimizes alterations to regional anatomy during biopsy or resection surgeries and reduces the risk of significant blood loss. These factors significantly reduced the operative time (2 min/animal), improved postoperative animal survival, lower variability in experimental groups, and result in high viability of resected tissues and cells for future analyses. This process is facilitated by a blade speed of ~1,400 cycles/min, which allows the harvesting of tissues into a sterile closed system that can be filled with a physiologic solution of choice. Given the emerging importance of studying and accurately modeling the impact of surgery, preservation and rigorous comparative analysis of regionalized tumor resection specimens, and intra-cavity-delivered therapeutics, this unique protocol will expand opportunities to explore unanswered questions about perioperative management and therapeutic discovery for brain tumor patients.

Published

2022

30. Designing a Murine Model of Human Glioblastoma Brain Tumor: Development of a Platform for Validation Using Ultrasound Elastography

Author

Griffin Mess, Rasika Thombre, Max Kerensky, Eli Curry, Fariba Aghabaglou, Safwan Alomari, Henry Brem, Nicholas Theodore, Betty Tyler, and Amir Manbachi

Abstract

Glioblastoma Multiforme (GBM) is a malignant brain cancer with low overall survival. Therefore, researchers are looking to augment its current therapeutic regimen, which includes surgical tumor resection, chemotherapy and radiation. A promising treatment modality, focused ultrasound, has been used as a non-invasive treatment for GBM through multiple approaches such as thermal ablation, immunomodulation, and blood brain barrier disruption. In order to develop these treatments for clinical trials, testing in animal models needs to be performed to investigate the efficacy of the treatment in complex biological environments, as well as to evaluate any side-effects. The more biologically relevant the animal model is to human anatomy, the more applicable the results will be for translation to clinical trials. Here, we report a human GBM rat model, which utilizes an IDH-wildtype, EGFRvIII mutant patient-derived xenograft in athymic rats. The in vivo tumor growth rate was assessed over a period of 20 days to evaluate reproducibility and to develop the model for future testing of FUS in the treatment of GBM.

Published

2022

31. Design and Development of System Components for Therapeutic Ultrasound Devices: Enhancing Focused Ultrasound Treatments Using Cones with Clinical and Ergonomic Considerations

Author

Rasika Thombre, Griffin Mess, Eli Curry, Richard Mejia, Ruixing Liang, Fariba Aghabaglou, Max Kerensky, Haley Abramson, Roslyn VanSickle, Betty Tyler, Nicholas Theodore, and Amir Manbachi

Abstract

Focused ultrasound (FUS) is an emerging technique with the potential to revolutionize traditional treatment methods in the fields of oncology and neurosurgery. Recently, FUS treatments have shown potential for altering neural activity in the spinal cord, with the intent to alleviate pain. Preliminary animal studies using FUS have demonstrated the need for transducer accessories that can simplify the implementation of the transducer in the clinic. The coupling cone that was supplied with the transducer was designed for larger target tissues. Thus, surgeons have expressed a desire to adapt the cone design to be easier to use for smaller targets, such as the spinal cord. Here, we developed 3D printed cones, with smaller aperture sizes, for FUS transducers to assist surgeons in localizing the focal point of the transducers in a faster, and more intuitive manner. The cones were designed to not alter the original focal region of the transducers. This was experimentally confirmed by measuring the size of the focal region for the transducer with the new cones and comparing this data to measurements provided by the manufacturer. The new coupling cones will make the FUS transducers more ergonomic for use in stimulating the spinal cord in an animal model.

Published

2022

32. Evaluating the Effects of Cerebrospinal Fluid Protein Content on the Performance of Differential Pressure Valves and Antisiphon Devices Using a Novel Benchtop Shunting Model

Author

Roger Bayston, Ian Suk, Hannah Antoine, Betty Tyler, Richard Um, Wataru Ishida, Risheng Xu, Xiaobu Ye, Riccardo Serra, Angad Grewal, Francesca Kroll, Kelly Beharry, Arba Cecia, Alexander Perdomo-Pantoja, Mark Luciano, Francis Loth, Audrey Monroe, Noah Gorelick, and Rajiv R. Iyer

Subjects

Supine position, Intracranial Pressure, business.industry, medicine.medical_treatment, Hydrostatic pressure, Models, Cardiovascular, Equipment Design, medicine.disease, Cerebrospinal Fluid Shunts, Hydrocephalus, Shunting, Flow control (fluid), Cerebrospinal fluid, Cerebrospinal Fluid Pressure, Humans, Medicine, Surgery, Neurology (clinical), business, Saline, Shunt (electrical), Biomedical engineering

Abstract

Background Hydrocephalus is managed by surgically implanting flow-diversion technologies such as differential pressure valves and antisiphoning devices; however, such hardware is prone to failure. Extensive research has tested them in flow-controlled settings using saline or de-aerated water, yet little has been done to validate their performance in a setting recreating physiologically relevant parameters, including intracranial pressures, cerebrospinal fluid (CSF) protein content, and body position. Objective To more accurately chart the episodic drainage characteristics of flow-diversion technology. A gravity-driven benchtop model of flow was designed and tested continuously during weeks-long trials. Methods Using a hydrostatic pressure gradient as the sole driving force, interval flow rates of 6 valves were examined in parallel with various fluids. Daily trials in the upright and supine positions were run with fluid output collected from distal catheters placed at alternating heights for extended intervals. Results Significant variability in flow rates was observed, both within specific individual valves across different trials and among multiple valves of the same type. These intervalve and intravalve variabilities were greatest during supine trials and with increased protein. None of the valves showed evidence of overt obstruction during 30 d of exposure to CSF containing 5 g/L protein. Conclusion Day-to-day variability of ball-in-cone differential pressure shunt valves may increase overdrainage risk. Narrow-lumen high-resistance flow control devices as tested here under similar conditions appear to achieve more consistent flow rates, suggesting their use may be advantageous, and did not demonstrate any blockage or trend of decreasing flow over the 3 wk of chronic use.

Published

2020

33. Minimizing cotton retention in neurosurgical procedures: which imaging modality can help?

Author

Micah Belzberg, Niki Tselepidakis, Cristina Madalo, Henry Brem, Noah Gorelick, Sean Glaister, Collin Shale, Judy Huang, Zachary Buono, Ian Suk, Benjamin Garlow, Alexandra Szwec, Isabella Ferrara, William Zhu, Betty Tyler, James Pitingolo, Renee Liu, Amir Manbachi, Brian Y. Hwang, Camilo A. Molina, Arushi Tandon, George Coles, Thomas Benassi, and Raphael Bechtold

Subjects

medicine.medical_specialty, Modality (human–computer interaction), business.industry, Radiography, Ultrasound, Cotton balls, Brain tissue, Article, Parenchyma, medicine, Ultrasound imaging, Neurosurgery, Radiology, business

Abstract

Cotton balls are used in neurosurgical procedures to assist with hemostasis and improve vision within the operative field. Although the surgeon can reshape pieces of cotton for multiple intraoperative uses, this customizability and scale also places them at perpetual risk of being lost, as blood-soaked cotton balls are visually similar to raw brain tissue. Retained surgical cotton can induce potentially life-threatening immunologic responses, impair postoperative imaging, lead to a textiloma or misdiagnosis, and/or require reoperation. This study investigated three imaging modalities (optical, acoustic, and radiographic) to find the most effective method of identifying foreign bodies during neurosurgery. First, we examined the use of dyes to increase contrast between cotton and surrounding parenchyma (optical approach). Second, we explored the ability to distinguish surgical cotton on or below the tissue surface from brain parenchyma using ultrasound imaging (acoustic approach). Lastly, we analyzed the ability of radiography to differentiate between brain parenchyma and cotton. Our preliminary testing demonstrated that dark-colored cotton is significantly more identifiable than white cotton on the surface level. Additional testing revealed that cotton has noticeable different acoustic characteristics (eg, speed of sound, absorption) from neural tissue, allowing for enhanced contrast in applied ultrasound imaging. Radiography, however, did not present sufficient contrast, demanding further examination. These solutions have the potential to significantly reduce the possibility of intraoperative cotton retention both on and below the surface of the brain, while still providing surgeons with traditional cotton material properties without affecting the surgical workflow.

Published

2022

34. DESIGN OF AN ULTRASOUND PROBE HOLDER TO MINIMIZE MOTION ARTIFACT DURING SONOGRAPHY

Author

Molly Acord, Betty Tyler, Nicholas Theodore, Ana Ainechi, Smruti Mahapatra, Fariba Aghabaglou, Tarana Parvez Kaovasia, Sufia Ainechi, Eli J. Curry, and Amir Manbachi

Subjects

Functional imaging, Artifact (error), Ultrasound probe, business.industry, Computer science, Ultrasound, business, Intraoperative imaging, Article, Biomedical engineering

Abstract

Standard diagnostic ultrasound imaging procedures heavily rely on a sonographer for image acquisition. Given the ultrasound probe is manually manipulated by the sonographer, there is a potential for noise artifacts like blurry acquired images caused by involuntary hand movements. Certain surgical procedures can also cause patients to exhibit involuntary “jumping” movements while on the operating table leading to further deterioration in ultrasound image quality. In this study, we attempt to mitigate these problems by fabricating a 3D-printed ultrasound probe holder. Due to the lightweight nature of the device, it can attach to surgical retractors without influencing the functionality of the retractor. Therefore, the 3D printed probe holder not only reduces relative motion between the probe and the patient, but also reduce the need for a sonographer during complex surgeries.

Published

2022

35. Dendrimer Technology in Glioma: Functional Design and Potential Applications

Author

Safwan Alomari, Andrew Hersh, Hallie Gaitsch, and Betty Tyler

Subjects

Cancer Research, Oncology

Abstract

Novel therapeutic and diagnostic methods are sorely needed for gliomas, which contribute yearly to hundreds of thousands of cancer deaths worldwide. Despite the outpouring of research efforts and funding aimed at improving clinical outcomes for patients with glioma, the prognosis for high-grade glioma, and especially glioblastoma, remains dire. One of the greatest obstacles to improving treatment efficacy and destroying cancer cells is the safe delivery of chemotherapeutic drugs and biologics to the tumor site at a high enough dose to be effective. Over the past few decades, a burst of research has leveraged nanotechnology to overcome this obstacle. There has been a renewed interest in adapting previously understudied dendrimer nanocarriers for this task. Dendrimers are small, highly modifiable, branched structures featuring binding sites for a variety of drugs and ligands. Recent studies have demonstrated the potential for dendrimers and dendrimer conjugates to effectively shuttle therapeutic cargo to the correct tumor location, permeate the tumor, and promote apoptosis of tumor cells while minimizing systemic toxicity and damage to surrounding healthy brain tissue. This review provides a primer on the properties of dendrimers; outlines the mechanisms by which they can target delivery of substances to the site of brain pathology; and delves into current trends in the application of dendrimers to drug and gene delivery, and diagnostic imaging, in glioma. Finally, future directions for translating these in vitro and in vivo findings to the clinic are discussed.

Published

2023

36. Combined intracranial Acriflavine, temozolomide and radiation extends survival in a rat glioma model

Author

Riccardo Serra, Antonella Mangraviti, Noah L. Gorelick, Tovi Shapira-Furman, Safwan Alomari, Arba Cecia, Namrata Darjee, Henry Brem, Yakir Rottenberg, Abraham J. Domb, and Betty Tyler

Subjects

Drug Implants, Brain Neoplasms, Cell Survival, Polymers, Pharmaceutical Science, Apoptosis, Radiotherapy Dosage, General Medicine, Glioma, Combined Modality Therapy, Xenograft Model Antitumor Assays, Rats, Inbred F344, Rats, Survival Rate, Cell Line, Tumor, Absorbable Implants, Temozolomide, Animals, Acriflavine, Biotechnology

Abstract

Glioblastomas have been historically difficult to treat with poor long-term survival. With novel strategies focused on targeting hypoxia-inducible factor (HIF) regulatory pathways, recent evidence has shown that Acriflavine (ACF) can effectively target glioma invasiveness and recurrence. However, local delivery of ACF and its combinatory effects with Temozolomide (TMZ) and radiation therapy (XRT) have not yet been optimized. In this study we test a novel polymeric matrix that can gradually release ACF at the tumor bed site in combination with systemic TMZ and XRT. In vitro cytotoxicity assays of ACF in combination with TMZ and XRT were performed on rodent and human cell lines with CCK-8 and flow cytometry. In vitro drug release was measured and intracranial safety was assessed in tumor-free animals. Finally, efficacy was assessed in an intracranial gliosarcoma model and combination therapy with TMZ and XRT evaluated. Combination therapy of ACF, TMZ, and XRT was able to reduce cell viability and induce apoptosis in glioma cells. In vitro and in vivo release of ACF was measured in benchtop and animal models. Efficacy was established in an in vivo gliosarcoma model in which intracranial ACF (p 0.01) significantly improved median survival and the combination therapy of ACF, TMZ and XRT (p 0.01) significantly improved median survival and led to long-term survival (LTS). We provide evidence that ACF, combined with TMZ and XRT, led to LTS in an intracranial model of rat gliosarcoma. These findings, in combination with the use of a novel polymeric matrix that allows more gradual drug delivery, constitute a first step in the translation of this novel strategy to human use.

Published

2021

37. High-Intensity Focused Ultrasound: A Review of Mechanisms and Clinical Applications

Author

Jordan J. Green, Ian Suk, Jayanidhi Kedda, Betty Tyler, and Vismaya S Bachu

Subjects

Extracorporeal Shockwave Therapy, medicine.medical_specialty, Modality (human–computer interaction), Therapeutic ultrasound, business.industry, medicine.medical_treatment, Ultrasound, Biomedical Engineering, High-intensity focused ultrasound, Article, Drug Delivery Systems, Treatment modality, Central Nervous System Diseases, Neoplasms, medicine, Medical imaging, Animals, Humans, Medical physics, Biomedical technology, business, Organ system, Ultrasonography

Abstract

High Intensity Focused Ultrasound (HIFU) is an emerging and increasingly useful modality in the treatment of cancer and other diseases. Although traditional use of ultrasound at lower frequencies has primarily been for diagnostic imaging purposes, the development of HIFU has allowed this particular modality to expand into therapeutic use. This non-invasive and acoustic method involves the use of a piezoelectric transducer to deliver high-energy pulses in a spatially coordinated manner, while minimizing damage to tissue outside the target area. This review describes the history of the development of diagnostic and therapeutic ultrasound and explores the biomedical applications utilizing HIFU technology including thermally ablative treatment, therapeutic delivery mechanisms, and neuromodulatory phenomena. The application of HIFU across various tumor types in multiple organ systems is explored in depth, with particular attention to successful models of HIFU in the treatment of various medical conditions. Basic mechanisms, preclinical models, previous clinical use, and ongoing clinical trials are comparatively discussed. Recent advances in HIFU across multiple medical fields reveal the growing importance of this biomedical technology for the care of patients and for the development of possible pathways for the future use of HIFU as a commonplace treatment modality.

Published

2021

38. Multi-layered core-sheath fiber membranes for controlled drug release in the local treatment of brain tumor

Author

Daewoo Han, Riccardo Serra, Charles G. Eberhart, Noah Gorelick, Betty Tyler, Umailla Fatima, Henry Brem, and Andrew J. Steckl

Subjects

0301 basic medicine, Drug, Biodistribution, Polymers, medicine.medical_treatment, media_common.quotation_subject, Brain tumor, lcsh:Medicine, Antineoplastic Agents, 02 engineering and technology, Article, Biomaterials, 03 medical and health sciences, Drug Delivery Systems, In vivo, Absorbable Implants, medicine, Animals, Cytotoxicity, lcsh:Science, media_common, Carmustine, Chemotherapy, Multidisciplinary, Brain Neoplasms, Chemistry, lcsh:R, Membranes, Artificial, 021001 nanoscience & nanotechnology, medicine.disease, Rats, Inbred F344, Rats, Drug Liberation, 030104 developmental biology, Surgical oncology, Delayed-Action Preparations, Drug delivery, Cancer research, Female, lcsh:Q, Glioblastoma, 0210 nano-technology, medicine.drug

Abstract

Interstitial chemotherapy plays a pivotal role in the treatment of glioblastoma multiforme (GBM), an aggressive form of primary brain cancer, by enhancing drug biodistribution to the tumor and avoiding systemic toxicities. The use of new polymer structures that extend the release of cytotoxic agents may therefore increase survival and prevent recurrence. A novel core-sheath fiber loaded with the drug carmustine (BCNU) was evaluated in an in vivo brain tumor model. Three-dimensional discs were formed from coaxially electrospun fiber membranes and in vitro BCNU release kinetics were measured. In vivo survival was assessed following implantation of discs made of compressed core-sheath fibers (NanoMesh) either concurrently with or five days after intracranial implantation of 9L gliosarcoma. Co-implantation of NanoMesh and 9L gliosarcoma resulted in statistically significant long-term survival (>150 days). Empty control NanoMesh confirmed the safety of these novel implants. Similarly, Day 5 studies showed significant median, overall, and long-term survival rates, suggesting optimal control of tumor growth, confirmed with histological and immunohistochemical analyses. Local chemotherapy by means of biodegradable NanoMesh implants is a new treatment paradigm for the treatment for brain tumors. Drug delivery with coaxial core-sheath structures benefits from high drug loading, controlled long-term release kinetics, and slow polymer degradation. This represents a promising evolution for the current treatment of GBM.

Published

2019

39. Local Delivery of the Poly-ADP-Ribose-Polymerase-Inhibitor Olaparib From a Biodegradable Paste Potentiates Radiotherapy and Prolongs Survival

Author

Kevin M. Shakesheff, Gareth J. Veal, Henry Brem, Ruman Rahman, Stuart Smith, Noah Gorelick, Riccardo Serra, Betty Tyler, Jonathan Rowlinson, and Richard Grundy

Subjects

Temozolomide, business.industry, Poly ADP ribose polymerase, medicine.medical_treatment, Poly (ADP-Ribose) Polymerase Inhibitor, Olaparib, Radiation therapy, chemistry.chemical_compound, chemistry, Apoptosis, Ribose, medicine, Cancer research, Surgery, Neurology (clinical), business, Etoposide, medicine.drug

Published

2019

40. Captopril as an Adjuvant to Temozolomide Prolongs Survival in a Rat Intracranial Gliosarcoma Model via Downregulation of Matrix Metalloproteinase-2

Author

Yuan Wang, Leon Pinheiro, Alexander Perdomo-Pantoja, Iddo Paldor, Antonella Mangraviti, Veronica Vigilar, Henry Brem, Joshua Casaos, and Betty Tyler

Subjects

Temozolomide, Gliosarcoma, business.industry, medicine.medical_treatment, Captopril, Matrix metalloproteinase, medicine.disease, Downregulation and upregulation, medicine, Cancer research, Surgery, Neurology (clinical), business, Adjuvant, medicine.drug

Published

2019

41. Overall Survival in Malignant Glioma Is Significantly Prolonged by Neurosurgical Delivery of Etoposide and Temozolomide from a Thermo-Responsive Biodegradable Paste

Author

Gareth J. Veal, Toby W.A. Gould, A.A. Ritchie, Stuart Smith, Henry Brem, Riccardo Serra, Kevin M. Shakesheff, Betty Tyler, Ruman Rahman, Philip Berry, Noah Gorelick, Nicolas Skuli, John Choi, Richard Grundy, Annette Otto, Jonathan Rowlinson, and Maria de los Angeles Estevez-Cebrero

Subjects

0301 basic medicine, Cancer Research, Polyesters, medicine.medical_treatment, macromolecular substances, Polyethylene Glycols, 03 medical and health sciences, chemistry.chemical_compound, Drug Delivery Systems, 0302 clinical medicine, Cell Line, Tumor, Glioma, Antineoplastic Combined Chemotherapy Protocols, PEG ratio, Temozolomide, medicine, Animals, Humans, Etoposide, Drug Carriers, Chemotherapy, Drug delivery, Efficacy, Etoposide, Glioma, PLGA/PEG, Temozolomide, technology, industry, and agriculture, medicine.disease, Delivery mode, Xenograft Model Antitumor Assays, Disease Models, Animal, Drug Liberation, PLGA, Treatment Outcome, 030104 developmental biology, Oncology, chemistry, 030220 oncology & carcinogenesis, Cancer research, Nanoparticles, Drug carrier, medicine.drug

Abstract

Purpose: High-grade glioma (HGG) treatment is limited by the inability of otherwise potentially efficacious drugs to penetrate the blood–brain barrier. We evaluate the unique intracavity delivery mode and translational potential of a blend of poly(DL-lactic acid-co-glycolic acid; PLGA) and poly(ethylene glycol; PEG) paste combining temozolomide and etoposide to treat surgically resected HGG. Experimental Design: To prolong stability of temozolomide prodrug, combined in vitro drug release was quantitatively assessed from low pH–based PLGA/PEG using advanced analytic methods. In vitro cytotoxicity was measured against a panel of HGG cell lines and patient-derived cultures using metabolic assays. In vivo safety and efficacy was evaluated using orthotopic 9L gliosarcoma allografts, previously utilized preclinically to develop Gliadel. Results: Combined etoposide and temozolomide in vitro release (22 and 7 days, respectively) was achieved from a lactic acid–based PLGA/PEG paste, used to enhance stability of temozolomide prodrug. HGG cells from central-enhanced regions were more sensitive to each compound relative to primary lines derived from the HGG-invasive margin. Both drugs retained cytotoxic capability upon release from PLGA/PEG. In vivo studies revealed a significant overall survival benefit in postsurgery 9L orthotopic gliosarcomas, treated with intracavity delivered PLGA/PEG/temozolomide/etoposide and enhanced with adjuvant radiotherapy. Long-term survivorship was observed in over half the animals with histologic confirmation of disease-free brain. Conclusions: The significant survival benefit of intracavity chemotherapy demonstrates clinical applicability of PLGA/PEG paste-mediated delivery of temozolomide and etoposide adjuvant to radiotherapy. PLGA/PEG paste offers a future platform for combination delivery of molecular targeted compounds.

Published

2019

42. Evaluation of an in vivo model for ventricular shunt infection: a pilot study using a novel antimicrobial-loaded polymer

Author

Betty Tyler, Karen C. Carroll, Audrey Monroe, Caroline M. Garrett, Rajiv R. Iyer, Noah Gorelick, Sean T. Zuckerman, Horst A. von Recum, Ari M. Blitz, Mark G. Luciano, Jeffrey R. Capadona, and Sarah E. Beck

Subjects

Male, medicine.medical_specialty, Microbiological culture, Polymers, medicine.drug_class, Antibiotics, Pilot Projects, Ventriculoperitoneal Shunt, Article, 03 medical and health sciences, Dogs, 0302 clinical medicine, Anti-Infective Agents, In vivo, Ventriculitis, Animals, Medicine, business.industry, General Medicine, Staphylococcal Infections, medicine.disease, Surgery, Hydrocephalus, Disease Models, Animal, Catheter, 030220 oncology & carcinogenesis, Equipment Contamination, Vancomycin, business, 030217 neurology & neurosurgery, Shunt (electrical), medicine.drug

Abstract

OBJECTIVEVentricular shunt infection remains an issue leading to high patient morbidity and cost, warranting further investigation. The authors sought to create an animal model of shunt infection that could be used to evaluate possible catheter modifications and innovations.METHODSThree dogs underwent bilateral ventricular catheter implantation and inoculation with methicillin-sensitive Staphylococcus aureus (S. aureus). In 2 experimental animals, the catheters were modified with a polymer containing chemical “pockets” loaded with vancomycin. In 1 control animal, the catheters were polymer coated but without antibiotics. Animals were monitored for 9 to 11 days, after which the shunts were explanted. MRI was performed after shunt implantation and prior to catheter harvest. The catheters were sonicated prior to microbiological culture and also evaluated by electron microscopy. The animals’ brains were evaluated for histopathology.RESULTSAll animals underwent successful catheter implantation. The animals developed superficial wound infections, but no neurological deficits. Imaging demonstrated ventriculitis and cerebral edema. Harvested catheters from the control animal demonstrated > 104 colony-forming units (CFUs) of S. aureus. In the first experimental animal, one shunt demonstrated > 104 CFUs of S. aureus, but the other demonstrated no growth. In the second experimental animal, one catheter demonstrated no growth, and the other grew trace S. aureus. Brain histopathology revealed acute inflammation and ventriculitis in all animals, which was more severe in the control.CONCLUSIONSThe authors evaluated an animal model of ventricular shunting and reliably induced features of shunt infection that could be microbiologically quantified. With this model, investigation of pathophysiological and imaging correlates of infection and potentially beneficial shunt catheter modifications is possible.

Published

2019

43. Biodegradable wafers releasing Temozolomide and Carmustine for the treatment of brain cancer

Author

Michael A. Peters, Yakir Rottenberg, Abraham J. Domb, Noah Gorelick, Arba Cecia, Tovi Shapira-Furman, Robert Langer, Henry Brem, Marisol Doglioli, Riccardo Serra, Betty Tyler, Valentina Tagliaferri, and Awanish Kumar

Subjects

Drug, Gliosarcoma, Polyesters, media_common.quotation_subject, Brain tumor, Pharmaceutical Science, 02 engineering and technology, Pharmacology, 03 medical and health sciences, chemistry.chemical_compound, Polylactic Acid-Polyglycolic Acid Copolymer, In vivo, Antineoplastic Combined Chemotherapy Protocols, Temozolomide, medicine, Animals, Wafer, Antineoplastic Agents, Alkylating, 030304 developmental biology, media_common, Drug Implants, 0303 health sciences, Carmustine, Brain Neoplasms, business.industry, 021001 nanoscience & nanotechnology, medicine.disease, Rats, Inbred F344, PLGA, chemistry, Delayed-Action Preparations, Female, Glioblastoma, 0210 nano-technology, business, Decanoic Acids, medicine.drug

Abstract

Glioblastoma multiforme (GBM) has few clinically approved therapeutic regimens. One of these therapeutic options includes placing biodegradable wafers releasing BCNU (Gliadel®) into the tumor bed at the time of surgical removal of the tumor. Due to the significant benefit this polymer technology has had clinically, we have prepared wafers releasing Temozolomide (TMZ), an anticancer drug used systemically for treating GBM. TMZ delivered via polymer wafer could be used as a complementary treatment with or as an alternative to Gliadel®. TMZ is an alkylating agent which is water soluble. To remain comparable with the preclinical studies that led to Gliadel® the same size of wafers were formulated with TMZ. Wafers were loaded with 50% w/w TMZ in poly(lactic acid-glycolic acid) (PLGA) and showed reliable release of high dose TMZ for a period of 4 weeks. To achieve this 30-day release of the highly water soluble drug, we developed an encapsulation method, where the drug powder was first coated with the polymer to form core-shell particles in which the coating shell served as a rate controlling membrane for the drug particles. Wafers were also made with a co-loading of TMZ and BCNU. All wafers were tested in vivo by treating an intracranial 9 L gliosarcoma model in F344 rats. Rats that were either untreated or treated with blank wafer died within 11 days while the median survival for rats treated with systemic TMZ was 18 days. The group that received the BCNU alone wafer had a median survival of 15 days, the group that received the TMZ wafer alone had a median survival of 19 days, and the group treated with the BCNU-TMZ wafer had a median survival of 28 days with 25% of the animals living long term (p .0038 vs. Control; p .001 vs. Blank Polymer). These findings demonstrate the potential of this newly designed wafer for treating GBM. Moreover, this concept, can pave the way for other drug combinations that may improve the clinical application of numerous agents to treat solid tumors.

Published

2019

44. A miniature multi-contrast microscope for functional imaging in freely behaving animals

Author

John B. Issa, Arvind P. Pathak, Alice L. Zou, Nitish V. Thakor, Betty Tyler, Hang Yu, Janaka Senarathna, Stacy Gil, Darian Hadjiabadi, Qihong Wang, and Callie Deng

Subjects

0301 basic medicine, Microscope, Materials science, genetic structures, Science, Brain tumor, General Physics and Astronomy, Monitoring, Ambulatory, Neuroimaging, 02 engineering and technology, Mice, SCID, General Biochemistry, Genetics and Molecular Biology, Article, law.invention, 03 medical and health sciences, Mice, law, medicine, Animals, lcsh:Science, Microscopy, Multidisciplinary, Miniaturization, Brain Neoplasms, General Chemistry, Equipment Design, 021001 nanoscience & nanotechnology, medicine.disease, Neurovascular bundle, eye diseases, Functional imaging, Mice, Inbred C57BL, 030104 developmental biology, Cerebral blood flow, GCaMP, lcsh:Q, Female, Tonotopy, 0210 nano-technology, Perfusion, Biomedical engineering

Abstract

Neurovascular coupling, cerebrovascular remodeling and hemodynamic changes are critical to brain function, and dysregulated in neuropathologies such as brain tumors. Interrogating these phenomena in freely behaving animals requires a portable microscope with multiple optical contrast mechanisms. Therefore, we developed a miniaturized microscope with: a fluorescence (FL) channel for imaging neural activity (e.g., GCaMP) or fluorescent cancer cells (e.g., 9L-GFP); an intrinsic optical signal (IOS) channel for imaging hemoglobin absorption (i.e., cerebral blood volume); and a laser speckle contrast (LSC) channel for imaging perfusion (i.e., cerebral blood flow). Following extensive validation, we demonstrate the microscope’s capabilities via experiments in unanesthetized murine brains that include: (i) multi-contrast imaging of neurovascular changes following auditory stimulation; (ii) wide-area tonotopic mapping; (iii) EEG-synchronized imaging during anesthesia recovery; and (iv) microvascular connectivity mapping over the life-cycle of a brain tumor. This affordable, flexible, plug-and-play microscope heralds a new era in functional imaging of freely behaving animals., Measuring multiple neurophysiologic variables usually requires bulky benchtop optical systems and working with anesthetized animals. Here the authors present a miniature portable microscope for neurovascular imaging in awake rodents, combining fluorescence, intrinsic optical signals and laser speckle contrast.

Published

2019

45. Design and Fabrication of a Focused Ultrasound Device for Minimallyinvasive Neurosurgery: Reporting a Second, Miniaturized and Mrcompatible Prototype with Steering Capabilities

Author

Tarana Parvez Kaovasia, Tim Xiong, Mark G. Luciano, Molly Acord, Kyle P. Morrison, Nao J. Gamo, Fariba Aghabaglou, Eli J. Curry, Betty Tyler, and Amir Manbachi

Subjects

medicine.medical_specialty, Fabrication, Computer science, business.industry, Ultrasound, Mr compatible, medicine, Neurosurgery, business, Article, Focused ultrasound, Biomedical engineering

Abstract

Many surgeons are faced with inoperable or only partially operable brain lesions, such as tumors. Even when surgery is feasible, patient outcomes are greatly affected by blood loss or infection. This has led many physicians toward non- or minimally-invasive surgery, which demands specialized toolkits. Focused ultrasound has great potential for assisting in such procedures due to its ability to focus a few centimeters away from the surface of the transducer. In a prior study, we developed a focused ultrasound prototype that could fit within a BrainPath trocar, specifically made for minimally invasive brain surgery. Here, we present the design and fabrication of a second prototype that reduces size, is MR-compatible, and has electronic steering capabilities.

Published

2021

46. Automatic detection of cotton balls during brain surgery: where deep learning meets ultrasound imaging to tackle foreign objects

Author

Shenandoah Robinson, Yohannes Tsehay, Jeong Hun Kim, Betty Tyler, Molly Acord, Christina Diana Ghinda, Henry Brem, Judy Huang, Ana Ainechi, Venkat Kuppoor, Smruti Mahapatra, Jennifer K. Son, Aliaksei Pustavoitau, Amir Manbachi, Nicholas Theodore, Eli J. Curry, Manish Balamurugan, Fariba Aghabaglou, Kathryn Chung, and Tarana Parvez Kaovasia

Subjects

medicine.medical_specialty, Handheld ultrasound, business.industry, Computer science, Deep learning, Ultrasound, Cotton balls, Article, Object detection, Textilomas, Surgery, medicine, Ultrasound imaging, Ball (bearing), Artificial intelligence, business, human activities, psychological phenomena and processes

Abstract

Cotton balls are a versatile and efficient tool commonly used in neurosurgical procedures to absorb fluids and manipulate delicate tissues. However, the use of cotton balls is accompanied by the risk of accidental retention in the brain after surgery. Retained cotton balls can lead to dangerous immune responses and potential complications, such as adhesions and textilomas. In a previous study, we showed that ultrasound can be safely used to detect cotton balls in the operating area due to the distinct acoustic properties of cotton compared with the acoustic properties of surrounding tissue. In this study, we enhance the experimental setup using a 3D-printed custom depth box and a Butterfly IQ handheld ultrasound probe. Cotton balls were placed in variety of positions to evaluate size and depth detectability limits. Recorded images were then analyzed using a novel algorithm that implements recently released YOLOv4, a state-of-the-art, real-time object recognition system. As per the radiologists’ opinion, the algorithm was able to detect the cotton ball correctly 61% of the time, at approximately 32 FPS. The algorithm could accurately detect cotton balls up to 5mm in diameter, which corresponds to the size of surgical balls used by neurosurgeons, making the algorithm a promising candidate for regular intraoperative use.

Published

2021

47. The development of Smart Hospital Assistant: integrating artificial intelligence and a voice-user interface for improved surgical outcomes

Author

Amir Manbachi, Fariba Aghabaglou, Japesh Patel, Eli J. Curry, Jeong Hun Kim, Brian Y. Hwang, Nicholas Theodore, Yohannes Tsehay, Jeff Ehresman, Richard Um, Rajiv R Iyer, Ana Ainechi, Betty Tyler, Smruti Mahapatra, and Jonathan Liu

Subjects

Multimedia, business.industry, Computer science, Health technology, Surgical operation, computer.software_genre, Remote assistance, Article, Patient safety, Voice user interface, Smart hospital, Health care, Operating time, business, computer

Abstract

Efficiency and patient safety are top priorities in any surgical operation. One effective way to achieve these objectives is automating many of the logistical and routine tasks that occur in the operating room. Inspired by smart assistant technology already commonplace in the consumer sector, we engineered the Smart Hospital Assistant (SHA), a smart, voice-controlled virtual assistant that handles natural speech recognition while executing a plurality of functions to aid surgery. Simulated surgeries showed that the SHA reduced operating time, optimized surgical staff resources, and reduced the number of major touch points that can lead to surgical site infections. The SHA not only shows its potential in the operating room, but also in other healthcare environments that may benefit from having virtual smart assistant technology.

Published

2021

48. CDKS Blockade Enhances In Vivo Efficacy of EGFR Inhibition in Chordomas

Author

Riccardo Serra, Tianna Zhao, Peter C. Burger, Michelle Guo, Gary L. Gallia, Christine L. Hann, Lisa M. Rooper, and Betty Tyler

Subjects

biology, Cyclin-dependent kinase, In vivo, Chemistry, Egfr inhibition, biology.protein, Cancer research, Blockade

Published

2021

49. Captopril inhibits Matrix Metalloproteinase-2 and extends survival as a temozolomide adjuvant in an intracranial gliosarcoma model

Author

Sakibul Huq, Timothy F. Witham, Antonella Mangraviti, Betty Tyler, Yuan Wang, Henry Brem, Leon Pinheiro, Iddo Paldor, Joshua Casaos, Alexander Perdomo-Pantoja, and Veronica Vigilar

Subjects

Gliosarcoma, Captopril, Combination therapy, medicine.medical_treatment, Cell Culture Techniques, Angiotensin-Converting Enzyme Inhibitors, Pharmacology, 03 medical and health sciences, 0302 clinical medicine, In vivo, Glioma, medicine, Temozolomide, Tumor Cells, Cultured, Animals, Antineoplastic Agents, Alkylating, business.industry, Brain Neoplasms, General Medicine, medicine.disease, Rats, Inbred F344, Rats, Disease Models, Animal, 030220 oncology & carcinogenesis, Immunohistochemistry, Matrix Metalloproteinase 2, Surgery, Female, Neurology (clinical), business, Adjuvant, 030217 neurology & neurosurgery, circulatory and respiratory physiology, medicine.drug

Abstract

Background Captopril is a well-characterized, FDA-approved drug that has demonstrated promise as a repurposed oncology therapeutic. Captopril’s known anti-cancer effects include inhibition of Matrix Metalloproteinase-2 (MMP-2), an endopeptidase which selectively breaks down the extracellular matrix to promote cell migration. MMP-2 is a known therapeutic target in gliomas, tumors with significant clinical need. Using an aggressive gliosarcoma model, we assessed captopril’s effects on MMP-2 expression in vitro and in vivo as well as its efficacy as an adjuvant in combination therapy regimens in vivo. Methods Following captopril treatment, MMP-2 protein expression and migratory capabilities of 9 L gliosarcoma cells were assessed in vitro via western blots and scratch wound assays, respectively. Rats were intracranially implanted with 9 L gliosarcoma tumors, and survival was assessed in the following groups: control; captopril (30 mg/kg/day); temozolomide (TMZ) (50 mg/kg/day), and captopril+TMZ. In vivo experiments were accompanied by immunohistochemistry for MMP-2 from brain tissue. Results In vitro, captopril decreased MMP-2 protein expression and reduced migratory capacity in 9 L gliosarcoma cells. In a gliosarcoma animal model, captopril decreased MMP-2 protein expression and extended survival as a TMZ adjuvant relative to untreated controls, captopril monotherapy, and TMZ monotherapy groups (27.5 versus 14 (p Conclusions Captopril decreases gliosarcoma cell migration, which may be mediated by reduction in MMP-2 protein expression. Captopril provided a survival advantage as a TMZ adjuvant in a rat intracranial gliosarcoma model. Captopril may represent a promising potential adjuvant to TMZ therapy in gliosarcoma as a modulator of the MMP-2 pathway.

Published

2021

50. Disulfiram and copper combination therapy targets NPL4, cancer stem cells and extends survival in a medulloblastoma model

Author

Renyuan Bai, Henry Brem, Alessandro Olivi, Eric M. Jackson, Joshua Casaos, Betty Tyler, Sakibul Huq, Arba Cecia, Charles G. Eberhart, Antonella Mangraviti, Riccardo Serra, Tianna Zhao, and Noah Gorelick

Subjects

Carcinogenesis, Cancer Treatment, Aldehyde dehydrogenase, Apoptosis, Toxicology, Pathology and Laboratory Medicine, Pediatrics, Animal Cells, Cancer Stem Cells, Disulfiram, Medicine and Health Sciences, Multidisciplinary, biology, Cell Death, Chemistry, Brain Neoplasms, Stem Cells, Cell Cycle, Oncology, Cell Processes, Neoplastic Stem Cells, Medicine, Cellular Types, medicine.drug, Research Article, Combination therapy, Blastoma, Science, Malignant Tumors, Cancer stem cell, In vivo, medicine, Animals, Clonogenic assay, Cell Proliferation, Medulloblastoma, Toxicity, Cancers and Neoplasms, Biology and Life Sciences, Cell Biology, Aldehyde Dehydrogenase, medicine.disease, biology.protein, Cancer research, Copper

Abstract

Background Medulloblastoma (MB) is the most common brain malignancy in children, and is still responsible for significant mortality and morbidity. The aim of this study was to assess the safety and efficacy of Disulfiram (DSF), an FDA-approved inhibitor of Aldehyde-Dehydrogenase (ALDH), and Copper (Cu++) in human SSH-driven and Group 3 MB. The molecular mechanisms, effect on cancer-stem-cells (CSC) and DNA damage were investigated in xenograft models. Methods The cytotoxic and anti-CSC effects of DSF/Cu++ were evaluated with clonogenic assays, flow-cytometry, immunofluorescence, western-blotting. ONS76, UW228 (SHH-driven with Tp53m), D425med, D283 and D341 (Group 3) cell-lines were used. In vivo survival and nuclear protein localization protein-4 (NPL4), Ki67, Cleaved-Caspase-3, GFAP and NeuN expression were assessed in two Group 3 MB xenografts with immunohistochemistry and western-blotting. Results Significant in vitro cytotoxicity was demonstrated at nanomolar concentrations. DSF/Cu++ induced cell-death through NPL4 accumulation in cell-nucleus and buildup of poly-ubiquitylated proteins. Flow-cytometry demonstrated a significant decrease in ALDH+, Nestin+ and CD133+ following treatment, anti-CSC effect was confirmed in vitro and in vivo. DSF/Cu++ prolonged survival, and increased nuclear NPL4 expression in vivo. Conclusions Our data suggest that this combination may serve as a novel treatment, as monotherapy or in combination with existing therapies, for aggressive subtypes of pediatric MB.

Published

2021