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1. Evaluation of patients with severe pulmonary hypertension and a range of comorbidities prescribed inhaled treprostinil

Author

Aparna C. Swaminathan, Amber Meservey, Alice Parish, Cynthia L. Green, Kishan Parikh, Terry Fortin, Richard A. Krasuski, Jordan W. Whitson, Talal Dahhan, Yen-Rei Yu, Karla Kennedy, Susana Almeida-Peters, and Sudarshan Rajagopal

Subjects
pulmonary arterial hypertension, prostacyclin, World Symposium on Pulmonary Hypertension, pulmonary vasodilator, treprostinil, Surgery, RD1-811, Specialties of internal medicine, RC581-951
Abstract

Background: Patients with pulmonary arterial hypertension (PAH) and additional cardiac or pulmonary comorbidities have a poor prognosis and are frequently excluded from clinical trials. The purpose of this study was to evaluate outcomes of patients with pulmonary hypertension (PH) secondary to a range of World Symposium on PH (WSPH) groups treated with inhaled treprostinil (iTRE) in a real-world setting. Methods: Patients with PH who were started on treatment with iTRE at Duke University were classified by WSPH Group and included patients with Groups 1, 2, 3, combined Groups 2 and 3 (PH in the setting of left heart failure and chronic lung disease), Group 4, and Group 5 PH. Time to disease worsening, a composite of death, lung transplantation, or transition to intravenous prostacyclin was compared by WSPH Group, and iTRE treatment status using a multivariable Cox proportional hazards model adjusted for age, sex, and Registry to Evaluate Early and Long-Term PAH Disease Management Lite 2 risk score. Treatment with iTRE was defined as a time-varying covariate. Results: The cohort included 270 patients with PH: 30.6% Group 1; 10% Group 2; 32.2% Group 3; 11.1% combined Groups 2 and 3; and 15.9% with either Group 4 or 5 PH. At 3 and 6 months of follow-up, 24.8% and 38.9% of patients, respectively, were no longer treated with iTRE. Patients who discontinued treatment with iTRE had a significantly higher risk of disease worsening (adjusted hazard ratio: 5.02, 95% confidence interval: 3.44-7.31). There was no significant difference in disease worsening among WSPH Groups. Conclusions: In a real-world setting, many patients with PH secondary to a range of WSPH Groups tolerated treatment with iTRE. Future studies should phenotype patients with PH based on both comorbidities and therapeutic responsiveness.

Published
2024
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2. Improved efficacy against malignant brain tumors with EGFRwt/EGFRvIII targeting immunotoxin and checkpoint inhibitor combinations

Author

Vidyalakshmi Chandramohan, Xuhui Bao, Xin Yu, Scott Parker, Charlotte McDowall, Yen-Rei Yu, Patrick Healy, Annick Desjardins, Michael D. Gunn, Matthias Gromeier, Smita K. Nair, Ira H. Pastan, and Darell D. Bigner

Subjects
Immunotoxin, Immune checkpoint inhibitors, EGFR, T cells, Malignant gliomas, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Abstract Background D2C7-IT is a novel immunotoxin (IT) targeting wild-type epidermal growth factor receptor (EGFRwt) and mutant EGFR variant III (EGFRvIII) proteins in glioblastoma. In addition to inherent tumoricidal activity, immunotoxins induce secondary immune responses through the activation of T cells. However, glioblastoma-induced immune suppression is a major obstacle to an effective and durable immunotoxin-mediated antitumor response. We hypothesized that D2C7-IT-induced immune response could be effectively augmented in combination with αCTLA-4/αPD-1/αPD-L1 therapies in murine models of glioma. Methods To study this, we overexpressed the D2C7-IT antigen, murine EGFRvIII (dmEGFRvIII), in established glioma lines, CT-2A and SMA560. The reactivity and therapeutic efficacy of D2C7-IT against CT-2A-dmEGFRvIII and SMA560-dmEGFRvIII cells was determined by flow cytometry and in vitro cytotoxicity assays, respectively. Antitumor efficacy of D2C7-IT was examined in immunocompetent, intracranial murine glioma models and the role of T cells was assessed by CD4+ and CD8+ T cell depletion. In vivo efficacy of D2C7-IT/αCTLA-4/αPD-1 monotherapy or D2C7-IT+αCTLA-4/αPD-1 combination therapy was evaluated in subcutaneous unilateral and bilateral CT-2A-dmEGFRvIII glioma-bearing immunocompetent mice. Further, antitumor efficacy of D2C7-IT+αCTLA-4/αPD-1/αPD-L1/αTim-3/αLag-3/αCD73 combination therapy was evaluated in intracranial CT-2A-dmEGFRvIII and SMA560-dmEGFRvIII glioma-bearing mice. Pairwise differences in survival curves were assessed using the generalized Wilcoxon test. Results D2C7-IT effectively killed CT-2A-dmEGFRvIII (IC50 = 0.47 ng/mL) and SMA560-dmEGFRvIII (IC50 = 1.05 ng/mL) cells in vitro. Treatment of intracranial CT-2A-dmEGFRvIII and SMA560-dmEGFRvIII tumors with D2C7-IT prolonged survival (P = 0.0188 and P = 0.0057, respectively), which was significantly reduced by the depletion of CD4+ and CD8+ T cells. To augment antitumor immune responses, we combined D2C7-IT with αCTLA-4/αPD-1 in an in vivo subcutaneous CT-2A-dmEGFRvIII model. Tumor-bearing mice exhibited complete tumor regressions (4/10 in D2C7-IT+αCTLA-4 and 5/10 in D2C7-IT+αPD-1 treatment groups), and combination therapy-induced systemic antitumor response was effective against both dmEGFRvIII-positive and dmEGFRvIII-negative CT-2A tumors. In a subcutaneous bilateral CT-2A-dmEGFRvIII model, D2C7-IT+αCTLA-4/αPD-1 combination therapies showed dramatic regression of the treated tumors and measurable regression of untreated tumors. Notably, in CT-2A-dmEGFRvIII and SMA560-dmEGFRvIII intracranial glioma models, D2C7-IT+αPD-1/αPD-L1 combinations improved survival, and in selected cases generated cures and protection against tumor re-challenge. Conclusions These data support the development of D2C7-IT and immune checkpoint blockade combinations for patients with malignant glioma.

Published
2019
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3. Single-Cell Analysis Reveals Distinct Immune and Smooth Muscle Cell Populations that Contribute to Chronic Thromboembolic Pulmonary Hypertension

Author

Gayathri Viswanathan, Hélène Fradin Kirshner, Nour Nazo, Saba Ali, Asvin Ganapathi, Ian Cumming, Yonghua Zhuang, Issac Choi, Anmol Warman, Chanpreet Jassal, Susana Almeida-Peters, John Haney, David Corcoran, Yen-Rei Yu, and Sudarshan Rajagopal

Subjects
Pulmonary and Respiratory Medicine, Critical Care and Intensive Care Medicine
Published
2023

4. Determining the Architecture of Inflammation in Pulmonary Arterial Hypertension.

Author

Rajagopal, Sudarshan and Yen-Rei Yu

Subjects
PULMONARY arterial hypertension, PULMONARY hypertension, INFLAMMATION
Abstract

An editorial is presented on the pathogenesis of pulmonary arterial hypertension (PAH), emphasizing the role of inflammation and immunity, supported by evidence of immune dysregulation and increased biomarkers in PAH. Ferrian et al.'s study, provides a groundbreaking architectural map connecting immune subsets to pulmonary vascular remodeling, highlighting the presence of distinct microenvironments and a specific subset of monocyte-derived cells associated with PAH pathology.

Published
2024
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5. Single-Cell Analysis Reveals Distinct Immune and Smooth Muscle Cell Populations that Contribute to Chronic Thromboembolic Pulmonary Hypertension.

Author

Viswanathan, Gayathri, Kirshner, Hélène Fradin, Nazo, Nour, Ali, Saba, Ganapathi, Asvin, Cumming, Ian, Yonghua Zhuang, Choi, Issac, Warman, Anmol, Jassal, Chanpreet, Almeida-Peters, Susana, Haney, John, Corcoran, David, Yen-Rei Yu, and Rajagopal, Sudarshan

Subjects
CELL populations, MUSCLE cells, SMOOTH muscle, ENDARTERECTOMY, VASCULAR remodeling, PULMONARY hypertension, THROMBOEMBOLISM, PULMONARY embolism
Abstract

Rationale: Chronic thromboembolic pulmonary hypertension (CTEPH) is a sequela of acute pulmonary embolism (PE) in which the PE remodels into a chronic scar in the pulmonary arteries. This results in vascular obstruction, pulmonary microvasculopathy, and pulmonary hypertension. Objectives: Our current understanding of CTEPH pathobiology is primarily derived from cell-based studies limited by the use of specific cell markers or phenotypic modulation in cell culture. Therefore, our main objective was to identify the multiple cell types that constitute CTEPH thrombusy and to study their dysfunction. Methods: Here we used single-cell RNA sequencing of tissue removed at the time of pulmonary endarterectomy surgery from five patients to identify the multiple cell types. Using in vitro assays, we analyzed differences in phenotype between CTEPH thrombus and healthy pulmonary vascular cells. We studied potential therapeutic targets in cells isolated from CTEPH thrombus. Measurements and Main Results: Single-cell RNA sequencing identified multiple cell types, including macrophages, T cells, and smooth muscle cells (SMCs), that constitute CTEPH thrombus. Notably, multiple macrophage subclusters were identified but broadly split into two categories, with the larger group characterized by an upregulation of inflammatory signaling predicted to promote pulmonary vascular remodeling. CD41 and CD81 T cells were identified and likely contribute to chronic inflammation in CTEPH. SMCs were a heterogeneous population, with a cluster of myofibroblasts that express markers of fibrosis and are predicted to arise from other SMC clusters based on pseudotime analysis. Additionally, cultured endothelial, smooth muscle, and myofibroblast cells isolated from CTEPH fibrothrombotic material have distinct phenotypes from control cells with regard to angiogenic potential and rates of proliferation and apoptosis. Last, our analysis identified PAR1 (protease-activated receptor 1) as a potential therapeutic target that links thrombosis to chronic PE in CTEPH, with PAR1 inhibition decreasing SMC and myofibroblast proliferation and migration. Conclusions: These findings suggest a model for CTEPH similar to atherosclerosis, with chronic inflammation promoted by macrophages and T cells driving vascular remodeling through SMC modulation, and suggest new approaches for pharmacologically targeting this disease. [ABSTRACT FROM AUTHOR]

Published
2023
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6. Single-Cell Analysis Reveals Distinct Immune and Smooth Muscle Cell Populations that Contribute to Chronic Thromboembolic Pulmonary Hypertension

Author

Gayathri Viswanathan, Hélène Fradin Kirshner, Nour Nazo, Asvin Ganapathi, Ian Cummings, Issac Choi, Anmol Warman, Susana Almeida-Peters, John Haney, David Corcoran, Yen-Rei Yu, and Sudarshan Rajagopal

Abstract

Chronic thromboembolic pulmonary hypertension (CTEPH) is a sequelae of acute pulmonary embolism (PE) in which the PE remodels into a chronic scar in the pulmonary arteries. This results in vascular obstruction, small vessel arteriopathy and pulmonary hypertension. Our current understanding of CTEPH pathobiology is primarily derived from cell-based studies limited by the use of specific cell markers or phenotypic modulation in cell culture. Here we used single cell RNA sequencing (scRNAseq) of tissue removed at the time of pulmonary thromboendarterectomy (PTE) surgery to identify the multiple cell types, including macrophages, T cells, and smooth muscle cells, that comprise CTEPH thrombus. Notably, multiple macrophage subclusters were identified but broadly split into two categories, with the larger group characterized by an upregulation of inflammatory signaling predicted to promote pulmonary vascular remodeling. Both CD4+ and CD8+ T cells were identified and likely contribute to chronic inflammation in CTEPH. Smooth muscle cells were a heterogeneous population, with a cluster of myofibroblasts that express markers of fibrosis and are predicted to arise from other smooth muscle cell clusters based on pseudotime analysis. Additionally, cultured endothelial, smooth muscle and myofibroblast cells isolated from CTEPH thrombus have distinct phenotypes from control cells with regards to angiogenic potential and rates of proliferation and apoptosis. Lastly, our analysis identified protease-activated receptor 1 (PAR1) as a potential therapeutic target that links thrombosis to chronic PE in CTEPH, with PAR1 inhibition decreasing smooth muscle cell and myofibroblast proliferation and migration. These findings suggest a model for CTEPH similar to atherosclerosis, with chronic inflammation promoted by macrophages and T cells driving vascular remodeling through smooth muscle cell modulation, and suggest new approaches for pharmacologically targeting this disease.

Published
2022

7. NEDD9 Is a Novel and Modifiable Mediator of Platelet-Endothelial Adhesion in the Pulmonary Circulation.

Author

Alba, George A., Samokhin, Andriy O., Rui-Sheng Wang, Ying-Yi Zhang, Wertheim, Bradley M., Arons, Elena, Greenfield, Edward A., Slingsby, Martina H. Lundberg, Ceglowski, Julia R., Haley, Kathleen J., Bowman, Frederick P., Yen-Rei Yu, Haney, John. C., Eng, George, Mitchell, Richard N., Sheets, Anthony, Vargas, Sara O., Sachiko Seo, Channick, Richard N., and Leary, Peter J.

Subjects
MOLECULAR immunology, ENDOTHELIAL cells, PULMONARY circulation, BLOOD circulation, PULMONARY hypertension, BIOLOGICAL models, RESEARCH, PULMONARY embolism, CELL culture, ANIMAL experimentation, BLOOD platelets, RESEARCH methodology, CELL physiology, MEDICAL cooperation, EVALUATION research, CELLULAR signal transduction, COMPARATIVE studies, RESEARCH funding, EPITHELIAL cells, CARRIER proteins, MICE
Abstract

Rationale: Data on the molecular mechanisms that regulate platelet-pulmonary endothelial adhesion under conditions of hypoxia are lacking, but may have important therapeutic implications. Objectives: To identify a hypoxia-sensitive, modifiable mediator of platelet-pulmonary artery endothelial cell adhesion and thrombotic remodeling. Methods: Network medicine was used to profile protein-protein interactions in hypoxia-treated human pulmonary artery endothelial cells. Data from liquid chromatography-mass spectrometry and microscale thermophoresis informed the development of a novel antibody (Ab) to inhibit platelet-endothelial adhesion, which was tested in cells from patients with chronic thromboembolic pulmonary hypertension (CTEPH) and three animal models in vivo. Measurements and Main Results: The protein NEDD9 was identified in the hypoxia thrombosome network in silico. Compared with normoxia, hypoxia (0.2% O2) for 24 hours increased HIF-1α (hypoxia-inducible factor-1α)-dependent NEDD9 upregulation in vitro. Increased NEDD9 was localized to the plasma-membrane surface of cells from control donors and patients with CTEPH. In endarterectomy specimens, NEDD9 colocalized with the platelet surface adhesion molecule P-selectin. Our custom-made anti-NEDD9 Ab targeted the NEDD9-P-selectin interaction and inhibited the adhesion of activated platelets to pulmonary artery endothelial cells from control donors in vitro and from patients with CTEPH ex vivo. Compared with control mice, platelet-pulmonary endothelial aggregates and pulmonary hypertension induced by ADP were decreased in NEDD9-/- mice or wild-type mice treated with the anti-NEDD9 Ab, which also decreased chronic pulmonary thromboembolic remodeling in vivo. Conclusions: The NEDD9-P-selectin protein-protein interaction is a modifiable target with which to inhibit platelet-pulmonary endothelial adhesion and thromboembolic vascular remodeling, with potential therapeutic implications for patients with disorders of increased hypoxia signaling pathways, including CTEPH. [ABSTRACT FROM AUTHOR]

Published
2021
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8. Improved efficacy against malignant brain tumors with EGFRwt/EGFRvIII targeting immunotoxin and checkpoint inhibitor combinations.

Author

Chandramohan, Vidyalakshmi, Xuhui Bao, Xin Yu, Parker, Scott, McDowall, Charlotte, Yen-Rei Yu, Healy, Patrick, Desjardins, Annick, Gunn, Michael D., Gromeier, Matthias, Nair, Smita K., Pastan, Ira H., and Bigner, Darell D.

Subjects
BRAIN tumors, EPIDERMAL growth factor receptors, IPILIMUMAB, IMMUNE checkpoint proteins, GLIOMAS, T cells, METHYLGUANINE
Abstract

Background: D2C7-IT is a novel immunotoxin (IT) targeting wild-type epidermal growth factor receptor (EGFRwt) and mutant EGFR variant III (EGFRvIII) proteins in glioblastoma. In addition to inherent tumoricidal activity, immunotoxins induce secondary immune responses through the activation of T cells. However, glioblastoma-induced immune suppression is a major obstacle to an effective and durable immunotoxin-mediated antitumor response. We hypothesized that D2C7-IT-induced immune response could be effectively augmented in combination with αCTLA-4/αPD-1/αPD-L1 therapies in murine models of glioma. Methods: To study this, we overexpressed the D2C7-IT antigen, murine EGFRvIII (dmEGFRvIII), in established glioma lines, CT-2A and SMA560. The reactivity and therapeutic efficacy of D2C7-IT against CT-2A-dmEGFRvIII and SMA560- dmEGFRvIII cells was determined by flow cytometry and in vitro cytotoxicity assays, respectively. Antitumor efficacy of D2C7-IT was examined in immunocompetent, intracranial murine glioma models and the role of T cells was assessed by CD4+ and CD8+ T cell depletion. In vivo efficacy of D2C7-IT/αCTLA-4/αPD-1 monotherapy or D2C7-IT+αCTLA-4/ αPD-1 combination therapy was evaluated in subcutaneous unilateral and bilateral CT-2A-dmEGFRvIII glioma-bearing immunocompetent mice. Further, antitumor efficacy of D2C7-IT+αCTLA-4/αPD-1/αPD-L1/αTim-3/αLag-3/αCD73 combination therapy was evaluated in intracranial CT-2A-dmEGFRvIII and SMA560-dmEGFRvIII glioma-bearing mice. Pairwise differences in survival curves were assessed using the generalized Wilcoxon test. Results: D2C7-IT effectively killed CT-2A-dmEGFRvIII (IC50 = 0.47 ng/mL) and SMA560-dmEGFRvIII (IC50 = 1.05 ng/mL) cells in vitro. Treatment of intracranial CT-2A-dmEGFRvIII and SMA560-dmEGFRvIII tumors with D2C7-IT prolonged survival (P = 0.0188 and P = 0.0057, respectively), which was significantly reduced by the depletion of CD4+ and CD8+ T cells. To augment antitumor immune responses, we combined D2C7-IT with αCTLA-4/αPD-1 in an in vivo subcutaneous CT-2A-dmEGFRvIII model. Tumor-bearing mice exhibited complete tumor regressions (4/10 in D2C7-IT+αCTLA-4 and 5/10 in D2C7-IT+αPD-1 treatment groups), and combination therapy-induced systemic antitumor response was effective against both dmEGFRvIII-positive and dmEGFRvIII-negative CT-2A tumors. In a subcutaneous bilateral CT-2A-dmEGFRvIII model, D2C7-IT+αCTLA-4/αPD-1 combination therapies showed dramatic regression of the treated tumors and measurable regression of untreated tumors. Notably, in CT-2A-dmEGFRvIII and SMA560-dmEGFRvIII intracranial glioma models, D2C7-IT+αPD-1/αPD-L1 combinations improved survival, and in selected cases generated cures and protection against tumor re-challenge. Conclusions: These data support the development of D2C7-IT and immune checkpoint blockade combinations for patients with malignant glioma. [ABSTRACT FROM AUTHOR]

Published
2019
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10. Improving the Quality and Reproducibility of Flow Cytometry in the Lung: An Official American Thoracic Society Workshop Report.

Author

Tighe, Robert M., Redente, Elizabeth F., Yen-Rei Yu, Herold, Susanne, Sperling, Anne I., Curtis, Jeffrey L., Duggan, Ryan, Swaminathan, Suchitra, Hideki Nakano, Zacharias, William J., Janssen, William J., Freeman, Christine M., Brinkman, Ryan R., Singer, Benjamin D., Jakubzick, Claudia V., and Misharin, Alexander V.

Subjects
FLOW cytometry, LUNG diseases, REPRODUCIBLE research, CELLS, IMMUNOLOGIC diseases
Abstract

Defining responses of the structural and immune cells in biologic systems is critically important to understanding disease states and responses to injury. This requires accurate and sensitive methods to define cell types in organ systems. The principal method to delineate the cell populations involved in these processes is flow cytometry. Although researchers increasingly use flow cytometry, technical challenges can affect its accuracy and reproducibility, thus significantly limiting scientific advancements. This challenge is particularly critical to lung immunology, as the lung is readily accessible and therefore used in preclinical and clinical studies to define potential therapeutics. Given the importance of flow cytometry in pulmonary research, the American Thoracic Society convened a working group to highlight issues and technical challenges to the performance of high-quality pulmonary flow cytometry, with a goal of improving its quality and reproducibility. [ABSTRACT FROM AUTHOR]

Published
2019
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12. A novel role for primary cilia in airway remodeling.

Author

Trempus, Carol S., Weifeng Song, Lazrak, Ahmed, Zhihong Yu, Creighton, Judy R., Young, Bethany M., Heise, Rebecca L., Yen Rei Yu, Ingram, Jennifer L., Tighe, Robert M., Matalon, Sadis, and Garantziotis, Stavros

Subjects
ORGANELLES, HOMEOSTASIS, CARTILAGE cells
Abstract

Primary cilia (PC) are solitary cellular organelles that play critical roles in development, homeostasis, and disease pathogenesis by modulating key signaling pathways such as Sonic Hedgehog and calcium flux. The antenna-like shape of PC enables them also to facilitate sensing of extracellular and mechanical stimuli into the cell, and a critical role for PC has been described for mesenchymal cells such as chondrocytes. However, nothing is known about the role of PC in airway smooth muscle cells (ASMCs) in the context of airway remodeling. We hypothesized that PC on ASMCs mediate cell contraction and are thus integral in the remodeling process. We found that PC are expressed on ASMCs in asthmatic lungs. Using pharmacological and genetic methods, we demonstrated that PC are necessary for ASMC contraction in a collagen gel three-dimensional model both in the absence of external stimulus and in response to the extracellular component hyaluronan. Mechanistically, we demonstrate that the effect of PC on ASMC contraction is, to a small extent, due to their effect on Sonic Hedgehog signaling and, to a larger extent, due to their effect on calcium influx and membrane depolarization. In conclusion, PC are necessary for the development of airway remodeling by mediating calcium flux and Sonic Hedgehog signaling. [ABSTRACT FROM AUTHOR]

Published
2017
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13. Know Where You Are: Pulmonary Macrophage Locations in the Human Lung.

Author

Tighe, Robert M., Yen Rei Yu, and Yu, Yen Rei

Subjects
MACROPHAGES, STEREOLOGY, FLOW cytometry, LUNGS, TISSUE analysis
Abstract

The article reflects on an article published within the issue on tissue location of human macrophages using design-based stereology. It mentions performing simultaneous flow cytometry on the lung tissues to compare differences between quantification by stereology with flow cytometry-derived quantification. It also mentions implications of demonstration of pulmonary macrophages in distinct tissue locations in the airspace and lung tissue.

Published
2020
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14. Additional file 1: of Improved efficacy against malignant brain tumors with EGFRwt/EGFRvIII targeting immunotoxin and checkpoint inhibitor combinations

Author

Vidyalakshmi Chandramohan, Xuhui Bao, Yu, Xin, Parker, Scott, McDowall, Charlotte, Yen-Rei Yu, Healy, Patrick, Desjardins, Annick, Gunn, Michael, Gromeier, Matthias, Nair, Smita, Pastan, Ira, and Bigner, Darell

Subjects
3. Good health
Abstract

Figure S1. D2C7 epitope comparison between human (h) and mouse (ms) EGFR sequence. The diagram shows sequence alignment between the human and mouse EGFR protein with the mismatched amino acids highlighted. Figure S2. Toxicity assessment of D2C7-IT in C57BL/6J mice bearing intracranial CT2A-dmEGFRvIII-Luc tumors. Different doses (0.03-1 μg) of D2C7-IT were delivered intracranially by CED over a 3-day period to C57BL/6J mice (N = 8-9 mice/group) implanted with CT2A-dmEGFRvIII-Luc tumors. Animals were monitored for toxicity related death. Data are expressed as percentage of mice surviving versus time. Figure S3. Specificity assessment of D2C7-IT in C57BL/6J mice bearing intracranial CT2A-dmEGFRvIII-Luc (A) or parental CT2A (B) tumors. A total dose of 0.1 μg of D2C7-IT or control P588-IT were delivered intracranially by CED over a 3-day period to C57BL/6J mice (N = 10 mice/group) implanted with CT2A-dmEGFRvIII-Luc (A) or parental CT2A tumors (B). Animals were monitored for survival. Treatment schedule, survival curves, median survival. And p-values generated from the generalized Wilcoxon test are provided. Figure S4. Flow cytometric analysis of immune checkpoint molecule expression on T cells and tumor cells. Intracranial CT2A-dmEGFRvIII-Luc (A-D) and SMA560-dmEGFRvIII-Luc (E-H) tumors were analyzed for the expression of PD-1 on CD4+ and CD8+ T cells, FoxP3 on CD4+CD25+ T cells and PD-L1 on tumor cells. Figure S5. Immunofluorescence and immunohistochemistry analysis of checkpoint molecule expression in orthotopic glioma models. Tissue sections from intracranial CT2A-dmEGFRvIII-Luc (A) and SMA560-dmEGFRvIII-Luc (B) tumors were analyzed for the expression of PD-1 and FoxP3 on CD4+ and CD8+ T cells and PD-L1 on tumor cells. Figure S6. Anti-tumor efficacy of D2C7-IT and immune checkpoint inhibitor combinations in orthotopic glioma models. (A-D) Survival curve and median survival estimate data are shown for C57BL/6J mice bearing intracranial CT-2A-dmEGFRvIII-Luc tumors treated with vehicle control, D2C7-IT, αPD-L1 (A), αTim-3 (B), αLag-3 (C), and αCD73 (D) mono or combination therapies. The p-values generated from the generalized Wilcoxon test are provided for all studies and are not adjusted for multiple testing. Figure S7. Comparison of CD4+ T cells:Treg and CD8+ T cells:Treg ratio in orthotopic CT2A-dmEGFRvIII-Luc tumors after D2C7-IT, αCTLA-4, or αPD-1 mono and combination therapies. Intracranial CT2A-dmEGFRvIII-Luc (N=5/6 mice/group) tumors were investigated for the presence of CD4+CD25+FOXP3+ Tregs by flow cytometric analysis. Panels (A) and (B) represent CD4+ T cells:Treg and CD8+ T cells:Treg ratio after D2C7-IT or αPD-1 mono and combination therapies. Panels (C) and (D) represent CD4+ T cells:Treg and CD8+ T cells:Treg ratio after D2C7-IT or αCTLA-4 mono and combination therapies. (PPTX 6598 kb)

16. Additional file 1: of Improved efficacy against malignant brain tumors with EGFRwt/EGFRvIII targeting immunotoxin and checkpoint inhibitor combinations

Author

Vidyalakshmi Chandramohan, Xuhui Bao, Yu, Xin, Parker, Scott, McDowall, Charlotte, Yen-Rei Yu, Healy, Patrick, Desjardins, Annick, Gunn, Michael, Gromeier, Matthias, Nair, Smita, Pastan, Ira, and Bigner, Darell

Subjects
3. Good health
Abstract

Figure S1. D2C7 epitope comparison between human (h) and mouse (ms) EGFR sequence. The diagram shows sequence alignment between the human and mouse EGFR protein with the mismatched amino acids highlighted. Figure S2. Toxicity assessment of D2C7-IT in C57BL/6J mice bearing intracranial CT2A-dmEGFRvIII-Luc tumors. Different doses (0.03-1 μg) of D2C7-IT were delivered intracranially by CED over a 3-day period to C57BL/6J mice (N = 8-9 mice/group) implanted with CT2A-dmEGFRvIII-Luc tumors. Animals were monitored for toxicity related death. Data are expressed as percentage of mice surviving versus time. Figure S3. Specificity assessment of D2C7-IT in C57BL/6J mice bearing intracranial CT2A-dmEGFRvIII-Luc (A) or parental CT2A (B) tumors. A total dose of 0.1 μg of D2C7-IT or control P588-IT were delivered intracranially by CED over a 3-day period to C57BL/6J mice (N = 10 mice/group) implanted with CT2A-dmEGFRvIII-Luc (A) or parental CT2A tumors (B). Animals were monitored for survival. Treatment schedule, survival curves, median survival. And p-values generated from the generalized Wilcoxon test are provided. Figure S4. Flow cytometric analysis of immune checkpoint molecule expression on T cells and tumor cells. Intracranial CT2A-dmEGFRvIII-Luc (A-D) and SMA560-dmEGFRvIII-Luc (E-H) tumors were analyzed for the expression of PD-1 on CD4+ and CD8+ T cells, FoxP3 on CD4+CD25+ T cells and PD-L1 on tumor cells. Figure S5. Immunofluorescence and immunohistochemistry analysis of checkpoint molecule expression in orthotopic glioma models. Tissue sections from intracranial CT2A-dmEGFRvIII-Luc (A) and SMA560-dmEGFRvIII-Luc (B) tumors were analyzed for the expression of PD-1 and FoxP3 on CD4+ and CD8+ T cells and PD-L1 on tumor cells. Figure S6. Anti-tumor efficacy of D2C7-IT and immune checkpoint inhibitor combinations in orthotopic glioma models. (A-D) Survival curve and median survival estimate data are shown for C57BL/6J mice bearing intracranial CT-2A-dmEGFRvIII-Luc tumors treated with vehicle control, D2C7-IT, αPD-L1 (A), αTim-3 (B), αLag-3 (C), and αCD73 (D) mono or combination therapies. The p-values generated from the generalized Wilcoxon test are provided for all studies and are not adjusted for multiple testing. Figure S7. Comparison of CD4+ T cells:Treg and CD8+ T cells:Treg ratio in orthotopic CT2A-dmEGFRvIII-Luc tumors after D2C7-IT, αCTLA-4, or αPD-1 mono and combination therapies. Intracranial CT2A-dmEGFRvIII-Luc (N=5/6 mice/group) tumors were investigated for the presence of CD4+CD25+FOXP3+ Tregs by flow cytometric analysis. Panels (A) and (B) represent CD4+ T cells:Treg and CD8+ T cells:Treg ratio after D2C7-IT or αPD-1 mono and combination therapies. Panels (C) and (D) represent CD4+ T cells:Treg and CD8+ T cells:Treg ratio after D2C7-IT or αCTLA-4 mono and combination therapies. (PPTX 6598 kb)

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