Your search keyword '"Antonia D. Boyer"' showing total 15 results

1. Longitudinal assessment of tumor development using cancer avatars derived from genetically engineered pluripotent stem cells

Author

Tomoyuki Koga, Isaac A. Chaim, Jorge A. Benitez, Sebastian Markmiller, Alison D. Parisian, Robert F. Hevner, Kristen M. Turner, Florian M. Hessenauer, Matteo D’Antonio, Nam-phuong D. Nguyen, Shahram Saberi, Jianhui Ma, Shunichiro Miki, Antonia D. Boyer, John Ravits, Kelly A. Frazer, Vineet Bafna, Clark C. Chen, Paul S. Mischel, Gene W. Yeo, and Frank B. Furnari

Subjects

Science

Abstract

The dearth of glioblastoma model systems that accurately recapitulate the disease remains a challenge. Here, the authors develop cancer avatars using genetically engineered human induced pluripotent cells.

Published

2020

2. Author Correction: Longitudinal assessment of tumor development using cancer avatars derived from genetically engineered pluripotent stem cells

Author

Tomoyuki Koga, Isaac A. Chaim, Jorge A. Benitez, Sebastian Markmiller, Alison D. Parisian, Robert F. Hevner, Kristen M. Turner, Florian M. Hessenauer, Matteo D’Antonio, Nam-phuong D. Nguyen, Shahram Saberi, Jianhui Ma, Shunichiro Miki, Antonia D. Boyer, John Ravits, Kelly A. Frazer, Vineet Bafna, Clark C. Chen, Paul S. Mischel, Gene W. Yeo, and Frank B. Furnari

Subjects

Science

Abstract

An amendment to this paper has been published and can be accessed via a link at the top of the paper.

Published

2020

3. Longitudinal assessment of tumor development using cancer avatars derived from genetically engineered pluripotent stem cells

Author

Kristen M. Turner, Shahram Saberi, Vineet Bafna, Shunichiro Miki, Frank B. Furnari, Isaac A. Chaim, Tomoyuki Koga, Florian M. Hessenauer, Matteo D’Antonio, Kelly A. Frazer, John Ravits, Jorge A. Benitez, Clark C. Chen, Jianhui Ma, Alison Parisian, Paul S. Mischel, Sebastian Markmiller, Gene W. Yeo, Robert F. Hevner, Antonia D. Boyer, and Nam Nguyen

Subjects

0301 basic medicine, Cellular differentiation, General Physics and Astronomy, Mice, SCID, Genome, Mice, 0302 clinical medicine, Stem Cell Research - Nonembryonic - Human, Induced pluripotent stem cell, lcsh:Science, Cancer, Heterologous, Multidisciplinary, Tumor, Neurofibromin 1, Stem Cell Research - Induced Pluripotent Stem Cell - Human, Brain Neoplasms, Cell Differentiation, Glioma, Primary tumor, Neural stem cell, 3. Good health, Gene Expression Regulation, Neoplastic, Neoplastic Stem Cells, Female, Stem Cell Research - Nonembryonic - Non-Human, Genetic Engineering, Pluripotent Stem Cells, Science, Transplantation, Heterologous, Biology, SCID, General Biochemistry, Genetics and Molecular Biology, Article, Cell Line, 03 medical and health sciences, Rare Diseases, Clinical Research, Neurosphere, Extrachromosomal DNA, Cell Line, Tumor, medicine, Genetics, Animals, Humans, Author Correction, Cancer models, Transplantation, Neoplastic, Stem Cell Research - Induced Pluripotent Stem Cell, Human Genome, PTEN Phosphohydrolase, Neurosciences, General Chemistry, medicine.disease, Stem Cell Research, Brain Disorders, CNS cancer, Brain Cancer, 030104 developmental biology, Gene Expression Regulation, Mutation, Cancer research, lcsh:Q, Tumor Suppressor Protein p53, Glioblastoma, 030217 neurology & neurosurgery, Neoplasm Transplantation

Abstract

Many cellular models aimed at elucidating cancer biology do not recapitulate pathobiology including tumor heterogeneity, an inherent feature of cancer that underlies treatment resistance. Here we introduce a cancer modeling paradigm using genetically engineered human pluripotent stem cells (hiPSCs) that captures authentic cancer pathobiology. Orthotopic engraftment of the neural progenitor cells derived from hiPSCs that have been genome-edited to contain tumor-associated genetic driver mutations revealed by The Cancer Genome Atlas project for glioblastoma (GBM) results in formation of high-grade gliomas. Similar to patient-derived GBM, these models harbor inter-tumor heterogeneity resembling different GBM molecular subtypes, intra-tumor heterogeneity, and extrachromosomal DNA amplification. Re-engraftment of these primary tumor neurospheres generates secondary tumors with features characteristic of patient samples and present mutation-dependent patterns of tumor evolution. These cancer avatar models provide a platform for comprehensive longitudinal assessment of human tumor development as governed by molecular subtype mutations and lineage-restricted differentiation., The dearth of glioblastoma model systems that accurately recapitulate the disease remains a challenge. Here, the authors develop cancer avatars using genetically engineered human induced pluripotent cells.

Published

2020

4. Inhibition of Nuclear PTEN Tyrosine Phosphorylation Enhances Glioma Radiation Sensitivity through Attenuated DNA Repair

Author

Huilin Zhou, John DeGroot, Erik P. Sulman, Frank B. Furnari, Andrew K. Shiau, Webster K. Cavenee, Ciro Zanca, Shunichiro Miki, Timothy C. Gahman, Laura Orellana, Rachel Reed, Suely Kazue Nagahashi Marie, Clark C. Chen, Jianhui Ma, Thais F. Galatro, Richard D. Kolodner, Jorge A. Benitez, Claudio P. Albuquerque, Jie Li, Tomoyuki Koga, Erik Lindahl, Nissi Varki, Antonia D. Boyer, and Tim R. Fenton

Subjects

0301 basic medicine, Male, PTEN, Cancer Research, Fibroblast Growth Factor, DNA Repair, Radiation Tolerance, chemistry.chemical_compound, Mice, 0302 clinical medicine, Radiation sensitivity, Phosphorylation, health care economics and organizations, Cancer, biology, Brain Neoplasms, Glioma, humanities, Chromatin, medicine.anatomical_structure, Oncology, 6.1 Pharmaceuticals, 030220 oncology & carcinogenesis, Female, ionizing radiation, Type 2, Receptor, DNA damage, DNA repair, Oncology and Carcinogenesis, GBM, Article, 03 medical and health sciences, Rare Diseases, Genetics, medicine, Animals, Humans, Oncology & Carcinogenesis, Receptor, Fibroblast Growth Factor, Type 2, Cell Nucleus, Lung, business.industry, tyrosine phosphorylation, Neurosciences, PTEN Phosphohydrolase, Evaluation of treatments and therapeutic interventions, Tyrosine phosphorylation, Cell Biology, medicine.disease, Xenograft Model Antitumor Assays, Brain Disorders, Brain Cancer, 030104 developmental biology, Pyrimidines, chemistry, FGFR2, Cancer cell, Cancer research, biology.protein, Tyrosine, Rad51 Recombinase, business

Abstract

Ionizing radiation (IR) and chemotherapy are standard of care treatments for glioblastoma (GBM) patients and both result in DNA damage, however, the clinical efficacy is limited due to therapeutic resistance. We identified a mechanism of such resistance mediated by phosphorylation of PTEN on tyrosine 240 (pY240-PTEN) by FGFR2. pY240-PTEN is rapidly elevated and bound to chromatin through interaction with Ki-67 in response to IR treatment and facilitates the recruitment of RAD51 to promote DNA repair. Blocking Y240 phosphorylation confers radiation sensitivity to tumors and extends survival in GBM preclinical models. Y240F-Pten knock-in mice showed radiation sensitivity. These results suggest that FGFR-mediated pY240-PTEN is a key mechanism of radiation resistance and is an actionable target for improving radiotherapy efficacy.

Published

2019

5. Cancer avatars derived from genetically engineered pluripotent stem cells allow for longitudinal assessment of tumor development

Author

Shunichiro Miki, Paul S. Mischel, Isaac A. Chaim, Clark C. Chen, Kristen M. Turner, Matteo D’Antonio, Kelly A. Frazer, Vineet Bafna, Jorge A. Benitez, John Ravits, Nam-Phuong Nguyen, Frank B. Furnari, Jianhui Ma, Shahram Saberi, Tomoyuki Koga, Florian M. Hessenauer, Antonia D. Boyer, Sebastian Markmiller, Gene W. Yeo, and Alison Parisian

Subjects

0303 health sciences, Cas9, Computational biology, Disease, Biology, Somatic evolution in cancer, Neural stem cell, 3. Good health, Genetically modified organism, 03 medical and health sciences, 0302 clinical medicine, 030220 oncology & carcinogenesis, Extrachromosomal DNA, CRISPR, Induced pluripotent stem cell, 030304 developmental biology

Abstract

Many current cellular models aimed at elucidating cancer biology do not recapitulate pathobiology including tumor heterogeneity, an inherent feature of cancer that underlies treatment resistance. Here we introduce a new cancer modeling paradigm using genetically engineered human pluripotent stem cells (hiPSCs) that capture authentic cancer pathobiology. Orthotopic engraftment of neural progenitor cells derived from hiPSCs that have been genome-edited to contain tumor-associated genetic driver mutations revealed by The Cancer Genome Atlas project for glioblastoma (GBM) result in formation of high-grade gliomas. As observed in GBM patient samples, these models harbor inter-tumor heterogeneity resembling different GBM molecular subtypes, and intra-tumor heterogeneity. Further, re-engraftment of primary tumor neurospheres generates secondary tumors with features characteristic of patient samples and present mutation-dependent patterns of tumor evolution. Thus, these cancer avatar models provide a platform for a comprehensive longitudinal assessment of human tumor development as governed by molecular subtype mutations and lineage-restricted differentiation.

Published

2019

6. Author Correction: Longitudinal assessment of tumor development using cancer avatars derived from genetically engineered pluripotent stem cells

Author

Jorge A. Benitez, Gene W. Yeo, Kelly A. Frazer, Robert F. Hevner, Sebastian Markmiller, Jianhui Ma, Florian M. Hessenauer, Alison Parisian, John Ravits, Tomoyuki Koga, Frank B. Furnari, Shahram Saberi, Matteo D’Antonio, Shunichiro Miki, Vineet Bafna, Nam Nguyen, Antonia D. Boyer, Isaac A. Chaim, Kristen M. Turner, Clark C. Chen, and Paul S. Mischel

Subjects

Multidisciplinary, Genetically engineered, Science, General Physics and Astronomy, Cancer, General Chemistry, Computational biology, Biology, medicine.disease, General Biochemistry, Genetics and Molecular Biology, medicine, lcsh:Q, Induced pluripotent stem cell, lcsh:Science

Abstract

An amendment to this paper has been published and can be accessed via a link at the top of the paper.

Published

2020

7. Correction: Publisher Correction: PTEN regulates glioblastoma oncogenesis through chromatin-associated complexes of DAXX and histone H3.3

Author

Antonia D. Boyer, Nathan M. Jameson, Matteo D’Antonio, Stephen Kelly, Kelly A. Frazer, Frank B. Furnari, Alireza Khodadadi-Jamayran, Michael A. E. Andersen, Jianhui Ma, Ciro Zanca, Shahram Saberi, Maria F. Camargo, Hrvoje Miletic, Jorge A. Benitez, and Webster K. Cavenee

Subjects

0301 basic medicine, Multidisciplinary, Science, General Physics and Astronomy, General Chemistry, Biology, medicine.disease, medicine.disease_cause, Article, General Biochemistry, Genetics and Molecular Biology, Chromatin, Cell biology, 03 medical and health sciences, Histone H3, 030104 developmental biology, Histone, Death-associated protein 6, medicine, biology.protein, PTEN, Carcinogenesis, Glioblastoma

Abstract

Glioblastoma (GBM) is the most lethal type of human brain cancer, where deletions and mutations in the tumour suppressor gene PTEN (phosphatase and tensin homolog) are frequent events and are associated with therapeutic resistance. Herein, we report a novel chromatin-associated function of PTEN in complex with the histone chaperone DAXX and the histone variant H3.3. We show that PTEN interacts with DAXX and, in turn PTEN directly regulates oncogene expression by modulating DAXX-H3.3 association on the chromatin, independently of PTEN enzymatic activity. Furthermore, DAXX inhibition specifically suppresses tumour growth and improves the survival of orthotopically engrafted mice implanted with human PTEN-deficient glioma samples, associated with global H3.3 genomic distribution changes leading to upregulation of tumour suppressor genes and downregulation of oncogenes. Moreover, DAXX expression anti-correlates with PTEN expression in GBM patient samples. Since loss of chromosome 10 and PTEN are common events in cancer, this synthetic growth defect mediated by DAXX suppression represents a therapeutic opportunity to inhibit tumorigenesis specifically in the context of PTEN deletion., PTEN mutations are frequent in glioblastoma and often are associated with therapeutic resistance. Here, the authors demonstrate that PTEN regulates gene expression at the chromatin level by interacting with the histone chaperone DAXX and H3.3, and that DAXX inhibition inhibits PTEN-deficient GBM growth in vivo.

Published

2018

8. PAX3-FOXO1 controls expression of the p57Kip2 cell-cycle regulator through degradation of EGR1

Author

Wendy Roeb, Webster K. Cavenee, Antonia D. Boyer, and Karen C. Arden

Subjects

endocrine system, PAX3, Regulator, Electrophoretic Mobility Shift Assay, Mice, Transgenic, FOXO1, Biology, Polymerase Chain Reaction, Mice, Transcription (biology), Rhabdomyosarcoma, Animals, Humans, Paired Box Transcription Factors, Myocyte, Promoter Regions, Genetic, Cyclin-Dependent Kinase Inhibitor p57, PAX3 Transcription Factor, Transcription factor, Early Growth Response Protein 1, Regulation of gene expression, Muscle Neoplasms, Multidisciplinary, Forkhead Box Protein O1, Hydrolysis, Forkhead Transcription Factors, Biological Sciences, musculoskeletal system, Fusion protein, Molecular biology, Gene Expression Regulation, embryonic structures

Abstract

The chimeric protein PAX3-FOXO1, resulting from a translocation between chromosomes 2 and 13, is the most common genetic aberration in the alveolar subtype of the human skeletal muscle tumor, rhabdomyosarcoma. To understand how PAX3-FOXO1 contributes to tumor development, we isolated and characterized muscle cells from transgenic mice expressing PAX3-FOXO1 under control of the PAX3 promoter. We demonstrate that these myoblasts are unable to complete myogenic differentiation because of an inability to up-regulate p57Kip2 transcription. This defect is caused by reduced levels of the EGR1 transcriptional activator resulting from a direct, destabilizing interaction with PAX3-FOXO1. Neither PAX3 nor FOXO1 share the ability to regulate p57Kip2 transcription. Thus, the breakage and fusion of the genes encoding these transcription factors creates a unique chimeric protein that controls a key cell-cycle and -differentiation regulator.

Published

2007

9. CT10: A new cancer-testis (CT) antigen homologous to CT7 and the MAGE family, identified by representational-difference analysis

Author

Ali O. Gure, Elisabeth Stockert, Carrie S. Viars, Yao-Tseng Chen, Matthew J. Scanlan, Lloyd J. Old, Karen C. Arden, and Antonia D. Boyer

Subjects

Genetics, endocrine system, Cancer Research, PRAME, biology, Immunogenicity, Melanoma, Cancer, medicine.disease, Oncology, Antigen, Complementary DNA, Cancer research, medicine, biology.protein, Representational difference analysis, Antibody, neoplasms

Abstract

Assays relying on humoral or T-cell-based recognition of tumor antigens to identify potential targets for immunotherapy have led to the discovery of a significant number of immunogenic gene products, including cancer-testis (CT) antigens predominantly expressed in cancer cells and male germ cells. The search for cancer-specific antigens has been extended via the technique of representational-difference analysis and SK-MEL-37, a melanoma cell line expressing a broad range of CT antigens. Using this approach, we have isolated CT antigen genes, genes over-expressed in cancer, e.g., PRAME and KOC, and genes encoding neuro-ectodermal markers. The identified CT antigen genes include the previously defined MAGE-A6, MAGE-A4a, MAGE-A10, CT7/MAGE-C1, as well as a novel gene designated CT10, which shows strong homology to CT7/MAGE-C1 both at cDNA and at genomic levels. Chromosome mapping localized CT10 to Xq27, in close proximity to CT7/MAGE-C1 and MAGE-A genes. CT10 mRNA is expressed in testis and in 20 to 30% of various human cancers. A serological survey identified 2 melanoma patients with anti-CT10 antibody, demonstrating the immunogenicity of CT10 in humans. Int. J. Cancer 85:726–732, 2000. © 2000 Wiley-Liss, Inc.

Published

2000

10. Localization of Serine Kinases, SRPK1 (SFRSK1) and SRPK2 (SFRSK2), Specific for the SR Family of Splicing Factors in Mouse and Human Chromosomes

Author

Antonia D. Boyer, Carrie S. Viars, Huan You Wang, John R. Bermingham, Wen Lin, Xiang-Dong Fu, and Karen C. Arden

Subjects

Male, RNA Splicing, Hybrid Cells, Protein Serine-Threonine Kinases, Biology, SRPK1, Mice, Splicing factor, Genetics, medicine, Animals, Humans, Crosses, Genetic, In Situ Hybridization, Fluorescence, medicine.diagnostic_test, Chromosome Mapping, Chromosome, Chromosome Banding, Mice, Inbred C57BL, Muridae, Chromosome 17 (human), RNA splicing, Chromosomes, Human, Pair 6, Female, Human genome, Chromosome 22, Chromosomes, Human, Pair 7, Fluorescence in situ hybridization

Abstract

The serine- and arginine-rich (SR) splicing factors play an important role in both constitutive and alternative pre-mRNA splicing, and the functions of these splicing factors are regulated by phosphorylation. We have previously characterized SRPK1 (SFRSK1) and SRPK2 (SFRSK2), which are highly specific protein kinases for the SR family of splicing factors. Here we report the chromosomal localization of the mouse and human genes for both kinases. SRPK1 probes detected two loci that were mapped to mouse Chromosomes 17 and X using The Jackson Laboratory interspecific backcross DNA panel, and SRPK2 probes identified a single locus on mouse Chromosome 5. Using a somatic cell hybrid mapping panel and by fluorescence in situ hybridization, SRPK1 and SRPK2 were respectively mapped to human chromosomes 6p21.2-p21.3 (a region of conserved synteny to mouse Chromosome 17) and 7q22-q31.1 (a region of conserved synteny to mouse Chromosome 5). In addition, we also found multiple SRPK-related sequences on other human chromosomes, one of which appears to correspond to a SRPK2 pseudogene on human chromosome 8.

Published

1999

11. Genomic cloning and localization of CTAG, a gene encoding an autoimmunogenic cancer-testis antigen NY-ESO-1 to human chromosome Xq28

Author

L. J. Old, S. Tsang, Carrie S. Viars, Yao-Tseng Chen, Karen C. Arden, and Antonia D. Boyer

Subjects

Male, X Chromosome, Chromosome Mapping, Membrane Proteins, Proteins, Hybrid Cells, Biology, Molecular biology, Tumor antigen, Epidermoid carcinoma, Antigens, Neoplasm, Immunoscreening, Testis, Genetics, Cancer research, Humans, Cancer/testis antigens, CTAG, Cloning, Molecular, NY-ESO-1, Molecular Biology, Genetics (clinical), X chromosome, Genomic organization

Abstract

CTAG was initially cloned from an esophageal squamous cell carcinoma cDNA expression library by immunoscreening with autologous patient’s serum. CTAG mRNA is expressed in a proportion of human cancers in a lineage-nonspecific fashion, whereas its expression in normal tissues is restricted to testis and ovary only. This expression pattern suggests that the CTAG product (NY-ESO-1) is an aberrantly activated tumor antigen and can potentially be an antigenic target for tumor vaccination. In the present study, we isolated human genomic clones of CTAG and established its genomic organization. By somatic cell hybrid studies and fluorescence in-situ hybridization, we localized this gene to chromosome Xq28, a region that also contains members of MAGE, a gene family that encodes several immunogenic tumor antigens with the characteristic cancer/testis expression pattern.

Published

1997

12. CBIO-04DAXX INHIBITION SUPPRESSES TUMOR GROWTH IN PTEN-DEFICIENT HUMAN GLIOBLASTOMAS

Author

Fernanda Camargo Camargo, Nathan M. Jameson, Jianhui Ma, Webster K. Cavenee, Ciro Zanca, Frank B. Furnari, Antonia D. Boyer, and Jorge A. Benitez

Subjects

Cancer Research, biology, Oncogene, Tumor suppressor gene, Cancer, medicine.disease, Chromatin, Histone, Death-associated protein 6, Oncology, biology.protein, Cancer research, medicine, Tensin, PTEN, Neurology (clinical), Abstracts from the 20th Annual Scientific Meeting of the Society for Neuro-Oncology

Abstract

Glioblastoma (GBM) is the most lethal type of brain cancer, where deletions and/or mutations in the tumor suppressor gene PTEN (phosphatase and tensin homolog) are associated to responsiveness of cancer to radiotherapy and chemotherapy. Herein, we show that a PTEN-DAXX-H3.3 chromatin complex negatively regulates proliferation and tumor growth. PTEN directly regulates oncogene expression by coordinating DAXX and histone H3.3 deposition on chromatin and in turn, DAXX protects PTEN from acetylation and ubiquitination. Furthermore, DAXX disruption in PTEN-deficient glioblastoma patient derived xenograft models suppresses tumor growth and promotes therapy sensitivity. Since PTEN loss is a common alteration in cancer, DAXX inhibition presents an approach to ablate the growth of such cancers.

Published

2015

13. ADAMTS9, a novel member of the ADAM-TS/ metallospondin gene family

Author

Melody Clark, Laurie A. Turbeville, Gregory S. Kelner, Antonia D. Boyer, Richard A. Maki, and Karen C. Arden

Subjects

endocrine system, Protein family, Disintegrins, Molecular Sequence Data, ADAMTS9 Protein, Gene Expression, Biology, Homology (biology), Gene expression, Genetics, Gene family, Animals, Humans, Amino Acid Sequence, Cloning, Molecular, Gene, In Situ Hybridization, Fluorescence, DNA Primers, Metalloproteinase, Thrombospondin, Reverse Transcriptase Polymerase Chain Reaction, Nucleic acid sequence, Chromosome Mapping, Metalloendopeptidases, Rats, carbohydrates (lipids), ADAM Proteins, Chromosomes, Human, Pair 3, Thrombospondins

Abstract

ADAM-TS/metallospondin genes encode a new family of proteins with structural homology to the ADAM metalloprotease-disintegrin family. However, unlike other ADAMs, these proteins contain thrombospondin type 1 (TSP1) repeats at the carboxy-terminal end and are secreted proteins instead of being membrane bound. Members of the ADAM-TS family have been implicated in the cleavage of proteoglycans, the control of organ shape during development, and the inhibition of angiogenesis. We have cloned a new member of the ADAM-TS/metallospondin family designated here as ADAMTS9. This protein has a metalloprotease domain, a disintegrin-like domain, one internal TSP1 motif, and three carboxy-terminal TSP1-like submotifs. In contrast to other ADAM-TS family members, ADAMTS9 is expressed in all fetal tissues examined as well as some adult tissues. Using FISH and radiation hybrid analysis, we have localized ADAMTS9 to chromosome 3p14.2-p14.3, an area known to be lost in hereditary renal tumors.

Published

2000

14. Assignment<footref rid='foot01'>1</footref> of Seta to distal mouse X chromosome by radiation hybrid mapping

Author

Antonia D. Boyer, Virginia W. Sykes, Karen C. Arden, M. A. Hyatt, and Oliver Bogler

Subjects

Genetics, Gene mapping, Seta, Radiation hybrid mapping, Computational biology, Biology, Molecular Biology, Genetics (clinical), X chromosome

Published

2000

15. Glioblastoma cellular cross-talk converges on NF-κB to attenuate EGFR inhibitor sensitivity

Author

Afsheen Banisadr, Kelly A. Frazer, Ciro Zanca, Nathan M. Jameson, Jorge A. Benitez, Webster K. Cavenee, William A. Weiss, Amy Haseley Thorne, Vladislav V. Verkhusha, Antonia D. Boyer, Jianhui Ma, Frank B. Furnari, Jill Wykosky, Feng Liu, Tomoyuki Koga, Matteo D’Antonio, Genaro R. Villa, Gabriela F. Barnabe, Huijun Yang, Shiro Ikegami, Paul S. Mischel, Andrew K. Shiau, Olesja Eliseeva, Sihan Wu, Clark C. Chen, Timothy C. Gahman, Alison Parisian, and Maria G. Isaguliants

Subjects

0301 basic medicine, medicine.medical_treatment, Nude, Drug Resistance, Cell Communication, Medical and Health Sciences, NF-κB, Mice, tumor heterogeneity, Epidermal growth factor receptor, Cancer, EGFR inhibitors, biology, NF-kappa B, Nuclear Proteins, Biological Sciences, ErbB Receptors, Cytokine, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Signal Transduction, BRD4, EGFR, survivin, 03 medical and health sciences, Paracrine signalling, Rare Diseases, Survivin, Genetics, medicine, Animals, Humans, Autocrine signalling, Protein Kinase Inhibitors, Neoplastic, IL-6, Interleukin-6, Psychology and Cognitive Sciences, glioblastoma, Neurosciences, Brain Disorders, Bromodomain, Brain Cancer, 030104 developmental biology, Gene Expression Regulation, Mutation, Cancer research, biology.protein, Neoplasm, Transcription Factors, Developmental Biology

Abstract

In glioblastoma (GBM), heterogeneous expression of amplified and mutated epidermal growth factor receptor (EGFR) presents a substantial challenge for the effective use of EGFR-directed therapeutics. Here we demonstrate that heterogeneous expression of the wild-type receptor and its constitutively active mutant form, EGFRvIII, limits sensitivity to these therapies through an interclonal communication mechanism mediated by interleukin-6 (IL-6) cytokine secreted from EGFRvIII-positive tumor cells. IL-6 activates a NF-κB signaling axis in a paracrine and autocrine manner, leading to bromodomain protein 4 (BRD4)-dependent expression of the prosurvival protein survivin (BIRC5) and attenuation of sensitivity to EGFR tyrosine kinase inhibitors (TKIs). NF-κB and survivin are coordinately up-regulated in GBM patient tumors, and functional inhibition of either protein or BRD4 in in vitro and in vivo models restores sensitivity to EGFR TKIs. These results provide a rationale for improving anti-EGFR therapeutic efficacy through pharmacological uncoupling of a convergence point of NF-κB-mediated survival that is leveraged by an interclonal circuitry mechanism established by intratumoral mutational heterogeneity.