Your search keyword '"Tracy T. Batchelor"' showing total 664 results

1. Comprehensive mutational scanning of EGFR reveals TKI sensitivities of extracellular domain mutants

Author

Tikvah K. Hayes, Elisa Aquilanti, Nicole S. Persky, Xiaoping Yang, Erica E. Kim, Lisa Brenan, Amy B. Goodale, Douglas Alan, Ted Sharpe, Robert E. Shue, Lindsay Westlake, Lior Golomb, Brianna R. Silverman, Myshal D. Morris, Ty Running Fisher, Eden Beyene, Yvonne Y. Li, Andrew D. Cherniack, Federica Piccioni, J. Kevin Hicks, Andrew S. Chi, Daniel P. Cahill, Jorg Dietrich, Tracy T. Batchelor, David E. Root, Cory M. Johannessen, and Matthew Meyerson

Subjects

Science

Abstract

Abstract The epidermal growth factor receptor, EGFR, is frequently activated in lung cancer and glioblastoma by genomic alterations including missense mutations. The different mutation spectra in these diseases are reflected in divergent responses to EGFR inhibition: significant patient benefit in lung cancer, but limited in glioblastoma. Here, we report a comprehensive mutational analysis of EGFR function. We perform saturation mutagenesis of EGFR and assess function of ~22,500 variants in a human EGFR-dependent lung cancer cell line. This approach reveals enrichment of erlotinib-insensitive variants of known and unknown significance in the dimerization, transmembrane, and kinase domains. Multiple EGFR extracellular domain variants, not associated with approved targeted therapies, are sensitive to afatinib and dacomitinib in vitro. Two glioblastoma patients with somatic EGFR G598V dimerization domain mutations show responses to dacomitinib treatment followed by within-pathway resistance mutation in one case. In summary, this comprehensive screen expands the landscape of functional EGFR variants and suggests broader clinical investigation of EGFR inhibition for cancers harboring extracellular domain mutations.

Published

2024

2. Author Correction: Comprehensive mutational scanning of EGFR reveals TKI sensitivities of extracellular domain mutants

Author

Tikvah K. Hayes, Elisa Aquilanti, Nicole S. Persky, Xiaoping Yang, Erica E. Kim, Lisa Brenan, Amy B. Goodale, Douglas Alan, Ted Sharpe, Robert E. Shue, Lindsay Westlake, Lior Golomb, Brianna R. Silverman, Myshal D. Morris, Ty Running Fisher, Eden Beyene, Yvonne Y. Li, Andrew D. Cherniack, Federica Piccioni, J. Kevin Hicks, Andrew S. Chi, Daniel P. Cahill, Jorg Dietrich, Tracy T. Batchelor, David E. Root, Cory M. Johannessen, and Matthew Meyerson

Subjects

Science

Published

2024

3. PIK3CA activating mutations are associated with more disseminated disease at presentation and earlier recurrence in glioblastoma

Author

Shota Tanaka, Tracy T. Batchelor, A. John Iafrate, Dora Dias-Santagata, Darrell R. Borger, Leif W. Ellisen, Daniel Yang, David N. Louis, Daniel P. Cahill, and Andrew S. Chi

Subjects

Dissemination, Glioblastoma, Gliomatosis, Multicentric, PIK3CA, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Phosphatidylinositol 3-kinase signaling promotes cell growth and survival and is frequently activated in infiltrative gliomas. Activating mutations in PIK3CA gene are observed in 6–15% of glioblastomas, although their clinical significance is largely undescribed. The objective of this study was to examine whether PIK3CA mutations are associated with a specific clinical phenotype in glioblastoma. We retrospectively reviewed 157 consecutive newly diagnosed glioblastoma patients from December 2009 to June 2012 who underwent molecular profiling consisting of targeted hotspot genotyping, fluorescence in situ hybridization for gene amplification, and methylation-specific PCR for O6-methylguanine-DNA methyltransferase promoter methylation. Molecular alterations were correlated with clinical features, imaging and outcome. The Cancer Genome Atlas data was analyzed as a validation set. There were 91 males; median age was 58 years (range, 23–85). With a median follow-up of 20.9 months, median progression-free survival (PFS) and estimated overall survival (OS) were 11.9 and 24.0 months, respectively. Thirteen patients (8.3%) harbored PIK3CA mutation, which was associated with younger age (mean 49.4 vs. 58.1 years, p = 0.02). PIK3CA mutation correlated with shorter PFS (median 6.9 vs. 12.4 months, p = 0.01) and OS (median 21.2 vs. 24.2 months, p = 0.049) in multivariate analysis. A significant association between PIK3CA mutation and more disseminated disease at diagnosis, as defined by gliomatosis, multicentric lesions, or distant leptomeningeal lesions, was observed (46.2% vs. 11.1%, p = 0.004). In conclusion, despite the association with younger age, PIK3CA activating mutations are associated with earlier recurrence and shorter survival in adult glioblastoma. The aggressive course of these tumors may be related to their propensity for disseminated presentation.

Published

2019

4. Pharmacodynamics of mutant-IDH1 inhibitors in glioma patients probed by in vivo 3D MRS imaging of 2-hydroxyglutarate

Author

Ovidiu C. Andronesi, Isabel C. Arrillaga-Romany, K. Ina Ly, Wolfgang Bogner, Eva M. Ratai, Kara Reitz, A. John Iafrate, Jorg Dietrich, Elizabeth R. Gerstner, Andrew S. Chi, Bruce R. Rosen, Patrick Y. Wen, Daniel P. Cahill, and Tracy T. Batchelor

Subjects

Science

Abstract

Inhibitors of mutant isocitrate dehydrogenase 1 (IDH1) entered recently clinical trials for treatment of gliomas. Here, the authors apply a MRS imaging method for 2HG detection and assessement of the pharmacodynamic effects of the mutant IDH1 inhibitor (IDH305) in 8 mutant IDH1 glioma patients.

Published

2018

5. Early changes in glioblastoma metabolism measured by MR spectroscopic imaging during combination of anti-angiogenic cediranib and chemoradiation therapy are associated with survival

Author

Ovidiu C. Andronesi, Morteza Esmaeili, Ronald J. H. Borra, Kyrre Emblem, Elizabeth R. Gerstner, Marco C. Pinho, Scott R. Plotkin, Andrew S. Chi, April F. Eichler, Jorg Dietrich, S. Percy Ivy, Patrick Y. Wen, Dan G. Duda, Rakesh Jain, Bruce R. Rosen, Gregory A. Sorensen, and Tracy T. Batchelor

Subjects

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

Abstract

Metabolic imaging reveals anti-angiogenic (AA) therapy mechanisms in glioblastoma (GBM) GBM is the most common and aggressive type of malignant primary brain tumors (glioma). Patients with GBM have less than 5% survival at 5 years with the best existing treatment and progress is desperately needed to improve patient outcome. Imaging can guide development and clinical translation of new treatments, and can help to understand mechanisms of response and to optimize drug regimens in patients. AA therapy that targets the blood supply of tumors can benefit GBM patients as adjuvant therapy to standard chemoradiation, but the timing of combination therapy may be important to obtain the maximum benefit and minimize negative side effects. Tracking metabolic changes with magnetic resonance spectroscopic imaging (MRSI) during a phase II clinical trial of AA drug cediranib combined with chemoradiation shows that there is a therapeutic window within the first month where there is maximal synergy between the effects of the anti-angiogenesis and chemoradiation. Our data suggest that adjusting the dose of AA therapy during chemoradiation may be beneficial, and MRSI can be used as a precision medicine tool to identify the patients and time for adjusting the combination treatment.

Published

2017

6. Clinical and radiographic response following targeting of BCAN-NTRK1 fusion in glioneuronal tumor

Author

Christopher Alvarez-Breckenridge, Julie J. Miller, Naema Nayyar, Corey M. Gill, Andrew Kaneb, Megan D’Andrea, Long P. Le, Jesse Lee, Ju Cheng, Zongli Zheng, William E. Butler, Pratik Multani, Edna Chow Maneval, Sun Ha Paek, Brian D. Toyota, Dora Dias-Santagata, Sandro Santagata, Javier Romero, Alice T. Shaw, Anna F. Farago, Stephen Yip, Daniel P. Cahill, Tracy T. Batchelor, A. John Iafrate, and Priscilla K. Brastianos

Subjects

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

Abstract

Abstract Glioneuronal tumors constitute a histologically diverse group of primary central nervous system neoplasms that are typically slow-growing and managed conservatively. Genetic alterations associated with glioneuronal tumors include BRAF mutations and oncogenic fusions. To further characterize this group of tumors, we collected a cohort of 26 glioneuronal tumors and performed in-depth genomic analysis. We identified mutations in BRAF (34%) and oncogenic fusions (30%), consistent with previously published reports. In addition, we discovered novel oncogenic fusions involving members of the NTRK gene family in a subset of our cohort. One-patient with BCAN exon 13 fused to NTRK1 exon 11 initially underwent a subtotal resection for a 4th ventricular glioneuronal tumor but ultimately required additional therapy due to progressive, symptomatic disease. Given the patient’s targetable fusion, the patient was enrolled on a clinical trial with entrectinib, a pan-Trk, ROS1, and ALK (anaplastic lymphoma kinase) inhibitor. The patient was treated for 11 months and during this time volumetric analysis of the lesion demonstrated a maximum reduction of 60% in the contrast-enhancing tumor compared to his pre-treatment magnetic resonance imaging study. The radiologic response was associated with resolution of his clinical symptoms and was maintained for 11 months on treatment. This report of a BCAN-NTRK1 fusion in glioneuronal tumors highlights its clinical importance as a novel, targetable alteration.

Published

2017

7. Primary central nervous system lymphoma

Author

Sarah Löw, Catherine H. Han, and Tracy T. Batchelor

Subjects

Neurology. Diseases of the nervous system, RC346-429

Abstract

Primary central nervous system lymphoma (PCNSL) is a rare and aggressive extranodal non-Hodgkin lymphoma (NHL), confined to the brain, eyes, spinal cord or leptomeninges without systemic involvement. Overall prognosis, diagnosis and management of PCNSL differ from other types of NHL. Prompt diagnosis and initiation of treatment are vital to improving clinical outcomes. PCNSL is responsive to radiation therapy, however whole-brain radiotherapy (WBRT) inadequately controls the disease when used alone and its delayed neurotoxicity causes neurocognitive impairment, especially in elderly patients. High-dose methotrexate (HD-MTX)-based induction chemotherapy with or without autologous stem cell transplantation (ASCT) or reduced-dose WBRT leads to durable disease control and less neurotoxicity. The optimal treatment has yet to be defined, however HD-MTX-based induction chemotherapy is considered standard for newly diagnosed PCNSL. Ongoing randomized trials address the role of rituximab, and of consolidative treatment using ASCT or reduced-dose WBRT. Despite high tumor response rates to initial treatment, many patients have relapsing disease with very poor prognosis. The optimal treatment for refractory or relapsed PCNSL is poorly defined. The choice of salvage treatment depends on age, previous treatment and response, performance status and comorbidities at the time of relapse. Novel therapeutics targeting underlying tumor biology include small molecule inhibitors of B-cell receptor, cereblon, and mammalian target of rapamycin signaling, and immunotherapy programmed cell death 1 receptor inhibitors and chimeric antigen receptor T cells.

Published

2018

8. Tumor inflammation-associated neurotoxicity

Author

Jasia Mahdi, Jorg Dietrich, Karin Straathof, Claire Roddie, Brian J. Scott, Tom Belle Davidson, Laura M. Prolo, Tracy T. Batchelor, Cynthia J. Campen, Kara L. Davis, Juliane Gust, Michael Lim, Robbie G. Majzner, Julie R. Park, Sonia Partap, Sneha Ramakrishna, Rebecca Richards, Liora Schultz, Nicholas A. Vitanza, Leo D. Wang, Crystal L. Mackall, and Michelle Monje

Subjects

General Medicine, General Biochemistry, Genetics and Molecular Biology

Published

2023

9. Understanding the Genetic Risk of IDH-Mutant Glioma

Author

Tracy T. Batchelor and Kyle M. Walsh

Subjects

General Medicine

Published

2023

10. Neurologic Complications of Cancer

Author

Luis Nicolas Gonzalez Castro, Tracy T. Batchelor, and Lisa M. DeAngelis

Published

2022

11. Supplementary Figure 3 from Brain Tumor Cells in Circulation Are Enriched for Mesenchymal Gene Expression

Author

Daniel A. Haber, Shyamala Maheswaran, Mehmet Toner, David N. Louis, Tracy T. Batchelor, Jay S. Loeffler, William T. Curry, A. John Iafrate, Khalid Shah, Ravi Kapur, Lecia V. Sequist, S. Michael Rothenberg, Hiroaki Wakimoto, Andrew S. Chi, Deepak Bhere, Simeon Springer, Samantha M. Oliveira, Marissa W. Madden, Brian V. Nahed, and James P. Sullivan

Abstract

DNA-FISH analysis of non-EGFR-amplified GBM CTCs.

Published

2023

12. Supplementary Table S3 from Genomic Characterization of Brain Metastases Reveals Branched Evolution and Potential Therapeutic Targets

Author

William C. Hahn, Gad Getz, David N. Louis, José Baselga, Tracy T. Batchelor, Rameen Beroukhim, Eric S. Lander, Stacey Gabriel, Levi Garraway, Matthew Meyerson, Anat Stemmer-Rachamimov, Eric P. Winer, Nancy U. Lin, Michael S. Rabin, Carrie Sougnez, Sabina Signoretti, Toni K. Choueiri, Mai P. Hoang, Bruce E. Johnson, Aaron R. Thorner, Paul Van Hummelen, Corey M. Gill, Frederick G. Barker, Mara Rosenberg, Aaron Chevalier, Aaron McKenna, Sung-Hye Park, Sun Ha Paek, Ian F. Dunn, William T. Curry, Elena Martinez-Saez, Joan Seoane, Josep Tabernero, Keith L. Ligon, Kristian Cibulskis, Peleg M. Horowitz, Michael S. Lawrence, Eliezer M. Van Allen, Robert T. Jones, Amaro Taylor-Weiner, Daniel P. Cahill, Sandro Santagata, Scott L. Carter, and Priscilla K. Brastianos

Abstract

Summary of clinically informative (TARGET) genes.

Published

2023

13. Supplementary Methods, Figures S1 - S20 from Genomic Characterization of Brain Metastases Reveals Branched Evolution and Potential Therapeutic Targets

Author

William C. Hahn, Gad Getz, David N. Louis, José Baselga, Tracy T. Batchelor, Rameen Beroukhim, Eric S. Lander, Stacey Gabriel, Levi Garraway, Matthew Meyerson, Anat Stemmer-Rachamimov, Eric P. Winer, Nancy U. Lin, Michael S. Rabin, Carrie Sougnez, Sabina Signoretti, Toni K. Choueiri, Mai P. Hoang, Bruce E. Johnson, Aaron R. Thorner, Paul Van Hummelen, Corey M. Gill, Frederick G. Barker, Mara Rosenberg, Aaron Chevalier, Aaron McKenna, Sung-Hye Park, Sun Ha Paek, Ian F. Dunn, William T. Curry, Elena Martinez-Saez, Joan Seoane, Josep Tabernero, Keith L. Ligon, Kristian Cibulskis, Peleg M. Horowitz, Michael S. Lawrence, Eliezer M. Van Allen, Robert T. Jones, Amaro Taylor-Weiner, Daniel P. Cahill, Sandro Santagata, Scott L. Carter, and Priscilla K. Brastianos

Abstract

Supplementary Methods, Figures S1 - S20. Figure S1. Branched evolution leads to tissue-sampling bias in primary tumor samples. Figure S2. Results of ABSOLUTE on samples from patient 418. Figure S3. 2D Bayesian clustering analysis of point-mutation CCF distributions in case 418. Figure S4. Bayesian clustering of private point-mutation CCF distributions in all sequenced tissue samples from case 418. Figure S5. Genetic alterations supporting phylogeny construction in case 418. Figure S6. Phylogenetic tree for case 418 Figure S7. Evolutionary relationships between primary tumor-samples and brain metastasis samples Figure S8. Detection of homozygous deletion in CDKN2A in the brain metastasis of case 24. Figure S9. Amplification of FGFR1 and MYC detected in the brain metastasis of case 331. Figure S10. Additional alterations under investigation for association with various targeted therapies. Figure S11. Power for paired-detection of somatic mutations. Figure S12. Amplification of CCNE1 detected in the brain metastasis of case 314. Figure S13. Amplification of EGFR detected in the brain metastasis of case 314. Figure S14. Amplification of MYC detected in the brain metastasis of case 308. Figure S15. Amplification of MYC detected in the brain metastasis of case 138. Figure S16. Amplifications of CDK6 and MET detected in the brain metastasis of case 138. Figure S17. Amplifications of CCNE1 and AKT2 detected in the brain metastasis of case 138. Figure S18. Amplification of EGFR detected in a regional lymph node from case 296. Figure S19. Power for somatic mutation detection in 86 matched primary-tumor and brain-metastasis samples. Figure S20. Calling of amplifications in primary-tumor samples and paired brain metastases.

Published

2023

14. Supplementary Figure 5 from Brain Tumor Cells in Circulation Are Enriched for Mesenchymal Gene Expression

Author

Daniel A. Haber, Shyamala Maheswaran, Mehmet Toner, David N. Louis, Tracy T. Batchelor, Jay S. Loeffler, William T. Curry, A. John Iafrate, Khalid Shah, Ravi Kapur, Lecia V. Sequist, S. Michael Rothenberg, Hiroaki Wakimoto, Andrew S. Chi, Deepak Bhere, Simeon Springer, Samantha M. Oliveira, Marissa W. Madden, Brian V. Nahed, and James P. Sullivan

Abstract

Immunohistologic and DNA-FISH analysis of tumor cells and CTCs from a patient with metastatic GBM.

Published

2023

15. Supplementary File 1 from Genomic Characterization of Brain Metastases Reveals Branched Evolution and Potential Therapeutic Targets

Author

William C. Hahn, Gad Getz, David N. Louis, José Baselga, Tracy T. Batchelor, Rameen Beroukhim, Eric S. Lander, Stacey Gabriel, Levi Garraway, Matthew Meyerson, Anat Stemmer-Rachamimov, Eric P. Winer, Nancy U. Lin, Michael S. Rabin, Carrie Sougnez, Sabina Signoretti, Toni K. Choueiri, Mai P. Hoang, Bruce E. Johnson, Aaron R. Thorner, Paul Van Hummelen, Corey M. Gill, Frederick G. Barker, Mara Rosenberg, Aaron Chevalier, Aaron McKenna, Sung-Hye Park, Sun Ha Paek, Ian F. Dunn, William T. Curry, Elena Martinez-Saez, Joan Seoane, Josep Tabernero, Keith L. Ligon, Kristian Cibulskis, Peleg M. Horowitz, Michael S. Lawrence, Eliezer M. Van Allen, Robert T. Jones, Amaro Taylor-Weiner, Daniel P. Cahill, Sandro Santagata, Scott L. Carter, and Priscilla K. Brastianos

Abstract

Supplementary File 1. Power for detection of somatic point mutations in coding exons of TARGET genes. The description for the plots in Supplementary File 1 can be found in the Legend of Supplementary Figure S1.

Published

2023

16. Supplementary Methods, Figure Legends from Brain Tumor Cells in Circulation Are Enriched for Mesenchymal Gene Expression

Author

Daniel A. Haber, Shyamala Maheswaran, Mehmet Toner, David N. Louis, Tracy T. Batchelor, Jay S. Loeffler, William T. Curry, A. John Iafrate, Khalid Shah, Ravi Kapur, Lecia V. Sequist, S. Michael Rothenberg, Hiroaki Wakimoto, Andrew S. Chi, Deepak Bhere, Simeon Springer, Samantha M. Oliveira, Marissa W. Madden, Brian V. Nahed, and James P. Sullivan

Abstract

Methods and Supplementary Figure Legends

Published

2023

17. Supplementary Figure 2 from Brain Tumor Cells in Circulation Are Enriched for Mesenchymal Gene Expression

Author

Daniel A. Haber, Shyamala Maheswaran, Mehmet Toner, David N. Louis, Tracy T. Batchelor, Jay S. Loeffler, William T. Curry, A. John Iafrate, Khalid Shah, Ravi Kapur, Lecia V. Sequist, S. Michael Rothenberg, Hiroaki Wakimoto, Andrew S. Chi, Deepak Bhere, Simeon Springer, Samantha M. Oliveira, Marissa W. Madden, Brian V. Nahed, and James P. Sullivan

Abstract

STEAM cocktail staining specifically identifies GBM cells.

Published

2023

18. Supplementary Table 1 from Brain Tumor Cells in Circulation Are Enriched for Mesenchymal Gene Expression

Author

Daniel A. Haber, Shyamala Maheswaran, Mehmet Toner, David N. Louis, Tracy T. Batchelor, Jay S. Loeffler, William T. Curry, A. John Iafrate, Khalid Shah, Ravi Kapur, Lecia V. Sequist, S. Michael Rothenberg, Hiroaki Wakimoto, Andrew S. Chi, Deepak Bhere, Simeon Springer, Samantha M. Oliveira, Marissa W. Madden, Brian V. Nahed, and James P. Sullivan

Abstract

Clinical association of CTC frequency

Published

2023

19. Supplementary Figure 4 from Brain Tumor Cells in Circulation Are Enriched for Mesenchymal Gene Expression

Author

Daniel A. Haber, Shyamala Maheswaran, Mehmet Toner, David N. Louis, Tracy T. Batchelor, Jay S. Loeffler, William T. Curry, A. John Iafrate, Khalid Shah, Ravi Kapur, Lecia V. Sequist, S. Michael Rothenberg, Hiroaki Wakimoto, Andrew S. Chi, Deepak Bhere, Simeon Springer, Samantha M. Oliveira, Marissa W. Madden, Brian V. Nahed, and James P. Sullivan

Abstract

Unsupervised hierarchical clustering analysis of patient and xenograft single cell qRT-PCR expression data.

Published

2023

20. Supplementary Figure 1 from Brain Tumor Cells in Circulation Are Enriched for Mesenchymal Gene Expression

Author

Daniel A. Haber, Shyamala Maheswaran, Mehmet Toner, David N. Louis, Tracy T. Batchelor, Jay S. Loeffler, William T. Curry, A. John Iafrate, Khalid Shah, Ravi Kapur, Lecia V. Sequist, S. Michael Rothenberg, Hiroaki Wakimoto, Andrew S. Chi, Deepak Bhere, Simeon Springer, Samantha M. Oliveira, Marissa W. Madden, Brian V. Nahed, and James P. Sullivan

Abstract

GBM8 and GBM24 growth in culture.

Published

2023

21. Supplementary Table 2 from Brain Tumor Cells in Circulation Are Enriched for Mesenchymal Gene Expression

Author

Daniel A. Haber, Shyamala Maheswaran, Mehmet Toner, David N. Louis, Tracy T. Batchelor, Jay S. Loeffler, William T. Curry, A. John Iafrate, Khalid Shah, Ravi Kapur, Lecia V. Sequist, S. Michael Rothenberg, Hiroaki Wakimoto, Andrew S. Chi, Deepak Bhere, Simeon Springer, Samantha M. Oliveira, Marissa W. Madden, Brian V. Nahed, and James P. Sullivan

Abstract

Tumor genotypes and CTC frequency

Published

2023

22. Supplementary File 3 from Genomic Characterization of Brain Metastases Reveals Branched Evolution and Potential Therapeutic Targets

Author

William C. Hahn, Gad Getz, David N. Louis, José Baselga, Tracy T. Batchelor, Rameen Beroukhim, Eric S. Lander, Stacey Gabriel, Levi Garraway, Matthew Meyerson, Anat Stemmer-Rachamimov, Eric P. Winer, Nancy U. Lin, Michael S. Rabin, Carrie Sougnez, Sabina Signoretti, Toni K. Choueiri, Mai P. Hoang, Bruce E. Johnson, Aaron R. Thorner, Paul Van Hummelen, Corey M. Gill, Frederick G. Barker, Mara Rosenberg, Aaron Chevalier, Aaron McKenna, Sung-Hye Park, Sun Ha Paek, Ian F. Dunn, William T. Curry, Elena Martinez-Saez, Joan Seoane, Josep Tabernero, Keith L. Ligon, Kristian Cibulskis, Peleg M. Horowitz, Michael S. Lawrence, Eliezer M. Van Allen, Robert T. Jones, Amaro Taylor-Weiner, Daniel P. Cahill, Sandro Santagata, Scott L. Carter, and Priscilla K. Brastianos

Abstract

Supplementary File 3. Detailed plots of the data used for phylogenetic inference in each case. The description for the plots in Supplementary File 3 can be found in the Legend of Supplementary Figure S13-S17.

Published

2023

23. Supplementary File 2 from Genomic Characterization of Brain Metastases Reveals Branched Evolution and Potential Therapeutic Targets

Author

William C. Hahn, Gad Getz, David N. Louis, José Baselga, Tracy T. Batchelor, Rameen Beroukhim, Eric S. Lander, Stacey Gabriel, Levi Garraway, Matthew Meyerson, Anat Stemmer-Rachamimov, Eric P. Winer, Nancy U. Lin, Michael S. Rabin, Carrie Sougnez, Sabina Signoretti, Toni K. Choueiri, Mai P. Hoang, Bruce E. Johnson, Aaron R. Thorner, Paul Van Hummelen, Corey M. Gill, Frederick G. Barker, Mara Rosenberg, Aaron Chevalier, Aaron McKenna, Sung-Hye Park, Sun Ha Paek, Ian F. Dunn, William T. Curry, Elena Martinez-Saez, Joan Seoane, Josep Tabernero, Keith L. Ligon, Kristian Cibulskis, Peleg M. Horowitz, Michael S. Lawrence, Eliezer M. Van Allen, Robert T. Jones, Amaro Taylor-Weiner, Daniel P. Cahill, Sandro Santagata, Scott L. Carter, and Priscilla K. Brastianos

Abstract

Supplementary File 2. Detailed plots of SCNA calls in TARGET genes. The description for the plots in Supplementary File 2 can be found in the Legend of Supplementary Figure S3.

Published

2023

24. Supplementary Figure 6 from Targetable Signaling Pathway Mutations Are Associated with Malignant Phenotype in IDH-Mutant Gliomas

Author

Andrew S. Chi, Daniel P. Cahill, A. John Iafrate, Tracy T. Batchelor, Matthew G. Vander Heiden, Sarah-Maria Fendt, Darrell R. Borger, Leif W. Ellisen, Dora Dias-Santagata, James C. Kim, Nina Lelic, Lindsay K. Klofas, Juxiang Chen, Kensuke Tateishi, Dan Zhao, Franziska Loebel, William T. Curry, Shota Tanaka, and Hiroaki Wakimoto

Abstract

PDF file - 102KB, Supplementary Figure S6. Sphere formation assay of MGG152 expressing N-MYC shRNA.

Published

2023

25. Figure S3 from Dopamine Receptor D5 is a Modulator of Tumor Response to Dopamine Receptor D2 Antagonism

Author

Joshua E. Allen, Wolfgang Oster, Patrick Y. Wen, Tracy T. Batchelor, Isabel Arrillaga-Romany, Robert Wechsler-Reya, Jessica Rusert, Mark R. Gilbert, Deric M. Park, Jinkyu Jung, Neil Charter, Sean Deacon, Rohinton S. Tarapore, Jessica Durrant, Alexander VanEngelenburg, Faye Doherty, Olivier Elemento, Wafik S. El-Deiry, Sophie Oster, C. Leah B. Kline, Coryandar Gilvary, Neel S. Madhukar, and Varun V. Prabhu

Abstract

Figure S3

Published

2023

26. Data from Vaccination with Irradiated Autologous Tumor Cells Mixed with Irradiated GM-K562 Cells Stimulates Antitumor Immunity and T Lymphocyte Activation in Patients with Recurrent Malignant Glioma

Author

Glenn Dranoff, Martin C. Mihm, Patrick Y. Wen, Tracy T. Batchelor, Alexandra J. Golby, Elizabeth R. Gerstner, Pamela S. Jones, Pankaj Agarwalla, Tetsuro Sasada, Matthias Piesche, Ramana Gorrepati, and William T. Curry

Abstract

Purpose: Recurrent malignant glioma carries a dismal prognosis, and novel therapies are needed. We examined the feasibility and safety of vaccination with irradiated autologous glioma cells mixed with irradiated GM-K562 cells in patients undergoing craniotomy for recurrent malignant glioma.Experimental Design: We initiated a phase I study examining the safety of 2 doses of GM-K562 cells mixed with autologous cells. Primary endpoints were feasibility and safety. Feasibility was defined as the ability for 60% of enrolled subjects to initiate vaccination. Dose-limiting toxicity was assessed via a 3+3 dose-escalation format, examining irradiated tumor cells mixed with 5 × 106 GM-K562 cells or 1 × 107 GM-K562 cells. Eligibility required a priori indication for resection of a recurrent high-grade glioma. We measured biological activity by measuring delayed type hypersensitivity (DTH) responses, humoral immunity against tumor-associated antigens, and T-lymphocyte activation.Results: Eleven patients were enrolled. Sufficient numbers of autologous tumor cells were harvested in 10 patients, all of whom went on to receive vaccine. There were no dose-limiting toxicities. Vaccination strengthened DTH responses to irradiated autologous tumor cells in most patients, and vigorous humoral responses to tumor-associated angiogenic cytokines were seen as well. T-lymphocyte activation was seen with significantly increased expression of CTLA-4, PD-1, 4-1BB, and OX40 by CD4+ cells and PD-1 and 4-1BB by CD8+ cells. Activation was coupled with vaccine-associated increase in the frequency of regulatory CD4+ T lymphocytes.Conclusions: Vaccination with irradiated autologous tumor cells mixed with GM-K562 cells is feasible, well tolerated, and active in patients with recurrent malignant glioma. Clin Cancer Res; 22(12); 2885–96. ©2016 AACR.

Published

2023

27. Supplementary Table S2 from Myc-Driven Glycolysis Is a Therapeutic Target in Glioblastoma

Author

Hiroaki Wakimoto, Andrew S. Chi, Daniel P. Cahill, Sudhandra Sundaram, Nina Lelic, Maristela L. Onozato, Keith T. Flaherty, Tracy T. Batchelor, William T. Curry, Quan Ho, A. John Iafrate, and Kensuke Tateishi

Abstract

Supplementary Table 2. Relationship of NAMPT inhibitor sensitivity, MYC/MYCN amplification, and Myc/N-Myc protein expression status in glioblastoma tumorsphere lines

Published

2023

28. Supplementary Figure Legends from The Alkylating Chemotherapeutic Temozolomide Induces Metabolic Stress in IDH1-Mutant Cancers and Potentiates NAD+ Depletion–Mediated Cytotoxicity

Author

Daniel P. Cahill, Andrew S. Chi, Hiroaki Wakimoto, A. John Iafrate, Tracy T. Batchelor, David E. Fisher, Shota Tanaka, Ganesh M. Shankar, Nina Lelic, Mara V.A. Koerner, Julie J. Miller, Fumi Higuchi, and Kensuke Tateishi

Abstract

''Temozolomide induced PARP activation deregulates NAD metabolism. Additive cytotoxic effect of TMZ and NAMPT inhibitors in IDH1 mutant cancers. NAD and cell viability effects with TMZ and NAMPT inhibitors in endogenous IDH1 mutant cancers. Combination treatment with TMZ and NAMPT inhibitor in IDH1 mutant and wild-type cells. Cell death mechanisms that underlie combined TMZ and NAMPT inhibitor treatment in IDH1 mutant cells. In vivo effects of combined TMZ and NAMPT inhibitor treatment for endogenous IDH1 mutant cancer.''

Published

2023

29. Supplementary Figure 5 from Targetable Signaling Pathway Mutations Are Associated with Malignant Phenotype in IDH-Mutant Gliomas

Author

Andrew S. Chi, Daniel P. Cahill, A. John Iafrate, Tracy T. Batchelor, Matthew G. Vander Heiden, Sarah-Maria Fendt, Darrell R. Borger, Leif W. Ellisen, Dora Dias-Santagata, James C. Kim, Nina Lelic, Lindsay K. Klofas, Juxiang Chen, Kensuke Tateishi, Dan Zhao, Franziska Loebel, William T. Curry, Shota Tanaka, and Hiroaki Wakimoto

Abstract

PDF file - 266KB, Supplementary Figure S5. Maintenance of genotype upon serial xenotransplantation.

Published

2023

30. Lymphocyte Immunophenotyping methods from Vaccination with Irradiated Autologous Tumor Cells Mixed with Irradiated GM-K562 Cells Stimulates Antitumor Immunity and T Lymphocyte Activation in Patients with Recurrent Malignant Glioma

Author

Glenn Dranoff, Martin C. Mihm, Patrick Y. Wen, Tracy T. Batchelor, Alexandra J. Golby, Elizabeth R. Gerstner, Pamela S. Jones, Pankaj Agarwalla, Tetsuro Sasada, Matthias Piesche, Ramana Gorrepati, and William T. Curry

Abstract

Extended methods for flow cytometry for lymphocyte phenotyping.

Published

2023

31. ELISA for angiogenic cytokines from Vaccination with Irradiated Autologous Tumor Cells Mixed with Irradiated GM-K562 Cells Stimulates Antitumor Immunity and T Lymphocyte Activation in Patients with Recurrent Malignant Glioma

Author

Glenn Dranoff, Martin C. Mihm, Patrick Y. Wen, Tracy T. Batchelor, Alexandra J. Golby, Elizabeth R. Gerstner, Pamela S. Jones, Pankaj Agarwalla, Tetsuro Sasada, Matthias Piesche, Ramana Gorrepati, and William T. Curry

Abstract

Extended methods for ELISA assay for angiogenic cytokines.

Published

2023

32. Supplementary Figures 1-6 from The Alkylating Chemotherapeutic Temozolomide Induces Metabolic Stress in IDH1-Mutant Cancers and Potentiates NAD+ Depletion–Mediated Cytotoxicity

Author

Daniel P. Cahill, Andrew S. Chi, Hiroaki Wakimoto, A. John Iafrate, Tracy T. Batchelor, David E. Fisher, Shota Tanaka, Ganesh M. Shankar, Nina Lelic, Mara V.A. Koerner, Julie J. Miller, Fumi Higuchi, and Kensuke Tateishi

Abstract

'Temozolomide induced PARP activation deregulates NAD metabolism. Additive cytotoxic effect of TMZ and NAMPT inhibitors in IDH1 mutant cancers. NAD and cell viability effects with TMZ and NAMPT inhibitors in endogenous IDH1 mutant cancers. Combination treatment with TMZ and NAMPT inhibitor in IDH1 mutant and wild-type cells. Cell death mechanisms that underlie combined TMZ and NAMPT inhibitor treatment in IDH1 mutant cells. In vivo effects of combined TMZ and NAMPT inhibitor treatment for endogenous IDH1 mutant cancer.'

Published

2023

33. Supplementary Figures from Myc-Driven Glycolysis Is a Therapeutic Target in Glioblastoma

Author

Hiroaki Wakimoto, Andrew S. Chi, Daniel P. Cahill, Sudhandra Sundaram, Nina Lelic, Maristela L. Onozato, Keith T. Flaherty, Tracy T. Batchelor, William T. Curry, Quan Ho, A. John Iafrate, and Kensuke Tateishi

Abstract

Supplementary Figure S1. Nampt inhibitor effects in glioblastoma tumorsphere cells. Supplementary Figure S2. Characterization of Nampt inhibitor effects in MYC/MYCN driven glioblastoma cells. Supplementary Figure S3. Characterization of NAD+-synthesis pathways in glioblastoma cells. Supplementary Figure S4. Nampt inhibitors induce apoptosis and disrupt intracellular metabolism pathways in MYC/MYCN amplified glioblastoma cells. Supplementary Figure S5. Fluorescent in situ hybridization (FISH) for MYC and MYCN in standard cancer cell lines. Supplementary Figure S6. Effect of Nampt inhibitors in Myc-driven standard cancer cell lines. Supplementary Figure S7. In vivo efficacy of Nampt inhibitor in MYC amplified H1975 xenografts. Supplementary Figure S8. NAMPT inhibitors were well tolerated in SCID mice bearing flank or orthotopic xenografts.

Published

2023

34. Supplementary Figure 2 from Targetable Signaling Pathway Mutations Are Associated with Malignant Phenotype in IDH-Mutant Gliomas

Author

Andrew S. Chi, Daniel P. Cahill, A. John Iafrate, Tracy T. Batchelor, Matthew G. Vander Heiden, Sarah-Maria Fendt, Darrell R. Borger, Leif W. Ellisen, Dora Dias-Santagata, James C. Kim, Nina Lelic, Lindsay K. Klofas, Juxiang Chen, Kensuke Tateishi, Dan Zhao, Franziska Loebel, William T. Curry, Shota Tanaka, and Hiroaki Wakimoto

Abstract

PDF file - 404KB, Supplementary Figure S2. IDH1-mutant glioma orthotopic xenografts recapitulate histopathological features of the respective patient tumors.

Published

2023

35. Data from Loss of the Mismatch Repair Protein MSH6 in Human Glioblastomas Is Associated with Tumor Progression during Temozolomide Treatment

Author

David N. Louis, A. John Iafrate, William T. Curry, Michael R. Stratton, P. Andrew Futreal, Tracy T. Batchelor, Linsey B. Reavie, Candice A. Romany, Patrick J. Codd, Rebecca A. Betensky, Kymberly K. Levine, and Daniel P. Cahill

Abstract

Purpose: Glioblastomas are treated by surgical resection followed by radiotherapy [X-ray therapy (XRT)] and the alkylating chemotherapeutic agent temozolomide. Recently, inactivating mutations in the mismatch repair gene MSH6 were identified in two glioblastomas recurrent post-temozolomide. Because mismatch repair pathway inactivation is a known mediator of alkylator resistance in vitro, these findings suggested that MSH6 inactivation was causally linked to these two recurrences. However, the extent of involvement of MSH6 in glioblastoma is unknown. We sought to determine the overall frequency and clinical relevance of MSH6 alterations in glioblastomas.Experimental Design: The MSH6 gene was sequenced in 54 glioblastomas. MSH6 and O6-methylguanine methyltransferase (MGMT) immunohistochemistry was systematically scored in a panel of 46 clinically well-characterized glioblastomas, and the corresponding patient response to treatment evaluated.Results:MSH6 mutation was not observed in any pretreatment glioblastoma (0 of 40), whereas 3 of 14 recurrent cases had somatic mutations (P = 0.015). MSH6 protein expression was detected in all pretreatment (17 of 17) cases examined but, notably, expression was lost in 7 of 17 (41%) recurrences from matched post–XRT + temozolomide cases (P = 0.016). Loss of MSH6 was not associated with O6-methylguanine methyltransferase status. Measurements of in vivo tumor growth using three-dimensional reconstructed magnetic resonance imaging showed that MSH6-negative glioblastomas had a markedly increased rate of growth while under temozolomide treatment (3.17 versus 0.04 cc/mo for MSH6-positive tumors; P = 0.020).Conclusions: Loss of MSH6 occurs in a subset of post–XRT + temozolomide glioblastoma recurrences and is associated with tumor progression during temozolomide treatment, mirroring the alkylator resistance conferred by MSH6 inactivation in vitro. MSH6 deficiency may therefore contribute to the emergence of recurrent glioblastomas during temozolomide treatment.

Published

2023

36. Supplementary Figure 3 from Targetable Signaling Pathway Mutations Are Associated with Malignant Phenotype in IDH-Mutant Gliomas

Author

Andrew S. Chi, Daniel P. Cahill, A. John Iafrate, Tracy T. Batchelor, Matthew G. Vander Heiden, Sarah-Maria Fendt, Darrell R. Borger, Leif W. Ellisen, Dora Dias-Santagata, James C. Kim, Nina Lelic, Lindsay K. Klofas, Juxiang Chen, Kensuke Tateishi, Dan Zhao, Franziska Loebel, William T. Curry, Shota Tanaka, and Hiroaki Wakimoto

Abstract

PDF file - 347KB, Supplementary Figure S3. Proliferation index of IDH1-mutant glioma orthotopic xenografts (MIB-1).

Published

2023

37. Supplementary Table 2 from Targetable Signaling Pathway Mutations Are Associated with Malignant Phenotype in IDH-Mutant Gliomas

Author

Andrew S. Chi, Daniel P. Cahill, A. John Iafrate, Tracy T. Batchelor, Matthew G. Vander Heiden, Sarah-Maria Fendt, Darrell R. Borger, Leif W. Ellisen, Dora Dias-Santagata, James C. Kim, Nina Lelic, Lindsay K. Klofas, Juxiang Chen, Kensuke Tateishi, Dan Zhao, Franziska Loebel, William T. Curry, Shota Tanaka, and Hiroaki Wakimoto

Abstract

XLS file - 24KB, Supplementary Table S2. Primers used for sequencing.

Published

2023

38. Data from Treatment Response Assessment in IDH-Mutant Glioma Patients by Noninvasive 3D Functional Spectroscopic Mapping of 2-Hydroxyglutarate

Author

Daniel P. Cahill, Bruce R. Rosen, Andrew S. Chi, William G. Kaelin, Elizabeth R. Gerstner, Tracy T. Batchelor, Jorg Dietrich, A. John Iafrate, Matthew G. Vander Heiden, Małgorzata Marjańska, Wolfgang Bogner, Franziska Loebel, and Ovidiu C. Andronesi

Abstract

Purpose: Measurements of objective response rates are critical to evaluate new glioma therapies. The hallmark metabolic alteration in gliomas with mutant isocitrate dehydrogenase (IDH) is the overproduction of oncometabolite 2-hydroxyglutarate (2HG), which plays a key role in malignant transformation. 2HG represents an ideal biomarker to probe treatment response in IDH-mutant glioma patients, and we hypothesized a decrease in 2HG levels would be measureable by in vivo magnetic resonance spectroscopy (MRS) as a result of antitumor therapy.Experimental Design: We report a prospective longitudinal imaging study performed in 25 IDH-mutant glioma patients receiving adjuvant radiation and chemotherapy. A newly developed 3D MRS imaging was used to noninvasively image 2HG. Paired Student t test was used to compare pre- and posttreatment tumor 2HG values. Test–retest measurements were performed to determine the threshold for 2HG functional spectroscopic maps (fSM). Univariate and multivariate regression were performed to correlate 2HG changes with Karnofsky performance score (KPS).Results: We found that mean 2HG (2HG/Cre) levels decreased significantly (median = 48.1%; 95% confidence interval = 27.3%–56.5%; P = 0.007) in the posttreatment scan. The volume of decreased 2HG correlates (R2 = 0.88, P = 0.002) with clinical status evaluated by KPS.Conclusions: We demonstrate that dynamic measurements of 2HG are feasible by 3D fSM, and the decrease of 2HG levels can monitor treatment response in patients with IDH-mutant gliomas. Our results indicate that quantitative in vivo 2HG imaging may be used for precision medicine and early response assessment in clinical trials of therapies targeting IDH-mutant gliomas. Clin Cancer Res; 22(7); 1632–41. ©2015 AACR.

Published

2023

39. Supplementary Figure 1 from Targetable Signaling Pathway Mutations Are Associated with Malignant Phenotype in IDH-Mutant Gliomas

Author

Andrew S. Chi, Daniel P. Cahill, A. John Iafrate, Tracy T. Batchelor, Matthew G. Vander Heiden, Sarah-Maria Fendt, Darrell R. Borger, Leif W. Ellisen, Dora Dias-Santagata, James C. Kim, Nina Lelic, Lindsay K. Klofas, Juxiang Chen, Kensuke Tateishi, Dan Zhao, Franziska Loebel, William T. Curry, Shota Tanaka, and Hiroaki Wakimoto

Abstract

PDF file - 791KB, Supplementary Figure S1. Additional mouse orthotopic xenografts generated from patient IDH1 R132H-mutant gliomas.

Published

2023

40. Supplementary Data from A Hyperactive RelA/p65-Hexokinase 2 Signaling Axis Drives Primary Central Nervous System Lymphoma

Author

Tetsuya Yamamoto, Koichi Ichimura, Motoo Nagane, Tracy T. Batchelor, Andrew S. Chi, Hiroaki Wakimoto, Daniel P. Cahill, Hiroyuki Mano, Shoji Yamanaka, Akihide Ryo, Yukihiko Fujii, Julie J. Miller, Ichio Aoki, Hidetoshi Murata, Jun Suenaga, Ryohei Miyazaki, Makoto Ohtake, Mayuko Nishi, Naoki Ikegaya, Manabu Natsumeda, Shilpa S. Tummala, Alexandria L. Fink, Kentaro Ohki, Naoko Udaka, Norio Shiba, Yuko Matsushita, Jun Watanabe, Akio Miyake, Toshihide Ueno, Yukie Yoshii, Jo Sasame, Taishi Nakamura, Nobuyoshi Sasaki, Masahito Kawazu, Yohei Miyake, and Kensuke Tateishi

Abstract

Supplementary document

Published

2023

41. Data from Dopamine Receptor D5 is a Modulator of Tumor Response to Dopamine Receptor D2 Antagonism

Author

Joshua E. Allen, Wolfgang Oster, Patrick Y. Wen, Tracy T. Batchelor, Isabel Arrillaga-Romany, Robert Wechsler-Reya, Jessica Rusert, Mark R. Gilbert, Deric M. Park, Jinkyu Jung, Neil Charter, Sean Deacon, Rohinton S. Tarapore, Jessica Durrant, Alexander VanEngelenburg, Faye Doherty, Olivier Elemento, Wafik S. El-Deiry, Sophie Oster, C. Leah B. Kline, Coryandar Gilvary, Neel S. Madhukar, and Varun V. Prabhu

Abstract

Purpose:Dopamine receptor D2 (DRD2) is a G protein–coupled receptor antagonized by ONC201, an anticancer small molecule in clinical trials for high-grade gliomas and other malignancies. DRD5 is a dopamine receptor family member that opposes DRD2 signaling. We investigated the expression of these dopamine receptors in cancer and their influence on tumor cell sensitivity to ONC201.Experimental Design:The Cancer Genome Atlas was used to determine DRD2/DRD5 expression broadly across human cancers. Cell viability assays were performed with ONC201 in >1,000 Genomic of Drug Sensitivity in Cancer and NCI60 cell lines. IHC staining of DRD2/DRD5 was performed on tissue microarrays and archival tumor tissues of glioblastoma patients treated with ONC201. Whole exome sequencing was performed in RKO cells with and without acquired ONC201 resistance. Wild-type and mutant DRD5 constructs were generated for overexpression studies.Results:DRD2 overexpression broadly occurs across tumor types and is associated with a poor prognosis. Whole exome sequencing of cancer cells with acquired resistance to ONC201 revealed a de novo Q366R mutation in the DRD5 gene. Expression of Q366R DRD5 was sufficient to induce tumor cell apoptosis, consistent with a gain-of-function. DRD5 overexpression in glioblastoma cells enhanced DRD2/DRD5 heterodimers and DRD5 expression was inversely correlated with innate tumor cell sensitivity to ONC201. Investigation of archival tumor samples from patients with recurrent glioblastoma treated with ONC201 revealed that low DRD5 expression was associated with relatively superior clinical outcomes.Conclusions:These results implicate DRD5 as a negative regulator of DRD2 signaling and tumor sensitivity to ONC201 DRD2 antagonism.

Published

2023

42. Supplementary Table from PI3K/AKT/mTOR Pathway Alterations Promote Malignant Progression and Xenograft Formation in Oligodendroglial Tumors

Author

Daniel P. Cahill, Hiroaki Wakimoto, A. John Iafrate, Andrew S. Chi, Tracy T. Batchelor, Koichi Ichimura, Tetsuya Yamamoto, Dora Dias-Santagata, William T. Curry, Shoji Yamanaka, Akihide Ryo, Hidetoshi Murata, Naoko Udaka, Hiroki Taguchi, Takashi Shuto, Shigeo Mukaihara, Shigeo Matsunaga, Ryogo Minamimoto, Takahiro Tanaka, Kenji Fujimoto, Jo Sasame, Yohei Miyake, Mara V.A. Koerner, Nina Lelic, Alexandria L. Fink, Shilpa S. Tummala, Julie J. Miller, Mayuko Nishi, Shigeta Miyake, Yuko Matsushita, Erik A. Williams, Tareq A. Juratli, Taishi Nakamura, and Kensuke Tateishi

Abstract

Supplementary Table 1 Primers used for PCR amplification and sequencing Supplementary Table 2 Results of Multiplex PCR based MGH SNAPShot assay, Pyrosequencing and Sanger sequencing in YMG6 patient and xenograft cells Supplementary Table 3 Analysis of microsatellite instability in YMG6 parent and xenograft tumors Supplementary Table 4 Quantitative analysis for MGMT methylation status in YMG6 cells Supplementary Table 5 Multiplex PCR based MGH SnaPShot assay for oligodendroglial tumors Supplementary Table 6 Correlation of xenograft lethality and phosphorylation of PI3K pathway protein Supplementary Table 7 Phosphorylation in PI3K pathway in oligodendroglioma xenograft model Supplementary Table 8 Clinical characteristics in oligodendroglial tumor patients

Published

2023

43. Table S1 from Dopamine Receptor D5 is a Modulator of Tumor Response to Dopamine Receptor D2 Antagonism

Author

Joshua E. Allen, Wolfgang Oster, Patrick Y. Wen, Tracy T. Batchelor, Isabel Arrillaga-Romany, Robert Wechsler-Reya, Jessica Rusert, Mark R. Gilbert, Deric M. Park, Jinkyu Jung, Neil Charter, Sean Deacon, Rohinton S. Tarapore, Jessica Durrant, Alexander VanEngelenburg, Faye Doherty, Olivier Elemento, Wafik S. El-Deiry, Sophie Oster, C. Leah B. Kline, Coryandar Gilvary, Neel S. Madhukar, and Varun V. Prabhu

Abstract

Table S1

Published

2023

44. Supplementary Figure from A Hyperactive RelA/p65-Hexokinase 2 Signaling Axis Drives Primary Central Nervous System Lymphoma

Author

Tetsuya Yamamoto, Koichi Ichimura, Motoo Nagane, Tracy T. Batchelor, Andrew S. Chi, Hiroaki Wakimoto, Daniel P. Cahill, Hiroyuki Mano, Shoji Yamanaka, Akihide Ryo, Yukihiko Fujii, Julie J. Miller, Ichio Aoki, Hidetoshi Murata, Jun Suenaga, Ryohei Miyazaki, Makoto Ohtake, Mayuko Nishi, Naoki Ikegaya, Manabu Natsumeda, Shilpa S. Tummala, Alexandria L. Fink, Kentaro Ohki, Naoko Udaka, Norio Shiba, Yuko Matsushita, Jun Watanabe, Akio Miyake, Toshihide Ueno, Yukie Yoshii, Jo Sasame, Taishi Nakamura, Nobuyoshi Sasaki, Masahito Kawazu, Yohei Miyake, and Kensuke Tateishi

Abstract

Supplementary Figure S1-S7

Published

2023

45. Supplemental Figure from A Multicenter, Phase II, Randomized, Noncomparative Clinical Trial of Radiation and Temozolomide with or without Vandetanib in Newly Diagnosed Glioblastoma Patients

Author

Patrick Y. Wen, Keith L. Ligon, Tracy T. Batchelor, Rakesh K. Jain, Katrina H. Smith, Mary Gerard, Christine S. McCluskey, Brian M. Alexander, Stephanie E. Weiss, Rameen Beroukhim, Andrew D. Norden, Jan Drappatz, Shakti Ramkissoon, Jason T. Huse, Marek Ancukiewicz, Alona Muzikansky, Benjamin W. Purow, Tom Mikkelsen, Eric T. Wong, Andrew B. Lassman, David Schiff, Dan G. Duda, Thomas J. Kaley, and Eudocia Q. Lee

Abstract

Supplemental Figure: Mean plasma concentrations of vandetanib.

Published

2023

46. Supplementary Data clean from Treatment Response Assessment in IDH-Mutant Glioma Patients by Noninvasive 3D Functional Spectroscopic Mapping of 2-Hydroxyglutarate

Author

Daniel P. Cahill, Bruce R. Rosen, Andrew S. Chi, William G. Kaelin, Elizabeth R. Gerstner, Tracy T. Batchelor, Jorg Dietrich, A. John Iafrate, Matthew G. Vander Heiden, Małgorzata Marjańska, Wolfgang Bogner, Franziska Loebel, and Ovidiu C. Andronesi

Abstract

This file contains 3 Tables and 9 Figures with additional results and details of analysis related to the main results presented in the manuscript. The complete list of figures and tables is provided below. Table 1S. Baseline metabolite levels relative to creatine. Table 2S. Demographic, genomic, molecular, histological, radiological and clinical data. Table 3S. Fractional changes for all imaging biomarkers. Table 4S. General Linear Model with change of KPS as dependent variable and grade, age and fractional volume of decreased 2HG/Cre as covariates. Figure 1S. 3D MRSI pulse sequence for 2HG imaging, detailed diagram. Figure 2S. Quantum mechanics simulations of 2HG spectral editing for MEGA-LASER, MEGA-PRESS and PRESS-97 sequences. Figure 3S. Simulations of 2HG editing for MEGA-LASER and PRESS-97 sequences in the presence of B1 field inhomogeneity. Figure 4S. Mitigation of subtraction artifacts caused by motion and scanner instability in J-difference MR spectroscopy using real-time prospective motion correction, shim update and reacquisition. Figure 5S. Metabolic maps before image interpolation. Figure 6S. Examples of OFF and difference (DIFF) MEGA-LASER spectra from 3D MRSI voxels located in the tumor and contralateral normal appearing white matter, pre- and post-treatment respectively. Figure 7S. Distributions of Δ2HG/Cre in the test-retest and post-pre longitudinal data sets. Figure 8S. Comparison of functional spectroscopic maps (fSM) and functional diffusion maps (fDM). Figure 9S. Relation between residual tumor measured by FLAIR hyperintensity volume and the SNR and CRLB of 2HG. Notes. Details related to data analysis in Figures 7S and 9S.

Published

2023

47. Supplemental Tables 1-3 from A Multicenter, Phase II, Randomized, Noncomparative Clinical Trial of Radiation and Temozolomide with or without Vandetanib in Newly Diagnosed Glioblastoma Patients

Author

Patrick Y. Wen, Keith L. Ligon, Tracy T. Batchelor, Rakesh K. Jain, Katrina H. Smith, Mary Gerard, Christine S. McCluskey, Brian M. Alexander, Stephanie E. Weiss, Rameen Beroukhim, Andrew D. Norden, Jan Drappatz, Shakti Ramkissoon, Jason T. Huse, Marek Ancukiewicz, Alona Muzikansky, Benjamin W. Purow, Tom Mikkelsen, Eric T. Wong, Andrew B. Lassman, David Schiff, Dan G. Duda, Thomas J. Kaley, and Eudocia Q. Lee

Abstract

Supplemental Tables 1-3. Supplementary Table 1: Correlations in the vandetanib/RT/TMZ arm between best radiographic responses with pre-treatment and on-treatment changes in blood biomarkers. Supplementary Table 2: Correlations in the vandetanib/RT/TMZ arm between overall survival with pre-treatment and on-treatment changes in blood biomarkers. Supplementary Table 3: Comparison of PFS or OS by log-rank p-value based on tissue biomarker analysis

Published

2023

48. Supplementary Figure 4 from Targetable Signaling Pathway Mutations Are Associated with Malignant Phenotype in IDH-Mutant Gliomas

Author

Andrew S. Chi, Daniel P. Cahill, A. John Iafrate, Tracy T. Batchelor, Matthew G. Vander Heiden, Sarah-Maria Fendt, Darrell R. Borger, Leif W. Ellisen, Dora Dias-Santagata, James C. Kim, Nina Lelic, Lindsay K. Klofas, Juxiang Chen, Kensuke Tateishi, Dan Zhao, Franziska Loebel, William T. Curry, Shota Tanaka, and Hiroaki Wakimoto

Abstract

PDF file - 323KB, Supplementary Figure S4. Sequencing of the IDH1 R132 locus in IDH1-mutant glioma xenografts.

Published

2023

49. Data from Targetable Signaling Pathway Mutations Are Associated with Malignant Phenotype in IDH-Mutant Gliomas

Author

Andrew S. Chi, Daniel P. Cahill, A. John Iafrate, Tracy T. Batchelor, Matthew G. Vander Heiden, Sarah-Maria Fendt, Darrell R. Borger, Leif W. Ellisen, Dora Dias-Santagata, James C. Kim, Nina Lelic, Lindsay K. Klofas, Juxiang Chen, Kensuke Tateishi, Dan Zhao, Franziska Loebel, William T. Curry, Shota Tanaka, and Hiroaki Wakimoto

Abstract

Purpose: Isocitrate dehydrogenase (IDH) gene mutations occur in low-grade and high-grade gliomas. We sought to identify the genetic basis of malignant phenotype heterogeneity in IDH-mutant gliomas.Methods: We prospectively implanted tumor specimens from 20 consecutive IDH1-mutant glioma resections into mouse brains and genotyped all resection specimens using a CLIA-certified molecular panel. Gliomas with cancer driver mutations were tested for sensitivity to targeted inhibitors in vitro. Associations between genomic alterations and outcomes were analyzed in patients.Results: By 10 months, 8 of 20 IDH1-mutant gliomas developed intracerebral xenografts. All xenografts maintained mutant IDH1 and high levels of 2-hydroxyglutarate on serial transplantation. All xenograft-producing gliomas harbored “lineage-defining” mutations in CIC (oligodendroglioma) or TP53 (astrocytoma), and 6 of 8 additionally had activating mutations in PIK3CA or amplification of PDGFRA, MET, or N-MYC. Only IDH1 and CIC/TP53 mutations were detected in non–xenograft-forming gliomas (P = 0.0007). Targeted inhibition of the additional alterations decreased proliferation in vitro. Moreover, we detected alterations in known cancer driver genes in 13.4% of IDH-mutant glioma patients, including PIK3CA, KRAS, AKT, or PTEN mutation or PDGFRA, MET, or N-MYC amplification. IDH/CIC mutant tumors were associated with PIK3CA/KRAS mutations whereas IDH/TP53 tumors correlated with PDGFRA/MET amplification. Presence of driver alterations at progression was associated with shorter subsequent progression-free survival (median 9.0 vs. 36.1 months; P = 0.0011).Conclusion: A subset of IDH-mutant gliomas with mutations in driver oncogenes has a more malignant phenotype in patients. Identification of these alterations may provide an opportunity for use of targeted therapies in these patients. Clin Cancer Res; 20(11); 2898–909. ©2014 AACR.

Published

2023

50. Data from Myc-Driven Glycolysis Is a Therapeutic Target in Glioblastoma

Author

Hiroaki Wakimoto, Andrew S. Chi, Daniel P. Cahill, Sudhandra Sundaram, Nina Lelic, Maristela L. Onozato, Keith T. Flaherty, Tracy T. Batchelor, William T. Curry, Quan Ho, A. John Iafrate, and Kensuke Tateishi

Abstract

Purpose: Deregulated Myc drives an oncogenic metabolic state, including pseudohypoxic glycolysis, adapted for the constitutive production of biomolecular precursors to feed rapid tumor cell growth. In glioblastoma, Myc facilitates renewal of the tumor-initiating cell reservoir contributing to tumor maintenance. We investigated whether targeting the Myc-driven metabolic state could be a selectively toxic therapeutic strategy for glioblastoma.Experimental Design: The glycolytic dependency of Myc-driven glioblastoma was tested using 13C metabolic flux analysis, glucose-limiting culture assays, and glycolysis inhibitors, including inhibitors of the NAD+ salvage enzyme nicotinamide phosphoribosyl-transferase (NAMPT), in MYC and MYCN shRNA knockdown and lentivirus overexpression systems and in patient-derived glioblastoma tumorspheres with and without MYC/MYCN amplification. The in vivo efficacy of glycolyic inhibition was tested using NAMPT inhibitors in MYCN-amplified patient-derived glioblastoma orthotopic xenograft mouse models.Results: Enforced Myc overexpression increased glucose flux and expression of glycolytic enzymes in glioblastoma cells. Myc and N-Myc knockdown and Myc overexpression systems demonstrated that Myc activity determined sensitivity and resistance to inhibition of glycolysis. Small-molecule inhibitors of glycolysis, particularly NAMPT inhibitors, were selectively toxic to MYC/MYCN–amplified patient-derived glioblastoma tumorspheres. NAMPT inhibitors were potently cytotoxic, inducing apoptosis and significantly extended the survival of mice bearing MYCN-amplified patient-derived glioblastoma orthotopic xenografts.Conclusions: Myc activation in glioblastoma generates a dependency on glycolysis and an addiction to metabolites required for glycolysis. Glycolytic inhibition via NAMPT inhibition represents a novel metabolically targeted therapeutic strategy for MYC or MYCN-amplified glioblastoma and potentially other cancers genetically driven by Myc. Clin Cancer Res; 22(17); 4452–65. ©2016 AACR.

Published

2023