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1. SUPRAMAX-study: supramaximal resection versus maximal resection for glioblastoma patients: study protocol for an international multicentre prospective cohort study (ENCRAM 2201)

Author

Sandro M Krieg, Susan M Chang, Steven De Vleeschouwer, Mitchel Berger, Arnaud J P E Vincent, Brian V Nahed, Philippe Schucht, Martin J van den Bent, Jasper Kees Wim Gerritsen, Christine Jungk, Marike Lianne Daphne Broekman, Djaina D Satoer, Jacob S Young, and Sebastian Ille

Subjects
Medicine
Abstract

Introduction A greater extent of resection of the contrast-enhancing (CE) tumour part has been associated with improved outcomes in glioblastoma. Recent results suggest that resection of the non-contrast-enhancing (NCE) part might yield even better survival outcomes (supramaximal resection, SMR). Therefore, this study evaluates the efficacy and safety of SMR with and without mapping techniques in high-grade glioma (HGG) patients in terms of survival, functional, neurological, cognitive and quality of life outcomes. Furthermore, it evaluates which patients benefit the most from SMR, and how they could be identified preoperatively.Methods and analysis This study is an international, multicentre, prospective, two-arm cohort study of observational nature. Consecutive glioblastoma patients will be operated with SMR or maximal resection at a 1:1 ratio. Primary endpoints are (1) overall survival and (2) proportion of patients with National Institute of Health Stroke Scale deterioration at 6 weeks, 3 months and 6 months postoperatively. Secondary endpoints are (1) residual CE and NCE tumour volume on postoperative T1-contrast and FLAIR (Fluid-attenuated inversion recovery) MRI scans; (2) progression-free survival; (3) receipt of adjuvant therapy with chemotherapy and radiotherapy; and (4) quality of life at 6 weeks, 3 months and 6 months postoperatively. The total duration of the study is 5 years. Patient inclusion is 4 years, follow-up is 1 year.Ethics and dissemination The study has been approved by the Medical Ethics Committee (METC Zuid-West Holland/Erasmus Medical Center; MEC-2020-0812). The results will be published in peer-reviewed academic journals and disseminated to patient organisations and media.

Published
2024
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2. The creation of the Global Scales for Early Development (GSED) for children aged 0–3 years: combining subject matter expert judgements with big data

Author

Sunil Sazawal, Salahuddin Ahmed, Fan Jiang, Tarun Dua, Melissa Gladstone, Fahmida Tofail, Vanessa Cavallera, Alexandra Brentani, Yvonne Schönbeck, Iris Eekhout, Maureen M Black, Rasheda Khanam, Magdalena Janus, Ann M Weber, Marta Rubio-Codina, Stef van Buuren, Susan M Chang, Arsene Zongo, Dana McCoy, Yunting Zhang, Gareth McCray, Patricia Kariger, Imran Nisar, Ambreen Nizar, Abdullah Baqui, Katelyn Hepworth, Marcus Waldman, Abbie Raikes, Kieran Bromley, Arunangshu Dutta, Symone B Detmar, Romuald Anago, Pacifico Mercadante, Raghbir Kaur, Samuel N Kembou, and Gill A Lancaster

Subjects
Medicine (General), R5-920, Infectious and parasitic diseases, RC109-216
Abstract

Introduction With the ratification of the Sustainable Development Goals, there is an increased emphasis on early childhood development (ECD) and well-being. The WHO led Global Scales for Early Development (GSED) project aims to provide population and programmatic level measures of ECD for 0–3 years that are valid, reliable and have psychometrically stable performance across geographical, cultural and language contexts. This paper reports on the creation of two measures: (1) the GSED Short Form (GSED-SF)—a caregiver reported measure for population-evaluation—self-administered with no training required and (2) the GSED Long Form (GSED-LF)—a directly administered/observed measure for programmatic evaluation—administered by a trained professional.Methods We selected 807 psychometrically best-performing items using a Rasch measurement model from an ECD measurement databank which comprised 66 075 children assessed on 2211 items from 18 ECD measures in 32 countries. From 766 of these items, in-depth subject matter expert judgements were gathered to inform final item selection. Specifically collected were data on (1) conceptual matches between pairs of items originating from different measures, (2) developmental domain(s) measured by each item and (3) perceptions of feasibility of administration of each item in diverse contexts. Prototypes were finalised through a combination of psychometric performance evaluation and expert consensus to optimally identify items.Results We created the GSED-SF (139 items) and GSED-LF (157 items) for tablet-based and paper-based assessments, with an optimal set of items that fit the Rasch model, met subject matter expert criteria, avoided conceptual overlap, covered multiple domains of child development and were feasible to implement across diverse settings.Conclusions State-of-the-art quantitative and qualitative procedures were used to select of theoretically relevant and globally feasible items representing child development for children aged 0–3 years. GSED-SF and GSED-LF will be piloted and validated in children across diverse cultural, demographic, social and language contexts for global use.

Published
2023
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4. Multiplatform molecular analyses refine classification of gliomas arising in patients with neurofibromatosis type 1

Author

Calixto-Hope G. Lucas, Emily A. Sloan, Rohit Gupta, Jasper Wu, Drew Pratt, Harish N. Vasudevan, Ajay Ravindranathan, Jairo Barreto, Erik A. Williams, Anny Shai, Nicholas S. Whipple, Carol S. Bruggers, Ossama Maher, Burt Nabors, Michael Rodriguez, David Samuel, Melandee Brown, Jason Carmichael, Rufei Lu, Kanish Mirchia, Daniel V. Sullivan, Melike Pekmezci, Tarik Tihan, Andrew W. Bollen, Arie Perry, Anuradha Banerjee, Sabine Mueller, Nalin Gupta, Shawn L. Hervey-Jumper, Nancy Ann Oberheim Bush, Mariza Daras, Jennie W. Taylor, Nicholas A. Butowski, John de Groot, Jennifer L. Clarke, David R. Raleigh, Joseph F. Costello, Joanna J. Phillips, Alyssa T. Reddy, Susan M. Chang, Mitchel S. Berger, and David A. Solomon

Subjects
Cellular and Molecular Neuroscience, Neurology (clinical), Pathology and Forensic Medicine
Abstract

Gliomas arising in the setting of neurofibromatosis type 1 (NF1) are heterogeneous, occurring from childhood through adulthood, can be histologically low-grade or high-grade, and follow an indolent or aggressive clinical course. Comprehensive profiling of genetic alterations beyond NF1 inactivation and epigenetic classification of these tumors remain limited. Through next-generation sequencing, copy number analysis, and DNA methylation profiling of gliomas from 47 NF1 patients, we identified 2 molecular subgroups of NF1-associated gliomas. The first harbored biallelic NF1 inactivation only, occurred primarily during childhood, followed a more indolent clinical course, and had a unique epigenetic signature for which we propose the terminology “pilocytic astrocytoma, arising in the setting of NF1”. The second subgroup harbored additional oncogenic alterations including CDKN2A homozygous deletion and ATRX mutation, occurred primarily during adulthood, followed a more aggressive clinical course, and was epigenetically diverse, with most tumors aligning with either high-grade astrocytoma with piloid features or various subclasses of IDH-wildtype glioblastoma. Several patients were treated with small molecule MEK inhibitors that resulted in stable disease or tumor regression when used as a single agent, but only in the context of those tumors with NF1 inactivation lacking additional oncogenic alterations. Together, these findings highlight recurrently altered pathways in NF1-associated gliomas and help inform targeted therapeutic strategies for this patient population.

Published
2022

5. Prognostic validation of a new classification system for extent of resection in glioblastoma: A report of the RANO resect group

Author

Philipp Karschnia, Jacob S Young, Antonio Dono, Levin Häni, Tommaso Sciortino, Francesco Bruno, Stephanie T Juenger, Nico Teske, Ramin A Morshed, Alexander F Haddad, Yalan Zhang, Sophia Stoecklein, Michael Weller, Michael A Vogelbaum, Juergen Beck, Nitin Tandon, Shawn Hervey-Jumper, Annette M Molinaro, Roberta Rudà, Lorenzo Bello, Oliver Schnell, Yoshua Esquenazi, Maximilian I Ruge, Stefan J Grau, Mitchel S Berger, Susan M Chang, Martin van den Bent, Joerg-Christian Tonn, and Neurology

Subjects
Cancer Research, classification, Oncology, SDG 3 - Good Health and Well-being, glioblastoma, outcome, surgical resection, Neurology (clinical), EOR
Abstract

Background Terminology to describe extent of resection in glioblastoma is inconsistent across clinical trials. A surgical classification system was previously proposed based upon residual contrast-enhancing (CE) tumor. We aimed to (1) explore the prognostic utility of the classification system and (2) define how much removed non-CE tumor translates into a survival benefit. Methods The international RANO resect group retrospectively searched previously compiled databases from 7 neuro-oncological centers in the USA and Europe for patients with newly diagnosed glioblastoma per WHO 2021 classification. Clinical and volumetric information from pre- and postoperative MRI were collected. Results We collected 1,008 patients with newly diagnosed IDHwt glioblastoma. 744 IDHwt glioblastomas were treated with radiochemotherapy per EORTC-26981/22981 (TMZ/RT→TMZ) following surgery. Among these homogenously treated patients, lower absolute residual tumor volumes (in cm3) were favorably associated with outcome: patients with “maximal CE resection” (class 2) had superior outcome compared to patients with “submaximal CE resection” (class 3) or “biopsy” (class 4). Extensive resection of non-CE tumor (≤5 cm3 residual non-CE tumor) was associated with better survival among patients with complete CE resection, thus defining class 1 (“supramaximal CE resection”). The prognostic value of the resection classes was retained on multivariate analysis when adjusting for molecular and clinical markers. Conclusions The proposed “RANO categories for extent of resection in glioblastoma” are highly prognostic and may serve for stratification within clinical trials. Removal of non-CE tumor beyond the CE tumor borders may translate into additional survival benefit, providing a rationale to explicitly denominate such “supramaximal CE resection.”

Published
2023

6. A Remote Parenting Program and Parent and Staff Perspectives: A Randomized Trial

Author

Joanne A. Smith, Susan M. Chang, Alexandra Brentani, Günther Fink, Florencia Lopez-Boo, Belen Michel Torino, Marta Rubio Codina, and Susan P. Walker

Subjects
Pediatrics, Perinatology and Child Health
Abstract

OBJECTIVES To assess impact and implementation of remote delivery of a parenting program following suspension of in-person visits during the coronavirus disease 2019 pandemic. METHODS Impact of remote delivery of the Reach Up parenting program on parenting practices was evaluated by randomized trial in Jamaica. Mothers with children aged 5 to 24 months who met 1 of 7 at-risk criteria were enrolled at health centers. Participants were randomly assigned to intervention or control using random number tables generated by a statistician. Intervention comprised a manual for parents with illustrated play activities, phone calls, and short message service messages. The control group received usual care. Parent practices were measured using an adapted Family Care Indicators telephone-administered questionnaire by interviewers unaware of group assignment. Qualitative interviews were conducted with staff and parents in Jamaica and Brazil and staff in Ecuador to identify facilitators and barriers to remote delivery of Reach Up. RESULTS Two hundred forty-seven participants were assessed at endline (control n = 130; intervention n = 117). Intervention increased parent activities that support child development, effect size 0.34 SD (95% confidence interval 0.03–0.53), and use of praise, odds 2 times higher with intervention. There were no benefits to interactive language or play materials. Qualitative results showed parents appreciated program continuation and felt motivated to help their child, and methods were acceptable to staff. Barriers included poor mobile phone access, difficulty contacting parents, and feedback limitations without in-person contact. CONCLUSIONS Remote delivery methods have potential to contribute to scaling of parenting programs.

Published
2023

7. Data from The Phenotypes of Proliferating Glioblastoma Cells Reside on a Single Axis of Variation

Author

Aaron A. Diaz, Manish K. Aghi, Joanna J. Phillips, Susan M. Chang, Harsh Wadhwa, Sumedh Shah, Arnold Kriegstein, Elizabeth Di Lullo, Beatriz Alvarado, Gary Kohanbash, Francisca Catalan, Karin Shamardani, Garima Yagnik, Sören Müller, Husam Babikir, and Lin Wang

Abstract

Although tumor-propagating cells can be derived from glioblastomas (GBM) of the proneural and mesenchymal subtypes, a glioma stem-like cell (GSC) of the classic subtype has not been identified. It is unclear whether mesenchymal GSCs (mGSC) and/or proneural GSCs (pGSC) alone are sufficient to generate the heterogeneity observed in GBM. We performed single-cell/single-nucleus RNA sequencing of 28 gliomas, and single-cell ATAC sequencing for 8 cases. We found that GBM GSCs reside on a single axis of variation, ranging from proneural to mesenchymal. In silico lineage tracing using both transcriptomics and genetics supports mGSCs as the progenitors of pGSCs. Dual inhibition of pGSC-enriched and mGSC-enriched growth and survival pathways provides a more complete treatment than combinations targeting one GSC phenotype alone. This study sheds light on a long-standing debate regarding lineage relationships among GSCs and presents a paradigm by which personalized combination therapies can be derived from single-cell RNA signatures, to overcome intratumor heterogeneity.Significance:Tumor-propagating cells can be derived from mesenchymal and proneural glioblastomas. However, a stem cell of the classic subtype has yet to be demonstrated. We show that classic-subtype gliomas are comprised of proneural and mesenchymal cells. This study sheds light on a long-standing debate regarding lineage relationships between glioma cell types.See related commentary by Fine, p. 1650.This article is highlighted in the In This Issue feature, p. 1631

Published
2023

10. Interview with Dr. Mellinghoff from Differential Sensitivity of Glioma- versus Lung Cancer–Specific EGFR Mutations to EGFR Kinase Inhibitors

Author

Ingo K. Mellinghoff, Timothy F. Cloughesy, Minesh P. Mehta, Paul S. Mischel, John G. Kuhn, William H. Yong, Lisa M. DeAngelis, Andrew B. Lassman, Nian Wu, Steve Horvath, Howard A. Fine, Michael D. Prados, Susan M. Chang, Kathleen R. Lamborn, Patrick Y. Wen, Jan Drappatz, David A. Reardon, Mark R. Gilbert, W. K. Alfred Yung, Frank Lieberman, Linda M. Liau, Adriana Heguy, Cameron W. Brennan, Alicia Pedraza, Julie Dang, Daisuke Kuga, Akio Iwanami, Shaojun Zhu, Hui Tao, Nicolas Yannuzzi, Milan G. Chheda, Barbara Oldrini, Sara Kubek, Phioanh Leia Nghiemphu, Christian Grommes, Carl Campos, Daniel Rohle, H. Ian Robins, and Igor Vivanco

Abstract

mp3 file (11 MB). In the May edition of the Cancer Discovery podcast, Science Writer Elizabeth McKenna talks with Ingo K. Mellinghoff about his paper, which suggests that the disappointing clinical activity of first-generation EGFR inhibitors in glioblastoma versus lung cancer may be attributed to the different conformational requirements of mutant EGFR in these two cancer types.

Published
2023

11. Supplementary Figures 1-10 from Differential Sensitivity of Glioma- versus Lung Cancer–Specific EGFR Mutations to EGFR Kinase Inhibitors

Author

Ingo K. Mellinghoff, Timothy F. Cloughesy, Minesh P. Mehta, Paul S. Mischel, John G. Kuhn, William H. Yong, Lisa M. DeAngelis, Andrew B. Lassman, Nian Wu, Steve Horvath, Howard A. Fine, Michael D. Prados, Susan M. Chang, Kathleen R. Lamborn, Patrick Y. Wen, Jan Drappatz, David A. Reardon, Mark R. Gilbert, W. K. Alfred Yung, Frank Lieberman, Linda M. Liau, Adriana Heguy, Cameron W. Brennan, Alicia Pedraza, Julie Dang, Daisuke Kuga, Akio Iwanami, Shaojun Zhu, Hui Tao, Nicolas Yannuzzi, Milan G. Chheda, Barbara Oldrini, Sara Kubek, Phioanh Leia Nghiemphu, Christian Grommes, Carl Campos, Daniel Rohle, H. Ian Robins, and Igor Vivanco

Abstract

PDF file - 689K

Published
2023

12. Supplementary Tables 1-8 from Differential Sensitivity of Glioma- versus Lung Cancer–Specific EGFR Mutations to EGFR Kinase Inhibitors

Author

Ingo K. Mellinghoff, Timothy F. Cloughesy, Minesh P. Mehta, Paul S. Mischel, John G. Kuhn, William H. Yong, Lisa M. DeAngelis, Andrew B. Lassman, Nian Wu, Steve Horvath, Howard A. Fine, Michael D. Prados, Susan M. Chang, Kathleen R. Lamborn, Patrick Y. Wen, Jan Drappatz, David A. Reardon, Mark R. Gilbert, W. K. Alfred Yung, Frank Lieberman, Linda M. Liau, Adriana Heguy, Cameron W. Brennan, Alicia Pedraza, Julie Dang, Daisuke Kuga, Akio Iwanami, Shaojun Zhu, Hui Tao, Nicolas Yannuzzi, Milan G. Chheda, Barbara Oldrini, Sara Kubek, Phioanh Leia Nghiemphu, Christian Grommes, Carl Campos, Daniel Rohle, H. Ian Robins, and Igor Vivanco

Abstract

PDF file - 104K

Published
2023

13. Supplementary Figure and Table Legends, Methods from Differential Sensitivity of Glioma- versus Lung Cancer–Specific EGFR Mutations to EGFR Kinase Inhibitors

Author

Ingo K. Mellinghoff, Timothy F. Cloughesy, Minesh P. Mehta, Paul S. Mischel, John G. Kuhn, William H. Yong, Lisa M. DeAngelis, Andrew B. Lassman, Nian Wu, Steve Horvath, Howard A. Fine, Michael D. Prados, Susan M. Chang, Kathleen R. Lamborn, Patrick Y. Wen, Jan Drappatz, David A. Reardon, Mark R. Gilbert, W. K. Alfred Yung, Frank Lieberman, Linda M. Liau, Adriana Heguy, Cameron W. Brennan, Alicia Pedraza, Julie Dang, Daisuke Kuga, Akio Iwanami, Shaojun Zhu, Hui Tao, Nicolas Yannuzzi, Milan G. Chheda, Barbara Oldrini, Sara Kubek, Phioanh Leia Nghiemphu, Christian Grommes, Carl Campos, Daniel Rohle, H. Ian Robins, and Igor Vivanco

Abstract

PDF file - 133K

Published
2023

14. Spectroscopic imaging of D-2-hydroxyglutarate and other metabolites in pre-surgical patients with IDH-mutant lower-grade gliomas

Author

Adam W. Autry, Marisa Lafontaine, Llewellyn Jalbert, Elizabeth Phillips, Joanna J. Phillips, Javier Villanueva-Meyer, Mitchel S. Berger, Susan M. Chang, and Yan Li

Subjects
IDH, Cancer Research, Magnetic Resonance Spectroscopy, Oncology and Carcinogenesis, Receptors, Antigen, T-Cell, Glutarates, Rare Diseases, Clinical Research, Receptors, Humans, Oncology & Carcinogenesis, Cancer, Brain Neoplasms, Neurosciences, Image-guided, Glioma, T-Cell, Isocitrate Dehydrogenase, Brain Disorders, Brain Cancer, MRSI, Neurology, Oncology, D-2-Hydroxyglutarate, Antigen, Mutation, Biomedical Imaging, Neurology (clinical), Tumor Suppressor Protein p53, Lower-grade glioma, Inositol
Abstract

Purpose Prognostically favorable IDH-mutant gliomas are known to produce oncometabolite D-2-hydroxyglutarate (2HG). In this study, we investigated metabolite-based features of patients with grade 2 and 3 glioma using 2HG-specific in vivo MR spectroscopy, to determine their relationship with image-guided tissue pathology and predictive role in progression-free survival (PFS). Methods Forty-five patients received pre-operative MRIs that included 3-D spectroscopy optimized for 2HG detection. Spectral data were reconstructed and quantified to compare metabolite levels according to molecular pathology (IDH1R132H, 1p/19q, and p53); glioma grade; histological subtype; and T2 lesion versus normal-appearing white matter (NAWM) ROIs. Levels of 2HG were correlated with other metabolites and pathological parameters (cellularity, MIB-1) from image-guided tissue samples using Pearson’s correlation test. Metabolites predictive of PFS were evaluated with Cox proportional hazards models. Results Quantifiable levels of 2HG in 39/42 (93%) IDH+ and 1/3 (33%) IDH– patients indicated a 91.1% apparent detection accuracy. Myo-inositol/total choline (tCho) showed reduced values in astrocytic (1p/19q-wildtype), p53-mutant, and grade 3 (vs. 2) IDH-mutant gliomas (p p p p p p = 0.002), total NAA (R = − 0.61; p = 0.002) and cellularity (R = 0.37; p = 0.04) but not MIB-1. Increasing levels of 2HG/tCr (p = 0.0007, HR 5.594) and thresholding (≥ 0.905, median value; p = 0.02) predicted adverse PFS. Conclusion In vivo 2HG detection can reasonably be achieved on clinical scanners and increased levels may signal adverse PFS.

Published
2022

15. Figure S1 from Prospective Feasibility Trial for Genomics-Informed Treatment in Recurrent and Progressive Glioblastoma

Author

Michael D. Prados, David W. Craig, John D. Carpten, Michael E. Berens, Jeffrey M. Trent, Winnie S. Liang, Sara Nasser, Sen Peng, Gerald M. Maggiora, Annette M. Molinaro, Mitchel S. Berger, Susan M. Chang, Jennifer L. Clarke, Jennie W. Taylor, Nicholas A. Butowski, Ingo K. Mellinghoff, Timothy F. Cloughesy, Patrick Y. Wen, Keith L. Ligon, Howard Colman, John F. de Groot, John G. Kuhn, Joanna J. Phillips, Rebecca F. Halperin, Nhan L. Tran, and Sara A. Byron

Abstract

Study Workflow Diagram. Key steps in the study are outlined, including the number of patients at each stage. BEV: bevacizumab.

Published
2023

16. Supplementary Table 1B from Individual Patient-Specific Immunity against High-Grade Glioma after Vaccination with Autologous Tumor Derived Peptides Bound to the 96 KD Chaperone Protein

Author

Andrew T. Parsa, Michael D. Prados, Michael W. McDermott, Mitchel S. Berger, Jennifer Clarke, Susan M. Chang, Nicholas Butowski, Anne Fedoroff, Valerie Kivett, Jessica Oehlke, Brian Ahn, Seunggu J. Han, and Courtney A. Crane

Abstract

PDF file, 48K, Overall Survival Characteristics of Treated Patients.

Published
2023

17. Supplementary Tables 1 - 4 from SSBP2 Variants Are Associated with Survival in Glioblastoma Patients

Author

Margaret R. Wrensch, Robert B. Jenkins, Kathleen M. Egan, John K. Wiencke, James E. Browning, Melissa H. Madden, Steve Brem, Jeffrey J. Olson, Louis Burt Nabors, Reid C. Thompson, Jan C. Buckner, Brian Patrick O'Neill, Daniel H. Lachance, Brooke L. Fridley, Matthew L. Kosel, Mitchel S. Berger, Susan M. Chang, Michael D. Prados, Tarik Tihan, Joe L. Wiemels, Helen M. Hansen, Joseph S. Patoka, Ivan Smirnov, Lucie S. McCoy, Terri Rice, Paul A. Decker, and Yuanyuan Xiao

Abstract

PDF file, 406KB, Supplementary Table 1.115 TCGA SOC sample IDs used in the validation phase.; Supplementary Table 2. Proportionality tests based on the scaled Schoenfeld residules for the SNP effect in the log-additive Cox Proportional Hazards model adjusted for age and sex.; Supplementary Table 3. Validation of survival association with three SNPs in glioblastoma multiforme patients from three independent studies (Mayo Clinic10, GliomaSE11 and The Cancer Genome Atlas (TCGA17); Supplementary Table 4. Imputation analyiss of SSBP2 region:chr5: 80,680,000 -- 80,980,000, University of California, San Francisco Adult Glioma Study (AGS), Mayo Clinic, and The MACH, Hapmap 2, human genome build 18, 3 sites (University of California, San Francisco, Mayo Clinic and The Cancer Genome Atlas).

Published
2023

18. Supplementary Figure 2 from Individual Patient-Specific Immunity against High-Grade Glioma after Vaccination with Autologous Tumor Derived Peptides Bound to the 96 KD Chaperone Protein

Author

Andrew T. Parsa, Michael D. Prados, Michael W. McDermott, Mitchel S. Berger, Jennifer Clarke, Susan M. Chang, Nicholas Butowski, Anne Fedoroff, Valerie Kivett, Jessica Oehlke, Brian Ahn, Seunggu J. Han, and Courtney A. Crane

Abstract

PDF file, 9905K, Representative phenotypic analysis of circulating lymphocytes in a clinical responder (Patient #009).

Published
2023

19. Data from Individual Patient-Specific Immunity against High-Grade Glioma after Vaccination with Autologous Tumor Derived Peptides Bound to the 96 KD Chaperone Protein

Author

Andrew T. Parsa, Michael D. Prados, Michael W. McDermott, Mitchel S. Berger, Jennifer Clarke, Susan M. Chang, Nicholas Butowski, Anne Fedoroff, Valerie Kivett, Jessica Oehlke, Brian Ahn, Seunggu J. Han, and Courtney A. Crane

Abstract

Purpose: Cancer immunotherapy offers hope of a highly specific nontoxic adjuvant treatment. Heat shock protein peptide complexes (HSPPCs) found in cancer cells carry tumor-specific antigenic proteins and can facilitate adaptive and innate immune responses. Here we show that peptides bound to a 96 kD chaperone protein (HSP-96) from brain tissue containing glioblastoma multiforme (GBM) can be used to safely immunize patients with recurrent GBM.Experimental Design: Multimodality immunomonitoring was completed on 12 patients with recurrent GBM before and after immunization with an autologous HSPPC vaccine derived from surgically resected tumor. Clinical endpoints included safety assessments and overall survival.Results: No adverse events attributable to the vaccine were found. Testing of peripheral blood leukocytes before and after vaccination revealed a significant peripheral immune response specific for the peptides bound to HSP-96, in 11 of the 12 patients treated. Brain biopsies of immune responders after vaccination revealed focal CD4, CD8, and CD56 IFNγ positive cell infiltrates, consistent with tumor site specific immune responses. Immune responders had a median survival of 47 weeks after surgery and vaccination, compared with 16 weeks for the single nonresponder.Conclusions: These data provide the first evidence in humans of individual patient-specific immune responses against autologous tumor derived peptides bound to HSP-96. Clin Cancer Res; 19(1); 205–14. ©2012 AACR.

Published
2023

20. Data from SSBP2 Variants Are Associated with Survival in Glioblastoma Patients

Author

Margaret R. Wrensch, Robert B. Jenkins, Kathleen M. Egan, John K. Wiencke, James E. Browning, Melissa H. Madden, Steve Brem, Jeffrey J. Olson, Louis Burt Nabors, Reid C. Thompson, Jan C. Buckner, Brian Patrick O'Neill, Daniel H. Lachance, Brooke L. Fridley, Matthew L. Kosel, Mitchel S. Berger, Susan M. Chang, Michael D. Prados, Tarik Tihan, Joe L. Wiemels, Helen M. Hansen, Joseph S. Patoka, Ivan Smirnov, Lucie S. McCoy, Terri Rice, Paul A. Decker, and Yuanyuan Xiao

Abstract

Purpose: Glioblastoma is a devastating, incurable disease with few known prognostic factors. Here, we present the first genome-wide survival and validation study for glioblastoma.Experimental Design: Cox regressions for survival with 314,635 inherited autosomal single-nucleotide polymorphisms (SNP) among 315 San Francisco Adult Glioma Study patients for discovery and three independent validation data sets [87 Mayo Clinic, 232 glioma patients recruited from several medical centers in Southeastern United States (GliomaSE), and 115 The Cancer Genome Atlas patients] were used to identify SNPs associated with overall survival for Caucasian glioblastoma patients treated with the current standard of care, resection, radiation, and temozolomide (total n = 749). Tumor expression of the gene that contained the identified prognostic SNP was examined in three separate data sets (total n = 619). Genotype imputation was used to estimate hazard ratios (HR) for SNPs that had not been directly genotyped.Results: From the discovery and validation analyses, we identified a variant in single-stranded DNA-binding protein 2 (SSBP2) on 5q14.1 associated with overall survival in combined analyses (HR, 1.64; P = 1.3 × 10−6). Expression of SSBP2 in tumors from three independent data sets also was significantly related to patient survival (P = 5.3 × 10−4). Using genotype imputation, the SSBP2 SNP rs17296479 had the strongest statistically significant genome-wide association with poorer overall patient survival (HR, 1.79; 95% CI, 1.45-2.22; P = 1.0 × 10−7).Conclusion: The minor allele of SSBP2 SNP rs17296479 and the increased tumor expression of SSBP2 were statistically significantly associated with poorer overall survival among glioblastoma patients. With further confirmation, previously unrecognized inherited variations influencing survival may warrant inclusion in clinical trials to improve randomization. Unaccounted for genetic influence on survival could produce unwanted bias in such studies. Clin Cancer Res; 18(11); 3154–62. ©2012 AACR.

Published
2023

21. Supplementary Figure 1 from Individual Patient-Specific Immunity against High-Grade Glioma after Vaccination with Autologous Tumor Derived Peptides Bound to the 96 KD Chaperone Protein

Author

Andrew T. Parsa, Michael D. Prados, Michael W. McDermott, Mitchel S. Berger, Jennifer Clarke, Susan M. Chang, Nicholas Butowski, Anne Fedoroff, Valerie Kivett, Jessica Oehlke, Brian Ahn, Seunggu J. Han, and Courtney A. Crane

Abstract

PDF file, 17162K, Model of HSPPC-96 mechanism of action.

Published
2023

22. Data from Prospective Feasibility Trial for Genomics-Informed Treatment in Recurrent and Progressive Glioblastoma

Author

Michael D. Prados, David W. Craig, John D. Carpten, Michael E. Berens, Jeffrey M. Trent, Winnie S. Liang, Sara Nasser, Sen Peng, Gerald M. Maggiora, Annette M. Molinaro, Mitchel S. Berger, Susan M. Chang, Jennifer L. Clarke, Jennie W. Taylor, Nicholas A. Butowski, Ingo K. Mellinghoff, Timothy F. Cloughesy, Patrick Y. Wen, Keith L. Ligon, Howard Colman, John F. de Groot, John G. Kuhn, Joanna J. Phillips, Rebecca F. Halperin, Nhan L. Tran, and Sara A. Byron

Abstract

Purpose: Glioblastoma is an aggressive and molecularly heterogeneous cancer with few effective treatment options. We hypothesized that next-generation sequencing can be used to guide treatment recommendations within a clinically acceptable time frame following surgery for patients with recurrent glioblastoma.Experimental Design: We conducted a prospective genomics-informed feasibility trial in adults with recurrent and progressive glioblastoma. Following surgical resection, genome-wide tumor/normal exome sequencing and tumor RNA sequencing were performed to identify molecular targets for potential matched therapy. A multidisciplinary molecular tumor board issued treatment recommendations based on the genomic results, blood–brain barrier penetration of the indicated therapies, drug–drug interactions, and drug safety profiles. Feasibility of generating genomics-informed treatment recommendations within 35 days of surgery was assessed.Results: Of the 20 patients enrolled in the study, 16 patients had sufficient tumor tissue for analysis. Exome sequencing was completed for all patients, and RNA sequencing was completed for 14 patients. Treatment recommendations were provided within the study's feasibility time frame for 15 of 16 (94%) patients. Seven patients received treatment based on the tumor board recommendations. Two patients reached 12-month progression-free survival, both adhering to treatments based on the molecular profiling results. One patient remained on treatment and progression free 21 months after surgery, 3 times longer than the patient's previous time to progression. Analysis of matched nonenhancing tissue from 12 patients revealed overlapping as well as novel putatively actionable genomic alterations.Conclusions: Use of genome-wide molecular profiling is feasible and can be informative for guiding real-time, central nervous system–penetrant, genomics-informed treatment recommendations for patients with recurrent glioblastoma. Clin Cancer Res; 24(2); 295–305. ©2017 AACR.See related commentary by Wick and Kessler, p. 256

Published
2023

23. Supplementary Figure 3 from Individual Patient-Specific Immunity against High-Grade Glioma after Vaccination with Autologous Tumor Derived Peptides Bound to the 96 KD Chaperone Protein

Author

Andrew T. Parsa, Michael D. Prados, Michael W. McDermott, Mitchel S. Berger, Jennifer Clarke, Susan M. Chang, Nicholas Butowski, Anne Fedoroff, Valerie Kivett, Jessica Oehlke, Brian Ahn, Seunggu J. Han, and Courtney A. Crane

Abstract

PDF file, 8781K, Representative phenotypic analysis of circulating lymphocytes in a clinical non-responder (Patient #003).

Published
2023

25. Supplementary Table 1 from Phase I Study of Vorinostat in Combination with Temozolomide in Patients with High-Grade Gliomas: North American Brain Tumor Consortium Study 04-03

Author

Patrick Y. Wen, Michael D. Prados, Igor Espinoza-Delgado, Matthew M. Ames, Xiabu Ye, Serena Desideri, Jihong Xu, Renee M. McGovern, Andrew B. Lassman, Frank S. Lieberman, H. Ian Robins, Mark R. Gilbert, W. K. Alfred Yung, Jan Drappatz, Susan M. Chang, Timothy F. Cloughesy, Kathleen R. Lamborn, John G. Kuhn, Joel M. Reid, Vinay K. Puduvalli, and Eudocia Q. Lee

Abstract

PDF file, 80K, Supplementary Table 1: Temozolomide 150 mg/m2 Pharmacokinetic Parameters (first cycle).

Published
2023

26. Supplementary Table 2 from Phase I Study of Vorinostat in Combination with Temozolomide in Patients with High-Grade Gliomas: North American Brain Tumor Consortium Study 04-03

Author

Patrick Y. Wen, Michael D. Prados, Igor Espinoza-Delgado, Matthew M. Ames, Xiabu Ye, Serena Desideri, Jihong Xu, Renee M. McGovern, Andrew B. Lassman, Frank S. Lieberman, H. Ian Robins, Mark R. Gilbert, W. K. Alfred Yung, Jan Drappatz, Susan M. Chang, Timothy F. Cloughesy, Kathleen R. Lamborn, John G. Kuhn, Joel M. Reid, Vinay K. Puduvalli, and Eudocia Q. Lee

Abstract

PDF file, 62K, Supplementary Table 2: Grade 3 or 4 events with relationship unrelated to unlikely to combination therapy (Vorinostat + TMZ).

Published
2023

27. Supplementary Table 2 from Individual Patient-Specific Immunity against High-Grade Glioma after Vaccination with Autologous Tumor Derived Peptides Bound to the 96 KD Chaperone Protein

Author

Andrew T. Parsa, Michael D. Prados, Michael W. McDermott, Mitchel S. Berger, Jennifer Clarke, Susan M. Chang, Nicholas Butowski, Anne Fedoroff, Valerie Kivett, Jessica Oehlke, Brian Ahn, Seunggu J. Han, and Courtney A. Crane

Abstract

PDF file, 29K, Vaccine Administration Schedule and Characteristics of Adverse Events.

Published
2023

28. Data from Phase I Study of Vorinostat in Combination with Temozolomide in Patients with High-Grade Gliomas: North American Brain Tumor Consortium Study 04-03

Author

Patrick Y. Wen, Michael D. Prados, Igor Espinoza-Delgado, Matthew M. Ames, Xiabu Ye, Serena Desideri, Jihong Xu, Renee M. McGovern, Andrew B. Lassman, Frank S. Lieberman, H. Ian Robins, Mark R. Gilbert, W. K. Alfred Yung, Jan Drappatz, Susan M. Chang, Timothy F. Cloughesy, Kathleen R. Lamborn, John G. Kuhn, Joel M. Reid, Vinay K. Puduvalli, and Eudocia Q. Lee

Abstract

Purpose: A phase I, dose-finding study of vorinostat in combination with temozolomide (TMZ) was conducted to determine the maximum tolerated dose (MTD), safety, and pharmacokinetics in patients with high-grade glioma (HGG).Experimental Design: This phase I, dose-finding, investigational study was conducted in two parts. Part 1 was a dose-escalation study of vorinostat in combination with TMZ 150 mg/m2/day for 5 days every 28 days. Part 2 was a dose-escalation study of vorinostat in combination with TMZ 150 mg/m2/day for 5 days of the first cycle and 200 mg/m2/day for 5 days of the subsequent 28-day cycles.Results: In part 1, the MTD of vorinostat administered on days 1 to 7 and 15 to 21 of every 28-day cycle, in combination with TMZ, was 500 mg daily. Dose-limiting toxicities (DLT) included grade 3 anorexia, grade 3 ALT, and grade 5 hemorrhage in the setting of grade 4 thrombocytopenia. In part 2, the MTD of vorinostat on days 1 to 7 and 15 to 21 of every 28-day cycle, combined with TMZ, was 400 mg daily. No DLTs were encountered, but vorinostat dosing could not be escalated further due to thrombocytopenia. The most common serious adverse events were fatigue, lymphopenia, thrombocytopenia, and thromboembolic events. There were no apparent pharmacokinetic interactions between vorinostat and TMZ. Vorinostat treatment resulted in hyperacetylation of histones H3 and H4 in peripheral mononuclear cells.Conclusion: Vorinostat in combination with temozolomide is well tolerated in patients with HGG. A phase I/II trial of vorinostat with radiotherapy and concomitant TMZ in newly diagnosed glioblastoma is underway. Clin Cancer Res; 18(21); 6032–9. ©2012 AACR.

Published
2023

30. Diagnosis and management of complications from the treatment of primary central nervous system tumors in adults

Author

Michael Weller, Emilie Le Rhun, Martin Van den Bent, Susan M Chang, Timothy F Cloughesy, Roland Goldbrunner, Yong-Kil Hong, Rakesh Jalali, Michael D Jenkinson, Giuseppe Minniti, Motoo Nagane, Evangelia Razis, Patrick Roth, Roberta Rudà, Ghazaleh Tabatabai, Patrick Y Wen, Susan C Short, and Matthias Preusser

Subjects
Cancer Research, Oncology, Neurology (clinical)
Abstract

Central nervous system (CNS) tumor patients commonly undergo multimodality treatment in the course of their disease. Adverse effects and complications from these interventions have not been systematically studied, but pose significant challenges in clinical practice and impact function and quality of life, especially in the management of long-term brain tumor survivors. Here, the European Association of Neuro-Oncology (EANO) has developed recommendations to prevent, diagnose, and manage adverse effects and complications in the adult primary brain CNS tumor (except lymphomas) patient population with a specific focus on surgery, radiotherapy, and pharmacotherapy. Specifically, we also provide recommendations for dose adaptations, interruptions, and reexposure for pharmacotherapy that may serve as a reference for the management of standard of care in clinical trials. We also summarize which interventions are unnecessary, inactive or contraindicated. This consensus paper should serve as a reference for the conduct of standard therapy within and outside of clinical trials.

Published
2023

31. Objective response rate targets for recurrent glioblastoma clinical trials based on the historic association between objective response rate and median overall survival

Author

Benjamin M Ellingson, Patrick Y Wen, Susan M Chang, Martin van den Bent, Michael A Vogelbaum, Gang Li, Shanpeng Li, Jiyoon Kim, Gilbert Youssef, Wolfgang Wick, Andrew B Lassman, Mark R Gilbert, John F de Groot, Michael Weller, Evanthia Galanis, Timothy F Cloughesy, and Neurology

Subjects
Cancer Research, SDG 3 - Good Health and Well-being, Oncology, Neurology (clinical)
Abstract

Durable objective response rate (ORR) remains a meaningful endpoint in recurrent cancer; however, the target ORR for single-arm recurrent glioblastoma trials has not been based on historic information or tied to patient outcomes. The current study reviewed 68 treatment arms comprising 4793 patients in past trials in recurrent glioblastoma in order to judiciously define target ORRs for use in recurrent glioblastoma trials. ORR was estimated at 6.1% [95% CI 4.23; 8.76%] for cytotoxic chemothera + pies (ORR = 7.59% for lomustine, 7.57% for temozolomide, 0.64% for irinotecan, and 5.32% for other agents), 3.37% for biologic agents, 7.97% for (select) immunotherapies, and 26.8% for anti-angiogenic agents. ORRs were significantly correlated with median overall survival (mOS) across chemotherapy (R2 = 0.4078, P < .0001), biologics (R2 = 0.4003, P = .0003), and immunotherapy trials (R2 = 0.8994, P < .0001), but not anti-angiogenic agents (R2 = 0, P = .8937). Pooling data from chemotherapy, biologics, and immunotherapy trials, a meta-analysis indicated a strong correlation between ORR and mOS (R2 = 0.3900, P < .0001; mOS [weeks] = 1.4xORR + 24.8). Assuming an ineffective cytotoxic (control) therapy has ORR = 7.6%, the average ORR for lomustine and temozolomide trials, a sample size of ≥40 patients with target ORR>25% is needed to demonstrate statistical significance compared to control with a high level of confidence (P < .01) and adequate power (>80%). Given this historic data and potential biases in patient selection, we recommend that well-controlled, single-arm phase II studies in recurrent glioblastoma should have a target ORR >25% (which translates to a median OS of approximately 15 months) and a sample size of ≥40 patients, in order to convincingly demonstrate antitumor activity. Crucially, this response needs to have sufficient durability, which was not addressed in the current study.

Published
2023

32. Isocitrate dehydrogenase (IDH) mutant gliomas: A Society for Neuro-Oncology (SNO) consensus review on diagnosis, management, and future directions

Author

Julie J Miller, L Nicolas Gonzalez Castro, Samuel McBrayer, Michael Weller, Timothy Cloughesy, Jana Portnow, Ovidiu Andronesi, Jill S Barnholtz-Sloan, Brigitta G Baumert, Mitchell S Berger, Wenya Linda Bi, Ranjit Bindra, Daniel P Cahill, Susan M Chang, Joseph F Costello, Craig Horbinski, Raymond Y Huang, Robert B Jenkins, Keith L Ligon, Ingo K Mellinghoff, L Burt Nabors, Michael Platten, David A Reardon, Diana D Shi, David Schiff, Wolfgang Wick, Hai Yan, Andreas von Deimling, Martin van den Bent, William G Kaelin, Patrick Y Wen, and Neurology

Subjects
Cancer Research, Oncology, SDG 3 - Good Health and Well-being, Neurology (clinical)
Abstract

Isocitrate dehydrogenase (IDH) mutant gliomas are the most common adult, malignant primary brain tumors diagnosed in patients younger than 50, constituting an important cause of morbidity and mortality. In recent years, there has been significant progress in understanding the molecular pathogenesis and biology of these tumors, sparking multiple efforts to improve their diagnosis and treatment. In this consensus review from the Society for Neuro-Oncology (SNO), the current diagnosis and management of IDH-mutant gliomas will be discussed. In addition, novel therapies, such as targeted molecular therapies and immunotherapies, will be reviewed. Current challenges and future directions for research will be discussed.

Published
2023

33. EWSR1-BEND2 fusion defines an epigenetically distinct subtype of astroblastoma

Author

Susan M. Chang, Rohit Gupta, Soonmee Cha, Huiling Xu, Melissa Gener, Jasper Wu, Nida Zia, Damien Kee, Ajay Ravindranathan, Kathan Shah, Calixto-Hope G Lucas, Arie Perry, David A. Solomon, Kevin Ginn, Nausheen Yaqoob, Adriana Florez, Jennifer Clarke, Jairo Barreto, Mitchel S. Berger, Owen W.J. Prall, and Hyun S Ko

Subjects
Adult, Male, Pathology, medicine.medical_specialty, Oncogene Proteins, Fusion, Brain Neoplasms, Astroblastoma, Infant, Newborn, Biology, medicine.disease, Neoplasms, Neuroepithelial, Pathology and Forensic Medicine, Cellular and Molecular Neuroscience, Young Adult, Correspondence, medicine, Humans, Female, Neurology (clinical), Spinal Cord Neoplasms, RNA-Binding Protein EWS, Child
Published
2021

35. Conserved features of TERT promoter duplications reveal an activation mechanism that mimics hotspot mutations in cancer

Author

Carter J. Barger, Abigail K. Suwala, Katarzyna M. Soczek, Albert S. Wang, Min Y. Kim, Chibo Hong, Jennifer A. Doudna, Susan M. Chang, Joanna J. Phillips, David A. Solomon, and Joseph F. Costello

Subjects
Multidisciplinary, General Physics and Astronomy, General Chemistry, General Biochemistry, Genetics and Molecular Biology, Promoter Regions, Rare Diseases, Genetic, Mutation, Genetics, Humans, 2.1 Biological and endogenous factors, Aetiology, Promoter Regions, Genetic, Glioblastoma, Telomerase, Cancer
Abstract

Mutations in the TERT promoter represent the genetic underpinnings of tumor cell immortality. Beyond the two most common point mutations, which selectively recruit the ETS factor GABP to activate TERT, the significance of other variants is unknown. In seven cancer types, we identify duplications of wildtype sequence within the core promoter region of TERT that have strikingly similar features including an ETS motif, the duplication length and insertion site. The duplications recruit a GABP tetramer by virtue of the native ETS motif and its precisely spaced duplicated counterpart, activate the promoter and are clonal in a TERT expressing multifocal glioblastoma. We conclude that recurrent TERT promoter duplications are functionally and mechanistically equivalent to the hotspot mutations that confer tumor cell immortality. The shared mechanism of these divergent somatic genetic alterations suggests a strong selective pressure for recruitment of the GABP tetramer to activate TERT.

Published
2022

36. Objective response rate (ORR) targets for recurrent glioblastoma clinical trials based on the historic association between ORR and median overall survival

Author

Benjamin M, Ellingson, Patrick Y, Wen, Susan M, Chang, Martin, van den Bent, Michael A, Vogelbaum, Gang, Li, Shanpeng, Li, Jiyoon, Kim, Gilbert, Youssef, Wolfgang, Wick, Andrew B, Lassman, Mark R, Gilbert, John F, de Groot, Michael, Weller, Evanthia, Galanis, and Timothy F, Cloughesy

Abstract

Durable objective response rate (ORR) remains a meaningful endpoint in recurrent cancer; however, the target ORR for single arm recurrent glioblastoma trials has not been based on historic information or tied to patient outcomes. The current study reviewed 68 treatment arms comprising 4,793 patients in past trials in recurrent glioblastoma in order to judiciously define target ORRs for use in recurrent glioblastoma trials. ORR was estimated at 6.1%[95% CI 4.23; 8.76%] for cytotoxic chemotherapies (ORR=7.59% for CCNU, 7.57% for TMZ, 0.64% for CPT-11, and 5.32% for other agents), 3.37% for biologic agents, 7.97% for (select) immunotherapies, and 26.8% for anti-angiogenic agents. ORRs were significantly correlated with median overall survival (mOS) across chemotherapy (R2=0.4078,P0.0001), biologics (R2=0.4003,P=0.0003), and immunotherapy trials (R2=0.8994,P0.0001), but not anti-angiogenic agents (R2=0, P=0.8937). Pooling data from chemotherapy, biologics, and immunotherapy trials, a meta-analysis indicated a strong correlation between ORR and mOS (R2=0.3900, P0.0001; mOS[weeks]=1.4xORR+24.8). Assuming an ineffective cytotoxic (control) therapy has ORR=7.6%, the average ORR for lomustine and temozolomide trials, a sample size of ≥40 patients with target ORR25% is needed to demonstrate statistical significance compared to control with a high level of confidence (P0.01) and adequate power (80%). Given this historic data and potential biases in patient selection, we recommend that well-controlled, single-arm phase II studies in recurrent glioblastoma should have a target ORR25% (which translates to a median OS of approximately 15 months) and a sample size of ≥40 patients, in order to convincingly demonstrate antitumor activity. Crucially, this response needs to have sufficient durability, which was not addressed in the current study.

Published
2022

37. 215 Extent of Resection in Glioblastoma: Prognostic Validation of a New Classification from the RANO Resect Group

Author

Philipp Karschnia, Jacob Young, Antonio Gabriel Dono Ostorga, Levin Häni, Tommaso Sciortino, Francesco Bruno, Stephanie T. Jünger, Nico Teske, Ramin A. Morshed, Alexander F. Haddad, Yalan Zhang, Sophia Stöcklein, Michael Weller, Michael A. Vogelbaum, Juergen Beck, Nitin Tandon, Shawn L. Hervey-Jumper, Annette Molinaro, Roberta Rudà, Lorenzo Bello, Oliver Schnell, Yoshua Esquenazi, Maximilian I. Ruge, Stefan J. Grau, Mitchel Berger, Susan M. Chang, Martin van den Bent, and Joerg-Christian Tonn

Subjects
Surgery, Neurology (clinical)
Published
2023

38. TMET-04. DETECTING DYNAMIC PYRUVATE TUMOR METABOLISM IN PATIENTS WITH GLIOMA USING HYPERPOLARIZED CARBON-13 METABOLIC IMAGING

Author

Yan Li, Janine Lupo, Adam Autry, Sana Vaziri, Jeremy Gordon, Marisa Lafontaine, Chen Hsin-Yu, Yaewon Kim, Jasmine Hu, Wendy Ma, Javier Villanueva-Meyer, Peder Larson, Duan Xu, Nancy Ann Oberheim Bush, Jennifer Clarke, Daniel Vigneron, and Susan M Chang

Subjects
Cancer Research, Oncology, Neurology (clinical)
Abstract

INTRODUCTION Hyperpolarized carbon-13 (HP-13C) MR enables rapid dynamic imaging of metabolic pathways in the human brain using non-toxic, non-radioactive metabolites as tracers. This study presents our unique experience on the benefit of using [1-13C]pyruvate and [2-13C]pyruvate MR for evaluating patients with glioma. METHODS 132 scans (71 using an integrated 13C /1H coil) including steady-state 1H-MRSI (~10 min) and dynamic HP-13C imaging (60 sec) following injection of HP [1-13C]pyruvate (N=125) or [2-13C]pyruvate (N=7) were acquired from 46 patients with glioma (18F/28M; 15 IDH-mutant, 27 IDH-wildtype, 4 IDH-status-unknown). Maps of temporally-summed 13C-metabolite signals, ratios, and kinetic rate constants were calculated for contrast-enhancing, nonenhancing, and normal-appearing-white-matter (NAWM) regions and compared to steady-state metabolic metrics. RESULTS The only adverse event, in a single patient, was a burning sensation after the injection that resolved after saline flush. The mean time-to-injection of HP probes was 58.6±14.0 sec. Signal-to-noise ratios of [1-13C]lactate and [13C]bicarbonate within the NAWM from the HP [1-13C]pyruvate data were 53±39 and 13±6, respectively. The SD/mean of repeated injections (N=3) for lactate/pyruvate and pyruvate-to-lactate conversion rates were 3.8±3.1% and 6.5±3.1% in the NAWM, respectively. Patients with progressive GBM had significantly higher lactate/pyruvate and lower bicarbonate/lactate (p< 0.05) in contrast- and non-enhancing lesions compared to NAWM. Significantly elevated lactate/pyruvate and reduced bicarbonate/lactate (p< 0.01) were found in contrast-enhancing compared to nonenhancing regions, whereas choline/NAA and steady-state 1H-lactate levels were similar. HP [2-13C]pyruvate data showed reduced glutamate/pyruvate and pyruvate-to-glutamate conversion rates in T2 lesions compared to contralateral normal-appearing brain in IDH-mutant gliomas, consistent with known metabolic reprogramming. CONCLUSION This study demonstrates the potential benefit of dynamic HP-13C MRI for evaluating patients with glioma, which provides unique and spatially distinct contrast compared to steady-state metabolic imaging. Ongoing studies will further characterize dynamic metabolism in specific glioma subtypes and provide biomarkers for evaluating responses to treatment.

Published
2022

39. NIMG-61. IMPROVED GENERALIZABILITY OF RADIOPATHOMIC PROBABILISTIC MAPPING OF TREATMENT-INDUCED EFFECTS WITH PHYSIOLOGIC MR IMAGING AND DEEP LEARNING IN PATIENTS WITH RECURRENT GLIOBLASTOMA

Author

Jacob Ellison, Nate Tran, Annette Molinaro, Valentina Pedoia, Joanna J Phillips, Anny Shai, Devika Nair, Marisa Lafontaine, Angela Jakary, Tracy Luks, Javier Villanueva-Meyer, Susan M Chang, Mitchel S Berger, Shawn L Hervey-Jumper, Manish Aghi, and Janine Lupo

Subjects
Cancer Research, Oncology, Neurology (clinical)
Abstract

Although physiologic (diffusion-weighted and perfusion-weighted) MRI has shown promise in identifying regions of recurrent tumor (rTumor) in patients with glioblastoma suspected of progression, distinguishing treatment-induced effects (TxE) from rTumor on anatomical MRI remains a challenge. Whereas prior larger-scale machine learning (ML)-based studies mostly utilize anatomical imaging alone and/or perform lesion-level predictions, this study aimed to develop a non-invasive, radiopathomic tool for regional probabilistic mapping of TxE using 208 tissue-samples (55 pathologically-confirmed TxE, 153 recurrent glioblastoma) acquired from 107 patients with known spatial coordinates on pre-surgical MRI. We tested the hypothesis that applying a deep-learning (DL) model that included physiological MRI can: 1) more accurately identify areas of TxE that mimic rTumor on anatomical MRI and 2) better generalize to an independent test set than ML-models or a DL-model that uses anatomical MRI alone. An 80/20 split for training/validation was used after 1/3 of the patients were withheld for testing. Oversampling of TxE samples was employed to address class imbalance and an equal proportion of TxE samples was maintained across all datasets. Three ML-models, their ensemble, and a deep 4D-convolutional-neural-network were trained based on normalized anatomical (post-contrast T1, T2-FLAIR), diffusion-weighted (ADC, FA), and DSC perfusion-weighted (PeakHeight, %recovery) images cropped to 10mm-cubic patches centered on the coordinates from where tissue was obtained. Although Random Forest and voting-ensembled ML-models using all imaging and the anatomical DL-model had the best validation performance (AUC=0.81-0.82), these models did not generalize (test AUC=0.58-0.59). The DL-model including physiologic images had slightly lower validation AUC (0.78) but the best overall test AUC (0.795), indicating superior generalizability. Elevated blood volume (nPeakHeight) was the most important feature. Our DL-model’s interpretability was also demonstrated by disrupting class separation after shuffling voxels within each input patch. These results suggest that using deep-learning with physiologic MRI can improve intratumoral classification of TxE from rTumor.

Published
2022

40. Assessment of higher-order singular value decomposition denoising methods on dynamic hyperpolarized [1

Author

Sana, Vaziri, Adam W, Autry, Marisa, Lafontaine, Yaewon, Kim, Jeremy W, Gordon, Hsin-Yu, Chen, Jasmine Y, Hu, Janine M, Lupo, Susan M, Chang, Jennifer L, Clarke, Javier E, Villanueva-Meyer, Nancy Ann Oberheim, Bush, Duan, Xu, Peder E Z, Larson, Daniel B, Vigneron, and Yan, Li

Abstract

Real-time metabolic conversion of intravenously-injected hyperpolarized [1-Dynamic HP-Both denoising methods improved metabolite SNR and regional signal coverage. In patient data, the average increase in peak dynamic metabolite SNR was 2-fold using TRI and 4-5 folds using GL-HOSVD denoising compared to acquired data. Denoising reduced kPost-processing denoising methods significantly improved the SNR of dynamic HP

Published
2022

41. Prospective genomically guided identification of 'early/evolving' and 'undersampled' IDH-wildtype glioblastoma leads to improved clinical outcomes

Author

Yalan Zhang, Calixto-Hope G Lucas, Jacob S Young, Ramin A Morshed, Lucie McCoy, Nancy Ann Oberheim Bush, Jennie W Taylor, Mariza Daras, Nicholas A Butowski, Javier E Villanueva-Meyer, Soonmee Cha, Margaret Wrensch, John K Wiencke, Julieann C Lee, Melike Pekmezci, Joanna J Phillips, Arie Perry, Andrew W Bollen, Manish K Aghi, Philip Theodosopoulos, Edward F Chang, Shawn L Hervey-Jumper, Mitchel S Berger, Jennifer L Clarke, Susan M Chang, Annette M Molinaro, and David A Solomon

Subjects
Adult, Cancer Research, precision medicine, Oncology and Carcinogenesis, Astrocytoma, molecular neuro-oncology, molecular diagnostics, Rare Diseases, Clinical Research, Genetics, Humans, Oncology & Carcinogenesis, Prospective Studies, Cancer, screening and diagnosis, Brain Neoplasms, Human Genome, glioblastoma, Neurosciences, Glioma, Isocitrate Dehydrogenase, Brain Disorders, Brain Cancer, Detection, Oncology, Mutation, Neurology (clinical), genomic profiling, Glioblastoma, Biotechnology, 4.2 Evaluation of markers and technologies
Abstract

Background Genomic profiling studies of diffuse gliomas have led to new improved classification schemes that better predict patient outcomes compared to conventional histomorphology alone. One example is the recognition that patients with IDH-wildtype diffuse astrocytic gliomas demonstrating lower-grade histologic features but genomic and/or epigenomic profile characteristic of glioblastoma typically have poor outcomes similar to patients with histologically diagnosed glioblastoma. Here we sought to determine the clinical impact of prospective genomic profiling for these IDH-wildtype diffuse astrocytic gliomas lacking high-grade histologic features but with molecular profile of glioblastoma. Methods Clinical management and outcomes were analyzed for 38 consecutive adult patients with IDH-wildtype diffuse astrocytic gliomas lacking necrosis or microvascular proliferation on histologic examination that were genomically profiled on a prospective clinical basis revealing criteria for an integrated diagnosis of “diffuse astrocytic glioma, IDH-wildtype, with molecular features of glioblastoma, WHO grade IV” per cIMPACT-NOW criteria. Results We identified that this diagnosis consists of two divergent clinical scenarios based on integration of radiologic, histologic, and genomic features that we term “early/evolving” and “undersampled” glioblastoma, IDH-wildtype. We found that prospective genomically guided identification of early/evolving and undersampled IDH-wildtype glioblastoma resulted in more aggressive patient management and improved clinical outcomes compared to a biologically matched historical control patient cohort receiving standard-of-care therapy based on histomorphologic diagnosis alone. Conclusions These results support routine use of genomic and/or epigenomic profiling to accurately classify glial neoplasms, as these assays not only improve diagnostic classification but critically lead to more appropriate patient management that can improve clinical outcomes.

Published
2022

42. Diffuse hemispheric glioma, H3 G34-mutant: Genomic landscape of a new tumor entity and prospects for targeted therapy

Author

Alyssa Reddy, Susan M. Chang, Mitchel S. Berger, Joanna J. Phillips, Arie Perry, Jennie Taylor, David A. Solomon, Nancy Ann Oberheim Bush, Nalin Gupta, Sabine Mueller, Jennifer Clarke, and Calixto-Hope G Lucas

Subjects
Cancer Research, Brain Neoplasms, medicine.medical_treatment, Mutant, Genomics, Glioma, Biology, medicine.disease, Targeted therapy, Histones, Oncology, Mutation, medicine, Cancer research, Humans, AcademicSubjects/MED00300, AcademicSubjects/MED00310, Neurology (clinical), Letters to the Editor
Published
2021

43. Glioblastoma Clinical Trials: Current Landscape and Opportunities for Improvement

Author

Rifaquat Rahman, Minesh P. Mehta, David A. Reardon, Louis B. Nabors, Timothy F. Cloughesy, John Sampson, Evanthia Galanis, Susan M. Chang, Roger Stupp, Mustafa Khasraw, Eudocia Q. Lee, Shawn Kothari, Manmeet S Ahluwalia, Stephen J Bagley, Patrick Y. Wen, Stuart A. Grossman, Simon Khagi, Erik P. Sulman, Michael Weller, Gavin P. Dunn, and University of Zurich

Subjects
Adult, Cancer Research, medicine.medical_specialty, Phase iii trials, Clinical Trials and Supportive Activities, Oncology and Carcinogenesis, MEDLINE, Context (language use), 610 Medicine & health, Article, Adult glioblastoma, Rare Diseases, Clinical Research, Medicine, Humans, Medical physics, Oncology & Carcinogenesis, Cancer, business.industry, Brain Neoplasms, Neurosciences, medicine.disease, Brain Disorders, 10040 Clinic for Neurology, Clinical trial, Brain Cancer, Oncology, Research Design, business, Early phase, Glioblastoma
Abstract

Therapeutic advances for glioblastoma have been minimal over the past 2 decades. In light of the multitude of recent phase III trials that have failed to meet their primary endpoints following promising preclinical and early-phase programs, a Society for Neuro-Oncology Think Tank was held in November 2020 to prioritize areas for improvement in the conduct of glioblastoma clinical trials. Here, we review the literature, identify challenges related to clinical trial eligibility criteria and trial design in glioblastoma, and provide recommendations from the Think Tank. In addition, we provide a data-driven context with which to frame this discussion by analyzing key study design features of adult glioblastoma clinical trials listed on ClinicalTrials.gov as “recruiting” or “not yet recruiting” as of February 2021.

Published
2022

44. Randomized trial of neoadjuvant vaccination with tumor-cell lysate induces T cell response in low-grade gliomas

Author

Hirokazu Ogino, Jennie W. Taylor, Takahide Nejo, David Gibson, Payal B. Watchmaker, Kaori Okada, Atsuro Saijo, Meghan R. Tedesco, Anny Shai, Cynthia M. Wong, Jane E. Rabbitt, Michael R. Olin, Christopher L. Moertel, Yasuhiko Nishioka, Andres M. Salazar, Annette M. Molinaro, Joanna J. Phillips, Nicholas A. Butowski, Jennifer L. Clarke, Nancy Ann Oberheim Bush, Shawn L. Hervey-Jumper, Philip Theodosopoulos, Susan M. Chang, Mitchel S. Berger, and Hideho Okada

Subjects
Adult, Male, and promotion of well-being, Clinical Trials and Supportive Activities, Immunology, T cells, Cancer immunotherapy, CD8-Positive T-Lymphocytes, Brain cancer, Cancer Vaccines, Medical and Health Sciences, Vaccine Related, Rare Diseases, Clinical Research, Tumor Microenvironment, Humans, Polylysine, Aged, Cancer, Vaccines, Prevention, Vaccination, Neurosciences, Evaluation of treatments and therapeutic interventions, General Medicine, Glioma, Middle Aged, Prevention of disease and conditions, Neoadjuvant Therapy, Brain Disorders, Poly I-C, Orphan Drug, Good Health and Well Being, Oncology, 3.4 Vaccines, Carboxymethylcellulose Sodium, 6.1 Pharmaceuticals, Female, Immunization, Clinical Medicine, Infection, Biotechnology
Abstract

BACKGROUND Long-term prognosis of WHO grade II low-grade gliomas (LGGs) is poor, with a high risk of recurrence and malignant transformation into high-grade gliomas. Given the relatively intact immune system of patients with LGGs and the slow tumor growth rate, vaccines are an attractive treatment strategy. METHODS We conducted a pilot study to evaluate the safety and immunological effects of vaccination with GBM6-AD, lysate of an allogeneic glioblastoma stem cell line, with poly-ICLC in patients with LGGs. Patients were randomized to receive the vaccines before surgery (arm 1) or not (arm 2) and all patients received adjuvant vaccines. Coprimary outcomes were to evaluate safety and immune response in the tumor. RESULTS A total of 17 eligible patients were enrolled — 9 in arm 1 and 8 in arm 2. This regimen was well tolerated with no regimen-limiting toxicity. Neoadjuvant vaccination induced upregulation of type-1 cytokines and chemokines and increased activated CD8+ T cells in peripheral blood. Single-cell RNA/T cell receptor sequencing detected CD8+ T cell clones that expanded with effector phenotype and migrated into the tumor microenvironment (TME) in response to neoadjuvant vaccination. Mass cytometric analyses detected increased tissue resident–like CD8+ T cells with effector memory phenotype in the TME after the neoadjuvant vaccination. CONCLUSION The regimen induced effector CD8+ T cell response in peripheral blood and enabled vaccine-reactive CD8+ T cells to migrate into the TME. Further refinements of the regimen may have to be integrated into future strategies. TRIAL REGISTRATION ClinicalTrials.gov NCT02549833. FUNDING NIH (1R35NS105068, 1R21CA233856), Dabbiere Foundation, Parker Institute for Cancer Immunotherapy, and Daiichi Sankyo Foundation of Life Science.

Published
2022

45. Isocitrate Dehydrogenase Mutant Grade II and III Glial Neoplasms

Author

Martin J. van den Bent, Kurt A. Jaeckle, Susan M. Chang, Ingo K. Mellinghoff, and Neurology

Subjects
Adult, Myeloid, Mutant, Low-grade glioma, Response assessment in neuro-oncology, Acute, Cardiorespiratory Medicine and Haematology, IDH2, Rare Diseases, medicine, Genetics, Humans, Oligodendroglial Tumor, Epigenetics, Oncology & Carcinogenesis, Cancer, Leukemia, business.industry, Brain Neoplasms, Myeloid leukemia, Glioma, Hematology, medicine.disease, Cancer metabolism, Isocitrate Dehydrogenase, Brain Disorders, Brain Cancer, Isocitrate dehydrogenase, Orphan Drug, Oncology, Mutation, Cancer research, Chondrosarcoma, business
Abstract

Mutations in isocitrate dehydrogenase (IDH) 1 or IDH2 occur in most of the adult low-grade gliomas and, less commonly, in cholangiocarcinoma, chondrosarcoma, acute myeloid leukemia, and other human malignancies. Cancer-associated mutations alter the function of the enzyme, resulting in production of R(-)-2-hydroxyglutarate and broad epigenetic dysregulation. Small molecule IDH inhibitors have received regulatory approval for the treatment of IDH mutant (mIDH) leukemia and are under development for the treatment of mIDH solid tumors. This article provides a current view of mIDH adult astrocytic and oligodendroglial tumors, including their clinical presentation and treatment, and discusses novel approaches and challenges toward improving the treatment of these tumors.

Published
2022

46. Assessment of higher-order singular value decomposition denoising methods on dynamic hyperpolarized [1-13C]pyruvate MRI data from patients with glioma

Author

Sana Vaziri, Adam W. Autry, Marisa Lafontaine, Yaewon Kim, Jeremy W. Gordon, Hsin-Yu Chen, Jasmine Y. Hu, Janine M. Lupo, Susan M. Chang, Jennifer L. Clarke, Javier E. Villanueva-Meyer, Nancy Ann Oberheim Bush, Duan Xu, Peder E.Z. Larson, Daniel B. Vigneron, and Yan Li

Subjects
Denoising, Cognitive Neuroscience, Carbon-13, Neurosciences, Bioengineering, Glioma, Magnetic Resonance Imaging, Bicarbonates, Hyperpolarized, Rare Diseases, Neurology, Pyruvic Acid, Humans, Biomedical Imaging, Radiology, Nuclear Medicine and imaging, Signal-to-noise ratio, Neurology (clinical), Lactic Acid, Higher-order singular value decomposition, Cancer
Abstract

BackgroundReal-time metabolic conversion of intravenously-injected hyperpolarized [1-13C]pyruvate to [1-13C]lactate and [13C]bicarbonate in the brain can be measured using dynamic hyperpolarized carbon-13 (HP-13C) MRI. However, voxel-wise evaluation of metabolism in patients with glioma is challenged by the limited signal-to-noise ratio (SNR) of downstream 13C metabolites, especially within lesions. The purpose of this study was to evaluate the ability of higher-order singular value decomposition (HOSVD) denoising methods to enhance dynamic HP [1-13C]pyruvate MRI data acquired from patients with glioma.MethodsDynamic HP-13C MRI were acquired from 14 patients with glioma. The effects of two HOSVD denoising techniques, tensor rank truncation-image enhancement (TRI) and global-local HOSVD (GL-HOSVD), on the SNR and kinetic modeling were analyzed in [1-13C]lactate data with simulated noise that matched the levels of [13C]bicarbonate signals. Both methods were then evaluated in patient data based on their ability to improve [1-13C]pyruvate, [1-13C]lactate and [13C]bicarbonate SNR. The effects of denoising on voxel-wise kinetic modeling of kPL and kPB was also evaluated. The number of voxels with reliable kinetic modeling of pyruvate-to-lactate (kPL) and pyruvate-to-bicarbonate (kPB) conversion rates within regions of interest (ROIs) before and after denoising was then compared.ResultsBoth denoising methods improved metabolite SNR and regional signal coverage. In patient data, the average increase in peak dynamic metabolite SNR was 2-fold using TRI and 4-5 folds using GL-HOSVD denoising compared to acquired data. Denoising reduced kPL modeling errors from a native average of 23% to 16% (TRI) and 15% (GL-HOSVD); and kPB error from 42% to 34% (TRI) and 37% (GL-HOSVD) (values were averaged voxelwise over all datasets). In contrast-enhancing lesions, the average number of voxels demonstrating within-tolerance kPL modeling error relative to the total voxels increased from 48% in the original data to 84% (TRI) and 90% (GL-HOSVD), while the number of voxels showing within-tolerance kPB modeling error increased from 0% to 15% (TRI) and 8% (GL-HOSVD).ConclusionPost-processing denoising methods significantly improved the SNR of dynamic HP-13C imaging data, resulting in a greater number of voxels satisfying minimum SNR criteria and maximum kinetic modeling errors in tumor lesions. This enhancement can aid in the voxel-wise analysis of HP-13C data and thereby improve monitoring of metabolic changes in patients with glioma following treatment.

Published
2022

47. Comparing China Reach and the Jamaica Home Visiting Program

Author

Jin Zhou, James J. Heckman, Bei Liu, Mai Lu, Susan M. Chang, and Sally Grantham-McGregor

Subjects
Pediatrics, Perinatology and Child Health
Abstract

OBJECTIVES Delayed child skill development is a common phenomenon in low- and middle-income countries. Effective and low-cost strategies suitable for application to less-developed countries are needed. We summarize empirical findings from recent papers that study a replication of the Jamaica Reach Up and Learn home visiting program in China, China REACH, and compare child skill growth profiles in the China Reach Up and Jamaica interventions. METHODS Different interventions often use different measures for assessing early childhood skill development. To estimate the growth of underlying skills across programs, we address the challenge that different programs use different assessments. We use a modified version of the Rasch model to anchor scores on common items to estimate skill development. RESULTS Language skill growth curves are comparable for both interventions. This pattern is consistent for the treatment and control groups across the interventions. Skill growth curves are not statistically significantly different between China REACH and Jamaican interventions. We find evidence of the importance of early investment. CONCLUSIONS The China REACH intervention significantly improves the development of multiple skills. At the same ages, treatment effect sizes and skill growth curves are comparable across the Jamaica and China REACH interventions, despite differences in scale and cultural settings. The scale of the program is much greater in China than in Jamaica, showing that the Jamaican curriculum can be effectively expanded to larger populations. Annual costs per child are roughly $500 (2015 US dollars).

Published
2022

48. Longitudinal MR spectroscopy to detect progression in patients with lower-grade glioma in the surveillance phase

Author

Lauro N, Avalos, Tracy L, Luks, Tyler, Gleason, Pablo, Damasceno, Yan, Li, Janine M, Lupo, Joanna, Phillips, Nancy Ann, Oberheim Bush, Jennie W, Taylor, Susan M, Chang, and Javier E, Villanueva-Meyer

Subjects
lower-grade glioma, screening and diagnosis, Neurosciences, Bioengineering, Brain Disorders, 4.1 Discovery and preclinical testing of markers and technologies, Brain Cancer, Detection, Rare Diseases, Oncology, Clinical Research, magnetic resonance spectroscopic imaging, Biomedical Imaging, Surgery, progression, Neurology (clinical), Cancer, 4.2 Evaluation of markers and technologies
Abstract

Background Monitoring lower-grade gliomas (LrGGs) for disease progression is made difficult by the limits of anatomical MRI to distinguish treatment related tissue changes from tumor progression. MR spectroscopic imaging (MRSI) offers additional metabolic information that can help address these challenges. The goal of this study was to compare longitudinal changes in multiparametric MRI, including diffusion weighted imaging, perfusion imaging, and 3D MRSI, for LrGG patients who progressed at the final time-point and those who remained clinically stable. Methods Forty-one patients with LrGG who were clinically stable were longitudinally assessed for progression. Changes in anatomical, diffusion, perfusion and MRSI data were acquired and compared between patients who remained clinically stable and those who progressed. Results Thirty-one patients remained stable, and 10 patients progressed. Over the study period, progressed patients had a significantly greater increase in normalized choline, choline-to-N-acetylaspartic acid index (CNI), normalized creatine, and creatine-to-N-acetylaspartic acid index (CRNI), than stable patients. CRNI was significantly associated with progression status and WHO type. Progressed astrocytoma patients had greater increases in CRNI than stable astrocytoma patients. Conclusions LrGG patients in surveillance with tumors that progressed had significantly increasing choline and creatine metabolite signals on MRSI, with a trend of increasing T2 FLAIR volumes, compared to LrGG patients who remained stable. These data show that MRSI can be used in conjunction with anatomical imaging studies to gain a clearer picture of LrGG progression, especially in the setting of clinical ambiguity.

Published
2022

49. T2 FLAIR hyperintensity volume Is associated with cognitive function and quality of life in clinically stable patients with lower grade gliomas

Author

Tracy L. Luks, Javier E. Villanueva-Meyer, Christina Weyer-Jamora, Karin Gehring, Angela Jakary, Shawn L. Hervey-Jumper, Steve E. Braunstein, Paige M. Bracci, Melissa S. Brie, Ellen M. Smith, Susan M. Chang, Jennie W. Taylor, and Cognitive Neuropsychology

Subjects
cognition, Aging, SURGERY, Clinical Sciences, neuropsychology, Neurodegenerative, Basic Behavioral and Social Science, Rare Diseases, Clinical Research, DEFICITS, NEUROCOGNITIVE DYSFUNCTION, glioma, Behavioral and Social Science, Acquired Cognitive Impairment, Psychology, BATTERY, RC346-429, Cancer, neuroimaging, Rehabilitation, Neurosciences, CHEMOTHERAPY, IMPAIRMENT, CANCER, Brain Disorders, PREVALENCE, Brain Cancer, Neurology, Biomedical Imaging, Neurology (clinical), Neurology. Diseases of the nervous system, neuro-oncology, DIFFUSE GLIOMA, RADIOTHERAPY
Abstract

Survival outcomes for patients with lower grade gliomas (LrGG) continue to improve. However, damage caused both by tumor growth and by the consequences of treatment often leads to significantly impaired cognitive function and quality of life (QoL). While neuropsychological testing is not routine, serial clinical MRIs are standard of care for patients with LrGG. Thus, having a greater understanding of MRI indicators of cognitive and QoL impairment risk could be beneficial to patients and clinicians. In this work we sought to test the hypothesis that in clinically stable LrGG patients, T2 FLAIR hyperintensity volumes at the time of cognitive assessment are associated with impairments of cognitive function and QoL and could be used to help identify patients for cognitive and QoL assessments and interventions. We performed anatomical MR imaging, cognitive testing and QoL assessments cross-sectionally in 30 clinically stable grade 2 and 3 glioma patients with subjective cognitive concerns who were 6 or more months post-treatment. Larger post-surgical T2 FLAIR volume at testing was significantly associated with lower cognitive performance, while pre-surgical tumor volume was not. Older patients had lower cognitive performance than younger patients, even after accounting for normal age-related declines in performance. Patients with Astrocytoma, IDH mutant LrGGs were more likely to show lower cognitive performance than patients with Oligodendroglioma, IDH mutant 1p19q co-deleted LrGGs. Previous treatment with combined radiation and chemotherapy was associated with poorer self-reported QoL, including self-reported cognitive function. This study demonstrates the importance of appreciating that LrGG patients may experience impairments in cognitive function and QoL over their disease course, including during periods of otherwise sustained clinical stability. Imaging factors can be helpful in identifying vulnerable patients who would benefit from cognitive assessment and rehabilitation.

Published
2022

50. TERT promotor status does not add prognostic information in IDH-wildtype glioblastomas fulfilling other diagnostic WHO criteria

Author

Philipp Karschnia, Jacob S Young, Antonio Dono, Levin Häni, Stephanie T Juenger, Tommaso Sciortino, Francesco Bruno, Nico Teske, Ramin A Morshed, Alexander F Haddad, Yalan Zhang, Sophia Stoecklein, Michael A Vogelbaum, Juergen Beck, Nitin Tandon, Shawn Hervey-Jumper, Annette M Molinaro, Roberta Rudà, Lorenzo Bello, Oliver Schnell, Yoshua Esquenazi, Maximilian I Ruge, Stefan J Grau, Martin van den Bent, Michael Weller, Mitchel S Berger, Susan M Chang, Joerg-Christian Tonn, Neurology, University of Zurich, and Tonn, Joerg-Christian

Subjects
2728 Neurology (clinical), 610 Medicine & health, 2730 Oncology, General Medicine, 10040 Clinic for Neurology, 2746 Surgery
Abstract

In IDH-wildtype glioblastomas which meet the histopathological or molecular diagnosis criteria, it remains unclear whether the presence of TERT promotor mutations provides additional prognostic information. Based on a multicenter cohort of 466 IDH-wildtype glioblastomas (including 396 with and 70 patients without TERT promotor mutations), we found that TERT promotor mutations were neither associated with progression-free survival nor overall survival. This held true in various treatment-based or molecular subgroups. This argues against standardized analysis for TERT promotor mutation status for the purpose of prognostic or therapeutic relevance in newly diagnosed IDH-wildtype glioblastoma that otherwise meets the histopathological and molecular diagnosis criteria.

Published
2022

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