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1. Supplementary materials-Neutrophil chemotaxis videos from Phase I Study of Zotiraciclib in Combination with Temozolomide for Patients with Recurrent High-grade Astrocytomas

Author

Mark R. Gilbert, John I. Gallin, Douglas B. Kuhns, William D. Figg, Katherine R. Calvo, Terri S. Armstrong, Javier Gonzales, Heather Leeper, Marta Penas-Prado, Eric M. Burton, Brett J. Theeler, Orwa Aboud, Christine Cordova, Nicole Lollo, Christine Siegel, Nancy Garren, Ramya Antony, Lisa Boris, Kelly Mentges, Ewa Grajkowska, Matthew Lindsley, Christine Bryla, Salman Ahmad, Elizabeth Vera, Tito R. Mendoza, Madison K. Butler, Guangyang Yu, Ying Pang, Yu-Ting Su, Tristan M. Sissung, Cody J. Peer, Danielle Fink, Debra A. Long Priel, Ying Yuan, and Jing Wu

Abstract

Neutrophils chemotaxis video

Published
2023

2. Supplementary materials-Clinical trial protocol from Phase I Study of Zotiraciclib in Combination with Temozolomide for Patients with Recurrent High-grade Astrocytomas

Author

Mark R. Gilbert, John I. Gallin, Douglas B. Kuhns, William D. Figg, Katherine R. Calvo, Terri S. Armstrong, Javier Gonzales, Heather Leeper, Marta Penas-Prado, Eric M. Burton, Brett J. Theeler, Orwa Aboud, Christine Cordova, Nicole Lollo, Christine Siegel, Nancy Garren, Ramya Antony, Lisa Boris, Kelly Mentges, Ewa Grajkowska, Matthew Lindsley, Christine Bryla, Salman Ahmad, Elizabeth Vera, Tito R. Mendoza, Madison K. Butler, Guangyang Yu, Ying Pang, Yu-Ting Su, Tristan M. Sissung, Cody J. Peer, Danielle Fink, Debra A. Long Priel, Ying Yuan, and Jing Wu

Abstract

Clinical trial protocol

Published
2023

3. Supplementary Data from Phase I Study of Zotiraciclib in Combination with Temozolomide for Patients with Recurrent High-grade Astrocytomas

Author

Mark R. Gilbert, John I. Gallin, Douglas B. Kuhns, William D. Figg, Katherine R. Calvo, Terri S. Armstrong, Javier Gonzales, Heather Leeper, Marta Penas-Prado, Eric M. Burton, Brett J. Theeler, Orwa Aboud, Christine Cordova, Nicole Lollo, Christine Siegel, Nancy Garren, Ramya Antony, Lisa Boris, Kelly Mentges, Ewa Grajkowska, Matthew Lindsley, Christine Bryla, Salman Ahmad, Elizabeth Vera, Tito R. Mendoza, Madison K. Butler, Guangyang Yu, Ying Pang, Yu-Ting Su, Tristan M. Sissung, Cody J. Peer, Danielle Fink, Debra A. Long Priel, Ying Yuan, and Jing Wu

Abstract

Supplementary Figures and Tables

Published
2023

4. Data from Phase I Study of Zotiraciclib in Combination with Temozolomide for Patients with Recurrent High-grade Astrocytomas

Author

Mark R. Gilbert, John I. Gallin, Douglas B. Kuhns, William D. Figg, Katherine R. Calvo, Terri S. Armstrong, Javier Gonzales, Heather Leeper, Marta Penas-Prado, Eric M. Burton, Brett J. Theeler, Orwa Aboud, Christine Cordova, Nicole Lollo, Christine Siegel, Nancy Garren, Ramya Antony, Lisa Boris, Kelly Mentges, Ewa Grajkowska, Matthew Lindsley, Christine Bryla, Salman Ahmad, Elizabeth Vera, Tito R. Mendoza, Madison K. Butler, Guangyang Yu, Ying Pang, Yu-Ting Su, Tristan M. Sissung, Cody J. Peer, Danielle Fink, Debra A. Long Priel, Ying Yuan, and Jing Wu

Abstract

Purpose:To investigate the toxicity profile and establish an optimal dosing schedule of zotiraciclib with temozolomide in patients with recurrent high-grade astrocytoma.Patients and Methods:This two-stage phase I trial determined the MTD of zotiraciclib combined with either dose-dense (Arm1) or metronomic (Arm2) temozolomide using a Bayesian Optimal Interval design; then a randomized cohort expansion compared the progression-free survival rate at 4 months (PFS4) of the two arms for an efficient determination of a temozolomide schedule to combine with zotiraciclib at MTD. Pharmacokinetic and pharmacogenomic profiling were included. Patient-reported outcome was evaluated by longitudinal symptom burden.Results:Fifty-three patients were enrolled. Dose-limiting toxicities were neutropenia, diarrhea, elevated liver enzymes, and fatigue. MTD of zotiraciclib was 250 mg in both arms and thus selected for the cohort expansion. Dose-dense temozolomide plus zotiraciclib (PSF4 40%) compared favorably with metronomic temozolomide (PFS4 25%). Symptom burden worsened at cycle 2 but stabilized by cycle 4 in both arms. A significant decrease in absolute neutrophil count and neutrophil reactive oxygen species production occurred 12–24 hours after an oral dose of zotiraciclib but both recovered by 72 hours. Pharmacokinetic/pharmacogenomic analyses revealed that the CYP1A2_5347T>C (rs2470890) polymorphism was associated with higher AUCinf value.Conclusions:Zotiraciclib combined with temozolomide is safe in patients with recurrent high-grade astrocytomas. Zotiraciclib-induced neutropenia can be profound but mostly transient, warranting close monitoring rather than treatment discontinuation. Once validated, polymorphisms predicting drug metabolism may allow personalized dosing of zotiraciclib.

Published
2023

5. Association of hyperglycemia and molecular subclass on survival in IDH-wildtype glioblastoma

Author

Elisa K Liu, Varshini Vasudevaraja, Vladislav O Sviderskiy, Yang Feng, Ivy Tran, Jonathan Serrano, Christine Cordova, Sylvia C Kurz, John G Golfinos, Erik P Sulman, Daniel A Orringer, Dimitris Placantonakis, Richard Possemato, and Matija Snuderl

Subjects
General Medicine
Abstract

Background Hyperglycemia has been associated with worse survival in glioblastoma. Attempts to lower glucose yielded mixed responses which could be due to molecularly distinct GBM subclasses. Methods Clinical, laboratory, and molecular data on 89 IDH-wt GBMs profiled by clinical next-generation sequencing and treated with Stupp protocol were reviewed. IDH-wt GBMs were sub-classified into RTK I (Proneural), RTK II (Classical) and Mesenchymal subtypes using whole-genome DNA methylation. Average glucose was calculated by time-weighting glucose measurements between diagnosis and last follow-up. Results Patients were stratified into three groups using average glucose: tertile one (115 mg/dL). Comparison across glucose tertiles revealed no differences in performance status (KPS), dexamethasone dose, MGMT methylation, or methylation subclass. Overall survival (OS) was not affected by methylation subclass (P = .9) but decreased with higher glucose (P = .015). Higher glucose tertiles were associated with poorer OS among RTK I (P = .08) and mesenchymal tumors (P = .05), but not RTK II (P = .99). After controlling for age, KPS, dexamethasone, and MGMT status, glucose remained significantly associated with OS (aHR = 5.2, P = .02). Methylation clustering did not identify unique signatures associated with high or low glucose levels. Metabolomic analysis of 23 tumors showed minimal variation across metabolites without differences between molecular subclasses. Conclusion Higher average glucose values were associated with poorer OS in RTKI and Mesenchymal IDH-wt GBM, but not RTKII. There were no discernible epigenetic or metabolomic differences between tumors in different glucose environments, suggesting a potential survival benefit to lowering systemic glucose in selected molecular subtypes.

Published
2022

6. Phase I Study of Zotiraciclib in Combination with Temozolomide for Patients with Recurrent High-grade Astrocytomas

Author

Ying Yuan, Brett Theeler, Eric M. Burton, Cody J. Peer, Douglas B. Kuhns, Salman Ahmad, Marta Penas-Prado, Nicole Lollo, Jing Wu, Matthew Lindsley, Christine Cordova, William D. Figg, John I. Gallin, Ramya Antony, Danielle Fink, Mark R. Gilbert, Javier Gonzales, Lisa Boris, Madison Butler, Tito R. Mendoza, Elizabeth Vera, Debra A. Long Priel, Ewa Grajkowska, Tristan M. Sissung, Ying Pang, Christine Bryla, Heather E. Leeper, Orwa Aboud, Katherine R. Calvo, Guangyang Yu, Terri S. Armstrong, Yu Ting Su, Kelly Mentges, Christine Siegel, and Nancy Garren

Subjects
0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Maximum Tolerated Dose, Clinical Trials and Supportive Activities, Oncology and Carcinogenesis, Astrocytoma, Neutropenia, Article, 03 medical and health sciences, Rare Diseases, 0302 clinical medicine, Pharmacokinetics, Clinical Research, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, Temozolomide, medicine, Humans, Oncology & Carcinogenesis, Dosing, Survival rate, Cancer, Brain Neoplasms, business.industry, Evaluation of treatments and therapeutic interventions, Bayes Theorem, medicine.disease, Discontinuation, Dacarbazine, 030104 developmental biology, 6.1 Pharmaceuticals, 030220 oncology & carcinogenesis, Absolute neutrophil count, Patient Safety, Digestive Diseases, business, medicine.drug
Abstract

Purpose: To investigate the toxicity profile and establish an optimal dosing schedule of zotiraciclib with temozolomide in patients with recurrent high-grade astrocytoma. Patients and Methods: This two-stage phase I trial determined the MTD of zotiraciclib combined with either dose-dense (Arm1) or metronomic (Arm2) temozolomide using a Bayesian Optimal Interval design; then a randomized cohort expansion compared the progression-free survival rate at 4 months (PFS4) of the two arms for an efficient determination of a temozolomide schedule to combine with zotiraciclib at MTD. Pharmacokinetic and pharmacogenomic profiling were included. Patient-reported outcome was evaluated by longitudinal symptom burden. Results: Fifty-three patients were enrolled. Dose-limiting toxicities were neutropenia, diarrhea, elevated liver enzymes, and fatigue. MTD of zotiraciclib was 250 mg in both arms and thus selected for the cohort expansion. Dose-dense temozolomide plus zotiraciclib (PSF4 40%) compared favorably with metronomic temozolomide (PFS4 25%). Symptom burden worsened at cycle 2 but stabilized by cycle 4 in both arms. A significant decrease in absolute neutrophil count and neutrophil reactive oxygen species production occurred 12–24 hours after an oral dose of zotiraciclib but both recovered by 72 hours. Pharmacokinetic/pharmacogenomic analyses revealed that the CYP1A2_5347T>C (rs2470890) polymorphism was associated with higher AUCinf value. Conclusions: Zotiraciclib combined with temozolomide is safe in patients with recurrent high-grade astrocytomas. Zotiraciclib-induced neutropenia can be profound but mostly transient, warranting close monitoring rather than treatment discontinuation. Once validated, polymorphisms predicting drug metabolism may allow personalized dosing of zotiraciclib.

Published
2021

7. Functional connectivity of the default mode, dorsal attention and fronto-parietal executive control networks in glial tumor patients

Author

Rajan Jain, Ruoyu Luie Wang, Sylvia Kurz, Daniel A. Orringer, Douglas Kondziolka, John G. Golfinos, Guillaume Madelin, Yulin Ge, Christine Cordova, Pradeep Kumar Gupta, Mickael Tordjman, and Mariana Lazar

Subjects
Adult, Male, Cancer Research, medicine.medical_specialty, Neurology, Adolescent, Precuneus, Glial tumor, Corpus callosum, Article, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Task-positive network, Glioma, Image Interpretation, Computer-Assisted, Humans, Medicine, Default mode network, Aged, Brain Mapping, Resting state fMRI, Brain Neoplasms, business.industry, Default Mode Network, Middle Aged, medicine.disease, Magnetic Resonance Imaging, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Female, Neurology (clinical), business, Neuroscience, 030217 neurology & neurosurgery
Abstract

PURPOSE: Resting state functional magnetic resonance imaging (rsfMRI) is an emerging tool to explore the functional connectivity of different brain regions. We aimed to assess the disruption of functional connectivity of the Default Mode Network (DMN), Dorsal Attention Network(DAN) and Fronto-Parietal Network (FPN) in patients with glial tumors. METHODS: rsfMRI data acquired on 3T-MR of treatment-naive glioma patients prospectively recruited (2015–2019) and matched controls from the 1000 functional-connectomes-project were analyzed using the CONN functional toolbox. Seed-Based Connectivity Analysis (SBCA) and Independent Component Analysis (ICA, with 10 to 100 components) were performed to study reliably the three networks of interest. RESULTS: 35 patients with gliomas (17 WHO grade I-II, 18 grade III-IV) and 70 controls were included. Global increased DMN connectivity was consistently found with SBCA and ICA in patients compared to controls (Cluster1: Precuneus, height: p < 10(−6); Cluster2: subcallosum; height: p < 10(−5)). However, an area of decreased connectivity was found in the posterior corpus callosum, particularly in high-grade gliomas (height: p < 10(−5)). The DAN demonstrated small areas of increased connectivity in frontal and occipital regions (height: p < 10(−6)). For the FPN, increased connectivity was noted in the precuneus, posterior cingulate gyrus, and frontal cortex. No difference in the connectivity of the networks of interest was demonstrated between low- and high-grade gliomas, as well as when stratified by their IDH1-R132H (isocitrate dehydrogenase) mutation status. CONCLUSION: Altered functional connectivity is reliably found with SBCA and ICA in the DMN, DAN, and FPN in glioma patients, possibly explained by decreased connectivity between the cerebral hemispheres across the corpus callosum due to disruption of the connections.

Published
2021

8. The prevalence of altered body image in patients with primary brain tumors: an understudied population

Author

Veeraj Shah, Kathleen Wall, Christine Siegel, Christine Bryla, Tito R. Mendoza, Elizabeth Vera, Peter Mathen, Nicole Leggiero, Orwa Aboud, Jennifer Reyes, Marta Penas-Prado, Alvina Acquaye, Kevin Camphausen, Ramya Antony, Mark R. Gilbert, Eric Burton, Sonja Crandon, Lindsay Rowe, Jing Wu, Terri Armstrong, Christine Cordova, Yamini Vyas, and Lisa Boris

Subjects
Male, Cancer Research, Neurology, Disease, Anxiety, 0302 clinical medicine, Quality of life, Prevalence, Prospective Studies, Depression (differential diagnoses), Cancer, MD Anderson Symptom Inventory - Brain Tumor, education.field_of_study, Brain Neoplasms, Depression, Middle Aged, Prognosis, Body image, Mental Health, Oncology, 030220 oncology & carcinogenesis, Female, medicine.symptom, Psychosocial, Adult, medicine.medical_specialty, Oncology and Carcinogenesis, Population, Psychological distress, Brain tumors, Young Adult, 03 medical and health sciences, Clinical Research, Internal medicine, Behavioral and Social Science, Body Image, medicine, Humans, Oncology & Carcinogenesis, education, Aged, business.industry, Neurosciences, United States, Brain Disorders, Cross-Sectional Studies, Good Health and Well Being, Clinical Study, Neurology (clinical), business, 030217 neurology & neurosurgery, Follow-Up Studies
Abstract

Purpose Body image (BI) is an important issue for cancer patients, as patients with BI concerns are susceptible to depression, anxiety, difficulty coping, and poor quality of life (QoL). While this concern has been documented in patients with other malignancies, no data exists of this QoL issue in patients with primary brain tumors (PBT). Methods A cross-sectional survey of 100 PBT patients was conducted on an IRB approved prospective protocol using structured questionnaires. Participants completed the body image scale (BIS), Appearance Scheme Inventory Revised (ASI-R), MD Anderson Symptom Inventory Brain Tumor (MDASI-BT), and Patient-Reported Outcomes Measurement Information System (PROMIS) Depression, Anxiety, and Psychosocial Impact Positive measures. Results The prevalence of clinically significant body image dissatisfaction (BIS ≥ 10) was 28% (95% CI 19–37%), median BIS score was 5 (range 0–27). The median ASI-R composite score was 2.9 (range 1.5–4.7). BIS was significantly correlated with the ASI-R (r = 0.53, 95% CI 0.37 to 0.65). The mean PROMIS Depression score was 48.4 (SD = 8.9), PROMIS Anxiety score was 49.4 (SD = 9.9), and PROMIS Psychosocial Illness Impact Positive score was 48.9 (SD = 9.7). BIS was significantly correlated with age, and trended with BMI and sex. The PROMIS Psychosocial Illness Impact Positive and PROMIS Anxiety scores were the most strongly related to BIS. Conclusions This study, the first to explore altered body image in PBT patients, revealed clinically significant body image dissatisfaction in nearly 1/3 of patients, similar to other malignancies. These findings underscore the potential contribution of disease and treatment-related body image concerns on psychosocial wellbeing in patients with PBT.

Published
2020

9. NCOG-11. ASSOCIATION OF HYPERGLYCEMIA AND TUMOR SUBCLASS ON SURVIVAL IN IDH-WILDTYPE GLIOBLASTOMA

Author

Erik P. Sulman, Varshini Vasudevaraja, Matija Snuderl, Jonathan Serrano, Yang Feng, Dimitris G. Placantonakis, Elisa Liu, Vladislav O. Sviderskiy, Ivy Tran, Sylvia Kurz, John G. Golfinos, Richard Possemato, and Christine Cordova

Subjects
Cancer Research, Wild type, O-6-methylguanine-DNA methyltransferase, Methylation, Biology, 26th Annual Meeting & Education Day of the Society for Neuro-Oncology, Subclass, Isocitrate dehydrogenase, Oncology, DNA methylation, Cancer research, medicine, Neurology (clinical), Epigenetics, Dexamethasone, medicine.drug
Abstract

BACKGROUND RNA expression and DNA methylation studies have identified different subclasses of isocitrate dehydrogenase (IDH)-wildtype (wt) glioblastoma (GBM). However, the prognostic significance of molecular subclasses is unclear. Although hyperglycemia has been previously associated with worse survival, attempts to lower glucose have yielded mixed responses. The role of hyperglycemia may be confounded by molecular heterogeneity and have different impact in molecularly distinct GBM subclasses. METHODS Clinical, laboratory, and molecular data on 89 IDH-wt GBMs profiled by clinical next-generation sequencing and treated with Stupp protocol were reviewed. IDH-wt GBMs were subclassified into RTKI (Proneural), RTKII (Classical) and Mesenchymal subtypes using DNA methylation. Average glucose was calculated by time-weighting plasma glucose measurements between diagnosis and last follow-up. RESULTS Patients were stratified into three groups using average glucose: tertile one (< 100mg/dL), tertile two (100-115mg/dL), and tertile three ( > 115mg/dL). Comparison across glucose tertiles revealed no significant differences in Karfnosky Performance Status (KPS), dexamethasone dose, MGMT methylation, or methylation subclass. Overall survival (OS) was not affected by methylation subclass (log-rank p=0.9) but decreased with higher glucose (log-rank p=0.015). Higher glucose tertiles were associated with poorer OS among RTK I (log-rank p=0.08) and mesenchymal tumors (log-rank p=0.05), but not RTK II (log-rank p=0.99). After controlling for age, KPS, dexamethasone dose, and MGMT status, glucose remained significantly associated with survival (adjusted hazard ratio=5.2, p=0.02). DNA methylation clustering did not identify a unique signature associated with high or low glucose levels. Metabolomic analysis of 23 tumors showed minimal variation across metabolites within the cohort with no differences across molecular subclasses. CONCLUSION Higher average glucose values were associated with poorer OS in RTKI and Mesenchymal IDH-wt GBM, but not RTKII. There were no discernible epigenetic or metabolomic differences between tumors in different glucose environments, suggesting a potential survival benefit with systemic glucose lowering in selected molecular subtype.

Published
2021

10. CTNI-57. RADIONUCLIDE THERAPY WITH 177LU-DOTATATE (LUTATHERA) IN ADULTS WITH ADVANCED INTRACRANIAL MENINGIOMA - INTERIM ANALYSIS RESULTS OF A SINGLE-ARM, OPEN-LABEL, MULTICENTER PHASE II STUDY

Author

Sylvia Kurz, Elcin Zan, Christine Cordova, Marissa Barbaro, Andrea Troxel, Joshua Silverman, Matija Snuderl, David Zagzag, John Golfinos, David Kondziolka, and Erik Sulman

Subjects
Cancer Research, Oncology, Neurology (clinical)
Abstract

BACKGROUND While most meningiomas are considered benign tumors, a subset of these tumors are characterized by a more aggressive clinical course and require multimodal treatment. Beyond surgical and radiotherapeutic options, there are no effective medical treatments available. Somatostatin receptor 2 (SSTR2) is expressed by the majority of meningiomas. 177Lu-DOTATATE is a SSTR2-targeting radionuclide that has been successful in neuroendocrine tumors. Here we report the results of the interim analysis of an ongoing clinical trial (NCT03971461) that is evaluating the effect of 177Lu-DOTATATE in treating progressive intracranial meningiomas. METHODS In this Simon two-stage design phase II study, adults with advanced intracranial meningiomas received 177Lu-DOTATATE 7.4 GBq (200 mCi) every eight weeks for four doses. 68Ga-DOTATATE PET-MRI was performed before and at the end of treatment. The primary endpoint was progression-free survival at 6 months (PFS-6). Correlative studies evaluated the association of PFS-6, objective response rate, progression-free survival, overall survival with radiographic tumor measurements, 68Ga-DOTATATE uptake on PET-MRI, SSTR2 expression in tumor, and meningioma methylation subclass. RESULTS Fourteen patients (F = 11, M = 3) with progressive meningiomas (WHO I = 3, II = 10, III = 1) have been enrolled. Median age was 63.1 (range 49-78) years. All patients previously underwent tumor resection and at least one course of radiation. Treatment with 177Lu-DOTATATE was well tolerated, no treatment-limiting toxicities were observed. Six of 14 patients (42%) achieved PFS-6. Radiographically, all six patients had achieved Stable Disease. A functional alteration of tumoral SSTR2 expression by 68Ga-DOTATATE PET-MR imaging was observed in three patients. CONCLUSIONS Treatment with SSTR2-targeting 177Lu-DOTATATE is well tolerated. In this interim analysis, six of 14 patients achieved PFS-6. This exceeds the predefined threshold to continue to stage two of this study. This clinical trial is now open to patient enrollment at two study sites in the US.

Published
2022

11. Proceedings of the Comprehensive Oncology Network Evaluating Rare CNS Tumors (NCI-CONNECT) Oligodendroglioma Workshop

Author

Marta, Penas-Prado, Jing, Wu, Daniel P, Cahill, Daniel J, Brat, Joseph F, Costello, Paul G, Kluetz, J Gregory, Cairncross, Martin, van den Bent, Roel G W, Verhaak, Orwa, Aboud, Peter, Burger, Susan M, Chang, Christine, Cordova, Raymond Y, Huang, Lindsay S, Rowe, Martin J B, Taphoorn, Mark R, Gilbert, Terri S, Armstrong, Kareem, Zaghloul, and Neurology

Subjects
0301 basic medicine, Medical education, business.industry, Clinical study design, Cancer, Review, medicine.disease, Call to action, Data sharing, Outreach, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, SDG 3 - Good Health and Well-being, 030220 oncology & carcinogenesis, General partnership, Health care, medicine, Oligodendroglioma, business
Abstract

Background Oligodendroglioma is a rare primary central nervous system (CNS) tumor with highly variable outcome and for which therapy is usually not curative. At present, little is known regarding the pathways involved with progression of oligodendrogliomas or optimal biomarkers for stratifying risk. Developing new therapies for this rare cancer is especially challenging. To overcome these challenges, the neuro-oncology community must be particularly innovative, seeking multi-institutional and international collaborations, and establishing partnerships with patients and advocacy groups thereby ensuring that each patient enrolled in a study is as informative as possible. Methods The mission of the National Cancer Institute’s NCI-CONNECT program is to address the challenges and unmet needs in rare CNS cancer research and treatment by connecting patients, health care providers, researchers, and advocacy organizations to work in partnership. On November 19, 2018, the program convened a workshop on oligodendroglioma, one of the 12 rare CNS cancers included in its initial portfolio. The purpose of this workshop was to discuss scientific progress and regulatory challenges in oligodendroglioma research and develop a call to action to advance research and treatment for this cancer. Results The recommendations of the workshop include a multifaceted and interrelated approach covering: biology and preclinical models, data sharing and advanced molecular diagnosis and imaging; clinical trial design; and patient outreach and engagement. Conclusions The NCI-CONNECT program is well positioned to address challenges in oligodendroglioma care and research in collaboration with other stakeholders and is developing a list of action items for future initiatives.

Published
2020

12. NCI-CONNECT: Comprehensive Oncology Network Evaluating Rare CNS Tumors-Histone Mutated Midline Glioma Workshop Proceedings

Author

John D. Heiss, Ali Shilatifard, Mark R. Gilbert, Marta Penas-Prado, Michelle Monje, Yamini Dalal, Carlos G Romo, Orwa Aboud, Christine Cordova, Kevin Camphausen, Elizabeth Finch, Kenneth Aldape, Roger J. Packer, Mario L. Suvà, Brett Theeler, and Terri Armstrong

Subjects
0301 basic medicine, Oncology, medicine.medical_specialty, Pediatric Cancer, Review, Disease, Glial tumor, 03 medical and health sciences, Rare Diseases, 0302 clinical medicine, Internal medicine, Glioma, H3F3A gene, Genetics, Medicine, CNS TUMORS, histone-mutated glioma, Cancer, Pediatric, clinical trials, biology, business.industry, Neurosciences, medicine.disease, rare brain tumors, Brain Disorders, Brain Cancer, Clinical trial, Orphan Drug, 030104 developmental biology, Histone, biology.protein, business, NCI-CONNECT, 030217 neurology & neurosurgery
Abstract

Histone mutations occur in approximately 4% of different cancer types. In 2012, mutations were found in the gene encoding histone variant H3.3 (H3F3A gene) in pediatric diffuse intrinsic pontine gliomas and pediatric hemispheric gliomas. Tumors with mutations in the H3F3A gene are generally characterized as histone mutated gliomas (HMGs) or diffuse midline gliomas. HMGs are a rare subtype of glial tumor that is malignant and fast growing, carrying a poor prognosis. In 2017, the Beau Biden Cancer Moonshot Program appropriated $1.7 billion toward cancer care in 10 select areas. The National Cancer Institute (NCI) was granted support to focus specifically on rare central nervous system (CNS) tumors through NCI-CONNECT. Its mission is to address the challenges and unmet needs in CNS cancer research and treatment by connecting patients, providers, researchers, and advocacy organizations to work in partnership. On September 27, 2018, NCI-CONNECT convened a workshop on histone mutated midline glioma, one of the 12 CNS cancers included in its initial portfolio. Three leaders in the field provided an overview of advances in histone mutated midline glioma research. These experts shared observations and experiences related to common scientific and clinical challenges in studying these tumors. Although the clinical focus of this workshop was on adult patients, one important objective was to start a collaborative dialogue between pediatric and adult clinicians and researchers. Meeting participants identified needs for diagnostic and treatment standards, disease biology and biological targets for this cancer, disease-specific trial designs, and developed a list of action items and future direction.

Published
2020

13. Advances in Molecular Classification and Therapeutic Opportunities in Meningiomas

Author

Sylvia Kurz and Christine Cordova

Subjects
0301 basic medicine, DNA Copy Number Variations, Bioinformatics, Meningioma, Phosphatidylinositol 3-Kinases, 03 medical and health sciences, 0302 clinical medicine, Molecular classification, Meningeal Neoplasms, Tumor Microenvironment, otorhinolaryngologic diseases, medicine, Humans, Epigenetics, neoplasms, Loss function, Neurofibromin 2, Tumor biology, business.industry, DNA Methylation, Who grade, medicine.disease, nervous system diseases, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Mutation, DNA methylation, business, Who classification, Signal Transduction
Abstract

Our understanding of the genetic and epigenetic alterations in meningioma and the underlying tumor biology of meningioma has significantly changed over the past decade and resulted in revision of prognostically relevant meningioma subclasses within and beyond the WHO classification of CNS tumors. The 2016 WHO classification of CNS tumors recognizes WHO grade I, II, and III based on histopathological features. Recent work has identified genetic alterations with prognostic implications, including mutations of the TERT promoter, loss of function of the DMD gene, and inactivation of the tumor suppressor BAP-1. Studies of DNA methylation patterns in meningiomas have resulted in a novel and prognostically relevant meningioma subclassification schema. There have been major advances in our understanding of prognostically relevant genetic and epigenetic changes in meningioma which will hopefully allow for improvement in clinical trial design and the development of more effective therapies for meningioma.

Published
2020

14. State of the Art Treatment and Surveillance Imaging of Glioblastomas

Author

Christine Cordova, Stefan E. Margiewicz, Andrew S. Chi, and Rajan Jain

Subjects
Brain Neoplasms, business.industry, Brain, Angiogenesis Inhibitors, Magnetic Resonance Imaging, Data science, 03 medical and health sciences, 0302 clinical medicine, Fluorodeoxyglucose F18, Positron-Emission Tomography, 030220 oncology & carcinogenesis, Humans, Medicine, Radiology, Nuclear Medicine and imaging, Immunotherapy, State (computer science), Radiopharmaceuticals, Surveillance imaging, Glioblastoma, business, 030217 neurology & neurosurgery
Published
2018

15. CTIM-20. FINAL RESULTS OF CONTROLLED IL-12 MONOTHERAPY AND IN COMBINATION WITH PD-1 INHIBITOR IN ADULT SUBJECTS WITH RECURRENT GLIOBLASTOMA

Author

Nate Demars, John S. Yu, Kamal Chadha, John Loewy, Nancy Ann Oberheim-Bush, Rimas V. Lukas, Christina Amidei, Jill Buck, Nira Hadar, Taylor Estupinan, Laurence J.N. Cooper, Robert Cavaliere, E. Antonio Chiocca, Christine Cordova, Clark C. Chen, Joseph Landolfi, and John Miao

Subjects
Oncology, Cancer Research, medicine.medical_specialty, biology, business.industry, Recurrent glioblastoma, 26th Annual Meeting & Education Day of the Society for Neuro-Oncology, Programmed cell death 1, Internal medicine, biology.protein, Interleukin 12, Medicine, Neurology (clinical), business
Abstract

Ad-RTS-hIL-12(Ad) is a gene therapy candidate conditionally expressing IL-12 under the transcriptional control of veledimex(V) acting via the RheoSwitch Therapeutic System® gene switch. Veledimex plasma and tumor PK demonstrated a dose-response relationship and crossing the BBB. PD-1+ T-cells were increased in tumor biopsy samples after treatment with Controlled-IL-12 in a phase-l study. This finding was the rationale for conducting 2 trials of Controlled-IL-12 in combination with PD-1-inhibitor to enhance T-cell-mediated anti-tumor effects. Data from two completed phase-I studies (presented in SNO2020), and an ongoing phase-II study of Controlled-IL-12 with cemiplimab study for the treatment of recurrent glioblastoma (rGBM) will be discussed. Ziopharm has conducted 3 phase-I (NCT02026271/NCT03679754 (monotherapy), NCT03636477 (combination with nivolumab)) and one phase-ll (NCT04006119) multicenter, open-label, single-arm trial in subjects with rGBM is evaluating Ad (single intratumoral injection, 2 x 1011-viral-particles, Day0) with oral V dosing (20mg, Days 0-14) with cemiplimab infusions (350 mg IV) on Days -7, 15, then Q3W. Systemic biomarkers (serum cytokines, and immune-activation-markers), local effects (tumor cytokines, T-cell immunobiology, pathology), neoepitope, and imaging will be assessed. Subject characteristics (Controlled IL-12 monotherapy (n=75); combination (Controlled IL-12 with anti-PD-1s) (n=61) were consistent across all 3 studies. Safety profiles were comparable between monotherapy and in combination with anti-PD-1s. Adverse reactions (ARs) after nivolumab or cemiplimab were consistent with labeling of anti-PD-1s. ARs related to Controlled IL-12 were all manageable and reversible with no synergistic toxicities in combination with anti-PD-1s. Increases in serum cytokine levels and pathology findings consistent with immune-mediated anti-tumor effect were observed in subjects who received Controlled-IL-12 monotherapy and in combination with anti-PD-1s. Final survival data and results from neoepitope analysis will be presented. Further investigation is warranted to understand the impact of monotherapy vs. combination, concurrent steroids use and unifocal vs. multifocal disease on overall survival in subjects with rGBM receiving Controlled-IL-12.

Published
2021

16. CTNI-53. SINGLE ARM, OPEN-LABEL, MULTICENTER PHASE II STUDY OF THE RADIONUCLIDE 177LU-DOTATATE (LUTATHERA) IN ADULTS WITH ADVANCED INTRACRANIAL MENINGIOMA

Author

Matija Snuderl, David Zagzag, Andrea B. Troxel, Douglas Kondziolka, Joshua S. Silverman, Christine Cordova, Erik P. Sulman, Elcin Zan, Zacharia Sawaged, Jasone Gurewitz, Hector Sevillano-Torres, Sylvia Kurz, and John G. Golfinos

Subjects
Cancer Research, Oncology, business.industry, Troponin I, Clinical Trials: Non-Immunologic, 177Lu-DOTATATE, Medicine, Phases of clinical research, Neurology (clinical), Intracranial meningioma, Open label, business, Nuclear medicine
Abstract

BACKGROUND Meningiomas are the most common primary intracranial neoplasm. Once surgical and radiotherapeutic options are exhausted, there are no effective medical treatments available. A majority of meningiomas express somatostatin receptor 2 (SSTR2), representing a promising treatment target. 177Lu-DOTATATE is a SSTR2-targeting radionuclide that has been successful in SSTR2-expressing neuroendocrine tumors. Here we hypothesize that 177Lu-DOTATATE is effective in treating progressive intracranial meningiomas. METHODS In this ongoing phase II study (NCT03971461), adults with advanced intracranial meningiomas received 177Lu-DOTATATE 7.4 GBq (200 mCi) every 8 weeks for 4 doses. 68Ga-DOTATATE PET-MRI was obtained before and at the end of treatment (EOT). The primary endpoint was progression-free survival at 6 months (PFS-6). Correlative studies evaluated the association of PFS-6, objective response rate, progression-free survival, overall survival with radiographic tumor measurements, 68Ga-DOTATATE uptake on PET-MRI, SSTR2 expression in tumor, and meningioma methylation subclass. RESULTS Nine patients (F = 7, M = 2) with progressive meningiomas (WHO I = 2, II = 6, III = 1) have been enrolled. Median age was 63 (range 49–78) years. All patients previously underwent tumor resection and at least one course of radiation. Treatment with 177Lu-DOTATATE was well tolerated, although CTCAE grade 3/4 electrolyte derangements and cytopenias were observed. Six patients reached PFS-6, three patients experienced progressive disease. Four patients had EOT 68Ga-DOTATATE PET-MRI evaluations in which anatomic measurements and 68Ga-DOTATATE standardized uptake values (SUV) pre- and post-treatment were assessed: one patient had reduced SUV measurements in all target lesions indicating altered SSTR2 expression and functional treatment response, one patient had stable disease, one patient had a mixed treatment response, and one patient experienced progressive disease. CONCLUSIONS SSTR2-targeting 177Lu-DOTATATE represents a promising treatment option for patients with progressive intracranial meningiomas. Treatment is well tolerated and can lead to functional alteration of tumoral SSTR2 expression by 68Ga-DOTATATE PET-MR imaging.

Published
2020

17. RARE-35. MRI FINDINGS AT PROGRESSION IN ADULT PATIENTS WITH MEDULLOBLASTOMA

Author

Terri Armstrong, Christine Cordova, Orwa Aboud, Nicole Leggiero, Elizabeth Vera, Christine Bryla, Jennifer Reyes, Lisa Boris, Kathleen Wall, Christine Siegel, Sonja Crandon, Yamini Vyas, Mark R. Gilbert, Jing Wu, Eric Burton, Ramya Antony, Brett Theeler, and Marta Penas-Prado

Subjects
Medulloblastoma, Cancer Research, medicine.medical_specialty, Oncology, Adult patients, business.industry, Rare Tumors, Medicine, Neurology (clinical), Radiology, business, medicine.disease, Mri findings
Abstract

Progression (PD) in medulloblastoma (MB) represents a diagnostic challenge due to imaging heterogeneity among/within patients. SHH (Sonic hedgehog)-MB is thought to recur mostly within the tumor bed (TB). In children, DWI restriction (DWIr) is more sensitive than contrast enhancement(CE) for first PD. Whether this is applicable to adults is unknown. METHODS Retrospective review of adults (age ≥18) with MB enrolled to Natural History study at NCI-NOB. Descriptive statistics of imaging at diagnosis and PD(CE, T2/FLAIR signal without CE, DWIr) and imaging patterns for each PD. RESULTS:14 adults with MB: 5 diagnosed in childhood (8–16 yrs), 9 as adults (18–45 yrs); Subtypes: 7 SHH, 3 non-WNT/non-SHH, 4 unknown. Eleven experienced ≥1 PD (6/7 SHH, 2/3 non-WNT/non-SHH, 3/4 unknown); median PD of 5 (range 1–9). Median age at first PD 31 years (range 10–46) with 5 first PDs >5 years after diagnosis. In 10 patients with available baseline MRI, 9 had CE, and 8 DWIr (2 without DWI sequences). Of 48 total PDs, the commonest patterns were: brain LMD alone (n=14), TB alone or distant brain parenchyma alone (each n=7), distant brain parenchyma with brain LMD (n=6), and TB with either distant brain parenchyma or LMD (n=3). Of the 82 PD lesions, 23% (n=14) of brain lesions lacked DWIr, and 37% (n=23) had T2/FLAIR signal without CE. PD tissue confirmation obtained at 18 time points:16 cases with confirmed recurrence had heterogeneous characteristics; in 12 with brain PD: CE in 5, T2/FLAIR without CE in 3 (unknown: 4). 2 CE lesions revealed meningioma (one- atypical meningioma- had DWIr). CONCLUSIONS Imaging findings in adult patients with MB are highly heterogeneous. Despite high specificity of DWIr for PD in children, it failed for 23% of brain lesions across multiple patients. Most SHH-MB had PD outside the TB, unlike what is widely accepted in the literature.

Published
2019

18. HOUT-22. EVALUATING CLINICAL IMPACT UTILIZING THE RANO-PRO COLLABORATIVE’S STANDARDIZED PRIORITY CONSTRUCTS

Author

Ramya Antony, Nicole Leggiero, Christine Bryla, Marta Penas-Prado, Jing Wu, Terri Armstrong, Elizabeth Vera, Brett Theeler, Mark R. Gilbert, Sonja Crandon, Jennifer Reyes, Kathleen Wall, Christine Cordova, Christine Siegel, Lisa Boris, Eric Burton, and Orwa Aboud

Subjects
Cancer Research, medicine.medical_specialty, Oncology, Descriptive statistics, business.industry, Treatment outcome, Disease progression, Medical imaging, medicine, Medical physics, Neurology (clinical), business, Health Outcome Measures
Abstract

Increasing recognition of the symptom burden and functional limitations among primary brain tumor (PBT) patients has led to proposing clinical outcomes assessments as an additional measure of a treatment’s effectiveness. The RANO-PRO Collaborative recommended core symptoms for evaluation in clinical care and research for malignant glioma are weakness, walking, seizures, communication, memory, and treatment-specific symptoms. We evaluated these symptoms using the MDASI-Brain Tumor (BT) in the PBT patient sample of the NCI-NOB Natural History Study, in relation to disease progression, by descriptive statistics, and independent- and paired-samples t-tests. The sample included 434 PBT patients (59% male, median age=50 (18–83), 82% white, 43% with a prior recurrence). In the 60% with a malignant glioma, weakness, walking, seizures, difficulty remembering, and fatigue were significantly worse in the group with progression at time of imaging compared to the group with stable disease (p< 0.05). In a subset of 114 patients with progression after study entry, reported severity in all symptoms (except seizures) significantly worsened from study entry to time of progression (-1.7< mean difference< -0.1, p< 0.02, 0.3< r< 0.5). Walking, weakness, difficulty remembering, and fatigue each had a difference greater than 1-point, the minimally important difference for MDASI-BT. No one core symptom accounted for the severity change; each was reported by 17%-35% of patients as their largest change in severity. Utilizing the symptom with the largest change increased the magnitude of the worsening and its effect size (mean difference=-2.9, r=0.5). The analysis was repeated in the larger PBT sample with similar statistical findings but with smaller mean differences. RANO-PRO Collaborative core symptoms were shown to worsen at time of progression on imaging, highlighting the importance of continual symptom assessment and validating this core symptom group. Further analysis will focus on degree of change with each core symptom and validation in other datasets.

Published
2019

19. AB044. P-12. Phase 1 study of hepatic arterial infusion (HAI) therapy with floxuridine (FUDR) combined with systemic gemcitabine and oxaliplatin in patients with locally advanced intrahepatic cholangiocarcinoma (ICC)

Author

Andrea Wang-Gillam, Kathryn J. Fowler, William G. Hawkins, Benjamin R. Tan, Chet W. Hammill, Kian-Huat Lim, Manik Amin, Patrick M. Grierson, Ashley Morton, Aabha Oza, M.B. Majella Doyle, Christine Cordova, Katrina S. Pedersen, William C. Chapman, and Ryan C. Fields

Subjects
medicine.medical_specialty, business.industry, Locally advanced, Gastroenterology, Gemcitabine, Oxaliplatin, Hepatic arterial infusion, Floxuridine, Internal medicine, Poster Abstracts, medicine, In patient, business, Intrahepatic Cholangiocarcinoma, medicine.drug
Abstract

BACKGROUND: The standard of care for unresectable intrahepatic cholangiocarcinoma (ICC) is palliative systemic chemotherapy with cisplatin and gemcitabine. The use of hepatic arterial infusion (HAI) floxuridine (FUDR) with systemic chemotherapy may improve outcomes. We conducted a phase 1 study of HAI FUDR with systemic gemcitabine and oxaliplatin. METHODS: We enrolled patients in three cohorts: FUDR 0.16 mg/kg/day ×14 days (Cohort 1), FUDR 0.12 mg/kg/day ×14 days with gemcitabine 1,000 mg/m(2) on days 1, 8, 15 (Cohort 2), and FUDR 0.10 mg/kg/day ×14 days with gemcitabine 800 mg/m(2) days 1, 15 and oxaliplatin 85 mg/m(2) days 1, 15 (Cohort 3). The primary endpoint was the recommended phase 2 dose (RP2D). Dose limiting toxicities (DLTs) were assessed during cycle 1. Secondary objectives were response rate and survival. RESULTS: We enrolled 24 patients, 6 male, age range 42–81 years (median 64). No DLTs were observed in Cohort 1. In Cohort 2, the addition of gemcitabine 1,000 mg/m(2) days 1, 8, 15 resulted in grade 3 LFT elevation in 2 patients; for subsequent patients, the gemcitabine dose was reduced to 800 mg/m(2). No DLT were observed in Cohort 3. Most patients experienced stable disease (SD) or partial response (PR). Conversion to resectable disease occurred in all cohorts. CONCLUSIONS: Administration of FUDR via HAI pump in combination with systemic gemcitabine and oxaliplatin is well-tolerated in patients with unresectable cholangiocarcinoma. Preliminary analysis suggests a high rate of response and disease control, with some patients proceeding to resection. Based on Cohort 3, the RP2D is FUDR 0.10 mg/kg/day ×14 days, with gemcitabine 800 mg/m(2) days 1, 15 and oxaliplatin 85 mg/m(2) days 1, 15 for future studies. Future studies of this promising regimen will utilize this dosing schedule.

Published
2019

20. 18F-FDG PET-CT and trephine biopsy assessment of bone marrow involvement in lymphoma

Author

Metin Ozdemirli, Samer Nassif, Christine Cordova, Giuseppe Esposito, Hongkun Wang, Bruce D. Cheson, Elizabeth M. Hill, and Chaitra S. Ujjani

Subjects
medicine.medical_specialty, medicine.diagnostic_test, business.industry, Follicular lymphoma, Retrospective cohort study, Hematology, medicine.disease, 030218 nuclear medicine & medical imaging, Lymphoma, 03 medical and health sciences, 0302 clinical medicine, Trephine biopsy, medicine.anatomical_structure, immune system diseases, hemic and lymphatic diseases, 030220 oncology & carcinogenesis, Biopsy, medicine, Radiology, Bone marrow, Stage (cooking), Young adult, business
Abstract

The ability of positron emission tomography-computerized tomography (PET-CT) to accurately detect bone marrow involvement (BMI) has been suggested in Hodgkin lymphoma (HL) and diffuse large B-cell lymphoma (DLBCL), but its abilities in other histologies is less established. The aim of this retrospective study was to confirm the role of PET-CT in detecting BMI in DLBCL and HL, and to explore its usefulness in other subtypes. Of the 149 newly diagnosed patients, common subtypes included DLBCL, follicular lymphoma (FL) and HL. In DLBCL, the sensitivity and specificity of PET-CT at diagnosis were 75% and 92%. In FL, the sensitivity and specificity of PET-CT were 67% and 85% at diagnosis, and 73% and 89% at relapse. In HL, the sensitivity and specificity were 100% and 74%. PET-CT was able to detect BMI in patients with negative biopsies. Most of the patients in which PET-CT failed to identify BMI were already advanced stage by imaging. In this analysis, PET-CT was highly accurate for detecting BMI at diagnosis in DLBCL and HL and highly specific in FL at diagnosis and relapse. Results also suggested the diagnostic advantage of PET-CT over bone marrow biopsy in detecting BMI. Prospective evaluation is necessary and may eliminate biopsies in future patients.

Published
2016

21. Osimertinib Dose Escalation Induces Regression of Progressive EGFR T790M–Mutant Leptomeningeal Lung Adenocarcinoma

Author

Abraham Chachoua, Joshua S. Silverman, Matija Snuderl, Douglas Kondziolka, Rajan Jain, Andrew S. Chi, Timothy M. Shepherd, and Christine Cordova

Subjects
0301 basic medicine, Pulmonary and Respiratory Medicine, Oncology, medicine.medical_specialty, Lung, business.industry, Mutant, EGFR T790M, medicine.disease, 03 medical and health sciences, ErbB Receptors, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Internal medicine, Dose escalation, Medicine, Adenocarcinoma, Osimertinib, business
Published
2017

22. Abstract A65: Longitudinal detection of TERT-mutant plasma cell-free circulating tumor DNA in newly diagnosed glioblastoma patients

Author

Amie Patel, David Zagzag, Broderick Corless, John G. Golfinos, Malcolm Delara, George Karlin-Neumann, Christine Cordova, Jennifer M. Wiggins, Minerva Utate, Andrew S. Chi, Zacharia Sawaged, Jessica Schafrick, Sylvia Kurz, Matija Snuderl, Rajan Jain, David Polsky, Dimitris G. Placantonakis, Joshua S. Silverman, and Mahrukh M. Syeda

Subjects
Oncology, Cancer Research, medicine.medical_specialty, business.industry, Mutant, Newly diagnosed, Plasma cell, medicine.disease, medicine.anatomical_structure, Circulating tumor DNA, Internal medicine, medicine, Digital polymerase chain reaction, business, Pseudoprogression, Whole blood, Glioblastoma
Abstract

Introduction: Liquid biopsies, especially plasma cell-free circulating tumor DNA (ctDNA), provide a potential opportunity to be a noninvasive biomarker for the diagnosis and monitoring of glioblastoma (GBM) patients. Previously, we detected TERT promoter hotspot mutations (C228T and C250T) in ctDNA of IDH wild-type (IDHwt) TERT promoter mutant GBM patients with 100% specificity using mutation-specific droplet digital PCR (ddPCR) assays. Here, we examine the association between mutant TERT ctDNA levels and clinical outcomes in newly diagnosed GBM patients undergoing chemoradiation. Methods: We analyzed 76 serially collected plasma samples from 17 patients with suspected IDHwt GBM based on MRI before surgery. Twenty mL of whole blood was collected in EDTA tubes at predetermined times: pre- and postoperatively, at the end of chemoradiation, and 1, 3, and 6 months from the end of chemoradiation. TERT promoter mutations C228T or C250T were identified in FFPE tumor samples using ddPCR assays specific for these mutations. Plasma samples were analyzed for the patient’s tumor TERT mutation using the ddPCR assays. The analytically validated thresholds for positive ctDNA detection were 1.5 and 1.7 copies/mL for C228T and C250T, respectively. Results: Sixteen of 17 (94%) IDHwt tumors had TERT mutations (10 C228T, 6 C250T) with MGMT methylated, unmethylated, or unknown status in 10, 5, and 1, respectively. Fourteen of the 16 patients (87.5%) had detectable mutant ctDNA at one or more time points (range 1.66 to 22.13 copies/mL). Of the 2 patients with undetectable ctDNA, one had diffuse and non-avidly enhancing disease and the other only had pre/postop plasma samples collected. Six patients had detectable ctDNA preop, and most had a dominant rim-enhancing mass with additional nonenhancing or enhancing lesion(s). Ten patients had detectable ctDNA up to 4 days postop, half of whom had undergone gross total resection. For 3 of 5 patients for whom there was a question of pseudoprogression versus true progression, ctDNA kinetics matched the clinical outcome. One patient with MGMT unmethylated multifocal GBM achieved ctDNA zeroconversion at 6 months post radiation (RT), and did not progress for another five months. Another patient was negative at all time points until their 3-month post RT follow-up, at which time they developed a recurrence. Another patient achieved zeroconversion at the end of RT but developed a borderline positive ctDNA at 6 months after RT, 2 months before documented radiographic progression. Conclusions: In this pilot, prospective ctDNA monitoring study of IDHwt GBM, TERT mutant ctDNA was detected at one or more time points in the majority of patients. ctDNA kinetics were associated with clinical outcomes for some patients. These data suggest that additional, larger studies could refine how ctDNA monitoring may be used to enhance the clinical management of IDHwt GBM patients. Citation Format: Christine Cordova, Mahrukh M. Syeda, Broderick Corless, Jennifer M. Wiggins, Amie Patel, Sylvia C. Kurz, Malcolm Delara, Zacharia Sawaged, Minerva Utate, Dimitris Placantonakis, John Golfinos, Jessica Schafrick, Joshua S. Silverman, Rajan Jain, Matija Snuderl, David Zagzag, George Karlin-Neumann, David Polsky, Andrew S. Chi. Longitudinal detection of TERT-mutant plasma cell-free circulating tumor DNA in newly diagnosed glioblastoma patients [abstract]. In: Proceedings of the AACR Special Conference on Advances in Liquid Biopsies; Jan 13-16, 2020; Miami, FL. Philadelphia (PA): AACR; Clin Cancer Res 2020;26(11_Suppl):Abstract nr A65.

Published
2020

23. QOLP-36. THE IMPORTANCE OF SLEEP DISTURBANCE IN PRIMARY BRAIN TUMOR (PBT) PATIENTS: CLINICAL CHARACTERISTICS & CO-OCCURRENCE WITH TUMOR-RELATED & PSYCHOLOGICAL SYMPTOMS

Author

Dorela D. Shuboni-Mulligan, Marta Penas-Prado, Elizabeth Vera, Amanda King, Brett Theeler, Jennifer Reyes, Jing Wu, Carrie Gartland, Sonja Crandon, Christine Cordova, Kathleen Wall, Ramya Antony, Lisa Boris, Eric Burton, Nicole Leggiero, Ewa Grajkowska, Mark R. Gilbert, Terri Armstrong, Orwa Aboud, Christine Bryla, and Christine Siegel

Subjects
Oncology, Cancer Research, medicine.medical_specialty, Sleep disorder, business.industry, Brain tumor, medicine.disease, Dyssomnias, Quality of Life and Palliative Care, Quality of life, Tumor progression, Internal medicine, Glioma, medicine, Anxiety, Neurology (clinical), medicine.symptom, business, Psychopathology
Abstract

Sleep disturbance (SD) is a common symptom reported by PBT patients and research has demonstrated a link between sleep and stress circadian pathways. SD can impact perceived severity of other symptoms and development of psychopathology. This study explored the prevalence of moderate-severe SD in PBT patients, identifying associated clinical characteristics and co-occurrence with other tumor-related and psychological symptoms. Demographic, clinical characteristics, MDASI-Brain Tumor, and PROMIS Depression and Anxiety Short-Forms were collected at study entry. Descriptive statistics, Chi-square tests, and independent t-tests were used to report results. The sample included 424 patients (58% male, 81% Caucasian) with a median age of 49 years (range 18–81) and 58% with high-grade gliomas. Most had received treatment with surgery, radiation or chemotherapy prior to study entry, with 44% reporting a past recurrence. Moderate-severe SD (³ 5 on a 0–10 scale) was reported in 19% of patients and was associated with younger age (mean difference = 5 years), poor KPS (OR 2.2), current steroid use (OR 2.4), and tumor progression on MRI (OR 2). Those with moderate-severe SD had a higher overall symptom burden (mean difference = 2.3) and reported more moderate-severe symptoms (8 vs. 2). Patients reporting moderate-severe SD also reported higher severity in affective and cognitive symptom domains and mood-interference, with fatigue (72%), drowsiness (59%), and distress (56%) the most frequently co-occurring symptoms. Patients with moderate-severe SD also had increased prevalence of moderate-severe anxiety (32%) and depression (23%), compared to 10% in those without SD. PBT patients with moderate-severe SD are more symptomatic and have higher incidence of mood disturbance, suggesting a key role for sleep in the development of tumor-related and psychological symptoms. Future work delineating specific pathways involving sleep disturbance and co-occurring symptoms will be foundational for designing targeted sleep interventions to improve symptom burden and quality of life.

Published
2019

24. ACTR-62. PHASE I TRIAL OF TG02 PLUS DOSE-DENSE OR METRONOMIC TEMOZOLOMIDE FOR RECURRENT HIGH-GRADE ASTROCYTOMA IN ADULTS

Author

Yu-Ting Su, Elizabeth Vera, Tito R. Mendoza, Mark R. Gilbert, Christine Cordova, Marta Penas-Prado, Orwa Aboud, Tracy Lawhon, Christine Bryla, Christine Siegel, Lisa Boris, Jing Wu, Ying Yuan, Ann McCoy, Nancy Garren, Brett Theeler, Terri Armstrong, Ramya Antony, and Ewa Grajkowska

Subjects
Oncology, Cancer Research, medicine.medical_specialty, Temozolomide, business.industry, Astrocytoma, Neutropenia, medicine.disease, Diarrhea, Adult Clinical Trials - Non-Immunologic, Internal medicine, Maximum tolerated dose, Glioma, medicine, Combined Modality Therapy, Neurology (clinical), medicine.symptom, business, Febrile neutropenia, medicine.drug
Abstract

BACKGROUND Therapies targeting multiple survival pathways are desirable for high-grade gliomas. TG02 (Zotiraciclib), a CDK9 inhibitor, regulates transcription and metabolism of tumor cells and synergizes with temozolomide. A phase I/II trial was launched to test the TG02/temozolomide combined treatment in recurrent high-grade astrocytomas. Phase I results are reported here. METHODS Adults with recurrent high-grade astrocytoma, KPS≥60, adequate organ function, < 2 prior relapses were enrolled. Primary endpoint was dose limiting toxicity (DLT) in cycle1 in each arm. Bayesian optimal interval design was employed to determine the maximum tolerated dose (MTD) with the target DLT rate of 35% and the toxicity profile of the combination of TG02 (starting dose 200mg orally on days1,12,15, and 26) and temozolomide, either as a dose-dense (DD; 125mg/m2/d, 7on/7off, Arm1) or metronomic (MN; 50mg/m2/d, Arm2) dosing schedule on a 28-day cycle. RESULTS Thirty-eight patients were evaluable; median age 50.7, KPS 90. Of 18 evaluable patients in Arm1, at TG02 dose-level 200mg, 1/6 had a DLT: Gr3 diarrhea; at dose-level 250mg, 3/12 had DLTs: Gr4 neutropenia for over 5 days, Gr3 elevated ALT, and Gr3 fatigue. Of 20 evaluable patients in Arm2, at TG02 dose-level 200mg, 1/6 had a DLT: recurrent Gr3 neutropenia; at dose-level 250mg, 5/12 had a DLT: Gr3 elevated ALT, Gr3 fatigue, and Gr4 neutropenia; at dose-level 300mg,1 of 2 had a DLT: Gr4 febrile neutropenia, Gr4 elevated ALT, Gr4 elevated AST. TG02 dose-level of 250mg was declared as the MTD in both Arms. Using the MDASI-BT, patients with high symptom burden had increased symptoms during cycle1 but became stable as they continued treatment. CONCLUSION The combination of TG02 at the MTD of 250mg with DD or MN temozolomide was tolerated. Cohort expansion continues at the MTD in both arms. Objective responses have been observed, suggesting activity of this regimen and supporting continued investigation.

Published
2019

25. PATH-42. DETECTION OF TERT MUTATIONS IN CELL-FREE CIRCULATING TUMOR DNA (ctDNA) OF GLIOBLASTOMA PATIENTS USING DROPLET DIGITAL PCR

Author

Rajan Jain, Jessica Schafrick, Amie Patel, Broderick Corless, Mahrukh M. Syeda, David Polsky, Sylvia Eisele, Donato Pacione, George Karlin-Neumann, Timothy M. Shepherd, Dimitris G. Placantonakis, Malcolm Delara, Jafar J. Jafar, Girish M. Fatterpekar, Christine Cordova, Joshua Silverman, David Zagzag, John G. Golfinos, Matija Snuderl, Yongzhao Shao, and Andrew S. Chi

Subjects
Cancer Research, Mutation, Chemistry, medicine.disease, medicine.disease_cause, Molecular biology, Abstracts, Oncology, Circulating tumor DNA, Glioma, medicine, Digital polymerase chain reaction, Neurology (clinical), Glioblastoma
Published
2017

26. HOUT-04. ASSOCIATION OF COMMON PATIENT-REPORTED IMMUNOTHERAPY SYMPTOMATIC SIDE EFFECTS AND PSEUDOPROGRESSION IN PATIENTS WITH PRIMARY CENTRAL NERVOUS SYSTEM (CNS) TUMORS

Author

Jing Wu, Christine Cordova, Nicole Leggiero, Sonja Crandon, Lisa Boris, Yamini Vyas, Ramya Antony, Orwa Aboud, Terri Armstrong, Jennifer Reyes, Marta Penas-Prado, Kathleen Wall, Eric Burton, Christine Bryla, Elizabeth Vera, Brett Theeler, Christine Siegel, and Mark R. Gilbert

Subjects
Medulloblastoma, Oncology, Cancer Research, medicine.medical_specialty, medicine.diagnostic_test, business.industry, medicine.medical_treatment, Spinal Cord Neoplasm, Central nervous system, Magnetic resonance imaging, Immunotherapy, medicine.disease, Health Outcome Measures, medicine.anatomical_structure, Internal medicine, medicine, In patient, Neurology (clinical), CNS TUMORS, business, Pseudoprogression
Abstract

BACKGROUND Immunotherapy agents have unique symptomatic side effects; patient-reported outcomes (PROs) can help to characterize the benefits and burdens associated with therapy. Common immunotherapy-associated symptoms include pain, fatigue, shortness of breath, and irregular bowel patterns. The purpose of this study was to assess the severity of symptoms and their association with imaging changes in CNS tumor patients undergoing single agent or combination treatment with immune checkpoint inhibitors (ICIs). METHODS Patients completed the MDASI-BT or MDASI-SP at baseline and longitudinally (every 8 weeks), and results through cycle 4 are reported. Neuro-imaging was categorized as stable, possible ICI-related pseudoprogression, or progression by clinical team review. RESULTS 29 Brain Tumor (BT) and 6 Spinal Tumor patients participated; the majority of which were male (62%) and white (91%), ranging 24-74yo (mean = 46). Glioblastoma was the most common diagnosis (31%) followed by medulloblastoma (16%), with 56% of patients having greater than 2 recurrences prior to the study. At baseline, both brain and spine tumor patients reported moderate to severe fatigue (Brain=4, Spine=6) and pain (Spine=5) with shortness of breath and pain worsening over time. BT patients with pseudoprogression were more likely to report increased fatigue (87%) and pain (63%) compared to those with stable (29%) or true progressive (17%) disease on imaging. BT patients with pseudoprogression also reported worsening of cognitive (43%) and neurologic (57%) symptom burden. CONCLUSIONS In contrast to the common pseudoprogression after chemoradiation, treatment-specific symptoms were worse with ICI-related pseudoprogression by MRI where an immunologic reaction was the likely cause of the imaging worsening. These results suggest that commonly used symptom and functional assessments to distinguish true progression from pseudoprogression may not be helpful with immunotherapy. Additional studies including those with pathologic confirmation of progression or pseudoprogression combined with outcomes measures are needed to develop more accurate determinations of disease status.

Published
2019

27. RARE-10. IMPROVING CARE FOR ADULT PATIENTS WITH RARE CNS TUMORS: THE NATIONAL CANCER INSTITUTE-COMPREHENSIVE ONCOLOGY NETWORK EVALUATING RARE CNS TUMORS (NCI-CONNECT) PROGRAM AND CLINIC

Author

Mark R. Gilbert, Orwa Aboud, Jing Wu, Liz Vera, Christine Bryla, Tracy Ani, Christine Cordova, Sylvia Stearn, Nicole Leggiero, Terri Armstrong, Alvina Acquaye, Sonja Crandon, Margarita Raygada, Christine Siegel, Lisa Boris, Kristen Stevens-Brown, Marta Penas-Prado, Kathleen Wall, Brett Theeler, Eric M. Burton, Ramya Antony, and Jennifer Reyes

Subjects
Oncology, Cancer Research, medicine.medical_specialty, Adult patients, Rare Tumors, business.industry, Cancer, medicine.disease, Internal medicine, medicine, Neurology (clinical), CNS TUMORS, business
Abstract

BACKGROUND While rare cancers have provided insight into mechanisms of tumorigenesis and familial syndromes, patients with rare CNS tumors and providers face unique challenges, including diagnostic delays and errors, lack of standardized approaches to care/treatment, and limited social support. Scant data exists on the natural history, health status, and impact of these tumors on life quality. This report describes an innovative clinic designed to fulfill the mission of the NCI-CONNECT program: To advance our understanding and to improve approaches to care and treatment of rare CNS tumors. METHODS A specialized weekly clinic was established incorporating routine comprehensive analysis of tumor tissue, genetic counseling with individual pedigree assessment, group meetings with a health and wellness counselor and comprehensive clinical evaluation. Patients and caregivers both participated. Descriptive statistics report of NCI-CONNECT clinic patients from January 1-May 8, 2019 are presented. RESULTS 33 patients and 32 caregivers have participated to date, representing 6 of the 12 rare tumors studied in NCI-CONNECT: 19 ependymomas, 9 oligodendrogliomas, 2 PXAs, 1 papillary pineal tumor, 1 medulloblastoma, 1 gliosarcoma. The median time from receiving pathologic material to appointment was 22 days, with analysis including methylation and next generation sequencing testing. All 33 patients underwent genetic counseling, most (n=26) having at least ≥ 2 first- or second-degree relatives diagnosed with cancer (Germline mutations/genetic predisposition testing underway). 44 patients attended (33 with 8 repeat visits) the health and wellness group sessions, with education on coping/wellness techniques included. During this same period, 7 patients participated in a rare CNS basket trial using nivolumab. CONCLUSIONS We have developed an innovative clinic model to interrogate rare CNS tumors for therapeutic targets, understand individual risk, how the patient feels and functions and conduct clinical trials. This effort has the potential to accelerate our understanding of these rare tumors and provide guidance on care.

Published
2019

28. NIMG-32. CHALLENGES OF IMAGING INTERPRETATION TO PREDICT OLIGODENDROGLIOMA GRADE

Author

Elizabeth Vera, Martha Quezado, Ramya Antony, Christine Bryla, Lisa Boris, Nicole Leggiero, Jing Wu, Marta Penas-Prado, Brett Theeler, Mark R. Gilbert, Christine Siegel, Kathleen Wall, Orwa Aboud, Sonja Crandon, Christine Cordova, Eric Burton, Terri Armstrong, Jennifer Reyes, and Ritu Shah

Subjects
Cancer Research, medicine.medical_specialty, medicine.diagnostic_test, business.industry, Magnetic resonance imaging, medicine.disease, Oncology, Biopsy, Neuro-Imaging, Radiology Specialty, medicine, Medical imaging, Neurology (clinical), Radiology, Oligodendroglioma, business, Imaging interpretation, Diagnostic radiologic examination
Abstract

BACKGROUND A recent report examining 75 Oligodendrogliomas indicated that specific imaging features may help predict grading and guide target selection for biopsy when resection is not possible. This report attempted to validate these findings in a separate sample and evaluate interrater reliability. METHODS Two Neuro-Oncologists, blinded to radiology report and grading reviewed diagnostic pre-radiation MRI. Imaging features and reviewer interpretations were evaluated included contrast enhancement, necrosis, calcification, and restricted diffusion; examiner concordance is reported. RESULTS Sixty-two patients with diagnosis of Oligodendroglioma (50 WHO grade II, 12 WHO grade III); 54 were molecularly confirmed as IDH-mutant/1p19q co-deleted based on the NOB Natural History Study. Four patients (grade III) were excluded due to lack of imaging studies. Among 58 evaluable patients, their location was frontal (n=32), temporal (n=14), parietal (n=4), occipital (n=1), and multi-lobe (n=11). Extent of resection: gross total 9, subtotal 36, biopsy 17. Partial to extensive contrast enhancement was present in 18/58 patients (6 grade II, 33%; 12 grade III, 67%); Kappa interrater agreement k= 0.37 on grade II and k=0.50 on grade III; extensive enhancement was present in 4/58 (all grade III), k= 0.70. Necrosis noted in 7/58 patients (all grade III), k=0.61. Calcification noted in 7/17 patients reviewed (all grade III), k=1.0; restriction noted in only 2/39 patients reviewed (all grade III), k=1.0. CONCLUSIONS THE presence of extensive enhancement, necrosis, calcification and restricted diffusion were only present in grade III with substantial agreement between readers, but there was lower agreement for partial enhancement. Image reviewers commented on the variability of enhancement intensity in normal structures between scans, likely contributing to this poor concordance. Tumor areas with extensive enhancement and/or necrosis are associated with higher grade and can guide biopsy if resection is not feasible. Discrepancies in imaging interpretation may be ameliorated by implementing a standardized imaging protocol.

Published
2019

29. Phase I trial of TG02 plus dose-dense or metronomic temozolomide for recurrent anaplastic astrocytoma and glioblastoma in adults

Author

Marta Penas-Prado, Tracy Lawhon, Orwa Aboud, Jing Wu, Yu-Ting Su, Christine Bryla, Christine Siegel, Ramya Antony, Terri Armstrong, Ying Yuan, Ann McCoy, Nancy Garren, Brett Theeler, Ewa Grajkowska, Lisa Boris, Christine Cordova, and Mark R. Gilbert

Subjects
Cancer Research, Temozolomide, business.industry, medicine.disease, Survival pathways, 03 medical and health sciences, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, medicine, Cancer research, business, 030215 immunology, Anaplastic astrocytoma, medicine.drug, Glioblastoma
Abstract

2031 Background: Therapies targeting multiple survival pathways simultaneously may be more effective for high-grade gliomas, a disease highly resistant to treatment. Our preclinical studies have shown potent anti-glioma effects of TG02 and synergy with temozolomide (TMZ) through modulation of transcription and cellular metabolism. A phase I/II trial was launched to test the combination of TG02 and TMZ in recurrent malignant gliomas and herein we report the phase I results. Methods: Adults with recurrent high-grade astrocytoma, KPS ≥ 60, normal organ function, ≤ 2 prior relapses were enrolled. The primary endpoint was dose limiting toxicity (DLT) from the start of the combined treatment to 4 weeks after in each arm. Bayesian optimal interval (BOIN) design was employed to determine the maximum tolerated dose (MTD) with the target DLT rate of 35% and the toxicity profile of the combination of TG02 (starting dose 200mg orally on days 1, 12, 15, and 26) and TMZ, either as a dose-dense (DD; 125mg/m2/d, 7on/7off, Arm 1) or metronomic (MN; 50mg/m2/d, Arm 2) dosing schedule on a 28-day cycle. Results: Forty patients were enrolled; 38 were evaluable; 70% male; overall median age 50.7; median KPS 90. Of 18 evaluable patients in Arm 1 (DD TMZ), at TG02 dose level 200mg, 1/6 had a DLT: Gr3 diarrhea. At TG02 dose level 250mg, 3/12 had DLTs: Gr4 neutropenia for over 5 days, Gr3 elevated ALT, and Gr3 fatigue. Of 20 evaluable patients in Arm 2 (MN TMZ), at TG02 dose level 200mg, 1/6 had a DLT: recurrent Gr3 neutropenia. At TG02 dose level 250mg, 5/12 had a DLT: Gr3 elevated ALT, Gr3 fatigue, and Gr4 neutropenia. At TG02 dose level 300mg,1 out of 2 had a DLT: Gr4 febrile neutropenia, Gr4 elevated ALT, Gr4 elevated AST, which resulted in hospitalization. Therefore, the TG02 dose level of 250mg was declared as the MTD in both Arm 1 and Arm 2. Conclusions: The combination of TG02 at the MTD of 250mg with DD or MN TMZ has a tolerable toxicity profile. Cohort expansion continues at the MTD in both arms to conduct pharmacokinetics and pharmacogenetics to better elucidate the toxicity profile. Objective responses have been observed, suggesting activity of this regimen and supporting continued investigation with the phase II randomized component. Clinical trial information: NCT02942264.

Published
2019

30. Plasma cell-free circulating tumor DNA (ctDNA) detection in longitudinally followed glioblastoma patients using TERT promoter mutation-specific droplet digital PCR assays

Author

Amie Patel, Mahrukh M. Syeda, Broderick Corless, Sylvia Kurz, Joshua S. Silverman, Matija Snuderl, George Karlin-Neumann, Rajan Jain, Zacharia Sawaged, John G. Golfinos, Jessica Schafrick, Minerva Utate, Andrew S. Chi, David Polsky, Dimitris G. Placantonakis, Malcolm Delara, Christine Cordova, Jennifer M. Wiggins, David Zagzag, and Yongzhao Shao

Subjects
Cancer Research, business.industry, Less invasive, Plasma cell, medicine.disease, Tert promoter, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, Oncology, Circulating tumor DNA, 030220 oncology & carcinogenesis, Cancer research, Medicine, Digital polymerase chain reaction, Tert promoter mutation, business, 030215 immunology, Glioblastoma
Abstract

2026 Background: There is a critical need for more specific and less invasive diagnostic and pharmacodynamic biomarkers in glioblastoma (GBM) patients (pts). Previously, we detected TERT promoter hotspot mutations (C228T and C250T) in the ctDNA of IDH wildtype ( IDHwt) TERT promoter mutant GBM pts with 100% specificity using mutation-specific droplet digital PCR (ddPCR) assays. Here, we explored the dynamics and clinical associations of mutant TERT ctDNA levels in GBM pts undergoing therapy. Methods: We examined 14 pts with suspected IDHwt GBM based on preoperative MRI. Plasma was isolated and frozen from ~15 mL whole blood samples collected pre- and post-op, at end of radiation (RT), and 1, 3, and 6 m after end of RT. TERT promoter mutations were identified in FFPE tumor samples using ddPCR assays for C228T/C250T. Plasma samples were analyzed using ddPCR assays specific for the corresponding tumor mutation. The validated thresholds for positive detection were 1.5 (C228T) and 1.7 copies/mL (C250T). Results: 13/14 (92.9%) IDHwt tumors had TERT mutations (7 C228T and 6 C250T). Six of these 13 (46%) pts had positive plasma TERT ctDNA preop (4 C228T, 2 C250T). The mean cross sectional area of enhancing disease at presentation for positive or negative preop mutant ctDNA was similar. All 4 pts with multiple contrast enhancing lesions had positive preop mutant ctDNA. 2 pts who were negative initially developed detectable mutant ctDNA preceding progression. 3/4 pts with equivocal radiographic pseudoprogression had ctDNA dynamics that correlated with eventual clinical outcome. One patient with unresectable GBM had declining mutant ctDNA in later collections during clinical stability. Conclusions: We detected plasma TERT ctDNA in 46% of TERT mutant GBM pts before surgery, and in 100% of pts with multiple contrast enhancing lesions. TERT mutant ctDNA levels correlated with pseudoprogression or true disease progression and predicted progression before MRI. These data suggest that larger studies to test circulating cell-free TERT mutation as a diagnostic and pharmacodynamic biomarker in GBM are warranted.

Published
2019

31. ATIM-01. A PHASE II, OPEN-LABEL, SINGLE ARM, MULTICENTER STUDY OF AVELUMAB WITH HYPOFRACTIONATED RE-IRRADIATION IN ADULT SUBJECTS WITH TRANSFORMED IDH MUTANT GLIOBLASTOMA

Author

Donato Pacione, Amie Patel, Timothy F. Cloughesy, Daniel P. Cahill, Rajan Jain, Douglas Kondziolka, Jessica Schafrick, Dimitris G. Placantonakis, Timothy M. Shepherd, Malcolm Delara, Girish M. Fatterpekar, Tracy T. Batchelor, David Zagzag, Sylvia Eisele, Isabel Arrillaga-Romany, Christine Cordova, Joshua Silverman, John G. Golfinos, Matija Snuderl, Sunita Latchman, Jennie Taylor, and Andrew S. Chi

Subjects
Cancer Research, Carmustine, Pathology, medicine.medical_specialty, Temozolomide, business.industry, Salvage therapy, Phases of clinical research, medicine.disease, Chemotherapy regimen, Abstracts, Isocitrate dehydrogenase, Oncology, Glioma, Cancer research, medicine, Neurology (clinical), Progression-free survival, business, medicine.drug
Published
2017

32. Task-Related Effects on the Temporal and Spatial Dynamics of Resting-State Functional Connectivity in the Default Network

Author

Yulin Ge, Christine Cordova, Douglas Kondziolka, Daniel Orringer, Rajan Jain, and Guillaume Madelin

Subjects
Cingulate cortex, Adult, Male, Elementary cognitive task, Cerebellum, Computer science, Nerve net, lcsh:Medicine, Amygdala, 050105 experimental psychology, 03 medical and health sciences, 0302 clinical medicine, Cognition, Task Performance and Analysis, medicine, Humans, 0501 psychology and cognitive sciences, Neuroscience/Theoretical Neuroscience, Least-Squares Analysis, lcsh:Science, Default mode network, Neuroscience/Cognitive Neuroscience, Multidisciplinary, Resting state fMRI, Functional connectivity, 05 social sciences, lcsh:R, medicine.anatomical_structure, Posterior cingulate, lcsh:Q, Female, Nerve Net, Neuroscience, 030217 neurology & neurosurgery, Research Article
Abstract

Recent evidence points to two potentially fundamental aspects of the default network (DN), which have been relatively understudied. One is the temporal nature of the functional interactions among nodes of the network in the resting-state, usually assumed to be static. The second is possible influences of previous brain states on the spatial patterns (i.e., the brain regions involved) of functional connectivity (FC) in the DN at rest. The goal of the current study was to investigate modulations in both the spatial and temporal domains. We compared the resting-state FC of the DN in two runs that were separated by a 45 minute interval containing cognitive task execution. We used partial least squares (PLS), which allowed us to identify FC spatiotemporal patterns in the two runs and to determine differences between them. Our results revealed two primary modes of FC, assessed using a posterior cingulate seed – a robust correlation among DN regions that is stable both spatially and temporally, and a second pattern that is reduced in spatial extent and more variable temporally after cognitive tasks, showing switching between connectivity with certain DN regions and connectivity with other areas, including some task-related regions. Therefore, the DN seems to exhibit two simultaneous FC dynamics at rest. The first is spatially invariant and insensitive to previous brain states, suggesting that the DN maintains some temporally stable functional connections. The second dynamic is more variable and is seen more strongly when the resting-state follows a period of task execution, suggesting an after-effect of the cognitive activity engaged during task that carries over into resting-state periods.

Published
2010

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