Your search keyword '"Nicholas Butowski"' showing total 74 results

1. Targeting the IL4 receptor with MDNA55 in patients with recurrent glioblastoma: Results of a phase IIb trial

Author

John H Sampson, Achal Singh Achrol, Manish K Aghi, Krystof Bankiewicz, Martin Bexon, Steven Brem, Andrew Brenner, Chandtip Chandhasin, Sajeel Chowdhary, Melissa Coello, Benjamin M Ellingson, John R Floyd, Seunggu Han, Santosh Kesari, Yael Mardor, Fahar Merchant, Nina Merchant, Dina Randazzo, Michael Vogelbaum, Frank Vrionis, Eva Wembacher-Schroeder, Miroslaw Zabek, and Nicholas Butowski

Subjects

Cancer Research, Oncology, Neurology (clinical)

Abstract

BackgroundMDNA55 is an interleukin 4 receptor (IL4R)-targeting toxin in development for recurrent GBM, a universally fatal disease. IL4R is overexpressed in GBM as well as cells of the tumor microenvironment. High expression of IL4R is associated with poor clinical outcomes.MethodsMDNA55-05 is an open-label, single-arm phase IIb study of MDNA55 in recurrent GBM (rGBM) patients with an aggressive form of GBM (de novo GBM, IDH wild-type, and nonresectable at recurrence) on their 1st or 2nd recurrence. MDNA55 was administered intratumorally as a single dose treatment (dose range of 18 to 240 ug) using convection-enhanced delivery (CED) with up to 4 stereo-tactically placed catheters. It was co-infused with a contrast agent (Gd-DTPA, Magnevist®) to assess distribution in and around the tumor margins. The flow rate of each catheter did not exceed 10μL/min to ensure that the infusion duration did not exceed 48 h. The primary endpoint was mOS, with secondary endpoints determining the effects of IL4R status on mOS and PFS.ResultsMDNA55 showed an acceptable safety profile at doses up to 240 μg. In all evaluable patients (n = 44) mOS was 11.64 months (80% one-sided CI 8.62, 15.02) and OS-12 was 46%. A subgroup (n = 32) consisting of IL4R High and IL4R Low patients treated with high-dose MDNA55 (>180 ug) showed the best benefit with mOS of 15 months, OS-12 of 55%. Based on mRANO criteria, tumor control was observed in 81% (26/32), including those patients who exhibited pseudo-progression (15/26).ConclusionsMDNA55 demonstrated tumor control and promising survival and may benefit rGBM patients when treated at high-dose irrespective of IL4R expression level.Trial Registration: Clinicaltrials.gov NCT02858895.

Published

2023

2. Temozolomide-induced hypermutation is associated with distant recurrence and reduced survival after high-grade transformation of low-grade IDH-mutant gliomas

Author

Annette M. Molinaro, Jennie Taylor, Anny Shai, Joanna J. Phillips, Serah Choi, Stephanie Hilz, Tali Mazor, Mitchel S. Berger, Bruce H Wainer, David A. Solomon, Susan M. Chang, Michael W. McDermott, Nancy Ann Oberheim Bush, Yao Yu, Daphne A. Haas-Kogan, Nicholas Butowski, Chibo Hong, Jennifer Clarke, Michael Wahl, Joseph F. Costello, Javier Villanueva-Meyer, and Matthew R. Grimmer

Subjects

Oncology, Cancer Research, medicine.medical_specialty, tumor mutational burden, Multivariate analysis, medicine.medical_treatment, Oncology and Carcinogenesis, Somatic hypermutation, temozolomide, Disease, Rare Diseases, Recurrence, Clinical Research, Internal medicine, medicine, Humans, Oncology & Carcinogenesis, Cancer, Chemotherapy, low-grade glioma, Temozolomide, Brain Neoplasms, business.industry, Incidence (epidemiology), hypermutation, Distant recurrence, Neurosciences, Brain, Glioma, IDH-mutant, Brain Disorders, Brain Cancer, Radiation therapy, Neoplasm Recurrence, Orphan Drug, Local, Basic and Translational Investigations, Mutation, Neurology (clinical), business, medicine.drug

Abstract

Background Chemotherapy improves overall survival after surgery and radiotherapy for newly diagnosed high-risk IDH-mutant low-grade gliomas (LGGs), but a proportion of patients treated with temozolomide (TMZ) will develop recurrent tumors with TMZ-induced hypermutation. We aimed to determine the prevalence of TMZ-induced hypermutation at recurrence and prognostic implications. Methods We sequenced recurrent tumors from 82 patients with initially low-grade IDH-mutant gliomas who underwent reoperation and correlated hypermutation status with grade at recurrence and subsequent clinical outcomes. Results Hypermutation was associated with high-grade disease at the time of reoperation (OR 12.0 95% CI 2.5-115.5, P = .002) and was identified at transformation in 57% of recurrent LGGs previously exposed to TMZ. After anaplastic (grade III) transformation, hypermutation was associated with shorter survival on univariate and multivariate analysis (HR 3.4, 95% CI 1.2-9.9, P = .024), controlling for tumor grade, subtype, age, and prior radiotherapy. The effect of hypermutation on survival after transformation was validated in an independent, published dataset. Hypermutated (HM) tumors were more likely to develop discontiguous foci of disease in the brain and spine (P = .003). To estimate the overall incidence of high-grade transformation among low-grade IDH-mutant tumors, data from a phase II trial of TMZ for LGG were analyzed. Eight-year transformation-free survival was 53.8% (95% CI 42.8-69.2), and 61% of analyzed transformed cases were HM. Conclusions TMZ-induced hypermutation is a common event in transformed LGG previously treated with TMZ and is associated with worse prognosis and development of discontiguous disease after recurrence. These findings impact tumor classification at recurrence, prognostication, and clinical trial design.

Published

2021

3. CTNI-61. CLINICAL EFFICACY AND PREDICTIVE BIOMARKERS OF ONC201 IN H3K27M-MUTANT DIFFUSE MIDLINE GLIOMA

Author

Abed Rahman Kawakibi, Rohinton Tarapore, Sharon Gardner, Andrew Chi, Sylvia Kurz, Patrick Y Wen, Isabel Arrillaga-Romany, Tracy Batchelor, Nicholas Butowski, Ashley Sumrall, Nicole Shonka, Rebecca Harrison, John DeGroot, Minesh Mehta, Yazmin Odia, Matthew Hall, Doured Daghistani, Timothy Cloughesy, Benjamin Ellingson, Michelle Kim, Yoshie Umemura, Hugh Garton, Andrea Franson, Jonathan Schwartz, Sunjong Li, Rodrigo Cartaxo, Karthik Ravi, Evan Cantor, Jessica Cummings, Alyssa Paul, Dustin Walling, Matthew Dun, Jason Cain, Jiang Li, Mariella Filbin, Lili Zhao, Chandan Kumar-Sinha, Rajen Mody, Arul Chinnaiyan, Ryo Kurokawa, Drew Pratt, Sriram Venneti, Jacques Grill, Cassie Kline, Sabine Mueller, Adam C Resnick, Javad Nazarian, Sebastian Waszak, Joshua E Allen, and Carl Koschmann

Subjects

Cancer Research, Oncology, Neurology (clinical)

Abstract

Patients with H3K27M-mutated diffuse midline glioma (DMG) have no proven effective therapies beyond radiation. ONC201, a DRD2 antagonist and mitochondrial ClpP agonist, has shown promise in this population. Clinical and genetic variables associated with ONC201 response in H3K27M-mutant DMG continue to be investigated. A combined clinical and genetic study evaluated patients with H3K27M-DMG treated with single-agent ONC201 at the established phase 2 dose. Clinical outcomes of patients treated on two recently completed multi-site clinical studies (NCT03416530 and NCT03134131, n = 75) were compared with historical control data from patients with confirmed H3K27M-DMG (n = 391 total, n = 119 recurrent). Patients treated with ONC201 monotherapy following initial radiation, but prior to recurrence, demonstrated a median overall survival (OS) of 25.6 months from diagnosis and recurrent patients demonstrated a median OS of 16.2 months from recurrence, both of these more than doubling historical outcomes. Using a Cox model to correct for age, gender and tumor location, OS of ONC201-treated patients with H3K27M-mutant tumors remained significantly better than non-ONC201-treated historical controls (p = 0.0001). A survival and radiographic analysis based on tumor location, revealed stronger responses in thalamic patients. In patients with thalamic tumors treated after initial radiation (n = 16), median OS was not reached with median follow up of 22.1 months (historical control median OS of 12.5 months, n = 83, p = 0.0001). Significant correlations were found between baseline cerebral blood flow (CBF) on perfusion imaging and OS (Pearson’s r = 0.75, p = 0.003) and between nrCBF and PFS (r = 0.77, p = 0.002). Baseline tumor sequencing from treated patients (n = 20) demonstrates EGFR mutation (n = 3) and high EGFR expression as a marker of resistance and improved response in tumors with MAPK-pathway alterations (n = 5). In conclusion, ONC201 demonstrates unprecedented clinical and radiographic efficacy in H3K27M-mutant DMG with outcomes enriched in patients with thalamic tumors, treatment prior to recurrence, MAPK-pathway alterations, and patients with relatively high CBF.

Published

2022

4. INNV-33. FUNCTIONAL EX VIVO TESTING PROSPECTIVELY IDENTIFIES NEWLY DIAGNOSED GLIOBLASTOMA PATIENTS SENSITIVE TO TEMOZOLOMIDE TREATMENT IRRESPECTIVE OF MGMT METHYLATION STATUS

Author

Tessa DesRochers, Lindsay Lipinski, Ajay Abad, Robert Fenstermaker, Andrew Fabiano, Jeffery Edenfield, Charles Kanos, Navid Redjal, Analiz Rodriguez, Alireza Mansouri, Brad Zacharia, Nicholas Butowski, Jesse Jia-Xin Liu, Seunggu Han, Mateo Ziu, Adam Cohen, Ashley Smith, Cecile Rose Vibat, and Aubrey Ledford

Subjects

Cancer Research, Oncology, Neurology (clinical)

Abstract

Standard of care (SOC) therapy for newly diagnosed (ND) glioblastoma (GBM) patients consist of temozolomide (TMZ) concurrent with radiation therapy. It is well known that patients with an unmethylated MGMT promoter are less likely to respond to TMZ, however, this trend is not universal. We have previously shown that 3D Predict™ glioma can identify patient response to TMZ, often differentially than the methylation status would predict. Here we present expanded clinical data relating to functional ex vivo testing capable of identifying patients responsive to alkylating therapies such as TMZ, regardless of methylation status. METHODS Fresh tissue specimens taken from ND GBM patients enrolled into the 3D PREDICT clinical study were examined by 3D Predict glioma to evaluate ex vivo therapeutic response to TMZ. Overall Survival (OS) and Progression Free Survival (PFS) in patients having ≥ 6 months follow-up post-surgery or < 6 months follow up but experiencing progression/death as of September 1, 2022 will be presented. Prospective correlation of clinical response and test-predicted response will be demonstrated in this expanded cohort of ND GBM patients. IMPACT This data has the potential to change treatment for ND GBM patients by stratifying according to functional therapeutic response rather than epigenetic factors that are not completely predictive of clinical response. It is feasible that 3D Predict glioma could dramatically impact patient care by determining which unmethylated patients should be treated with TMZ, and methylated patients who would potentially derive greater benefit from clinical trials or other treatment regimens.

Published

2022

5. A randomized controlled phase III study of VB-111 combined with bevacizumab vs bevacizumab monotherapy in patients with recurrent glioblastoma (GLOBE)

Author

Jian Campian, Andrew Brenner, Patrick Y. Wen, Shifra Fain Shmueli, John de Groot, Tamar Rachmilewitz Minei, Laurence S. Freedman, Noa Lowenton-Spier, Leor Zach, Nicholas Butowski, Timothy F. Cloughesy, Benjamin M. Ellingson, and Yael C Cohen

Subjects

Cancer Research, medicine.medical_specialty, Bevacizumab, business.industry, Hazard ratio, Phases of clinical research, Gastroenterology, law.invention, Oncology, Randomized controlled trial, law, Concomitant, Internal medicine, medicine, Clinical endpoint, In patient, Neurology (clinical), business, Adverse effect, medicine.drug

Abstract

BackgroundOfranergene obadenovec (VB-111) is an anticancer viral therapy that demonstrated in a phase II study a survival benefit for patients with recurrent glioblastoma (rGBM) who were primed with VB-111 monotherapy that was continued after progression with concomitant bevacizumab.MethodsThis pivotal phase III randomized, controlled trial compared the efficacy and safety of upfront combination of VB-111 and bevacizumab versus bevacizumab monotherapy. Patients were randomized 1:1 to receive VB-111 1013 viral particles every 8 weeks in combination with bevacizumab 10 mg/kg every 2 weeks (combination arm) or bevacizumab monotherapy (control arm). The primary endpoint was overall survival (OS), and secondary endpoints were objective response rate (ORR) by Response Assessment in Neuro-Oncology (RANO) criteria and progression-free survival (PFS).ResultsEnrolled were 256 patients at 57 sites. Median exposure to VB-111 was 4 months. The study did not meet its primary or secondary goals. Median OS was 6.8 versus 7.9 months in the combination versus control arm (hazard ratio, 1.20; 95% CI: 0.91–1.59; P = 0.19) and ORR was 27.3% versus 21.9% (P = 0.26). A higher rate of grades 3–5 adverse events was reported in the combination arm (67% vs 40%), mainly attributed to a higher rate of CNS and flu-like/fever events. Trends for improved survival with combination treatment were seen in the subgroup of patients with smaller tumors and in patients who had a posttreatment febrile reaction.ConclusionsIn this study, upfront concomitant administration of VB-111 and bevacizumab failed to improve outcomes in rGBM. Change of treatment regimen, with the lack of VB-111 monotherapy priming, may explain the differences from the favorable phase II results.Clinical trials registrationNCT02511405

Published

2019

6. CTIM-29. PHASE 2 STUDY OF A NOVEL IMMUNOTHERAPY SL-701 IN ADULTS WITH RECURRENT GBM: IDENTIFICATION OF TREATMENT-INDUCED CD8+CD107A+ CD57+ PD-1- MEMORY T-CELLS THAT ARE ASSOCIATED WITH INCREASED SURVIVAL

Author

David Peereboom, Ross Lindsay, Michael Badruddoja, L Burt Nabors, Priya Kumthekar, Frank Lieberman, David Tran, Surasak Phuphanich, David Schiff, Jonathan Sherman, Nicholas Butowski, Erin Dunbar, Karen Fink, Fabio Iwamoto, Christopher Moertel, Michael Schulder, Tobias Walbert, Nassir Habboubi, Krzysztof Grzegorzewski, Christopher Brooks, and David A Reardon

Subjects

Cancer Research, Oncology, Neurology (clinical)

Abstract

Recurrent glioblastoma (GBM) is an aggressive disease with poor survival and limited treatment options. SL-701 is a novel immunotherapy comprised of synthetic peptides designed to elicit an anti-tumor immune response against GBM antigens IL-13Rα2, ephrinA2, and survivin. Here we describe an 18-color flow cytometry analysis from stage 2 of a Ph2 clinical trial of SL-701+poly-ICLC+bevacizumab (NCT02078648), in which 12-month overall survival (OS) was 50%. Of the 27 patients in stage 2, 24 (89%) developed heterogeneous T-cell responses against 1, 2, or 3 of the SL-701 CD8 peptides. Magnitude and kinetics of peptide responses were variable among these patients with no clear relationship to OS. Therefore, a phenotypic analysis of the T-cell response in all 27 patients was conducted using terraFlow, a unique data analysis approach utilizing machine learning to identify T-cell phenotypes associated with clinical response from all possible combinations of markers. In total, 10,184 unique SL-701 induced phenotypes were measured, including 223 phenotypes (P < 0.05) and 16 core phenotypes that uniquely represent differences between patients with OS above or below 12 months (P < 0.05). 50% of the core phenotypes were CD8+ CD57+ CD107a+ PD-1- SL-701-specific T-cells, which are highly-differentiated memory T-cells primed for cytotoxicity. The frequency of the CD57+ core phenotypes (8%-18%) was enhanced 1.6- to 2.3-fold in patients with an OS > 12 months (P < 0.05). Similarly, 2 core phenotypes identified cytotoxic CD4+ and CD8+ T cells, which were enhanced 1.9- and 2.5-fold in patients with an OS >12 months. The final 6 core phenotypes identified activated CD4+ CD154+ SL-701-specific T-cells (5%-19%) that were enhanced 0.3- to 0.5-fold in patients with an OS < 12 months (P < 0.05), suggesting helper T-cell responses in the absence of cytotoxic T-cell responses are associated with an OS < 12 months. Deep sequencing of SL-701-specific T-cells using whole transcriptome-based molecular cytometry is planned.

Published

2022

7. QOL-10. NOVEL MULTIMODAL STUDY OF THREE COGNITIVE REHABILITATION INTERVENTIONS IN LOWER GRADE GLIOMA

Author

Christina Weyer Jamora, Melissa Brie, Paige Bracci, Ellen Smith, Tracy Luks, Stephanie Phan, Steve Braunstein, Javier Villanueva-Meyer, Karen Gehring, Adrian Aguilera, Nancy Ann Oberheim Bush, Nicholas Butowski, Jennifer Clarke, Mariza Daras, John de Groot, Susan M Chang, Shawn L Hervey-Jumper, and Jennie Taylor

Subjects

Cancer Research, Oncology, Neurology (clinical)

Abstract

BACKGROUND Grade 2 and 3 glioma survivors (LrGG) are living longer, yet experience cognitive impairments with diminished quality of life (QOL). We present a novel multimodal study of three cognitive rehabilitation interventions in stable LrGG survivors. METHODS Participants were radiologically stable adult LrGG patients who were off medical treatment for ≥ 6 months with subjective and objective cognitive impairments ( >1SD in 2 or more domains). Patients were offered either In-person cognitive rehabilitation (strategy training including telehealth), or randomized to App-based cognitive rehabilitation (retraining and strategy training) versus Text messaging (strategy training). Intervention duration was 3 months. Neuropsychological testing (with parallel forms) and QOL assessments were conducted at baseline (T1), immediate post intervention (T2), and 6-month follow-up (T3), and analyzed with repeated measures regression or Wilcoxon signed rank tests. RESULTS Of the 33 analyzed (enrollment ongoing); 15/17 In-person, 5/8 App-based, and 8/8 Texting completed ≥ 80% or greater of interventions. Demographic and clinical characteristics were similar between cohorts. Median age was 48 years (range 27-63), 58% astrocytoma, 30% oligodendroglioma, 15% other (1 pilocytic astrocytoma, 4 diffuse glioma NOS), and 76% had prior radiotherapy. Rehabilitation interventions showed improvements in auditory working memory (T1-T2 In-person p= 0.02, eta2= 0.32-medium effect), verbal learning (T1-T3 App-based p= .06, eta2= 0.54-large effect; T1-T3 Texting p= .01, eta2= 0.75-large effect), and verbal memory (T1-T3 App-based p= .06, rho=0.31-medium effect). CONCLUSION Significant improvements in cognitive impairments were found with medium to large treatment effects within each cohort. Cognitive rehabilitation via In-person and Texting showed strongest feasibility and acceptability. In-person cognitive rehab showed earlier posttreatment improvements whereas treatment effects for App-based and Texting were noted, but took longer to realize gains. These interventions may show promise for addressing cognitive impairments in LrGG survivors and warrant further investigation.

Published

2022

8. CTNI-49. EARLY SIGNAL OF ACTIVITY FROM A PHASE 2 STUDY OF ST101, A FIRST-IN-CLASS PEPTIDE ANTAGONIST OF CCAAT/ENHANCER-BINDING PROTEIN Β (C/EBPΒ), IN RECURRENT GLIOBLASTOMA (GBM)

Author

Fabio Iwamoto, Vinai Gondi, Nicholas Butowski, Gerald Falchook, Anja Williams, Katherine B Peters, Jeff Evans, Nehal Lakhani, Meredith McKean, Stefan Symeonides, Benjamin Ellingson, Jim Rotolo, Gina Capiaux, Erol Wiegert, Rob Michel, Steve Kaesshaefer, and Alice Bexon

Subjects

Cancer Research, Oncology, Neurology (clinical)

Abstract

BACKGROUND C/EBPβ is a transcription factor that is active during embryofetal development but held in an inactive state in most mature cells (Zahnow 2009). C/EBPβ activates a proliferation/survival gene signature in multiple cancers, where it inversely correlates with disease prognosis and survival. ST101 is a cell-penetrating peptide antagonist of C/EBPβ. ST101 exposure leads to selective tumor cell death in multiple human cancer cell lines, including GBM, without impacting normal cell viability. In vivo, ST101 displays rapid uptake into multiple organs, the ability to cross the blood-brain barrier, and a long plasma half-life due to its resistance to degradation. It has potent anti-tumor activity in multiple GBM models, as a single agent or in combination, which supported moving into clinical development. TRIAL DESIGN: This phase 2 study is enrolling adult patients with GBM that has recurred or progressed after one standard treatment regimen (surgery, radiotherapy +/-temozolomide). Patients require measurable disease at baseline and at least 3 months from prior radiotherapy. Subjects receive the recommended phase 2 dose of ST101 (500mg IV weekly). Recruitment in the phase 2 portion of this trial began in January, 2022. RESULTS As of June 1, 2022, 14 GBM patients were enrolled. One patient has a confirmed mRANO partial response (PR) after 18 weeks of therapy, seven patients have not reached the first on-study assessment and six patients progressed. The median duration of therapy was 5 weeks. ST101 has a favorable safety profile with minor infusion related reactions being the most common adverse event. Based on the confirmed PR, the GBM cohort will be expanded. CONCLUSION This first-in-class C/EBPβ inhibitor, ST101, showed an early signal of activity in recurrent GBM. More extensive follow-up and clinical experience will be presented as this trial expands and matures.

Published

2022

9. Reirradiation of recurrent high-grade glioma and development of prognostic scores for progression and survival

Author

David R. Raleigh, Jennie Taylor, Jennifer Clarke, Shannon Fogh, Jared Hara, Christopher H. Chapman, Jean L. Nakamura, Susan M. Chang, Steve Braunstein, Penny K. Sneed, Nicholas Butowski, Annette M. Molinaro, and Nancy Ann Oberheim Bush

Subjects

Re-Irradiation, medicine.medical_specialty, recurrence, medicine.medical_treatment, Medicine (miscellaneous), Effective dose (radiation), Radiosurgery, Rare Diseases, glioma, Glioma, reirradiation, Medicine, Cancer, Performance status, Receiver operating characteristic, business.industry, glioblastoma, Neurosciences, Area under the curve, Original Articles, medicine.disease, Brain Disorders, Brain Cancer, prognosis, Fresh frozen plasma, Radiology, business

Abstract

Background Optimal techniques and patient selection for salvage reirradiation of high-grade glioma (HGG) are unclear. In this study, we identify prognostic factors for freedom from progression (FFP) and overall survival (OS) after reirradiation, risk factors for high-grade toxicity, and validate clinical prognostic scores. Methods A total of 116 patients evaluated between 2000 and 2018 received reirradiation for HGG (99 WHO grade IV, 17 WHO grade III). Median time to first progression after initial therapy was 10.6 months. Salvage therapies before reirradiation included surgery (31%) and systemic therapy (41%). Sixty-five patients (56%) received single-fraction stereotactic radiosurgery (SRS) as reirradiation. The median biologically effective dose (BED) was 47.25 Gy, and the median planning target volume (PTV) was 4.8 cc for SRS and 95.0 cc for non-SRS treatments. Systemic therapy was given concurrently to 52% and adjuvantly to 74% of patients. Results Median FFP was 4.9 months, and median OS was 11.0 months. Significant multivariable prognostic factors for FFP were performance status, time to initial progression, and BED; for OS they were age, time to initial progression, and PTV volume at recurrence. High-grade toxicity was correlated to PTV size at recurrence. Three-level prognostic scores were generated for FFP and OS, with cross-validated receiver operating characteristic area under the curve (AUC) of 0.640 and 0.687, respectively. Conclusions Clinical variables at the time of reirradiation for HGG can be used to prognosticate FFP and OS.

Published

2019

10. SYST-14 CLINICAL EFFICACY OF ONC201 IN RECURRENT H3 K27M-MUTANT DIFFUSE MIDLINE GLIOMA (DMG) PATIENTS

Author

Isabel Arrillaga-Romany, Sylvia Kurz, Rohinton Tarapore, Guangrong Lu, Ashley Sumrall, Nicholas Butowski, Rebecca Harrison, John DeGroot, Andrew Chi, Nicole Shonka, Yoshie Umemura, Yazmin Odia, Minesh Mehta, Phioanh Nghiemphu, Timothy Cloughesy, Lynne Taylor, Jerome Graber, Lindsay Kilburn, Karan Dixit, Clark Chen, Sharon Gardner, Dolly Aguilera, Tobey MacDonald, Andrew Cluster, Kathan Mehta, Albert Kheradpour, Allen Melemed, Joshua E Allen, Tracey Batchelor, Andrew Lassman, and Patrick Wen

Subjects

General Medicine

Abstract

BACKGROUND H3 K27M-mutant DMG predominantly affects children and young adults; no effective therapy is known. ONC201 is a first-in-class, anti-cancer DRD2 antagonist and ClpP agonist. METHODS Fifty pediatric and adult patients with recurrent H3 K27M DMG who received oral ONC201 monotherapy in clinical trials and expanded access were selected for a planned efficacy analysis. Eligibility criteria included measurable contrast-enhancing disease by RANO-HGG criteria (excluding pontine and spinal cord tumors), KPS/LPS≥60, ≥90 days from prior radiation, and adequate washout from prior anti-cancer therapy. The primary endpoint was overall response rate (ORR) by RANO-HGG criteria. Secondary endpoints included duration of response, time to response, progression-free survival (PFS), overall survival (OS), corticosteroid response rate, performance status response rate, and ORR by RANO-LGG criteria. Radiographic endpoints were assessed by dual-reader blinded independent central review. Data cutoff was May 31, 2021. RESULTS ORR was 20.0% (95%CI, 10.0–33.7) by RANO-HGG criteria. Median duration of response was 11.2 months (95%CI, 3.8–not reached) and median time to response was 8.3 months (range, 1.9–15.9). PFS at 6 months was 35.1% (95%CI, 21.2–49.3). The ORR was 26.0% (95%CI, 14.6–40.3) by RANO-LGG criteria. Fifteen patients (30.0%; 95%CI, 17.9–44.6) achieved an objective response by RANO-HGG and/or RANO-LGG criteria. Of 15 patients receiving ≥4 mg daily dexamethasone at baseline, 7 (46.7%; 95%CI, 21.3–73.4) achieved ≥50% confirmed reduction in dose. Of 34 patients with baseline KPS/LPS CONCLUSIONS ONC201 monotherapy exhibits durable and clinically meaningful efficacy in recurrent H3 K27M-mutant DMG.

Published

2022

11. CTNI-17. A PHASE 1 WITH DOSE EXPANSION/PHASE 2 STUDY OF SELINEXOR IN COMBINATION WITH STANDARD OF CARE THERAPY FOR NEWLY DIAGNOSED OR RECURRENT GLIOBLASTOMA

Author

Howard Colman, Frances Chow, Jatin P. Shah, Gregory Mundy, Andrew B. Lassman, Rebecca Harrison, Yasaman Damestani, Yang Liu, Vyshak Venur, Warren P. Mason, Nicholas Butowski, Minesh P. Mehta, Paul Duic, Sharon Tamir, Michael Schulder, John A. Boockvar, Kai Li, Yazmin Odia, Patrick Y. Wen, Erin M. Dunbar, Samuel Goldlust, Sharon Shacham, Scott R. Plotkin, Eric Sbar, and Priya Kumthekar

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Standard of care, Temozolomide, Bevacizumab, business.industry, Recurrent glioblastoma, O-6-methylguanine-DNA methyltransferase, Lomustine, 26th Annual Meeting & Education Day of the Society for Neuro-Oncology, medicine.disease, Glioma, Internal medicine, Troponin I, medicine, Neurology (clinical), business, medicine.drug

Abstract

BACKGROUND Glioblastoma (GBM) is the most common and aggressive primary brain tumor with median overall survival of 15 months and 5-7 months for patients with newly diagnosed or recurrent disease (nGBM or rGBM), respectively. Selinexor is a first-in-class, oral, selective inhibitor of nuclear export which blocks exportin 1 (XPO1), forcing the nuclear retention and reactivation of tumor suppressor proteins, ultimately causing cancer cell death. Increased XPO1 expression in gliomas is associated with higher pathological grade and poorer prognosis. Consistent with these data, selinexor inhibited tumor growth and prolonged survival in an animal model of GBM. Importantly, selinexor showed encouraging intra-tumoral penetration and single-agent efficacy in rGBM (KING study). The current trial tests the hypothesis that adding selinexor to standard therapy will improve clinical outcomes for patients with nGBM or rGBM. METHODS To facilitate the successful development of new therapies, consensus recommendations are to use biomarker enrichment and flexible design that allows expansion of promising cohorts. Accordingly, this phase 1a dose finding study is followed by a phase 1b dose expansion (and ultimately by a 1:1 randomized phase 2 efficacy exploration trial) to independently evaluate: radiation + selinexor in nGBM with unmethylated MGMT promoter (Arm A), radiation + temozolomide + selinexor for nGBM with methylated MGMT promoter (Arm B), and lomustine + selinexor in rGBM (Arm C). Bevacizumab or TTField + selinexor in rGBM (Arms D & E, respectively) are being considered. The Phase 1a primary endpoint is maximum tolerated dose/recommended phase 2 dose. The phase 1b primary endpoint is PFS at 3 months against historic controls. The phase 1b dose expansion is included to evaluate preliminary efficacy before launching into a randomized phase 2 trial. Patient quality of life during the trial will be objectively measured using digital devices (e.g. smartwatch/customized smartphone app). We are currently enrolling patients nationwide. Clinical Trial Registration number: NCT04421378.

Published

2021

12. BIOM-40. TARGETED GENE EXPRESSION PROFILING PREDICTS MENINGIOMA OUTCOMES AND RADIOTHERAPY RESPONSES

Author

Nancy Ann Oberheim-Bush, Tai-Chung Lam, Penny K. Sneed, C.H. Lucas, Gilberto K.K. Leung, Javier Villanueva-Meyer, David A. Solomon, Jenny Kan-Suen Pu, William S. Chen, Minh P. Nguyen, Abrar Choudhury, Lai-Fung Li, Nicholas Butowski, Jacob S. Young, Jason Chan, Michael McDermott, David R. Raleigh, Mitchel S. Berger, Arie Perry, Theresa Yu, Stephen Magill, Harish N. Vasudevan, Jessica Schulte, and Steve Braunstein

Subjects

Oncology, Cancer Research, medicine.medical_specialty, business.industry, medicine.medical_treatment, Postoperative radiotherapy, 26th Annual Meeting & Education Day of the Society for Neuro-Oncology, medicine.disease, Meningioma, Gene expression profiling, Radiation therapy, Internal medicine, DNA methylation, Gene expression, medicine, Neurology (clinical), business, Gene, Exome sequencing

Abstract

BACKGROUND Surgery is the mainstay of meningioma treatment, but improvements in meningioma risk stratification are needed and indications for postoperative radiotherapy are controversial. DNA methylation profiling, copy number variants (CNVs), exome sequencing, and RNA sequencing have improved understanding of meningioma biology, but have not superseded histologic grading, or revealed biomarkers for radiotherapy responses. To address these unmet needs, we optimized and validated a targeted gene expression biomarker predicting meningioma outcomes and responses to radiotherapy. METHODS Targeted gene expression profiling was performed on a discovery cohort of 173 meningiomas (median follow-up 8.1 years) and a validation cohort of 331 meningiomas (median follow-up 6.1 years) treated with surgery (n=504) and postoperative radiotherapy (n=73) at independent, international institutions (70% WHO grade 1, 24% WHO grade 2, 6% WHO grade 3). Optimized targeted gene expression models predicting clinical outcomes (34 genes) or radiotherapy responses (12 genes) were developed from the discovery cohort, and compared to histologic and molecular classification systems by performing DNA methylation profiling, CNV analysis, exome sequencing, and RNA sequencing on the same meningiomas. RESULTS Targeted gene expression profiling achieved a concordance-index of 0.75 ± 0.03 (SEM) for local freedom from recurrence (LFFR) and 0.72 ± 0.03 for overall survival (OS) in the validation cohort, outperforming WHO grade (5-year LFFR delta-AUC 0.15, 95% CI 0.076-0.229, p=0.001) and DNA methylation grouping (delta-AUC 0.075, 95% CI 0.006-0.130, p=0.01) for LFFR, disease-specific survival, and OS. The biomarker was independently prognostic after accounting for WHO grade, extent of resection, primary versus recurrent presentation, CNV status, DNA methylation group, and Ki67 labeling index, and identified meningiomas benefiting from radiotherapy (interaction p-value=0.0008), suggesting postoperative radiotherapy could be refined in 30.2% of cases. CONCLUSIONS Targeted gene expression profiling of 504 meningiomas improves discrimination of meningioma local recurrence, disease-specific survival, and overall survival, and predicts radiotherapy responses.

Published

2021

13. CTIM-28. MDNA55, AN INTERLEUKIN-4 RECEPTOR TARGETED IMMUNOTHERAPY, FOR RECURRENT GBM DELIVERED BY CONVECTION ENHANCED DELIVERY (CED)

Author

Nina Merchant, Dina Randazzo, Sajeel Chowdhary, Seunggu J. Han, Fahar Merchant, John Sampson, Krystof Bankiewiecz, Melissa Coello, Benjamin M. Ellingson, Andrew Brenner, Santosh Kesari, Achal S. Achrol, Nicholas Butowski, Michael A. Vogelbaum, John Floyd, Manish K. Aghi, Martin Bexon, Steven Brem, Miroslaw Zabek, Frank D. Vrionis, and Chandtip Chandhasin

Subjects

Cancer Research, Oncology, business.industry, Interleukin-4 receptor, Cancer research, Medicine, Neurology (clinical), 26th Annual Meeting & Education Day of the Society for Neuro-Oncology, business, Convection-Enhanced Delivery, Targeted immunotherapy

Abstract

BACKGROUND MDNA55 is an IL4R-targeted toxin in development for treatment of recurrent glioblastoma (rGBM). MDNA55 binds to IL4R expressed by tumor cells and non-malignant cells of the tumor microenvironment. METHOD MDNA55-05 was an open-label, single-arm study of MDNA55 delivered by CED as a single treatment in patients with 1st or 2nd recurrence following de novo GBM, IDH wild type status and not indicated for resection at relapse. Dose volumes (up to 60mL) and concentration of MDNA55 (1.5 to 9.0 μg/mL) were studied. RESULTS MDNA55 showed an acceptable safety profile at all doses tested. Median OS (mOS) amongst all subjects was 11.9 months, OS-24 was 20%, and PFS-12 was 27%. Among subjects expressing high levels of IL4R (irrespective of MDNA55 dose) and low levels of IL4R expression administered high dose (≥ 180μg) of MDNA55 (IL4Rhi + IL4Rlo/hd), mOS further improved to 14.0 months with OS-24 of 20%. Unmethylated MGMT promoter status did not affect MDNA55 treatment outcomes. In the IL4Rhi + IL4Rlo/hd population (N=17), mOS was 14.9 months with OS-24 of 22%. Following treatment with high concentrations of MDNA55 (6.0 or 9.0 μg/mL), transient (median of 3 cycles) low dose Avastin (5mg/kg q2w or 7.5mg/kg q3w) was used for symptom control and steroid sparring. Among these subjects, mOS amongst all comers (N=9) and the IL4Rhi + IL4Rlo/hd group (N=8) increased to 21.8 and 18.6 months with OS-24 of 44% and 38%, respectively. CONCLUSIONS MDNA55 shows potential to benefit all rGBM patients treated at high dose irrespective of IL4R expression. In the 1:1 randomized Phase 3 trial, the study will enrol two-thirds of subjects in the SOC arm from a matched external control arm. Unlike conventional RCTs, the hybrid design sets a new precedent for GBM trials, allowing robust OS analysis while significantly reducing the number of subjects randomized to SOC arm.

Published

2021

14. CTIM-18. LUMINOS-101: INITIAL SAFETY AND TOLERABILITY OF PVSRIPO AND PEMBROLIZUMAB COMBINATION THERAPY IN RECURRENT GLIOBLASTOMA

Author

Mitchel S. Berger, Shirley Ong, Daniel Landi, Andrew E. Sloan, Andrea Kelly, Adam Dickinson, E. Antonio Chiocca, Ketan R. Bulsara, A. Desjardins, J. Bradley Elder, Robin Buerki, Bruno Bockorny, Rafael A. Vega, Prakash Ambady, Allan H. Friedman, Lori Mixson, William T. Curry, Elizabeth R. Gerstner, Kevin Becker, Patrick Y. Wen, Chris A. Learn, LeAnn Jackson, Nicholas Butowski, Eric Sauvageau, W Garrett Nichols, and Robert Cavaliere

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Tolerability, Combination therapy, business.industry, Recurrent glioblastoma, Internal medicine, Medicine, Neurology (clinical), Pembrolizumab, business

Abstract

BACKGROUND Recurrent glioblastoma (rGBM) is rapidly fatal with current therapies. PVSRIPO is an intratumoral immunotherapy targeting CD155 on antigen-presenting and malignant cells of solid tumors. Preclinically, PVSRIPO treatment leads to systemic, tumor antigen-specific, polyfunctional T-cell–mediated anti-tumor response, predominately driven by type I/III interferons. This inflammatory signature generates anti-tumor immunity and upregulates the programmed death (PD)-1 immune checkpoint in the tumor microenvironment. Preclinical models (including GBM) have shown that PVSRIPO+anti-PD-1/L1 therapy was more efficacious than either agent alone, warranting further investigation. METHODS Adults with histologically confirmed rGBM (1-2 prior progressions), Karnofsky performance status (KPS) ≥70, and an active, supratentorial, contrast-enhancing lesion (1-5.5 cm), received PVSRIPO (5x107 TCID50) intratumorally via convection-enhanced delivery (Day 1), followed by 200 mg pembrolizumab IV at week 2, given every 3 weeks for up to 24 months, to evaluate the safety/efficacy of the combination. A safety lead-in period (n=3-6) with a minimum 21–28-day delay before treatment of subsequent patients was planned, with a data safety monitoring board (DSMB) evaluating safety/tolerability prior to expansion (up to N=30). RESULTS The first 3 patients enrolled (ages 55-60, KPS 90-100) all received PVSRIPO followed by pembrolizumab (1-5 cycles), as planned. At cutoff (26-106 days of follow-up), there were no dose-limiting toxicities, treatment-emergent (TE) serious adverse events (SAE), or TEAEs necessitating a delay in initial/subsequent pembrolizumab treatments. All patients experienced a related TEAE, all grade 1 or 2 in severity. One patient experienced an AE of special interest (peritumoral edema, resulting in headache and hemiparesis), successfully managed with low-dose bevacizumab and corticosteroids. The DSMB unanimously recommended the study proceed without modification. CONCLUSIONS Intratumoral PVSRIPO+pembrolizumab was reasonably well tolerated, warranting continued investigation of the safety and efficacy of this combination in patients with rGBM.

Published

2021

15. Attitudes toward fertility and fertility preservation in women with glioma

Author

Nicholas Butowski, Jane Rabbitt, Mitchell P. Rosen, Jessica L. Chan, Joseph M. Letourneau, Jennifer Clarke, E.E. Niemasik, Rachel K Stiner, Nikita Sinha, Susan M. Chang, and Michael D. Prados

Subjects

business.industry, media_common.quotation_subject, Oncology and Carcinogenesis, Neurosciences, Medicine (miscellaneous), Survey result, Fertility, Original Articles, medicine.disease, Affect (psychology), Chemotherapy regimen, 03 medical and health sciences, 0302 clinical medicine, 030220 oncology & carcinogenesis, Glioma, Female patient, medicine, Oncology & Carcinogenesis, Fertility preservation, business, 030217 neurology & neurosurgery, After treatment, Demography, media_common

Abstract

Background No studies have examined the fertility priorities of women undergoing treatment for their glioma. Glioma patients frequently undergo chemotherapy as part of their treatment; however, it is unknown whether patients truly are aware of its possible effects on their fertility. Our objective was to assess the fertility priorities of glioma patients and ascertain whether female glioma patients are being effectively counseled on the effects of chemotherapy on their fertility prior to beginning treatment. Methods The sample was composed of female patients from the Neuro-oncology clinic of the University of California, San Francisco. Participants completed a cross-sectional survey between October 2010 and December 2013 exploring their attitudes toward fertility and their experience with fertility counseling prior to chemotherapy initiation. Results Seventy-two women completed the survey. Analysis of the survey results showed that 30% of women receiving chemotherapy reported having a discussion regarding fertility preservation prior to beginning treatment. Of those who reported having this discussion, 80% were aware that chemotherapy could negatively affect their fertility. Many women reported that while fertility preservation was not important to them at the time of diagnosis, it was a priority for them at the time of survey completion. Although interest in having children tended to decrease after cancer treatment, the majority of respondents reported wanting a child after treatment. Conclusions The data obtained in this study suggest a lack of understanding of reproductive priorities, which may be addressed with a more comprehensive fertility discussion prior to beginning treatment.

Published

2018

16. IMMU-26. SAFETY AND EFFICACY OF PVSRIPO IN RECURRENT GLIOBLASTOMA: LONG-TERM FOLLOW-UP AND INITIAL MULTICENTER RESULTS

Author

Mitchel S. Berger, Patrick Y. Wen, Andrew E. Sloan, William T. Curry, Andrea Kelly, Robert Cavaliere, Allan H. Friedman, Adam Dickinson, E. Antonio Chiocca, Henry S. Friedman, Nicholas Butowski, Matthias Gromeier, Darell D. Bigner, W Garrett Nichols, Lori Mixson, Robin Buerki, A. Desjardins, Eric Sauvageau, David M. Ashley, Elizabeth R. Gerstner, Daniel Landi, Chris A. Learn, and Kristin Orr

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Long term follow up, business.industry, Recurrent glioblastoma, Internal medicine, Medicine, Neurology (clinical), 26th Annual Meeting & Education Day of the Society for Neuro-Oncology, business

Abstract

BACKGROUND Recurrent glioblastoma (rGBM) is rapidly fatal (median overall survival [mOS] of ~9 months; OS at 12 months [OS12] < 35%) with approved therapies (lomustine±bevacizumab). PVSRIPO is an intratumoral immunotherapy targeting CD155 on antigen-presenting and malignant cells of solid tumors. Preclinically, PVSRIPO delivers a systemic, tumor antigen-specific, polyfunctional T-cell mediated anti-tumor response. Interim, single-center, phase (Ph) 1 results showed greater long-term survival with PVSRIPO vs. criteria-matched external control rGBM patients (Desjardins 2018). Updates to Ph1 safety (at the Ph2 dose) and efficacy and interim multicenter (Ph2) results are presented. METHODS Adults with histologically-confirmed rGBM, Karnofsky performance status ≥ 70, and an active, supratentorial, contrast-enhancing lesion (1-5.5cm) received PVSRIPO (5x107 TCID50) intratumorally via convection-enhanced delivery on Day 1, with a planned follow-up of 24 months. Safety (treatment-emergent adverse events [TEAEs]), efficacy (reported as OS12, OS24, mOS), and blood/tissue were assessed. RESULTS 149 patients (>90% with 1-2 prior progressions, including failure of SOC and patients with prior bevacizumab failure) received the Ph2 dose of PVSRIPO (n=30 received other doses in Ph1 with safety summarized previously). Follow-up durations for surviving patients were 51-74 months (Ph1) and 10-44 months (Ph2). No dose-limiting toxicities occurred; up to 97% of patients experienced mostly grade 1-2 related TEAEs; ≤ 23% patients experienced grade ≥ 3 related events. Neurologic symptoms related to peritumoral edema were most common ( > 90% patients) and were effectively managed with low-dose bevacizumab/corticosteroids. Survival estimates were: OS12: 54%, 50%; OS24: 18%, 17%; mOS: 12.3 (95% CI 10,15.3), 12 (10.6,13.7) months, for the Ph1 and Ph2 trials, respectively. Baseline correlates of longer survival included smaller lesions and methylated MGMT-promoter status. CONCLUSIONS The multicenter/Ph2 study replicated the single-center/Ph1 results. Relative to published data with approved therapies, PVSRIPO was associated with greater long-term survival and mOS in patients with rGBM and was generally well-tolerated.

Published

2021

17. PATH-36. INTRATUMOR HETEROGENEITY AND BIOINFORMATIC DIFFERENCES INFLUENCE MENINGIOMA MOLECULAR CLASSIFICATION

Author

Stephanie Hilz, David R. Raleigh, Melike Pekmezci, Javier Villanueva-Meyer, William S. Chen, Abrar Choudhury, Harish N. Vasudevan, Stephen Magill, C.H. Lucas, Nicholas Butowski, Arie Perry, Nancy Ann Oberheim-Bush, Steve Braunstein, Michael McDermott, and David A. Solomon

Subjects

Cancer Research, Computational biology, Biology, medicine.disease, nervous system diseases, Copy Number Polymorphism, Meningioma, Molecular classification, Oncology, Intratumor heterogeneity, otorhinolaryngologic diseases, medicine, Neurology (clinical), neoplasms

Abstract

Molecular alterations such as CDKN2A inactivation and TERT promoter mutation are new criteria for grade 3 meningiomas in the 5th edition of the WHO Classification of Tumors of the Central Nervous System. However, consensus approaches to identify copy number variants (CNVs) and short somatic variants in meningiomas are lacking. Here, we performed integrated DNA methylation profiling, RNA-sequencing, and targeted DNA mutational profiling on 10 stereotactically-collected, regionally-distinct samples from 4 meningiomas. Targeted DNA sequencing revealed numerous private short somatic variants from multiple sites within individual meningiomas, including a TERT promoter mutation in only 1 of 2 samples from the same tumor. DNA methylation profiling revealed differences in biologic groups and immune cell enrichment between regionally-distinct samples within individual meningiomas. CNV status was evaluated using DNA methylation profiling and RNA sequencing on 14 stereotactically-collected, regionally-distinct samples from 2 meningiomas. Phylogenetic architectures from DNA methylation profiling and targeted DNA sequencing were highly concordant and shared 99.12% of CNVs while RNA sequencing identified only 39% of the CNVs called from DNA based approaches. Finally, CNV analysis based on single-cell RNA sequencing revealed partially overlapping CNVs across meningioma cells within an individual tumor, suggesting subclonal populations may influence CNV-based meningioma molecular classification and underlie limitations in defining CNVs from bulk RNA-sequencing. In sum, these data highlight the relative strengths and weaknesses of various approaches for molecular analysis of meningiomas complicated by intratumor heterogeneity due to non-tumor cells and subclonal populations of meningioma cells. Future efforts to incorporate molecular analysis into the diagnostic paradigm for meningiomas may require orthogonal validation across multiple platforms or image-guided meningioma sampling to select the most aggressive regions for molecular profiling.

Published

2021

18. CTIM-11. PHASE 2 STUDY OF SL-701, A NOVEL IMMUNOTHERAPY, IN ADULTS WITH RECURRENT GBM: A HIGH PARAMETER FLOW CYTOMETRY ANALYSIS OF CD8+ T CELLS AND POTENTIAL IMPLICATIONS FOR PATIENT ENRICHMENT STRATEGIES

Author

Michael Schulder, Krzysztof Grzegorzewski, Frank S. Lieberman, Nassir Habboubi, Erin M. Dunbar, Ross W. B. Lindsay, Tobias Walbert, Christopher Brooks, Fabio M. Iwamoto, Jonathan H. Sherman, Surasak Phuphanich, Karen Fink, L. Burt Nabors, Nicholas Butowski, David Schiff, Michael Badruddoja, Priya Kumthekar, David M. Peereboom, David Tran, David A. Reardon, and Christopher L. Moertel

Subjects

Cancer Research, medicine.diagnostic_test, Interferon type II, business.industry, medicine.medical_treatment, Immunotherapy, 26th Annual Meeting & Education Day of the Society for Neuro-Oncology, Flow cytometry, Immune system, Oncology, Antigen, Survivin, medicine, Cancer research, Cytotoxic T cell, Neurology (clinical), Immunocompetence, business, medicine.drug

Abstract

Treatment of glioblastoma (GBM) remains a critical challenge and unmet medical need due to limited treatment options. SL-701 is a novel immunotherapy comprised of synthetic peptides designed to elicit a target-specific anti-tumor immune response against the GBM antigens IL-13Rα2, ephrinA2, and survivin. A multicenter, 2-stage, phase 2 clinical trial (NCT02078648) that evaluated the safety and efficacy of SL-701 in 74 adults with recurrent GBM was previously reported. This report describes preliminary data to suggest a correlation of immunocompetence to clinical outcome. In stage 2 (SL-701 + bevacizumab + poly-ICLC) the overall survival at 12 months was 50%. Two of 28 patients enrolled in stage 2 achieved CR (duration of response: 7.8 and 8.8 months) and 2 achieved PR (duration of response: 7.9 and 8.8 months). In a preliminary analysis to assess CD8+ T-cell responses, long-term survivors were comprised largely of subjects with an SL-701-induced target-specific CD8+ T-cell response, indicating a potential correlation of immunocompetence to clinical outcome. By week 24, SL-701-induced target-specific CD8+ T cells expressing IFNg were detected in 8 of 27 patients (30%) who had sufficient samples, with co-expression of PD-1, TIM3, and LAG3 detected in 4 patients. To further understand the T-cell response to SL-701, deep sequencing of target-specific CD8+ T cells using whole transcriptome-based molecular cytometry and high parameter (25+ color) flow cytometry is currently underway and updated data will be reported.

Published

2021

19. CTIM-24. RANDOMIZED TRIAL OF NEOADJUVANT VACCINATION WITH TUMOR-CELL LYSATE INDUCES T CELL RESPONSE IN LOW-GRADE GLIOMAS

Author

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

Subjects

Cancer Research, Chemokine, biology, business.industry, medicine.medical_treatment, 26th Annual Meeting & Education Day of the Society for Neuro-Oncology, law.invention, Vaccination, Radiation therapy, Immune system, Cytokine, Oncology, Randomized controlled trial, law, medicine, Cancer research, biology.protein, Neurology (clinical), Stem cell, business, Neoadjuvant therapy

Abstract

BACKGROUND The prognosis of WHO grade II low-grade gliomas (LGG) is varied with potential for long survival.Given their relatively intact immune system and slow growth rate, vaccines are an attractive treatment strategy for LGG in an attempt to defer more toxic treatments. The goals of this pilot study were to evaluate safety and immunological effects of vaccination with GBM6-AD, an allogeneic glioblastoma stem cell line lysate, with poly-ICLC in LGG. METHODS Eligible patients were ≥ 18 years old, ≥ 70 KPS, with recurrent LGG or imaging consistent with LGG, and amenable to resection. Patients were randomized to vaccine prior to surgery (Arm 1) or not (Arm 2) and all received adjuvant vaccine. Co-primary outcomes were safety and immune response in the tumor, with exploratory outcomes of survival and immunologic effects in peripheral blood. RESULTS A total of 17 eligible patients were evaluable – nine into Arm 1 and eight into Arm 2. Median age was 33 years, with median time from initial diagnosis of 4.7 years (0 – 20). Two patients (11.8%) previously received radiotherapy and seven (41.2%) prior systemic therapy. No dose limiting toxicities or grade 3 AEs were observed. Neoadjuvant vaccination induced up regulation of type-1 cytokines and chemokines in peripheral blood, and CD8+ T cell clones that reacted to the vaccine were also detected in the tumor. Median follow-up time from first post-operative vaccine was 20.8 months with median PFS of 11.0 months and time to change in therapy of 23.7 months. Of the six patients to receive additional treatment, three had second surgery only one confirming malignant progression to anaplastic oligodendroglioma. CONCLUSION Treatment was well-tolerated with no regimen-limiting toxicity. GBM6-AD plus poly-ICLC induced effector CD8+ T cell response in peripheral blood and enables some vaccine-reactive CD8+ T cells to migrate into the TME. Further investigation is warranted.

Published

2021

20. NGMA-6. Quantitative MGMT Promoter Methylation Index Indicates Non-Linear, Prognostic Effect in Glioblastoma

Author

Akshay Ravi, Nancy Ann Oberheim Bush, Eduardo Rodriguez, Jennifer Clarke, Susan M. Chang, Hideho Okada, Aaron Scheffler, Mitchel S. Berger, Jennie Taylor, David A. Solomon, John S. Witte, Nicholas Butowski, David R. Gibson, and Farid F. Chehab

Subjects

Methyltransferase, O-6-methylguanine-DNA methyltransferase, Final Category: Next Generation Methods and Approaches, Methylation, Biology, Chemotherapy regimen, Supplement Abstracts, CpG site, Cancer research, AcademicSubjects/MED00300, AcademicSubjects/MED00310, Epigenetics, Progression-free survival, Gene

Abstract

Background Epigenetic inhibition of the O6-methylguanine-DNA-methyltransferase (MGMT) gene has emerged as a clinically relevant prognostic marker in glioblastoma (GBM). Methylation of the MGMT promoter has been shown to increase chemotherapy efficacy. While traditionally reported as a binary marker, recent methodological advancements have led to quantitative methods of measuring methylation, allowing for clearer insights into methylation’s functional relationship with survival. Methods A CLIA assay and bisulfite sequencing was utilized to develop a quantitative, 17-point MGMT promoter methylation index derived from the number of methylated CpG sites. Retrospective review of 242 newly diagnosed GBM patients was performed in order to discern how risk for mortality transforms as promoter methylation increases. Non-linearities were captured by fitting splines to Cox proportional hazard models, plotting smoothed residuals, and creating survival plots. Covariates included age, KPS, IDH1 mutation, and extent of resection. Results Median follow-up time and progression free survival were 15.9 and 9 months, respectively. 176 subjects experienced death. A one-unit increase in CpG methylation resulted in a 4% reduction in hazard (95% CI 0.93–0.99, P Conclusion The extent of MGMT methylation shares a non-linear relationship with survival, suggesting conformation of the marker’s protective effect. This finding challenges the current understanding of MGMT and underlines the clinical importance of determining its prognostic utility. Potential limitations include censoring, sample size, and extraneous mutations. Future research is warranted to examine whether the location of CpG site methylation contributes to a reduction in mortality hazard.

Published

2021

21. PATH-34. GENETIC PROFILING OF AGGRESSIVE MENINGIOMAS REVEAL DIVERSE SPECTRUM OF ACCOMPANYING ALTERATIONS BEYOND NF2 INACTIVATION

Author

Nancy Ann Oberheim Bush, Jessica Schulte, Tarik Tihan, Melike Pekmezci, Minh P. Nguyen, David R. Raleigh, Stephen T. Magill, Julieann C. Lee, Michael McDermott, Andrew W. Bollen, Nicholas Butowski, Arie Perry, Javier Villanueva-Meyer, David A. Solomon, and Philip V. Theodosopoulos

Subjects

Cancer Research, Mutation, MTOR Serine-Threonine Kinases, Molecular Pathology & Classification, Computational biology, Biology, medicine.disease, medicine.disease_cause, Meningioma, Oncology, PIK3CA gene, otorhinolaryngologic diseases, medicine, Neurology (clinical), Epigenetics, Akt1 gene, neoplasms

Abstract

BACKGROUND Meningiomas are the most common primary central nervous system tumor in adults. The majority are clinically indolent and WHO grade I. However, 20-30% are WHO grade II and 1-3% are WHO grade III, which have shorter progression-free (PFS) and overall survival. A subset of grade I meningiomas also follow an aggressive course, requiring serial resection and/or radiotherapy, similar to high-grade meningiomas. The objective of this study was to characterize the genetic alterations in meningiomas with an aggressive clinical course. METHODS Targeted next-generation sequencing (NGS) of 40 aggressive meningiomas was performed using the UCSF500 cancer panel, which assesses ~500 cancer-related genes. Information on patient demographics, tumor histopathology, and treatment history was also collected. RESULTS Meningiomas analyzed included 15 (38%) WHO grade I, 11 (28%) WHO grade II, and 13 (33%) WHO grade III. At the time of genetic profiling, 71% of patients had received prior treatment (68% surgery, 48% fractionated radiotherapy, 23% radiosurgery). The most commonly altered gene was NF2, with 71% of tumors demonstrating biallelic inactivation. Other common alterations included biallelic CDKN2A/B deletion (15%) and TERT amplification or promoter mutation (13%). Other recurrent alterations involved SUFU (8%), and ARID1A, ATM, BAP1, DMD, KDM6A, and PTEN (each 5%). Genes which are commonly altered in indolent WHO grade I meningiomas, such as AKT1, KLF4, PIK3CA, SMO, and TRAF7, were intact in this cohort. CONCLUSIONS The additional genetic alterations beyond NF2 inactivation that drive aggressive meningiomas are diverse and include homozygous deletion of CDKN2A (negative regulator of cyclin-dependent kinases 4/6), inactivating mutations in SUFU (a negative regulator of Hedgehog signaling), homozygous deletion of PTEN (a negative regulator of mTOR signaling), and mutations/deletions in epigenetic regulatory factors (e.g. ARID1A, KDM6A). Clinical trials are needed to assess the efficacy of therapeutics targeting these specific pathways in patients with meningiomas refractory to conventional treatments.

Published

2020

22. NCOG-21. INTERIM RESULTS OF THREE COGNITIVE REHABILITATION STRATEGIES IN PATIENTS WITH LOWER GRADE GLIOMAS

Author

Susan M. Chang, Jennie Taylor, Ellen Smith, Steve Braunstein, Karin Gehring, Nicholas Butowski, Jennifer Clarke, Melissa S Brie, Paige M. Bracci, Christina Weyer-Jamora, Adrian Aguilera, Javier Villanueva-Meyer, Tracy Luks, Nancy Ann Oberheim Bush, and Shawn L. Hervey-Jumper

Subjects

Cancer Research, Lower grade, medicine.medical_specialty, Oncology, business.industry, Interim, Physical therapy, medicine, In patient, Neurology (clinical), Cognitive rehabilitation therapy, business, Outcome Measures and Neuro-Cognitive Outcomes

Abstract

BACKGROUND Patients with lower grade (2 and 3) gliomas (LrGG) are living longer, but often with cognitive impairments from their tumor and treatments. However, cognitive assessments and access to cognitive rehabilitation are not a standard part of care. We present preliminary results of a pilot study investigating feasibility and efficacy of three cognitive rehabilitation strategies for stable LrGG patients – in-person manualized cognitive rehabilitation; iPad based cognitive rehabilitation program of retraining and compensation strategies (ReMind); or daily instructional text messages (Healthy SMS). METHODS Eligible patients were adults with clinically and radiologically stable LrGG, > 6 months from last treatment, and ≥1 standard deviation (SD) below normal on ≥ 2 domains of neuropsychological assessments. Patients were first offered in-person cognitive rehabilitation or randomized to ReMind or Healthy SMS if unable to attend in-person. Interventions lasted 3 months. Neuropsychological and HRQOL assessments, using PROMIS NeuroQOL, were conducted at baseline, 3, and 6 months post-intervention. Feasibility was defined as attending ≥80% of in-person sessions; completing ≥80% of ReMind tasks; or not opting out of Healthy SMS texts. RESULTS To date 23/60 patients have enrolled: 11 in-person and 12 randomized to ReMind (5) or Healthy SMS (7). Demographic and clinical characteristics were similar between cohorts. Median age at testing was 46 years, with 65% female, and 78% having received prior radiation (median 4.1 years, range 3.2 – 11.5). At baseline, processing speed was the most common domain of impairment with 43% ≥ 1.5 SD below normal and 36% patients reporting subjective cognitive impairment on HROQL assessment. Feasibility was 71% for in-person rehabilitation; 50% for ReMind; and 100% for Health SMS. CONCLUSION These preliminary results demonstrate that stable LrGG patients with subjective and objective cognitive impairments can reasonably engage in cognitive rehabilitation interventions. Updated data including post-intervention neuropsychological and HROQL related changes will be presented.

Published

2020

23. CTNI-17. CLINICAL EFFICACY AND PREDICTIVE BIOMARKERS OF ONC201 IN H3 K27M-MUTANT DIFFUSE MIDLINE GLIOMA

Author

Pankaj Vats, Alyssa Paul, Yoshie Umemura, Timothy F. Cloughesy, Chase Thomas, Nicole Shonka, Daniel Martinez, Isabel Arrillaga-Romany, Ian Wolfe, Benjamin M. Ellingson, Arul M. Chinnaiyan, Evan Cantor, Zachary Miklja, John de Groot, Abed Rahman Kawakibi, Andrew S. Chi, Chandan Kumar-Sinha, Rebecca Harrison, Adam C. Resnick, Nicholas Butowski, Guangrong Lu, Minesh P. Mehta, Joshua E. Allen, Ashley Sumrall, Matthew Hall, Rajen Mody, Carl Koschmann, Mariella G. Filbin, Ruby Siada, Sylvia Kurz, Rohinton Tarapore, Sebastian M Waszak, Doured Daghistani, Hugh J. L. Garton, Viveka Nand Yadav, Javad Nazarian, Amy K. Bruzek, Patrick Y. Wen, Sabine Mueller, Tracy T. Batchelor, Sharon Gardner, Jessica R. Cummings, Sriram Venneti, Jonathan Schwartz, Brendan Mullan, Patricia L. Robertson, Li Jiang, Andrea Franson, Yazmin Odia, and Rodrigo Cartaxo

Subjects

Drd2 gene, Cancer Research, Pathology, medicine.medical_specialty, business.industry, Mutant, Clinical Trials: Non-Immunologic, medicine.disease, Oncology, Circulating tumor DNA, Glioma, Troponin I, medicine, Neurology (clinical), Clinical efficacy, business, Predictive biomarker

Abstract

Patients with diffuse midline glioma (DMG) harboring H3 K27M mutation rarely survive longer than two years and have no proven therapies following first-line radiation. ONC201, a bitopic DRD2 antagonist and allosteric ClpP agonist, has shown encouraging efficacy in early phase studies in H3 K27M-mutant DMG. In order to define response rates in H3 K27M DMG patients and to clarify the genomic, anatomic and molecular predictors of response, we performed an integrated pre-clinical and clinical analysis of ONC201 treatment. ONC201 was effective in intra-uterine electroporation (IUE)-generated H3 K27M-mutant murine glioma models with excellent CNS penetration and survival benefit. Patients with H3 K27M-mutant DMG treated with ONC201 on active clinical trials (n=50, 27 thalamic, 23 brainstem) showed an overall survival (OS) of 28.1 (range: 5.9–105) months from diagnosis (enrollment by 4/29/19, data cut-off 12/28/19), compared to historical median OS of 12 months. Median OS for non-recurrent patients has not been reached (n=16, median follow-up: 16.8 from diagnosis). For non-recurrent thalamic patients (n=8), median PFS is 20.1 (range: 9.3–27.6) months from diagnosis (median time on drug: 14.5 months). Best response for thalamic patients by RANO: 1 CR, 5 PR, 7 SD, 8 PD, 6 not reported. Decreased H3 K27M cell-free tumor DNA in plasma and CSF at 6 months correlated with long-term response. Baseline tumor gene expression profiling in patients treated with ONC201 (n=14) identified EGFR and the cortical developmental transcription factor FOXG1 as the strongest biomarkers of radiographic response to ONC201. Analysis of 541 ONC201-treated human cancer cell lines from DepMap, provided evidence for an EGFR-dependent ONC201 resistance mechanism. Analysis of 38 glioma cell lines further supports FOXG1 as a glioma-specific predictive biomarker of ONC201 response. The unprecedented survival results and radiographic responses to ONC201 in H3K27M DMG make a compelling case for later phase and combinatorial studies.

Published

2020

24. CTNI-37. EFFICACY OF ONC201 IN PATIENTS WITH ONC201 FOR RECURRENT H3 K27M-MUTANT DIFFUSE MIDLINE GLIOMA

Author

Rebecca Harrison, Tracy T. Batchelor, Guangrong Lu, Andrew B. Lassman, Patrick Y. Wen, Rohinton Tarapore, Minesh P. Mehta, Lindsay Kilburn, John de Groot, Yoshie Umemura, Timothy F. Cloughesy, Karan Dixit, Nicole Shonka, Andrew S. Chi, Jerome J. Graber, Joshua E. Allen, Isabel Arrillaga-Romany, Nicholas Butowski, Lynne Taylor, Phioanh Nghiemphu, Yazmin Odia, Ashley Sumrall, and Sylvia Kurz

Subjects

Cancer Research, Pathology, medicine.medical_specialty, business.industry, Thalamus, Clinical Trials: Non-Immunologic, Fluid-attenuated inversion recovery, Spinal cord, medicine.disease, medicine.anatomical_structure, Cerebrospinal fluid, Oncology, Glioma, Troponin I, medicine, Neurology (clinical), Progression-free survival, business, Dexamethasone, medicine.drug

Abstract

H3 K27M-mutant diffuse midline gliomas (DMG) have a dismal prognosis. We report an integrated analysis for ONC201, a DRD2 antagonist and ClpP agonist, in patients with recurrent H3 K27M DMG administered as monotherapy in 3 clinical studies (NCT03295396, n=20; NCT02525692, n=6; or expanded access, n=4) by independent, central radiology review among 30 patients. At baseline, patients had measurable contrast-enhancing disease by RANO criteria, KPS>60, and were >90 days from prior radiation. Patients with primary lesions that involved the pons or spinal cord or had evidence of leptomeningeal or cerebrospinal fluid dissemination were excluded. ONC201 was orally administered at 625 mg (scaled by body weight for patients < 18 years old) weekly in 29 patients and every 3 weeks in 1 patient. Median age was 31 years (range 8–70; two patients < 18). There were 16 women and 14 men. Tumors were predominantly thalamic (73%), with other locations including the cerebellum (5%), brainstem (non-pontine) (3%), basal ganglia (3%), and midbrain (3%). Median time from prior radiation was 7.5 months. The most frequent drug-related adverse events were low grade nausea (10%) and fatigue (10%). Nine patients (30%) had >50% regression of T1 contrast enhancement and 11 (36.7%) patients had regression of T2/FLAIR. Objective response rate and progression-free survival by RANO criteria, as well overall survival will be reported. Among 8 patients with sustained radiographic regressions, 6 were tapered off dexamethasone and 4 had improvement in KPS. Five patients (16.7%) remain on treatment with a median of 9.5 months (range 7.3–12). In conclusion, single agent ONC201 is well tolerated and clinically active in recurrent H3 K27M DMG patients.

Published

2020

25. CTIM-13. CLINICAL EFFICACY OF MDNA55, AN INTERLEUKIN-4 RECEPTOR TARGETED IMMUNOTHERAPY, IN RECURRENT GBM DELIVERED BY CONVECTION ENHANCED DELIVERY (CED)

Author

Manish K. Aghi, Sajeel Chowdhary, Seunggu J. Han, Fahar Merchant, Melissa Coello, Nina Merchant, Martin Bexon, John Floyd, Chandtip Chandhasin, Achal S. Achrol, Krystof Bankiewiecz, Benjamin M. Ellingson, Frank D. Vrionis, John Sampson, Santosh Kesari, Andrew Brenner, Michael A. Vogelbaum, Nicholas Butowski, Miroslaw Zabek, Dina Randazzo, and Steven Brem

Subjects

Cancer Research, Tumor microenvironment, business.industry, medicine.medical_treatment, Immunotherapy, Institutional review board, medicine.disease, Clinical Trials: Immunologic, Progressive Neoplastic Disease, Oncology, Interleukin-4 receptor, Cancer research, medicine, Neurology (clinical), Clinical efficacy, Convection-Enhanced Delivery, Myelofibrosis, business

Abstract

BACKGROUND MDNA55 is an IL4R-targeted toxin in development for GBM, a universally fatal disease. IL4R is over-expressed in GBM, the tumor microenvironment, and high expression is associated with poor outcomes in GBM. METHOD MDNA55-05 is an open-label, single-arm study of MDNA55 delivered by CED as a single treatment in rGBM patients at 1st or 2nd recurrence with an aggressive form of GBM (de novo GBM, IDH wild-type, not-resectable at recurrence, ~ 50% expressing high levels of IL4R). Primary endpoint is mOS, secondary endpoint includes impact of IL4R status on mOS. A Synthetic Control Arm (SCA) served as an external comparator constructed from patient registries at neurosurgery centers under IRB-approved protocols. Propensity score weighting corrected for imbalances in baseline characteristics between the two groups. RESULTS MDNA55 showed an acceptable safety profile at doses up to 240μg. In all evaluable subjects (n=44) mOS was 11.6 and OS-12 was 46%. A sub-population (n=32) consisting of all IL4RHigh subjects + only IL4RLow subjects treated with high dose (median 180µg) showed most benefit: mOS is 15 months, OS-12 is 55%. Tumor control, assessed by mRANO criteria, was seen in 81% (26/32) of this sub-population, including those that had pseudo-progression (15/26). In these subjects, tumor control was associated with longer mPFS (4.7 months) and mOS (15.0 months) than those with progressive disease (mPFS 1.0 month, mOS 7.7 months). Comparison against the SCA demonstrated > 100% increase in mOS: 15.7 months vs 7.2 months (HR 0.52, 95% CI 0.30, 0.91). CONCLUSIONS MDNA55 demonstrates improved survival and tumor control in this study design and has potential to benefit all rGBM patients treated at high dose irrespective of IL4R expression. There are no approved therapies for rGBM that can extend survival by 50%; the potential for MDNA55 to extend survival by > 100% is promising for this devastating disease.

Published

2020

26. SURG-18. THE IMPACT OF NEUROLOGIC IMPAIRMENTS ON THE RELATIVE BENEFIT OF MAXIMAL EXTENT OF RESECTION IN NEWLY DIAGNOSED IDH-WILD TYPE GLIOBLASTOMA

Author

Yalan Zhang, Simon G Ammanuel, Jason C. Crane, Gayathri Warrier, Marisa Lafontaine, Margaret Wrensch, Jennifer Clarke, Jennie Taylor, Joanna J. Phillips, Anny Shai, Manish K. Aghi, Susan M. Chang, Desmond A. Brown, Mitchel S. Berger, Shawn L. Hervey-Jumper, Nancy Ann Oberheim Bush, Cecilia L Dalle Ore, Terri Rice, John K. Wiencke, Ramin A. Morshed, Nicholas Butowski, Philip V. Theodosopoulos, Annette M. Molinaro, and Yi Lin

Subjects

Oncology, Cancer Research, medicine.medical_specialty, business.industry, Wild type, Newly diagnosed, medicine.disease, Extent of resection, Internal medicine, Surgical Therapies, medicine, Neurology (clinical), business, Glioblastoma

Abstract

BACKGROUND The prognostic importance of maximal resection of contrast enhancing and non-contrast enhancing disease has been established. Nonetheless, glioblastomas exist within the framework of complex neural circuitry serving cognition, movement, and behavior consequential leading to neurological impairments. The prognostic importance of neurological impairments on survival remains poorly understood. METHODS This is a retrospective, single cohort study from UCSF including 316 eligible patients diagnosed over 20 years with 9.6 years of follow-up. All patients underwent surgical resection for newly diagnosed glioblastoma for whom survival, molecular, preoperative and postoperative MRI images, and clinical data were available. All patients had chemoradiation treated IDH-wild-type glioblastoma with available preoperative and 1-month post-surgical resection neurological outcomes. We employed survival models and recursive partitioning (RPA) to investigate multivariate relationships of overall survival (OS). RESULTS Preoperative neurological impairments were present in 75.6% (n= 239) and new post resection impairments were identified in 37.3% (n=117). Univariate analysis confirmed that new postoperative cognitive impairment [HR 7.91, 95% CI 2.47-25.33] and hemiplegia [HR 3.38, 95% CI 0.83-13.67] (not hemiparesis) impact OS. Risk stratified grouping by RPA demonstrated that gross total resection of contrast enhancing tumor in patients with no new postoperative neurological impairments confers the longest OS (median OS 27.1 months 95%CI 21.5-33.7). Patients with any residual tumor volume after surgery but no new neurological deficits experience a similar survival to younger patients (under 65) with 1 or more new postoperative neurological deficits (median OS 16.6 months 95%CI 15.2-19.2). Shortest OS is identified in patients with any volume of residual tumor plus 1 or more new postoperative neurological deficits and age over 65 (median OS 11.4 months, 95%CI 9.3-13.5). CONCLUSIONS This study confirms that new postoperative neurological impairments impact overall survival in patients with chemoradiation treated IDH-wild-type glioblastoma.

Published

2020

27. COVD-31. THE STATE OF NEURO-ONCOLOGY DURING THE COVID-19 PANDEMIC: A WORLDWIDE ASSESSMENT

Author

Martin J. van den Bent, David Schiff, Gelareh Zadeh, Erin Dunbar, Farshad Nassiri, Sameer Agnihotri, Alyx B. Porter, Katherine B. Peters, Monika E. Hegi, Terri Armstrong, Jeffrey S. Wefel, Shawn L. Hervey-Jumper, Alvina Acquaye, Michael Lim, Jennie Taylor, Quinn T. Ostrom, Nicholas Butowski, Susan M. Chang, Kathy Oliver, Scott L. Coven, Chas Haynes, Milan G. Chheda, Shelley M. Pressley, Maciej M. Mrugala, and Alissa A. Thomas

Subjects

Cancer Research, Telemedicine, medicine.medical_specialty, Coronavirus disease 2019 (COVID-19), business.industry, Standard treatment, education, Affect (psychology), Clinical trial, Oncology, Family medicine, Pandemic, AcademicSubjects/MED00300, Medicine, Anxiety, AcademicSubjects/MED00310, Neurology (clinical), Salary, Covid-19 and Neuro-Oncology, medicine.symptom, business

Abstract

To assess the impact of the pandemic on the field, we performed an international web-based survey of practitioners, scientists, and trainees from 21 neuro-oncology organizations across 6 continents from April 24 through May 17. Of 582 respondents, 258 (45%) were in the US, and 314 (55%) were international. 80.4% were affiliated with academic institutions. 94% respondents reported changes in clinical practice; 95% reported conversion to telemedicine for at least some appointments. However, almost 10% practitioners felt the need to see patients in person specifically because of billing concerns and perceived institutional pressure. Over 50% believed neuro-oncology patients were at increased risk of contracting COVID-19. 67% practitioners suspended enrollment for at least one clinical trial: 53% suspended phase II and 62% suspended phase III trial enrollment. 71% clinicians feared for their or their families’ safety, specifically because of their clinical duties. 20% percent said they did not have enough PPE to work safely; about the same percentage were unhappy with their institutions’ response to the pandemic. 43% believed the pandemic would negatively affect their academic career, and 52% fellowship program directors were worried about losing funding for their training programs. While 69% respondents reported increased stress, 44% were offered no psychosocial support. 37% had their salary reduced. 36% researchers had to temporarily close their laboratories. In contrast, the pandemic created positive changes in perceived patient and family satisfaction, quality of communication, and use of technology to deliver care and interactions with other practitioners. CONCLUSIONS: The pandemic has altered standard treatment schedules and limited investigational treatment options for patients. In some cases, clinicians felt institutional pressure to continue conducting billable in-person visits when telemedicine visits would have sufficed. A lack of institutional support created anxiety among clinicians and researchers. We make specific recommendations to guide clinical and scientific infrastructure moving forward.

Published

2020

28. CTNI-38. PAMIPARIB IN COMBINATION WITH RADIATION THERAPY (RT) AND/OR TEMOZOLOMIDE (TMZ) IN PATIENTS WITH NEWLY DIAGNOSED (ND) OR RECURRENT/REFRACTORY (R/R) GLIOBLASTOMA (GBM); PHASE 1B/2 STUDY UPDATE

Author

Tobias Walbert, Kent C. Shih, Manmeet S Ahluwalia, James Battiste, Ingo K. Mellinghoff, Michael Badruddoja, Amandeep Kalra, David Schiff, Dawit Aregawi, Vanitha Ramakrishnan, Katie Wood, Jian Campian, Jon Glass, Vinay K. Puduvalli, Michael Weller, Timothy F. Cloughesy, Howard Colman, Nicholas Butowski, Patrick Y. Wen, Kathy Zhang, Martin J. van den Bent, Anna F. Piotrowski, and Michael Pearlman

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Temozolomide, business.industry, medicine.medical_treatment, Clinical Trials: Non-Immunologic, O-6-methylguanine-DNA methyltransferase, medicine.disease, Radiation therapy, Refractory, Internal medicine, Troponin I, medicine, Neurology (clinical), Progression-free survival, Adverse effect, business, Febrile neutropenia, medicine.drug

Abstract

Pamiparib, an investigational, oral PARP 1/2 inhibitor, demonstrated preclinical brain penetration and synergistic cytotoxicity with TMZ. We report updated safety and antitumor data for pamiparib plus RT and/or TMZ in ND-GBM or R/R-GBM (SNO 2019, ACTR-39). This dose-escalation/expansion study includes three arms: A, pamiparib (2, 4, or 6 weeks) plus RT (6–7 weeks) in ND-GBM with unmethylated MGMT promoter (unmethylated-GBM); B, pamiparib (6 weeks) plus RT and increasing TMZ doses in Weeks 1 and 5 of RT in unmethylated ND-GBM; and C, pamiparib plus increasing TMZ doses in methylated/unmethylated R/R-GBM. Most patients in Arms A (expansion) and B received maintenance pamiparib plus TMZ after post-RT rest period at Arm C expansion. As of April 10, 2020, enrollment was complete (N=116; A, n=60; B, n=9; C, n=47). Median study follow-up was 11.3 mo (A/B) and 7.1 mo (C). Common grade ≥3 AEs were anemia (10%) in Arm A; decreased neutrophil and white blood cell count (each 22%) in B; anemia, fatigue, and decreased lymphocyte count (each 11%) in C. Brain edema (A) and pneumonia (C) (n=1 each) were fatal treatment-unrelated AEs. In ND-GBM, modified disease control rate (DCR following post-RT rest period) was 69.8% (95% CI, 55.7–81.7) overall, 68.8% (50.0–83.9) in A, and 80.0% (28.4–99.5) in B. Median duration of response was 5.1 mo (overall), 3.8 mo (A), and NE (B). In Arms A/B, median progression-free survival (PFS) and median overall survival (OS) were 4.4 mo and 12.7 mo, respectively; 12-mo OS rate, 54% (95% CI, 40–66). In R/R-GBM (Arm C), confirmed ORR was 9.1% (95% CI, 2.5–21.7); median PFS and OS were 1.9 mo and 7.3 mo, respectively; 6-mo PFS rate, 19% (95% CI, 9–32). These results showed a manageable safety profile for pamiparib +/- RT +/-TMZ; response and survival results support further evaluation of these combinations in GBM.

Published

2020

29. RTID-09. A RANDOMIZED, DOUBLE-BLINDED, PHASE 3 STUDY OF ENZASTAURIN ADDED TO TEMOZOLOMIDE DURING AND FOLLOWING RADIATION THERAPY IN NEWLY DIAGNOSED GLIOBLASTOMA PATIENTS WHO POSSESS THE NOVEL BIOMARKER, DGM1

Author

Thomas Heineman, Nicholas Butowski, Isabel Han, Wen Luo, Theresa Dewitt, Lan Ge, Wilson Wu, Ying Mao, and Daniel Pertschuk

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Temozolomide, Double blinded, business.industry, medicine.medical_treatment, Phases of clinical research, Newly diagnosed, medicine.disease, Randomized Trials in Development, Radiation therapy, chemistry.chemical_compound, Enzastaurin, chemistry, Internal medicine, medicine, Biomarker (medicine), Neurology (clinical), business, medicine.drug, Glioblastoma

Abstract

BACKGROUND Limited progress has been made in improving therapeutic outcomes for glioblastoma (GBM) patients. Enzastaurin (enza) is an oral PKC-β inhibitor that suppresses signaling through the PKC and PI3K/AKT pathways. Although enza did not significantly improve survival in a prior Phase 1/2 study, we have identified a novel genomic biomarker, DGM1, that may predict a response to enza in GBM. PRIMARY OBJECTIVE To assess whether enza added to temozolomide and radiation therapy (RT) improves overall survival (OS) in newly diagnosed GBM patients who possess the DGM1 biomarker. POPULATION Adults with newly diagnosed GBM regardless of DGM1 status who have undergone surgical resection and are candidates for chemoradiation. Approximately 318 patients will be enrolled. DGM1 status will be determined prior to analysis. DESIGN This is a randomized, double-blinded, placebo-controlled study. Patients will be stratified by MGMT and IDH1 status and by geographic region. Treatment will be divided into 3 phases. In the Concurrent Phase (6 weeks), patients will receive RT plus temozolomide and either enzastaurin or placebo. Patients will then enter the Single-Agent Phase and receive either enza or placebo (21-35 days). Then, patients will enter the Adjuvant Phase and receive temozolomide with either enza or placebo (6-12 cycles) followed by enza or placebo alone (to 24 cycles total). ANALYSIS The primary efficacy endpoint of OS will be analyzed using stratified log-rank test for all DGM1-positive randomized patients. The study has approximately 90% power to detect a HR of 0.63 assuming 196 OS events based on a 2.5% one-sided false positive error rate. Statistical significance would be achieved with an estimated observed HR < 0.76. Safety evaluation will include all patients receiving at least one dose of enza or placebo. If OS in DGM1-positive patients is statistically significant, OS in the overall population will be assessed.

Published

2020

30. ACTR-34. SINGLE AGENT ONC201 IN PREVIOUSLY-TREATED, PROGRESSIVE ADULT H3 K27M-MUTANT GLIOMA

Author

Isabel Arrillaga-Romany, Patrick Y. Wen, Yoshie Umemura, Timothy F. Cloughesy, John DeGroot, Erik P. Sulman, Andrew B. Lassman, Tracy T. Batchelor, Andrew S. Chi, Rohinton Tarapore, Rebecca Harrison, Nicholas Butowski, Nicole Shonka, Joshua E. Allen, P Leia Nghiemphu, Krystal Merdinger, Sylvia Kurz, Minesh P. Mehta, Ashley Sumrall, Fabio M. Iwamoto, Yazmin Odia, and Wolfgang Oster

Subjects

Drd2 gene, Cancer Research, business.industry, Treatment outcome, Mutant, Cancer, medicine.disease, Oncology, Dopamine receptor, Adult Clinical Trials - Non-Immunologic, Glioma, Cancer research, Medicine, Single agent, Neurology (clinical), business, Previously treated

Abstract

H3 K27M-mutant gliomas often manifest as midline gliomas, have a dismal prognosis, and have no established or effective treatments at recurrence. ONC201 is the first clinical bitopic DRD2 antagonist/ClpP agonist and is under evaluation in Phase II trials for gliomas and other cancers. We previously reported in vitro studies suggesting dysregulated dopamine receptor expression and enhanced ONC201 sensitivity among H3 K27M-mutant gliomas. Following these observations, adults with midline H3 K27M-mutant glioma patients were enrolled to a dedicated Phase II clinical trial (NCT03295396), a multi-arm Phase II trial (NCT0252569), and expanded access protocols under the Sponsor’s IND. An integrated radiographic analysis with an objective response rate primary endpoint in patients who received ONC201 monotherapy with confirmed H3 K27M-mutant glioma (not primarily in the pons or spinal cord and without leptomeningeal spread) that was progressive and measurable disease by RANO criteria, >90 days from completion of prior radiation, and had KPS >60. As of December 15, 2018, 15 patients have received single agent ONC201 who meet these criteria (n=9 NCT03295396; n=5 NCT0252569; n=1 expanded access). ONC201 was orally administered at 625 mg weekly, except for one patient dosed once every 3 weeks. As midline gliomas can exhibit a mixture of contrast-enhancing and non-contrast-enhancing disease, objective response was assessed by blinded independent central review using RANO-HGG and RANO-LGG criteria for each patient. Best response to date by RANO-HGG criteria is at least 27%: 1 CR, 3 PR, 7 SD, and 4 PD; by RANO-LGG is at least 36%: 1 CR, 1 PR, 3 minor response (MR), 4 SD, 5 PD, 1 unevaluable. By RANO-HGG, median onset of response is 2.6 months (range 1.3–3.4); median duration of response has not been reached with a median follow-up of 7.7 months (range 1.8–29.8). Updated radiographic response, pharmacodynamics, safety, and other clinical outcomes will be reported.

Published

2019

31. RTHP-33. A SINGLE INSTITUTION RETROSPECTIVE ANALYSIS ON SURVIVAL BASED ON TREATMENT PARADIGMS FOR PATIENTS WITH ANAPLASTIC OLIGODENDROGLIOMA

Author

Nancy Ann Oberheim-Bush, Jennie Taylor, Yalan Zhang, Susan M. Chang, Michael D. Prados, Jacob S. Young, Jennifer Clarke, Mitchel S. Berger, Nicholas Butowski, and Annette M. Molinaro

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Univariate analysis, Temozolomide, business.industry, medicine.medical_treatment, Anaplastic oligodendroglioma, Radiation Therapy, medicine.disease, Chemotherapy regimen, Radiation therapy, Glioma, Internal medicine, medicine, Retrospective analysis, Neurology (clinical), Single institution, business, medicine.drug

Abstract

Anaplastic oligodendrogliomas are a type of high grade glioma defined molecularly by the 1p19q co-deletion. Currently, there is no curative therapy, and some studies have estimated median survival is estimated to be approximately 5 years. Current standard of care includes surgical resection followed by radiation and chemotherapy. However, the benefit of up-front radiation with chemotherapy compared to chemotherapy alone following surgical resection has not been shown in a randomized control trial. Given the long-term cognitive consequences of radiation therapy and the high percentage of patients who lives beyond 15 years with AO, there is an effort to balance longevity with radiation toxicity. As such we performed a retrospective single institution analysis of survival of patients with anaplastic oligodendroglioma over 20 years. 159 patients were identified as diagnosed with an anaplastic oligodendroglioma between 1996–2016. Of those, 57 patients were found to have anaplastic olidodendroglioma at original diagnosis and had long term follow-up. Sixty-six percent of patients were between the ages of 30–50 and mean KPS was 87.3. At the time of analysis, 33% of patients had died. In this cohort, 60% of patients were initially treated with radiation and chemotherapy (either temozolomide or CCNU) at diagnosis and 40% were treated with chemotherapy alone. Median overall survival for the entire cohort was 142 months. The related risk of progression in the upfront chemotherapy only group is approximately 5.87 times higher than the patients who received radiation and chemotherapy (Hazard ratio=5.87, 1.92–17.90, p=0.002). However, there was no significant difference in overall survival in patients treated with upfront chemotherapy compared to patients treated upfront with chemotherapy and radiation (p=0.14). On univariate analysis, there was no association between age, KPS, EOR, or upfront vs. delayed radiation and survival. As such initial treatment with chemotherapy alone may be an option for some patients with anaplastic oligodendroglioma.

Published

2019

32. THER-01. PRECLINICAL DEVELOPMENT OF EO1001, A NOVEL IRREVERSIBLE BRAIN PENETRATING PAN-ErbB INHIBITOR

Author

Neil Sankar, Dennis Brown, Francis J. Giles, C. David James, Harry Pedersen, Sarath Kanekal, Nicholas Butowski, Zhen Zhong Wang, Wang Shen, Jann N. Sarkaria, Theodore Nicolaides, and Jeffrey A. Bacha

Subjects

Abstracts, ErbB Receptors, Hypokinesia, business.industry, ErbB, Cancer research, medicine, Medical Therapy (Chemotherapy, Targeted Therapy/Immunotherapy), medicine.symptom, Signal transduction, skin and connective tissue diseases, business

Abstract

Dysregulation of ErbB-mediated signaling is observed in up to 90% of solid tumors. ErbB family cross-talk is implicated in the development of resistance and metastasis, including CNS metastases. Inhibition of multiple ErbB receptors may result in improved patient outcomes. EO1001 is a novel, patented, oral, brain-penetrating, irreversible pan-ErbB inhibitor targeting EGFR (ErbB1), HER2 (ErbB2) and HER4 (ErbB4). METHODS: (1) In vitro testing. EO1001 demonstrates high specificity for the ErbB family of receptors with excellent, balanced equipotent activity against EGFR, HER2 and HER4 (0.4 to 7.4 nM). EO1001 inhibits signaling downstream of wild type EGFR, mutant EGFR (T790M, L858R and d746-750) and HER2. (2) PK and toxicity. In rodent studies in vivo, EO1001 exhibited a half-life of 16–20 hours. EO1001 rapidly enters the CNS and penetrates tumor tissue at higher concentrations relative to plasma. Safety of EO1001 was evaluated by repeat-dosing studies in SD rats and beagle dogs. Toxicities typical of the ErbB inhibitor class, including gastro-intestinal effects, weight loss and decreased activity were observed at higher dose groups in both species. Mortality was observed in SD rats at higher dose groups. (3) In vivo efficacy studies. EO1001 was studied following oral administration in several erbB-positive mouse xenograft models including N87 (Her2+), H1975 (EGFR/T790M), GBM12 (EGFR+), GBM39 (EGVRvIII+). Following oral administration, treatment with EO1001 resulted in a statistically significant improvement in outcomes compared to positive and negative controls in both CNS and systemic tumor models. EO1001 was well-tolerated with no gastrointestinal side effects observed at efficacious doses in these models. CONCLUSION: Based on research to date, EO1001 has the potential to be a best-in-class CNS-penetrating pan-ErbB inhibitor with a safety and pharmacokinetic profile amenable for use as a single agent and in combination with other agents. EO1001 is poised to enter phase 1-2a clinical testing in the second-half of 2019.

Published

2019

33. The effects of anti-angiogenic therapy on the formation of radiation-induced microbleeds in normal brain tissue of patients with glioma

Author

Annette M. Molinaro, Susan M. Chang, Sarah J. Nelson, Emma Essock-Burns, Janine M. Lupo, Nicholas Butowski, and Soonmee Cha

Subjects

Male, Oncology, Cancer Research, Pathology, Indoles, Angiogenesis, medicine.medical_treatment, Angiogenesis Inhibitors, Brain tissue, radiation therapy, 030218 nuclear medicine & medical imaging, anti-angiogenic therapy, chemistry.chemical_compound, 0302 clinical medicine, Enzastaurin, glioma, Medicine, Cancer, Neovascularization, Pathologic, medicine.diagnostic_test, Brain Neoplasms, Glioma, treatment effects, Middle Aged, Magnetic Resonance Imaging, Treatment Outcome, 030220 oncology & carcinogenesis, Susceptibility weighted imaging, Female, Adult, medicine.medical_specialty, Oncology and Carcinogenesis, Clinical Investigations, 03 medical and health sciences, Rare Diseases, Clinical Research, Internal medicine, Humans, Oncology & Carcinogenesis, Neovascularization, Aged, Cerebral Hemorrhage, Pathologic, Radiotherapy, business.industry, Neurosciences, Magnetic resonance imaging, medicine.disease, Brain Disorders, Brain Cancer, Radiation therapy, susceptibility-weighted imaging, chemistry, Concomitant, microbleeds, Neurology (clinical), business

Abstract

Background. Radiotherapy (RT) is an integral component in managing patients with glioma, but the damage it may cause to healthy brain tissue and quality of life is of concern. Susceptibility-weighted imaging (SWI) is highly sensitive to the detection of microbleeds that occur years after RT. This study’s goals were to characterize the evolution of radiation-induced microbleeds in normal-appearing brain and determine whether the administration of an anti-angiogenic agent altered this process. Methods. Serial high-resolution SWI was acquired on 17 patients with high-grade glioma between 8 months and 4.5 years posttreatment with RT and adjuvant chemotherapy. Nine of these patients were also treated with the anti-angiogenic agent enzastaurin. Microbleeds were identified as discrete foci of susceptibility not corresponding to vessels, tumor, or postoperative infarct, and counted in normal-appearing brain. Analysis of covariance was performed to compare slopes of regression of individual patients’ microbleed counts over time, Wilcoxon rank-sum tests examined significant differences in rates of microbleed formation between groups, and linear and quadratic mixed-effects models were employed. Results. The number of microbleeds increased with time for all patients, with initial onset occurring at 8– 22 months. No microbleeds disappeared once formed. The average rate of microbleed formation significantly increased after 2 years post-RT (P , .001). Patients receiving anti-angiogenic therapy exhibited fewer microbleeds overall (P , .05) and a significant reduction in initial rate of microbleed appearance (P ¼ .01). Conclusions. We have demonstrated a dramatic increase in microbleed formation after 2 years post-RT that was decelerated by the concomitant administration of anti-angiogenic therapy, which may aid in determining brain regions susceptible to RT.

Published

2015

34. PATH-05. IMPLEMENTATION OF A TARGETED NEXT-GENERATION SEQUENCING PANEL FOR THE DIAGNOSIS AND PRECISION MEDICINE TREATMENT OF ADULT PATIENTS WITH WHO GRADE IV DIFFUSE GLIOMAS

Author

Nancy Ann Oberheim Bush, Jennifer Clarke, Mitchel S. Berger, Yalan Zhang, Nicholas Butowski, Joanna J. Phillips, Tarik Tihan, Annette M. Molinaro, Shawn L. Hervey-Jumper, Arie Perry, Jennie Taylor, Philip V. Theodosopoulos, Manish K. Aghi, Melike Pekmezci, Susan M. Chang, Andrew W. Bollen, David A. Solomon, and Michael W. McDermott

Subjects

Cancer Research, medicine.medical_specialty, Adult patients, business.industry, Who grade, Precision medicine, DNA sequencing, Abstracts, Oncology, Path (graph theory), Medicine, Medical physics, Neurology (clinical), business, neoplasms

Abstract

BACKGROUND: Analysis of tumors via next-generation sequencing is now routinely used in clinical practice. The UCSF500 NGS panel became available starting in June 2015. In Dec 2017, a glioblastoma precision medicine initiative started at our institution to sequence all newly-diagnosed WHO grade IV diffuse gliomas. We review our experience over a 3-year period. METHODS: The UCSF500 Cancer Panel assesses approximately 500 cancer-associated genes for mutations, copy number alterations, and structural rearrangements, including fusions. The test can be run on tumor DNA alone or compared with normal DNA, allowing for discrimination of germline variants. Sequencing results are analyzed by a neuropathologist with genomics expertise (D.A.S.). Results from the 165 adult WHO grade IV diffuse glioma cases sequenced to date were analyzed, including 136 glioblastomas, IDH-wildtype; 19 glioblastomas, IDH-mutant; and 10 diffuse midline gliomas, H3 K27M-mutant. RESULTS: Among the 136 IDH-wildtype glioblastomas, the most common alterations were in TERT, EGFR, CDKN2A, PTEN, NF1, TP53, PIK3R1, PDGFRA, CDK4, MDM2, LZTR1, and STAG2. Among the 19 IDH-mutant glioblastomas, the most common additional alterations were in TP53, ATRX, CDKN2A, and PDGFRA. Paired germline sequencing was performed on 71 patients, ten of which were found to harbor a germline mutation associated with increased cancer risk, including the CHEK2, MSH2, and NF1 genes. Somatic hypermutation was present in nine cases, four at initial resection and five at recurrence with a temozolomide-associated mutational signature. Among the four treatment-naïve glioblastomas with hypermutation, two were Lynch syndrome-associated in patients with damaging germline mutations in MSH2, and two were sporadic tumors that harbored somatic mutations in mismatch repair genes. CONCLUSIONS: Genomic profiling in adult glioblastoma patients results in identification of potentially actionable genetic alterations and also previously unknown germline mutations associated with increased cancer risk. A subset of glioblastomas (approximately 5%) harbor somatic hypermutation, indicating potential utility of immune checkpoint inhibition.

Published

2018

35. ATIM-05. INTRATUMORAL DELIVERY OF MDNA55, AN INTERLEUKIN-4 RECEPTOR TARGETED IMMUNOTHERAPY, BY MRI-GUIDED CONVECTIVE DELIVERY FOR THE TREATMENT OF RECURRENT GLIOBLASTOMA

Author

Fahar Merchant, Krystof S. Bankiewicz, Martin Bexon, Achal S. Achrol, Nicholas Butowski, Andrew Brenner, Michael A. Vogelbaum, Dina Randazzo, Santosh Kesari, Rosemina Merchant, John Sampson, and Miroslaw Zabek

Subjects

Cancer Research, Tumor size, business.industry, Recurrent glioblastoma, medicine.medical_treatment, Immunotherapy, medicine.disease, Targeted immunotherapy, Abstracts, Oncology, Interleukin-4 receptor, Cancer research, Medicine, Neurology (clinical), business, Mri guided, Interleukin 4, Glioblastoma

Abstract

While intratumoral delivery of immunotherapies allows for targeted distribution and minimal systemic toxicity, optimal spatial distribution of therapeutic agents remains a challenge. MR-guided convection-enhanced delivery of MDNA55, interleukin-4 cytokine fused to Pseudomonas exotoxin, is currently being explored in a Phase 2 open label study in up to 52 patients with recurrent glioblastoma. MDNA55 is coinfused with a Gadolinium-based contrast agent (GdDTPA) and delivered as a single infusion using implantable flexible catheters. MRI was employed to monitor initial infusion, allowing adjustment of catheter depth as needed. The bulk of the delivery was performed outside the MRI scanner while patients were awake. MRI confirmation of distribution was performed within 4 hours post-infusion. Here we report preliminary results of tumor distribution in 23 subjects. Total volume of MDNA55 (ranging from 12 mL to 66 mL) was initially administered to subjects (n=12) based on tumor size. This achieved a mean coverage of 75% (range 46 – 94%) with 17% showing volume of distribution > 100 mL. Review by the Safety Committee determined that improvements to drug distribution could be further enhanced by moving to a fixed volume of 60 mL administered via 4 catheters and allowing placement outside the peritumoral area if necessary. Treatment in the next 11 subjects showed that infusion volumes exceeding 40 mL and placement of catheters outside the enhancing tumor led to increased volumes of drug distribution (45% showed volume of distribution > 100 mL) but did not improve the target percentage coverage of the tumor (mean 60%, range 22 – 97%) and its immediate penumbra. Therefore, under the current protocol version, all subjects are receiving individualized volume of MDNA55 (according to tumor size), but not exceeding 40 mL. Further optimization is underway to ensure adequate coverage and improve drug distribution.

Published

2018

36. QOLP-24. ATTITUDES TOWARD FERTILITY AND FERTILITY PRESERVATION IN WOMEN WITH GLIOMA

Author

E.E. Niemasik, Susan M. Chang, Rachel Stiner, Michael D. Prados, Nikita Sinha, Nicholas Butowski, Jane Rabbitt, Jennifer Clarke, Jessica L. Chan, Joseph M. Letourneau, and Mitchell P. Rosen

Subjects

Abstracts, Cancer Research, Oncology, media_common.quotation_subject, Glioma, medicine, Fertility, Neurology (clinical), Fertility preservation, Biology, medicine.disease, media_common, Demography

Abstract

BACKGROUND: No studies have examined the fertility priorities of women undergoing treatment for glioma. Glioma patients frequently undergo chemotherapy as part of their treatment, however it is unknown whether patients are aware of the possible effects of treatment on their fertility. Our objective was to assess the fertility priorities of glioma patients and ascertain whether female glioma patients are being effectively counseled on the effects of chemotherapy on fertility prior to beginning treatment. METHODS: The sample was composed of female patients from the Neuro-oncology clinic of the University of California, San Francisco. Participants completed a cross-sectional survey between October 2010 and December 2013 exploring their attitudes toward fertility and their experience with fertility counseling prior to chemotherapy initiation. RESULTS: Seventy-two women completed the survey. Analysis of the survey results showed that 30% of women receiving chemotherapy reported having a discussion regarding fertility preservation prior to beginning treatment. Of those who reported having this discussion, 80% were aware that chemotherapy could negatively affect their fertility. Many women reported that while fertility preservation was not important to them at the time of diagnosis, it was a priority for them at the time of survey completion. Although interest in having children tended to decrease after cancer treatment, the majority of respondents reported desiring a child after treatment. CONCLUSIONS: The data obtained in this study suggest a lack of understanding of reproductive priorities which may be addressed with a more comprehensive fertility discussion prior to beginning treatment.

Published

2018

37. PATH-09. CLINICAL CHARACTERISTICS OF ADULTS WITH H3 K27M-MUTANT GLIOMAS AT UCSF

Author

Robin A. Buerki, Sarah Lapointe, Nancy Ann Oberheim Bush, David A. Solomon, Jennie Taylor, Arie Perry, Joanna J. Phillips, Susan M. Chang, Nicholas Butowski, Jennifer Clarke, Annette M. Molinaro, and Javier Villanueva-Meyer

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Temozolomide, business.industry, Treatment outcome, Mutant, medicine.disease, Abstracts, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Glioma, medicine, 030212 general & internal medicine, Neurology (clinical), business, 030217 neurology & neurosurgery, medicine.drug, Glioblastoma

Abstract

BACKGROUND: Histone H3.3 or H3.1 mutant protein is commonly expressed in pediatric and adult diffuse midline gliomas, including diffuse intrinsic pontine gliomas (DIPGs), and portends a poor prognosis, regardless of histologic features. As such, “Diffuse midline glioma, H3-K27M-mutant” (DMG-H3K27M) was added to the 2016 WHO Classification as a grade IV entity. Knowledge of the clinical experience and natural history of this recently defined tumor in adults is limited. METHODS: We retrospectively reviewed the pathology of adult (age ≥ 18) DMG-H3K27Ms diagnosed at our institution either via H3-K27M mutant-specific immunohistochemistry or via the UCSF500 targeted next-generation sequencing panel that includes the H3F3A, HIST1H3B, and HIST1H3C genes. Treatment, outcome, and imaging characteristics were reviewed. RESULTS: We identified 26 adults with DMG-H3K27M and 2 with non-midline-H3K27M. Tumor locations included thalamus/basal ganglia (15), hypothalamus (2), pineal region (1), cerebellum (3), brainstem (2), spinal cord (2), mesial temporal (1), and non-midline sites (2). MRI imaging for 21/25 evaluable cases demonstrated enhancement. Of the 26 DMG-H3K27M cases, median age was 35 years (22–68 years). Of these, 17 patients had biopsy only. Median OS was 41 months (95%-CI 31-NA). In the 22 DMG-H3K27M patients with available clinical treatment data, 21 received radiation (19 with temozolomide) at initial diagnosis. At progression/recurrence, 11 patients received bevacizumab, 5 were re-treated with temozolomide, 8 received other chemotherapy, and 8 received > 1 course of re-irradiation. CONCLUSION: While still poor overall, clinical outcome in adults with DMG-H3K27M is often better than that of pediatric DIPGs and other IDH-wildtype high-grade gliomas, such as glioblastoma. This may reflect a different cell of origin or other distinct biologic differences. Further investigation of both DMG-H3K27M and non-midline H3K27M mutant tumors in adults is warranted to study the genetic and epigenetic features of these rare tumors, as well as optimal treatment strategies.

Published

2018

38. NIMG-47. VOLUMETRIC ANALYSIS OF PHASE 2 AND 3 TRIALS IN RECURRENT GLIOBLASTOMA TREATED WITH VB-111 WITH OR WITHOUT BEVACIZUMAB OR BEVACIZUMAB MONOTHERAPY

Author

Nicholas Butowski, Catalina Raymond, Dror Harats, Jodi Goldman, Andrew Brenner, Yael Cohen, Patrick Y. Wen, Benjamin M. Ellingson, Jacob Schlossman, Timothy F. Cloughesy, Jingwen Yao, Tamar Rachmilewitz Minei, and Caleb Tran

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Bevacizumab, business.industry, Internal medicine, Recurrent glioblastoma, Neuro-Imaging, medicine, Neurology (clinical), business, medicine.drug

Abstract

VB-111 is a non-replicating adenovirus carrying a pro-apoptotic transgene for TNFR1/Fas under the control of a modified murine promoter to pre-proendothelin 1. The transgene is expressed only in angiogenic endothelial cells, and therefore VB-111 results in targeted apoptosis of neovascular vessels. The current study characterizes the quantitative radiographic results and impact on OS in phase 2 and 3 trials of recurrent glioblastoma (GBM) patients treated with VB-111 with or without bevacizumab (BV) or BV monotherapy. MRI data from a phase 2 (NCT01260506) and randomized, double arm, controlled phase 3 (GLOBE; NCT02511405) trial of VB-111 in recurrent GBM were used in current study: Arm A) VB-111 monotherapy until progression followed by combination VB-111 and bevacizumab (BV) (“Primed Combination”; Phase 2; N=24); Arm B) VB-111 in combination with BV (“Unprimed Combination”; Phase 3; N=124); Arm C) BV monotherapy (“Control”; Phase 3; N=120). Contrast enhanced T1-weighted digital subtraction was used to quantify tumor volume at all time points. Baseline tumor volume was prognostic for OS in all treatment groups when controlling for therapy and age (Cox, P< 0.001, HR=1.02). In patients with smaller tumors (< 25mL), the “primed combination” cohort (Arm A) from the phase 2 trial had a significant OS advantage compared to both upfront combination of VB-111 and BV (Arm B; P=0.0094, HR=0.53; median OS = 7 vs. 15mo) as well as BV alone (Arm C; P=0.025, HR=0.58; median OS=8.5 vs. 15mo). Patients with a radiographic response (>65% reduction) had a significant survival difference from non-responders when controlling for age, baseline tumor volume, and treatment arm (P=0.0014, HR=0.58). Responders to VB-111 monotherapy or combination therapy after priming with VB-111 exhibited characteristic, expansive areas of necrosis in areas of initial disease.

Published

2019

39. ATIM-09. CLINICAL TRIAL IN PROGRESS: A STUDY OF NEOADJUVANT AND ADJUVANT VB-111 FOR TREATMENT OF RECURRENT GBM

Author

Tamar Rachmilewitz Minei, Timothy F. Cloughesy, Dror Harats, Patrick Y. Wen, and Nicholas Butowski

Subjects

Clinical trial, Oncology, Cancer Research, medicine.medical_specialty, business.industry, Adult Clinical Trials–Immunologic, Internal medicine, medicine.medical_treatment, medicine, Neurology (clinical), business, Adjuvant

Abstract

BACKGOUND Ofranergene obadenovec (VB-111) is a targeted anti-cancer viral based gene therapy with a dual mechanism: a broad antiangiogenic effect and induction of a tumor directed immune response. Previous study demonstrated a survival benefit for patients with recurrent glioblastoma (rGBM) treated with VB-111 monotherapy that was continued upon progression with combination treatment of VB-111 and bevacizumab. Glioblastoma is an immunologically “cold” microenvironment which fosters immunosuppression and antagonizes anti-tumor immune responses. The role of T-cell infiltration in combating cancer has been increasingly recognized and associated with improved participant outcomes. Based on these observations, this study will assess the hypothesis that neoadjuvant use of VB-111 will lead to a statistically significant increase in tumor infiltrating T lymphocyte (TIL) density within the tumor and enhanced systemic tumor-specific T cell responses. METHODS This is a multicenter, randomized, blinded, placebo-controlled, phase 2 surgical trial to evaluate early immunologic pharmacodynamic parameters for the viral cancer therapy VB-111 in rGBM. 45 participants with rGBM indicated for resection will randomized to one of three treatment arms: Neoadjuvant Arm: intravenous VB-111 prior to resection, and VB-111 every 6 weeks after resection. Adjuvant Arm: placebo prior to resection, and VB-111 every 6 weeks afterwards. The control arm will receive placebo prior to resection followed by standard of care. Upon evidence of contrast-enhancing progression, bevacizumab may be initiated as needed for supportive care and VB-111 will continue until progression is supported at two consecutive time points. Tumor samples will be obtained and archived at the time of surgery, and blood samples will be obtained as pharmacodynamic markers throughout the study to allow DNA sequencing of T cells. The primary endpoint is influence of neoadjuvant VB-111 on TIL density. Other endpoints include safety and tolerability, peripheral T cell response, tumor/microenvironment transcriptomic alteration, and PFS/OS. Study will open for enrolment in 2019.

Published

2019

40. DDIS-33. SELECTIVE AND COMPLETE INHIBITION OF mTORC1 BY BI-STERIC mTOR INHIBITORS DRIVES THERAPEUTIC RESPONSE IN GLIOBLASTOMA

Author

Tomoko Ozawa, William A. Weiss, Qi-Wen Fan, Edward G. Lorenzana, James Aggen, Kevan M. Shokat, Xujun Luo, Ozlem Aksoy, Mallika Singh, Douglas R. Wassarman, Nicholas Butowski, Robin Lea, Z. H. An, Jaqueline A.M. Smith, and David R. Raleigh

Subjects

Cancer Research, Everolimus, biology, Chemistry, P70-S6 Kinase 1, mTORC1, mTORC2, Oncology, Drug Discovery, medicine, Cancer research, biology.protein, PTEN, Neurology (clinical), biological phenomena, cell phenomena, and immunity, Sapanisertib, Mechanistic target of rapamycin, PI3K/AKT/mTOR pathway, medicine.drug

Abstract

Activation of phosphatidylinositol 3-kinase (PI3K)/PTEN pathway and oncogenic signaling via the mechanistic target of rapamycin (mTOR) occur in a majority of high-grade glial brain tumors. Allosteric mTOR inhibitors, such as rapamycin and other rapalogs, incompletely block mTORC1 by reducing phosphorylation of some substrates, including S6K1, but not 4EBP1. In contrast, ATP-competitive inhibitors, such as sapanisertib, fully inhibit mTORC1. However these inhibitors are also active against mTORC2 and lipid kinases, likely enhancing toxicity. A new class of selective mTORC1 inhibitor that interacts with both the ATP- and FKBP12/FRB-binding sites has been developed, which we term ‘bi-steric’. The prototype bi-steric inhibitor, RapaLink-1, blocks phosphorylation of many mTORC1 substrates, including 4EBP1. Importantly, RapaLink-1 showed improved efficacy in glioblastoma models in vivo as compared to rapamycin or sapanisertib (Fan et al., Cancer Cell 2017). Revolution Medicines has developed novel next-generation bi-steric mTORC1-selective inhibitors that exhibit potent and selective (>10-fold) inhibition of mTORC1 over mTORC2 in vitro in cell line models. Two of these compounds, RM-001 and RM-006, showed sustained blockade of mTORC1 signaling, including dephosphorylation of 4EBP1, following weekly ip dosing in an orthotopic U87MG-Luc model of glioblastoma. Repeated weekly administration of these agents resulted in significantly greater anti-tumor efficacy, as assessed via tumor burden (bioluminescence imaging) and overall survival in comparison to daily sapanisertib and the rapalog everolimus, and weekly dosing of the first generation bi-steric RapaLink-1, all at maximally tolerated doses. In summary, our data demonstrate that bi-steric mTORC1 selective inhibitors elict marked anti-tumor efficacy at doses that are well tolerated in a preclinical model of glioblastoma. Our study emphasizes the importance of mTOR as a central target in glioblastoma, and showcases the therapeutic potential of novel and selective clinical bi-steric mTORC1 inhibitors under development as investigational new drugs.

Published

2019

41. SCIDOT-02. A PHASE I STUDY OF CONVECTION-ENHANCED DELIVERY OF LIPOSOMAL-IRINOTECAN (ONIVYDE) USING REAL-TIME IMAGING WITH GADOLINIUM IN PATIENTS WITH RECURRENT HIGH GRADE GLIOMAS: RESULTS THUS FAR

Author

Krystof S. Bankiewicz, Susan M. Chang, Nancy Ann Oberheim Bush, Jennifer Clarke, Jennie Taylor, Manish K. Aghi, Alastair J. Martin, Nicholas Butowski, Mitchell S. Berger, Karishma Kumar, and John Bringas

Subjects

Cancer Research, medicine.medical_specialty, Gliosarcoma, Oligoastrocytoma, medicine.diagnostic_test, business.industry, Gadolinium, chemistry.chemical_element, Magnetic resonance imaging, medicine.disease, Irinotecan, Oncology, chemistry, Abstracts from the 3rd Sno-Scidot Joint Conference on Therapeutic Delivery to the CNS, Glioma, medicine, Medical imaging, Liposomal Irinotecan, Neurology (clinical), Radiology, business, medicine.drug

Abstract

BACKGROUND Chemotherapy for high grade gliomas (HGG) is limited by the blood-brain-barrier (BBB). Convection enhanced delivery (CED) improves chemotherapy delivery by utilizing fluid convection obviating the challenges of crossing the BBB while minimizing systemic toxicity. CED of nanoliposomal-irinotecan (Onivyde) showed to be a superior delivery route for anti-tumor activity in animal models. An advance of this trial is the development and use of real time CED, which utilizes MRI to visualize the CED process with the aid of co-convected contrast agents, monitoring delivery into the brain and affording for corrective action. METHODS This is a 3 + 3 single dose escalation trial with 2 cohorts: 20mg/ml and 40mg/ml. Onivyde and GAD were co-infused via the same catheters in a one-time delivery. The total dose was personalized based on the patient’s tumor volume, and ranged from 20–680 mg of Onivyde, given via up to 4 catheters. Tumor diameters were allowed to be 1 – 4 cm, with injection volumes ranging from 2 – 17 mL of infusate. RESULTS 13 patients have been treated on this protocol, all in under 5 hours. There were 9 GBs, 1 gliosarcoma, 2 AAs, and 1 oligoastrocytoma. Utilizing imaging software, we correlated pre-infusion modeling of the drug distribution with post-infusion imaging. A number of technical challenges were overcome by real time monitoring; the total volume of distribution (Vd), and the Vd to volume infused (Vi) ratio for each infusion was ~2. Of all patients, the only notable AE was encephalopathy, which was resolved. CONCLUSIONS Image-guided distribution allows for safe real-time placement and adjustment of CED cannula of Onivyde into patient’s brains. Such methods allow for maximum tumor coverage and warrant further studies with repeat dosing.

Published

2019

42. LTBK-08. TOCA 511 & TOCA FC VERSUS STANDARD OF CARE IN PATIENTS WITH RECURRENT HIGH GRADE GLIOMA

Author

George J. Kaptain, David Schiff, Nam D. Tran, Alexander Lossos, Ryan Merrell, David W. Macdonald, James Perry, Garth Nicholas, Raphael P. Davis, Karen Fink, J. Bradley Elder, Manmeet Ahluwalia, Tobias Walbert, Michael Salacz, Reid C. Thompson, Fairooz F. Kabbinavar, Jason Heth, Denise Damek, Thian Kheoh, Nina L. Martinez, Timothy F. Cloughesy, Daniela A. Bota, Marshall Pitz, Seema Nagpal, Yaron A. Moshel, Jay-Jiguang Zhu, Do-Hyun Nam, David Picconi, Fabio M. Iwamoto, Clark C. Chen, Nicholas Butowski, Gelareh Zadeh, Joseph Landolfi, Chul-Kee Park, Rohan Ramakrishna, Kevin Petrecca, H. Ian Robins, David Tran, Michael A. Vogelbaum, Steven Brem, Dimitris G. Placantonakis, David Cachia, Chetan Bettegowda, Vivek Mehta, Michael Pearlman, Deborah Heros, and Nimish Mohile

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Temozolomide, Bevacizumab, business.industry, Lomustine, Late Breaking Abstracts, medicine.disease, Chemotherapy regimen, Glioma, Internal medicine, Toca 511 & Toca FC, medicine, Neurology (clinical), business, Survival rate, medicine.drug, Anaplastic astrocytoma

Abstract

BACKGROUND Toca 511 (vocimagene amiretrorepvec) is a cancer-selective, retroviral replicating vector encoding a codon optimized, heat stabilized cytosine deaminase that converts Toca FC (extended-release 5-fluorocytosine, 5-FC) into the anticancer agent 5-fluorouracil. Three Ph1 studies in patients with recurrent high grade glioma have demonstrated a tolerable safety profile and encouraging efficacy. METHODS Toca 5 is a multi-national, randomized, open-label Ph3 trial (NCT02414165) of Toca 511 & Toca FC versus standard of care (SOC) options that comprises Investigator’s choice of single agent chemotherapy (lomustine, temozolomide) or bevacizumab in patients who have undergone resection for first or second recurrence of glioblastoma or anaplastic astrocytoma. 403 patients were randomized 1:1 to the Toca arm or the SOC arm and stratified by IDH1 status, KPS, and geographic region. Primary endpoint was overall survival (OS), and secondary endpoints were durable response rate, durable clinical benefit rate, duration of durable response, and 12-month survival rate. The study used group sequential design including 2 interim analyses and 1 final analysis, and the stratified log-rank test are used for the analysis. RESULTS 271 events were observed for this analysis. Median follow-up was 22.8 months, and the Toca arm missed the primary endpoint (OS) compared to the SOC arm (11.1 months median compared to 12.2 months, HR=1.06, p=0.6154). All secondary endpoints showed no meaningful difference between the arms of the trial. The safety, tolerability and adverse event profile of Toca 511 and Toca FC was as expected for this patient population, with low incidences of Grade 3–4 adverse events. Pre-planned subgroup analyses showed compelling OS improvement in patients with secondary recurrence, and favorable trends in IDH1 mutant and AA population. Detailed data will be presented at the time of the conference.

Published

2019

43. Heat-shock protein peptide complex–96 vaccination for recurrent glioblastoma: a phase II, single-arm trial

Author

Andrew T. Parsa, Susan M. Chang, Rajwant Kaur, Orin Bloch, Jeffrey N. Bruce, Jennifer Clarke, Courtney A. Crane, Mitchel S. Berger, Manish K. Aghi, Michael D. Prados, Andrew E. Sloan, Nicholas Butowski, Michael W. McDermott, and Yelena S. Fuks

Subjects

Male, Oncology, Cancer Research, medicine.medical_treatment, Phases of clinical research, 6.2 Cellular and gene therapies, Heat-Shock Proteins, Cancer, Brain Neoplasms, Vaccination, Middle Aged, Prognosis, Survival Rate, Local, 5.1 Pharmaceuticals, 6.1 Pharmaceuticals, Female, immunotherapy, Development of treatments and therapeutic interventions, Biotechnology, Adult, medicine.medical_specialty, Clinical Trials and Supportive Activities, Oncology and Carcinogenesis, Cancer Vaccines, Vaccine Related, Rare Diseases, Clinical Research, Heat shock protein, Internal medicine, medicine, Humans, Oncology & Carcinogenesis, Progression-free survival, Adverse effect, Survival rate, Neoplasm Staging, Aged, urogenital system, business.industry, Surrogate endpoint, Prevention, glioblastoma, Neurosciences, Evaluation of treatments and therapeutic interventions, Immunotherapy, Brain Disorders, nervous system diseases, Brain Cancer, Neoplasm Recurrence, Emerging Infectious Diseases, Immunology, Immunization, Neurology (clinical), business, Follow-Up Studies

Abstract

BackgroundOutcomes for patients with recurrent glioblastoma multiforme (GBM) are poor and may be improved by immunotherapy. We investigated the safety and efficacy of an autologous heat-shock protein peptide complex-96 (HSPPC-96) vaccine for patients with recurrent GBM.MethodsIn this open-label, single-arm, phase II study, adult patients with surgically resectable recurrent GBM were given vaccine after gross total resection. The primary endpoint was overall survival at 6 months. Secondary endpoints included overall survival, progression-free survival, safety, and immune profiling. Outcome analyses were performed in the intention-to-treat and efficacy populations.ResultsBetween October 3, 2007 and October 24, 2011, 41 patients underwent gross total resection of recurrent GBM and received a median of 6 doses of HSPPC-96 vaccine. Following treatment, 90.2% of patients were alive at 6 months (95% confidence interval [CI]: 75.9-96.8) and 29.3% were alive at 12 months (95% CI: 16.6-45.7). Median overall survival was 42.6 weeks (95% CI: 34.7-50.5). Twenty-seven (66%) patients were lymphopenic prior to therapy, and patients with lymphocyte counts below the cohort median demonstrated decreased overall survival (hazard ratio: 4.0; 95% CI: 1.4-11.8; P = .012). There were no treatment-related deaths. There were 37 serious (grades 3-5) adverse events reported, with 17 attributable to surgical resection and a single grade 3 constitutional event related to the vaccine.ConclusionThe HSPPC-96 vaccine is safe and warrants further study of efficacy for the treatment of recurrent GBM. Significant pretreatment lymphopenia may impact the outcomes of immunotherapy and deserves additional investigation.

Published

2013

44. Using susceptibility-weighted imaging to determine response to combined anti-angiogenic, cytotoxic, and radiation therapy in patients with glioblastoma multiforme

Author

Emma Essock-Burns, Nicholas Butowski, Susan M. Chang, Sarah J. Nelson, Annette M. Molinaro, Janine M. Lupo, and Soonmee Cha

Subjects

Male, Oncology, Cancer Research, Pathology, Indoles, Image Processing, medicine.medical_treatment, response to anti-angiogenic therapy, chemistry.chemical_compound, Computer-Assisted, Enzastaurin, glioma, Antineoplastic Combined Chemotherapy Protocols, Image Processing, Computer-Assisted, Cancer, screening and diagnosis, Brain Neoplasms, Chemoradiotherapy, Middle Aged, Prognosis, Magnetic Resonance Imaging, Dacarbazine, Survival Rate, Detection, Susceptibility weighted imaging, Biomedical Imaging, Female, 4.2 Evaluation of markers and technologies, medicine.drug, Adult, medicine.medical_specialty, Oncology and Carcinogenesis, Clinical Investigations, Rare Diseases, Internal medicine, Temozolomide, medicine, Humans, Oncology & Carcinogenesis, Progression-free survival, Neoplasm Staging, Aged, business.industry, Neurosciences, Brain Disorders, Brain Cancer, Radiation therapy, susceptibility-weighted imaging, chemistry, Concomitant, Neurology (clinical), Glioblastoma, business, Follow-Up Studies

Abstract

BackgroundThe goal of this study was to investigate whether the amount of hypointense signal on susceptibility-weighted imaging within the contrast-enhancing lesion (%SWI-h) on the pretreatment scan could determine response in patients with newly diagnosed glioblastoma multiforme who received external beam radiation therapy with concomitant anti-angiogenic therapy (enzastaurin) and cytotoxic chemotherapy (temozolomide).MethodsTwenty-five patients were imaged before therapy (postsurgical resection) and scanned serially every 2 months until progression. Standard clinical MR imaging and SWI were performed on a 3T scanner. %SWI-h was quantified for each patient's pretreatment scan. Time to progression and death were used to characterize patients into non-, immediate-, and sustained-response groups for both events. Cox proportional hazards models were used to assess the association between %SWI-h and both progression-free survival (PFS) and overall survival (OS). Classification and regression tree analysis were used to determine optimal cutoffs on which to split %SWI-h.ResultsFor both death- and progression-based response categories, %SWI-h was significantly higher in sustained responders than in nonresponders. Cox model coefficients showed an association between %SWI-h and PFS and OS, both in univariate analysis (PFS: hazard ratio [HR] = 0.966, 95% confidence interval [CI] = 0.942-0.988; and OS: HR = 0.945, 95% CI = 0.915-0.976) and when adjusting for baseline KPS, age, sex, and resection extent (PFS: HR = 0.968, 95% CI = 0.940 -0.994; and OS: HR = 0.943, 95% CI = 0.908 -0.976). A cutoff value of 38.1% significantly differentiated patients into 2 groups based on censored OS and into non- and intermediate-response categories based on time to progression.ConclusionsThese early differences suggest that SWI may be able to predict which patients would benefit most from similar combination therapies and may assist clinicians in making important decisions about patient care.

Published

2013

45. PATH-07. FAMILIAL MELANOMA-ASTROCYTOMA SYNDROME: SYNCHRONOUS DIFFUSE ASTROCYTOMA AND PLEOMORPHIC XANTHOASTROCYTOMA IN A PATIENT WITH GERMLINE CDKN2A/B DELETION AND A SIGNIFICANT FAMILY HISTORY

Author

Mitchel S. Berger, Arie Perry, Daniah Beleford, Andrew K Chan, Nicholas Butowski, David A. Solomon, Manish K. Aghi, Joseph T. Shieh, Joanna J. Phillips, Andrew W. Bollen, Winward Choy, and Seunggu J. Han

Subjects

Genetics, Pleomorphic xanthoastrocytoma, Cancer Research, Astrocytoma, Biology, Cdkn2a b, medicine.disease, Familial Melanoma, Germline, nervous system diseases, stomatognathic diseases, Abstracts, Oncology, Diffuse Astrocytoma, medicine, Cancer research, Neurology (clinical), Family history, neoplasms

Abstract

Familial melanoma-astrocytoma syndrome is a tumor predisposition syndrome caused by inactivating germline alteration of the CDKN2A tumor suppressor gene on chromosome 9p21. While some families with germline CDKN2A mutations are prone to development of just melanomas, other families develop both melanomas, astrocytomas, and occasionally other nervous system neoplasms including peripheral nerve sheath tumors and meningiomas. The histologic spectrum of the astrocytomas that arise as part of this syndrome is not well described, nor are the additional genetic alterations that drive these astrocytomas apart from the germline CDKN2A inactivation. Herein, we report the case of a young man with synchronous development of a pleomorphic xanthoastrocytoma, diffuse astrocytoma, and paraspinal mass radiographically consistent with a peripheral nerve sheath tumor. His paternal family history is significant for melanoma, glioblastoma, and oral squamous cell carcinoma. Genomic profiling revealed that he harbors a heterozygous deletion in the germline of chromosome 9p21.3 encompassing the CDKN2A and CDKN2B tumor suppressor genes. Both the pleomorphic xanthoastrocytoma and diffuse astrocytoma were found to have homozygous deletion of CDKN2A/B due to somatic loss of the other copy of chromosome 9p containing the remaining intact alleles. Additional somatic alterations included BRAF p.V600E mutation in the pleomorphic xanthoastrocytoma and PTPN11, ATRX, and NF1 mutations in the diffuse astrocytoma. The presence of germline CDKN2A/B inactivation together with the presence of multiple anatomically, histologically, and genetically distinct astrocytic neoplasms, both with accompanying somatic loss of heterozygosity for the CDKN2A/B deletion, led to a diagnosis of familial melanoma-astrocytoma syndrome. This remarkable case illustrates the histologic and genetic diversity that astrocytomas arising as part of this rare glioma predisposition syndrome can demonstrate.

Published

2017

46. RTHP-11. REIRRADIATION OF RECURRENT HIGH GRADE GLIOMAS: OUTCOMES AND PROGNOSTIC FACTORS

Author

Jean L. Nakamura, Penny K. Sneed, Christopher H. Chapman, Shannon Fogh, Jared Hara, Jennifer Clarke, Susan M. Chang, Nicholas Butowski, Steve Braunstein, and David R. Raleigh

Subjects

Abstracts, Cancer Research, Oncology, Neurology (clinical)

Abstract

PURPOSE/OBJECTIVE(S): Identify prognostic factors for progression-free survival (PFS) and overall survival (OS) after reirradiation (re-RT) for recurrent high grade glioma (HGG). MATERIALS/ METHODS: Patients with HGG received re-RT from 2010 to present. PFS and OS prognostic variables were examined using Cox models. Receiver operative curve (ROC) analysis identified predictive thresholds for continuous variables. RESULTS: 58 patients received surgery and adjuvant radiation for HGG (51 grade IV, 7 grade III). The median time to first progression after initial radiation was 11 months. 36% received single fraction stereotactic re-RT (SRS) (median 18 Gy) and 64% received fractionated re-RT (median 35 Gy in 10 fractions). The median planning target volume (PTV) was 16.8 mL. The median biologically effective dose (BED10) of re-RT was 47 Gy (range 15–72). 50% received chemotherapy and 36% received bevacizumab concurrent to re-RT. Toxicity ≥ grade 3 was 7%. The median PFS after re-RT was 4.7 months and the median OS was 11 months. Lower PFS was significantly associated with shorter time to first progression, lower KPS, and lower re-RT dose. Lower OS was associated with shorter time to first progression, lower KPS, and larger PTV. Other factors were not significantly associated with PFS or OS. ROC analysis of time to first progression and re-RT dose showed best predictive thresholds at time > 12 months and BED10 > 42 Gy. CONCLUSIONS: Reirradiation was tolerated with infrequent high grade toxicity. PFS and OS after re-RT were both predicted by time to progression after initial radiation. Published prognostic scores have used total time from first to second radiation courses; however in our series the period from initial progression to re-RT did not add prognostic information. There was evidence for a dose threshold irrespective of radiotherapy technique. Use of chemotherapy and bevacizumab with re-RT were not associated with improved outcomes.

Published

2018

47. PATH-08. THE IVY GLIOBLASTOMA PATIENT ATLAS - A NOVEL CLINICAL AND RADIO-GENOMICS RESOURCE FOR EARLY PHASE CLINICAL TRIAL DESIGN AND INTERPRETATION

Author

Benjamin M. Ellingson, Nikolaus Schultz, Anat Stemmer-Rachamimov, Timothy F. Cloughesy, Sarah Charbonneau, Keith L. Ligon, Howard Colman, Brian M. Alexander, Susan M. Chang, Robert J. Young, Patrick Y. Wen, Ingo K. Mellinghoff, John de Groot, Michael D. Prados, Jack Geduldig, Annette M. Molinaro, Shannon Block, William H. Yong, Joanna J. Phillips, Janine M. Lupo, Lisa M. DeAngelis, Isabel Arrillaga-Romany, Nicholas Butowski, Raymond Y. Huang, and David A. Reardon

Subjects

Radio communications, Cancer Research, medicine.medical_specialty, Temozolomide, business.industry, Clinical study design, Genomics, medicine.disease, Abstracts, medicine.anatomical_structure, Oncology, Atlas (anatomy), medicine, Medical physics, Neurology (clinical), Early phase, business, medicine.drug, Glioblastoma

Abstract

Newly diagnosed GBM represents a population of increased focus in early phase clinical trials. However, a key limitation of current genomic databases of GBM, such as TCGA, is that patient populations eligible for inclusion in these databases exhibit inherent biases and exhibit limitations on the quality of clinical and imaging data available for integration with genomics. To address these limitations and to better represent the genomics of patient populations commonly enrolled to early phase clinical trials, we prospectively consented and enrolled GBM patients to the Ivy Foundation Glioblastoma Patient Atlas Project. A total of 1591 patients from 7 participating sites of the Ben and Catherine Ivy Foundation Consortium for Early Phase Clinical Trials were consented to the project and clinical data was entered into a centrally managed clinical trials database. Overall 658 subjects had pre- and post-surgical imaging centrally reviewed and recorded and 387 subjects had sufficient tissue for completion of targeted exome sequencing of approximately 500 cancer causing genes (Oncopanel or Impact). More than 308 subjects had a complete set of genomics, imaging, and clinical data, including TMZ/RT use, KPS, progression, and steroid use. Histopathological features, MGMT, and IDH mutation status were also annotated. Of the subjects with full clinical data, 171 had expired by the time of last analysis of the cohort. Genomic and clinical characteristics unique to the early phase clinical trial population compared to TCGA and other cohorts of GBM were identified and radio-genomic and other advanced population-based analyses were performed. All clinical, genomic and imaging data are being utilized to create an Ivy cBio Portal for sharing of this rich dataset within the neurooncology community.

Published

2018

48. ATIM-06. PHASE 2 TRIAL OF SL-701 + BEVACIZUMAB IN PATIENTS WITH PREVIOUSLY TREATED GLIOBLASTOMA (GBM) MEETS PRIMARY ENDPOINT OF OS-12, WITH PRELIMINARY CORRELATION BETWEEN LONG-TERM SURVIVAL AND TARGET-SPECIFIC CD8+ T CELL IMMUNE RESPONSE

Author

Erin M. Dunbar, Christopher Brooks, Tobias Walbert, Frank S. Lieberman, Karen Fink, David Schiff, Fabio M. Iwamoto, Surasak Phuphanich, Priya Kumthekar, Michael Schulder, J. Bullington, David M. Peereboom, David Tran, Jonathan H. Sherman, Lynn S. Ashby, L. Burt Nabors, David A. Reardon, Michael Badruddoja, Nicholas Butowski, and Ross W. B. Lindsay

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Bevacizumab, medicine.medical_treatment, Human leukocyte antigen, Abstracts, 03 medical and health sciences, 0302 clinical medicine, Immune system, Internal medicine, Survivin, medicine, Clinical endpoint, Cytotoxic T cell, business.industry, Immunotherapy, medicine.disease, Cytokine release syndrome, 030104 developmental biology, 030220 oncology & carcinogenesis, Neurology (clinical), business, medicine.drug

Abstract

SL-701 is a novel immunotherapy comprised of synthetic peptides designed to elicit an anti-tumor immune response against GBM targets: interleukin-13 receptor alpha-2, EphrinA2 and Survivin. Updated Phase 2 data are reported. Patients with previously treated GBM, bevacizumab (bev)-naive, HLA-A2+, and KPS>60, were enrolled. SL-701 with adjuvant poly-ICLC was dosed biweekly with bev (10 mg/kg) for 6 months, then q28 days. Primary endpoint was OS-12, with statistical significance determined if lower bound of 2-sided 95% Clopper Exact confidence interval (CI) is >20%. Target-specific CD8+ T-cell frequency was assessed by flow cytometry. 28 patients received median of 13 SL-701 doses with bev. Most frequent treatment-related adverse events (TRAEs) were fatigue (39%) and injection site reaction (25%). Grade 3 TRAE was fatigue (3.6%); there were no other grade 3 TRAEs. Disease control rate (complete response [CR], partial response [PR], stable disease) was 54% (n=15), with 2 CRs and 2 PRs. Median duration of disease control was 8.8 months (95% CI 3.7, NE). Median OS was 11.7 months (95% CI: 7.1, NE). The primary endpoint was met with a 50% OS-12 (95% CI: 30.6, 69.4). Target-specific CD8+ T cell activity was detected at 8–24 wks, the majority occurring by wk 16. Long-term survivors were largely comprised of patients with target-specific CD8+ T-cell responses; median OS of these immune responders was not reached. The Phase 2 trial of SL-701 + bev in previously treated GBM met its primary endpoint with a 50% OS-12. The regimen was well-tolerated and demonstrated objective responses, including CRs. There was an even more pronounced survival signal, as well as an encouraging survival tail comprised largely of target-specific CD8+ T cell responders, and the median OS of these immune responders was not reached. Updates around next steps, including leveraging potential immune-related biomarkers in a registration-directed trial design, will be provided.

Published

2018

49. CHARACTERIZATION OF RADIOTHERAPY-INDUCED CEREBRAL MICROBLEEDS WITH ULTRA-HIGH FIELD MRI: EXPERIENCE IN YOUNG AND ADULT BRAIN TUMOUR POPULATION

Author

Melanie A. Morrison, Sabine Mueller, Christopher Hess, Janine Lupo, Erin Felton, Jennifer Clarke, Angela Jakary, Nicholas Butowski, and Susan Chang

Subjects

Cancer Research, education.field_of_study, medicine.medical_specialty, business.industry, medicine.medical_treatment, Population, Radiation therapy, Abstracts, Text mining, Oncology, Ultra high field, medicine, Neurology (clinical), Radiology, education, business

Abstract

MOTIVATION: In the treatment of brain tumours, radiation therapy (RT) is associated with long-term effects including vascular injury, changes in white matter, and cognitive decline. Vascular injury typically manifests as size-varying hemosiderin deposits in the brain called cerebral microbleeds (CMBs) which can be detected with susceptibility-weighted imaging (SWI) as early as 8 months following treatment. Similar forms of vascular injury have been related to the cognitive impairments experienced by other patient populations (e.g. stroke, vascular dementia); preliminary findings suggest a similar relationship for RT-induced CMBs, though their clinical relevance remains unclear. Further characterization of RT-induced CMBs in relation to cognition, treatment and clinical parameters is thus needed to develop a more thorough understanding of the impact of CMBs on patients with brain tumours, with the ultimate goal of mitigating CMB development and associated long-term effects without sacrificing treatment efficacy. METHODS: Ultra-high field MRI and SWI were used to detect CMBs with high sensitivity in patients treated with RT for an adult (focal) or pediatric (whole-brain) brain tumour. For the adult patients, predictors of CMB development were identified, and evolutionary changes in CMB burden were characterized across serial imaging data. Neurocognitive testing was performed for the pediatric patients and the distribution of CMBs was evaluated; global and local CMB burden were related to global and region-specific measures of cognitive function. RESULTS: Total CMB burden increased with time since RT, though individual CMBs decreased in size overtime. Risk factors for CMB development in adults included multiple surgical resections, tumour type (and subsequent RT regimen), and tumour location. Majority of CMBs were in the white matter, occipital, temporal, and frontal lobes. Increased presence of CMBs in the frontal lobe was associated with worse performance on tasks measuring execution function in children.

Published

2018

50. Assessment of perfusion MRI-derived parameters in evaluating and predicting response to antiangiogenic therapy in patients with newly diagnosed glioblastoma

Author

Emma Essock-Burns, Susan M. Chang, Janine M. Lupo, Nicholas Butowski, Sarah J. Nelson, Mei Yin C. Polley, and Soonmee Cha

Subjects

Cancer Research, medicine.medical_specialty, Indoles, Radiography, medicine.medical_treatment, Clinical Investigations, Perfusion scanning, chemistry.chemical_compound, Enzastaurin, Text mining, Image Processing, Computer-Assisted, Temozolomide, Humans, Medicine, Antineoplastic Agents, Alkylating, Brain Neoplasms, business.industry, Combined Modality Therapy, Magnetic Resonance Imaging, Surgery, Dacarbazine, Perfusion, Survival Rate, Radiation therapy, Treatment Outcome, Oncology, chemistry, Chemotherapy, Adjuvant, Disease Progression, Radiotherapy, Adjuvant, Neurology (clinical), Radiology, Glioblastoma, business, Adjuvant, medicine.drug

Abstract

The paradigm for treating patients with glioblastoma multiforme (GBM) is shifting from a purely cytotoxic approach to one that incorporates antiangiogenic agents. These are thought to normalize the tumor vasculature and have shown improved disease management in patients with recurrent disease. How this vascular remodeling evolves during the full course of therapy for patients with newly diagnosed GBM and how it relates to radiographic response and outcome remain unclear. In this study, we examined 35 patients who were newly diagnosed with GBM using dynamic susceptibility contrast (DSC) MRI in order to identify early predictors of radiographic response to antiangiogenic therapy and to evaluate changes in perfusion parameters that may be predictive of progression. After surgical resection, patients received enzastaurin and temozolomide, both concurrent with and adjuvant to radiotherapy. Perfusion parameters, peak height (PH) and percent recovery, were calculated from the dynamic curves to assess vascular density and leakage. Six-month radiographic responders showed a significant improvement in percent recovery between baseline and 2 months into therapy, whereas 6-month radiographic nonresponders showed significantly increased PH between baseline and 1 month. At 2 months into therapy, percent recovery was predictive of progression-free survival. Four months prior to progression, there was a significant increase in the standard deviation of percent recovery within the tumor region. DSC perfusion imaging provides valuable information about vascular remodeling during antiangiogenic therapy, which may aid clinicians in identifying patients who will respond at the pretherapy scan and as an early indicator of response to antiangiogenic therapy.

Published

2010