A Trial to Evaluate Multiple Regimens in Newly Diagnosed and Recurrent Glioblastoma

Part of paid clinical trials in Birmingham, Alabama.

Sponsor: Global Coalition for Adaptive Research
Study ID: NCT03970447
Phase: PHASE2/PHASE3
Status: Recruiting

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Conditions

Glioblastoma

Eligibility Criteria

Sex: ALL
Age: 18 Years - N/A
Healthy Volunteers: Not accepted

Interventions

Temozolomide — DRUG
Dosage Form: Capsule for oral administration Strengths: 5 mg, 20 mg, 100 mg, 140 mg, 180 mg, or 250 mg
Lomustine — DRUG
Dosage Form: Capsule for oral administration Strength: 5 mg, 10 mg, 40 mg, and 100 mg
Regorafenib — DRUG
Dosage Form: Tablet for oral administration Strength: 40 mg Standard Regimen: 160 mg orally (PO) every day (QD) for 3 weeks of every 4 week cycle (i.e., 3 weeks on, 1 week off)
Radiation — RADIATION
60 Gy
Paxalisib — DRUG
Dosage Form: Tablet for oral administration Strength: 15 mg Standard Regimen: 45 mg orally (PO) every day for 28 days for the first cycle. If tolerated, increase dose to 60 mg orally (PO) every day for 28 days for all subsequent cycles
VAL-083 — DRUG
Dosage Form: Infusion for intravenous administration Strength: 40 mg per vial Standard Regimen: 30 mg/m2 on Day 1, 2 and 3 of 21-day cycle. The drug is available in powder form. It is reconstituted with 5 mL of 0.9% Sodium Chloride for Injection, USP. This will produce a solution of 40 mg VAL-083 in 5 mL. The required volume of reconstituted VAL-083 for the patient is then calculated at the rate of 30 mg/m2. The corresponding volume is further diluted into 250 mL of 0.9% Sodium Chloride for Injection, USP, prior to intravenous administration.
VT1021 — DRUG
Dosage Form: Infusion for intravenous administration Strength: 10 mg/mL Standard Regimen Newly Diagnosed: Dose as confirmed through the dose finding phase, administered twice weekly (Mon and Thurs or Tues and Fri or Mon and Fri). Standard Regimen Recurrent: 12 mg/kg administered twice weekly (Mon and Thurs or Tues and Fri or Mon and Fri). The drug is available as a sterile solution of the acetate salt formulated with phosphate-buffered saline, mannitol, and 2.5% polysorbate 80. The required volume stock solution for the patient is calculated. The corresponding volume is diluted in 500 mL of either 0.9% saline or D5W, prior to intravenous administration.
Troriluzole — DRUG
Dosage Form: Capsule for oral administration Strength: 100 mg Standard Regimen: Dose as confirmed through the dose finding phase orally BID.
ADI-PEG 20 — BIOLOGICAL
Dosage Form: Solution for intramuscular injection Strength: 11.5 ± 1.0 mg/ml Standard Regimen: For newly diagnosed patients, 36mg/m2. For recurrent disease patients, dose as confirmed through the dose finding phase intramuscularly once a week
AZD1390 — DRUG
Standard Regimen Newly Diagnosed: Given once daily on days of radiation and once daily for 14 consecutive days after completion of radiation.
Tinostamustine — DRUG
Dosage form: Reconstituted powder for intravenous administration Strength: 2mg/mL Standard Regimen: Dose as confirmed through the dose finding phase, on Day 1 of 21-day cycle for up to 12 cycles in the maintenance phase.

Study Details

Glioblastoma (GBM) adaptive, global, innovative learning environment (GBM AGILE) is an international, seamless Phase II/III response adaptive randomization platform trial designed to evaluate multiple therapies in newly diagnosed (ND) and recurrent GBM. All institutions are enrolling Newly Diagnosed participants. Institutions also enrolling Recurrent participants are marked with an asterisk (\*).

Key Dates

Start date: Jul 30, 2019
Status verified: Jun 2026
Primary completion: Jun 30, 2028
Completion: Jun 30, 2030

Study Design

Enrollment: 2,250 participants (estimated)
Allocation: RANDOMIZED
Intervention model: SEQUENTIAL
Primary purpose: TREATMENT

Arms

Active Comparator: Control Arm
Newly Diagnosed GBM: Radiation therapy (XRT) 60 Gy for 6 weeks. Temozolomide 75 mg/m2 orally daily during radiation therapy. Rest Period 2-6 weeks from the last day of radiation, and the start of the first cycle of Maintenance Therapy 2-6 weeks after the last day of radiotherapy. The start of all subsequent maintenance therapy cycles (2-12) every 4 weeks + 7 days after the first daily dose of temozolomide of the preceding cycle. Total number of cycles should comply with institutional or country standards. During maintenance therapy, the first cycle of temozolomide will be at 150 mg/m2 for Days 1-5 of a 28-day cycle. Second and subsequent cycles of maintenance therapy will be at 200 mg/m2 for Days 1-5 of a 28-day cycle. Recurrent GBM: Lomustine started at 110 mg/m2/day on Day 1 of a 42-day cycle as per local standards. Treatment will continue for up to 6 total cycles.
Experimental: Regorafenib Treatment Arm- Enrollment concluded
Newly Diagnosed MGMT Unmethylated GBM: XRT 60 Gy for 6 weeks. Temozolomide 75 mg/m2 orally daily during radiation therapy. Rest Period 4 weeks from the last day of radiation. Maintenance period: Regorafenib (Dosage Form: Tablet for oral administration; Strength: 40 mg) 160 mg orally (PO) every day (QD) for 3 weeks of every 4 week cycle (i.e., 3 weeks on, 1 week off). Recurrent GBM: Regorafenib (Dosage Form: Tablet for oral administration; Strength: 40 mg) 160 mg orally (PO) every day (QD) for 3 weeks of every 4 week cycle (i.e., 3 weeks on, 1 week off).
Experimental: Paxalisib Treatment Arm- Enrollment concluded
Newly Diagnosed MGMT Unmethylated GBM: XRT 60 Gy for 6 weeks. Temozolomide 75 mg/m2 orally daily during radiation therapy. Rest Period 4 weeks from the last day of radiation. Maintenance period: Paxalisib (Dosage Form: Tablet for oral administration; Strength: 15 mg per tablet) 45 mg orally (PO) every day for 28 days for the first cycle. If tolerated, increase dose to 60 mg orally (PO) every day for 28 days for all subsequent cycles. Recurrent GBM: Paxalisib (Dosage Form: Tablet for oral administration; Strength: 15 mg per tablet) 45 mg orally (PO) every day for 21 days for the first cycle. If tolerated, increase dose to 60 mg orally (PO) every day for 21 days for all subsequent cycles.
Experimental: VAL-083 Treatment Arm- Enrollment concluded
Newly Diagnosed MGMT Methylated and Unmethylated GBM: XRT 60 Gy for 6 weeks. Temozolomide 75 mg/m2 orally daily during radiation therapy. Rest Period 4 weeks from the last day of radiation. Maintenance period: VAL-083 (Dosage Form: Infusion for intravenous administration; Strength: 30 mg/m2) on Day 1, 2 and 3 of 21-day cycle. Recurrent GBM: VAL-083 (Dosage Form: Infusion for intravenous administration; Strength: 30 mg/m2) on Day 1, 2 and 3 of 21-day cycle.
Experimental: VT1021 Treatment Arm - Dose Finding Phase
Newly diagnosed MGMT Methylated and Unmethylated GBM: Rolling 6 design. Treatment as outlined in section "Experimental: VT1021 Treatment Arm" with the first 6 patients receiving VT1021 at 12 mg/kg twice weekly in combination with temozolomide and radiation therapy. If there are two dose limiting toxicities reported, the dose will be de-escalated to 9 mg/kg two times a week. 6 patients will then be receiving 9 mg/kg two times a week and observed for DLTs for 4 weeks. Recurrent GBM: Dose Finding Phase is not applicable for patients with Recurrent GBM in the VT1021 treatment arm.
Experimental: VT1021 Treatment Arm - Enhanced Safety Management (ESM)
Experimental: VT1021 Treatment Arm - Enhanced Safety Management (ESM) Newly diagnosed MGMT Methylated and Unmethylated GBM: Supplemental safety assessments including bi-weekly collection of adverse events, dose modification profile, hematology, serum chemistry and coagulation panels. PK and PD assessments are done for patients as a part of ESM. ESM will continue until the Data Safety Monitoring Board (DSMB) suspends collection of additional data. Recurrent GBM: ESM is not applicable for patients with Recurrent GBM in the VT1021 treatment arm.
Experimental: VT1021 Treatment Arm
Newly diagnosed MGMT Methylated and Unmethylated GBM: XRT 60 Gy for 6 weeks. Temozolomide 75 mg/m2 orally daily and VT1021 (Dosage Form: Infusion for intravenous administration; Strength: 10 mg/mL; Dose: As confirmed through the dose finding phase) twice weekly during radiation therapy. Rest period: 2-6 weeks from last day of radiation. VT1021 dosing will continue during the rest period. Maintenance period: The first cycle of temozolomide will be at 150 mg/m2 for days 1-5 of a 28-day cycle. Second and subsequent cycles of maintenance therapy will be at 200 mg/m2 for days 1-5 of a 28-day cycle. Temozolomide will be administered for up to 6 cycles in the maintenance phase in combination with VT1021. After 6 cycles, VT1021 only. Recurrent GBM: VT1021 (Dosage Form: Infusion for intravenous administration; Strength: 10 mg/mL; Dose: 12mg/kg) twice weekly.
Experimental: Troriluzole Treatment Arm - Dose Finding Phase
Newly diagnosed MGMT Methylated and Unmethylated GBM: Rolling 6 design. The first 6 patients will receive troriluzole at 100 mg BID for the first two weeks followed by 200 mg BID for the next two weeks in combination with temozolomide and radiation therapy. If there are two dose limiting toxicities (DLTs) reported, the dose will be de-escalated to 100 mg in the morning and followed by 200 mg in the evening. 6 patients will receive this dose and observed for 4 weeks. If there are two DLTs reported, then this dose will be de-escalated to 100 mg BID. 6 patients will then be receiving this dose and observed for DLTs for 4 weeks. Recurrent GBM: Rolling 6 design. The first 6 patients receiving troriluzole 100 mg twice a day (BID) for the first two weeks followed by 200 mg BID for the next two weeks in combination with lomustine. The dose de-escalation is similar to that of newly diagnosed patients during the rolling 6 design.
Experimental: Troriluzole Treatment Arm - Enhanced Safety Management (ESM)
Newly diagnosed MGMT Methylated and Unmethylated GBM and Recurrent GBM: Supplemental safety assessments including bi-weekly collection of adverse events, dose modification profile, hematology, serum chemistry and coagulation panels. ESM will continue until the Data Safety Monitoring Board (DSMB) suspends collection of additional data.
Experimental: Troriluzole Treatment Arm
Newly diagnosed MGMT Methylated and Unmethylated GBM: XRT 60 Gy for 6 weeks. Temozolomide 75 mg/m2 orally daily and troriluzole (Dosage Form: Capsule for oral administration; Strength: 100 mg; Dose: As confirmed by dose finding phase) BID. Rest period: 2-6 weeks from last day of radiation. Troriluzole dosing will continue during the rest period. Maintenance period: The first cycle of temozolomide will be at 150 mg/m2 for days 1-5 of a 28-day cycle. Second and subsequent cycles of maintenance therapy will be at 200 mg/m2 for days 1-5 of a 28-day cycle. Temozolomide will be administered for up to 6 cycles in the maintenance phase in combination with troriluzole. After 6 cycles, troriluzole only. Recurrent GBM: Lomustine 100 mg/m2 orally on day 1 of a 42-day cycle in combination with troriluzole (Dosage Form: Capsule for oral administration; Strength: 100 mg; Dose: As confirmed by dose finding phase) BID. After 6 cycles, troriluzole only.
Experimental: ADI-PEG 20 Treatment Arm - Dose Finding Phase
Newly diagnosed MGMT Methylated and Unmethylated GBM: Dose Finding Phase is not applicable for newly diagnosed patients on the ADI-PEG 20 treatment arm. Recurrent GBM: Rolling 6 design. The first 6 patients will receive ADI-PEG 20 at 36 mg/m2 once a week in combination with lomustine 100 mg/m2 orally on day 1 of a 42-day cycle. 6 patients will receive this dose and be observed for 4 weeks. If there are two dose limiting toxicities (DLTs) reported, the dose will be de-escalated to 18 mg/m2 once a week. 6 patients will receive this dose and be observed for 4 weeks.
Experimental: ADI-PEG 20 Treatment Arm - Enhanced Safety Management (ESM)
Newly diagnosed MGMT Methylated and Unmethylated GBM: ESM is not applicable for newly diagnosed patients on the ADI-PEG 20 treatment arm. Recurrent GBM: Supplemental safety assessments including bi-weekly collection of adverse events, dose modification profile, hematology, serum chemistry and coagulation panels. ESM will continue until the Data Safety Monitoring Board (DSMB) suspends collection of additional data.
Experimental: ADI-PEG 20 Treatment Arm
Newly diagnosed MGMT Methylated and Unmethylated GBM: XRT 60 Gy over 6 weeks. Temozolomide (75 mg/m2 orally daily and ADI-PEG 20 (Dosage Form: Solution for intramuscular injection; Strength: 11.5 ± 1.0 mg/ml; Dose: 36 mg/m2) once a week. Rest period: 2-6 weeks from last day of radiation. ADI-PEG 20 dosing will continue during rest period. Maintenance period: The first cycle of temozolomide will be at 150 mg/m2 for days 1-5 of a 28-day cycle. Subsequent cycles will be at 200 mg/m2 for days 1-5 of a 28-day cycle. Temozolomide will be administered for up to 6 cycles in the maintenance phase in combination with ADI-PEG 20. After 6 cycles, ADI-PEG 20 only for up to 104 weeks of total treatment. Recurrent GBM: Lomustine 100 mg/m2 orally on day 1 of a 42-day cycle in combination with ADI-PEG 20 (Dosage Form: Solution for IM injection; Strength: 11.5 ± 1.0 mg/ml; Dose: As confirmed by dose finding phase, once a week. After 6 cycles, ADI-PEG 20 only for up to 104 weeks of total treatment.
Experimental: AZD1390 Treatment Arm
Newly Diagnosed MGMT Methylated and Unmethylated GBM: XRT 60 Gy for 6 weeks in combination with AZD1390 given on days of radiation followed by 14 days with daily AZD1390. Rest Period 2-4 weeks from the last day of AZD1390. The first cycle of temozolomide will be at 150 mg/m2 for days 1-5 of a 28-day cycle. Second and subsequent cycles of maintenance therapy will be at 200 mg/m2 for days 1-5 of a 28-day cycle, if there is no toxicity. Temozolomide will be administered for up to 6 cycles in the maintenance phase.
Experimental: Tinostamustine - Dose finding phase
Newly diagnosed MGMT Methylated and Unmethylated GBM: Tinostamustine Dosage Form: Infusion for intravenous administration; Rolling 6 design. Treatment as outlined in "Investigational: Tinostamustine Treatment Arm" with the first 6 patients receiving Tinostamustine at 80 mg/m2 over 60 minutes with two potential dose de-escalations. If there are two or more dose limiting toxicities at the tested dose, subsequent patients will be enrolled at the next lower dose level (60 mg/m2 and subsequently to 40 mg/m2). Recurrent GBM: Rolling 6 design. Tinostamustine Dosage Form: Infusion for intravenous administration; Strength: Starting dose 80 mg/m2 on Day 1 of 21-day cycle for up to 12 cycles. The first 6 patients will receive Tinostamustine at 80 mg/m2 over 60 minutes with two potential dose de-escalations if there are two or more dose limiting toxicities at the tested dose, subsequent patients will be enrolled at the next lower dose level (60 mg/m2 and subsequently to 40 mg/m2).
Experimental: Tinostamustine - Enhanced Safety Management
Newly diagnosed MGMT Methylated and Unmethylated GBM: Treatment as outlined in "Investigational: Tinostamustine Treatment Arm". Dose as determined by the dose finding phase. Recurrent GBM: Tinostamustine (Dosage Form: Infusion for intravenous administration; Strength: as determined though the dose finding phase on Day 1 of 21-day cycle for up to 12 cycles.
Experimental: Investigation arm: Tinostamustine
Newly diagnosed MGMT Methylated and Unmethylated GBM: XRT total of 60 Gy (2 Gy/fraction) over 6 weeks. Temozolomide 75 mg/m2 orally daily during radiation therapy. Rest Period 2-6 weeks from the last day of radiation. Tinostamustine treatment period: Tinostamustine (Dosage Form: Infusion for intravenous administration; Strength: as determined though the dose finding phase) on Day 1 of 21-day cycle for up to 12 cycles.

Primary Outcome Measure

Overall Survival (OS) [ Time Frame: From date of randomization until the date of death from any cause, or until 12 months following last patient randomization (approximately 2 years), whichever comes first. ]

Central Contacts

Patient Information
310-598-3199
[email protected]
Rachel Rosenstein-Sisson
[email protected]

Locations (42)

Facility	City	State	ZIP	Site coordinators
University of Alabama at Birmingham	Birmingham	Alabama	35249	Thiru Pillay [email protected] 205-934-1432 Yantong (Lily) Liu [email protected] 205-975-2283 Louis B Nabors, MD (PRINCIPAL_INVESTIGATOR)
University of California, San Diego	La Jolla	California	92093	Sheila Medina [email protected] (858) 246-1093 [email protected] David Piccioni, MD, PhD (PRINCIPAL_INVESTIGATOR)
Cedars Sinai - Samuel Oschin Comprehensive Cancer Institute	Los Angeles	California	90048	Shannon Cyhan [email protected] Jethro Hu, MD (PRINCIPAL_INVESTIGATOR)
University of California, Los Angeles	Los Angeles	California	90095	Quan Li [email protected] 310-825-1416 Phioanh Nghiemphu, MD (PRINCIPAL_INVESTIGATOR)
St. Joseph Hospital	Orange	California	92868	Andrea Torres [email protected] 714-734-6220 Lars Anker, MD (PRINCIPAL_INVESTIGATOR)
University of California, San Francisco	San Francisco	California	94143	UCSF Neuro Onc New Patient Coordinator [email protected] (415) 353-2193 Nicholas Butowski, MD (PRINCIPAL_INVESTIGATOR)
Stanford Cancer Center	Stanford	California	94305	-
University of Colorado Denver	Aurora	Colorado	80045	Katherine Harr [email protected] 303-724-9693 Denise Damek, MD (PRINCIPAL_INVESTIGATOR)
Yale Cancer Center / Smilow Cancer Hospital*	New Haven	Connecticut	06511	Amy L. Rodriguez [email protected] 203-785-5702 Nicholas Blondin, MD (PRINCIPAL_INVESTIGATOR)
Mayo Clinic Cancer Center	Jacksonville	Florida	32224	-
Sylvester Comprehensive Cancer Center*	Miami	Florida	33136	Leonela Wright [email protected] 305-243-0864 Macarena I De La Fuente, MD (PRINCIPAL_INVESTIGATOR)
Moffitt Cancer Center	Tampa	Florida	33612	Minnah Mohamed [email protected] 813-745-5848 Carie Bliss [email protected] 813-745-2131 Patrick Grogan, MD (PRINCIPAL_INVESTIGATOR)
Piedmont Atlanta Hospital	Atlanta	Georgia	30309	Dionne Jean [email protected] 404-425-7927 Takiyyah Hamiliton [email protected] 770-315-7744 Erin Dunbar, MD (PRINCIPAL_INVESTIGATOR)
Winship Cancer Institute of Emory University	Atlanta	Georgia	30322	-
LSU Health Sciences Center - New Orleans	New Orleans	Louisiana	70112	-
Dana Farber Cancer Institute	Boston	Massachusetts	02115	Amanda Dresser [email protected] 617-582-9314 Kathryn Partridge [email protected] 617-582-9314 Patrick Wen, MD (PRINCIPAL_INVESTIGATOR)
Massachusetts General Hospital	Boston	Massachusetts	02114	Lauren Hibyan [email protected] 617-643-8992 Marie Aste [email protected] 617-724-2262 Patrick Wen, MD (PRINCIPAL_INVESTIGATOR)
Henry Ford Health System	Detroit	Michigan	48202	-
Allina Health Systems/Abbott Northwestern Hospital	Minneapolis	Minnesota	55407	[email protected] 612-863-3452 Andrea Wasilewski, MD (PRINCIPAL_INVESTIGATOR)
Mayo Clinic Cancer Center - Rochester	Rochester	Minnesota	55905	-
University of Mississippi Medical Center	Jackson	Mississippi	39213	-
Washington University School of Medicine - Siteman Cancer Center	St Louis	Missouri	63110	-
Columbia University Medical Center	New York	New York	10032	Andrew Lassman, MD [email protected] 212-342-0571 Andrew Lassman, MD (PRINCIPAL_INVESTIGATOR)
Icahn School of Medicine at Mount Sinai	New York	New York	10029	Disha Jain [email protected] 929-638-2764 Lyndon Kim, MD (PRINCIPAL_INVESTIGATOR)
Memorial Sloan Kettering Cancer Center*	New York	New York	10065	Kerina Yang [email protected] 901-883-0840 Nancy Keith [email protected] 646-300-0216 Ingo Mellinghoff, MD (PRINCIPAL_INVESTIGATOR)
Perlmutter Cancer Center, NYU Langone Health	New York	New York	10016	Ewelina Rakoczy, Rachel Kim #[email protected] 212-731-6267 Jonathan Yang, MD, PhD (PRINCIPAL_INVESTIGATOR)
Duke University Medical Center	Durham	North Carolina	27710	Erin Severance [email protected] 919-668-6230 Katherine Peters, MD, PhD (PRINCIPAL_INVESTIGATOR)
Comprehensive Cancer Center of Wake Forest*	Winston-Salem	North Carolina	272157	Monique Mercado [email protected] 336-716-9123 Glenn Lesser, MD (PRINCIPAL_INVESTIGATOR)
Cleveland Clinic	Cleveland	Ohio	44195	Rachel Hufsey [email protected] 216-442-6671 Kathy Robinson [email protected] 216-444-8923 Mina Lobbous, MD (PRINCIPAL_INVESTIGATOR)
University Hospitals Cleveland Medical Center*	Cleveland	Ohio	44106	Melissa Brately [email protected] 216-983-3021 Carmen Gray [email protected] Herbert Newton, MD (PRINCIPAL_INVESTIGATOR)
Ohio State University Cancer Center	Columbus	Ohio	43210	-
University of Pennsylvania - Perelman Center for Advanced Medicine	Philadelphia	Pennsylvania	19104	ACC Clinical Trials [email protected] 215-349-8245 Leah Coghlan [email protected] Arati Desai, MD (PRINCIPAL_INVESTIGATOR)
Allegheny General Hospital	Pittsburgh	Pennsylvania	15212	-
University of Pittsburgh Medical Center - Hillman Cancer Center	Pittsburgh	Pennsylvania	15232	Theo Estep [email protected] 878-261-6727 Brynne Fedor [email protected] 878-261-6409 Jan Drappatz, MD (PRINCIPAL_INVESTIGATOR)
Medical University of South Carolina - Hollings Cancer Center	Charleston	South Carolina	29425	HCC Clinical Trials Office [email protected] 843-792-9321 Scott Lindhorst, MD (PRINCIPAL_INVESTIGATOR)
Texas Oncology - Austin	Austin	Texas	78705	-
University of Texas Southwestern Medical Center	Dallas	Texas	75390	-
University of Texas - MD Anderson Cancer Center	Houston	Texas	77030	Evguenia Gachimova, RN [email protected] (832)266-3519 Shiao-Pei Weathers, MD (PRINCIPAL_INVESTIGATOR)
University of Utah - Huntsman Cancer Institute	Salt Lake City	Utah	84112	Rachel Kingsford [email protected] 801-505-0115 Yuri Kida [email protected] 801-646-4397 Howard Colman, MD, PhD (PRINCIPAL_INVESTIGATOR)
University of Virginia Health	Charlottesville	Virginia	22908	CJ Woodburn [email protected] 434-243-9900 David Schiff, MD (PRINCIPAL_INVESTIGATOR)
University of Washington Medical Center	Seattle	Washington	98101	-
Froedtert Hospital/Medical College of Wisconsin	Milwaukee	Wisconsin	53226	-

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University of Alabama at Birmingham· Birmingham, AL University of California, San Diego· La Jolla, CA Cedars Sinai - Samuel Oschin Comprehensive Cancer Institute· Los Angeles, CA University of California, Los Angeles· Los Angeles, CA St. Joseph Hospital· Orange, CA University of California, San Francisco· San Francisco, CA

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