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This is a multicenter, Phase 2 study to assess the activity of tesevatinib in patients with recurrent glioblastoma.
This is a multicenter, Phase 2 study to assess the activity of tesevatinib in subjects (n = 40) with recurrent glioblastoma. This study will be conducted at up to 10 sites in the United States.
The availability of paraffin-embedded tumor sample diagnostic of glioblastoma is mandatory for entry into the study. Tumor samples will be evaluated for the EGFRvIII mutation and for EGFR gene amplification. Tissue from recurrent surgery is preferred, but tissue from initial surgery is sufficient for study entry. Baseline MRI is mandatory.
After completion of the screening assessments and confirmation of study eligibility by the Medical Monitor upon review of an inclusion package, tesevatinib will be orally administered to all patients at a dose of 300 mg once daily. A cycle will be considered as 28 days. Patients will be evaluated for efficacy according to the Response Assessment in Neuro-Oncology (RANO) criteria.
Patients who develop ≥ Grade 3 adverse event(s) considered by the investigator to be related to study drug will have study treatment interrupted until the drug-related toxicities have resolved to ≤ Grade 1. Once toxicities have resolved to ≤ Grade 1, the patient may resume study treatment at a reduced dose of 250 mg/day. No more than 1 dose reduction is permitted. Patients who require more than one dose reduction will have study drug discontinued and enter the Follow-up Period.
Patients for whom toxicity persists beyond 21 days despite dose interruption may resume study treatment only with permission from the responsible Medical Monitor.
If study treatment is withheld, the patient should be instructed not to make up the withheld doses.
Study treatment will continue until disease progression, unacceptable toxicity, patient or physician decision to discontinue, or death. Assessments for disease response will occur at Week 4 and Week 8 and then every 8 weeks thereafter using the RANO criteria.
Upon treatment discontinuation, patients will be followed every 8 weeks for survival.
Tumor samples will be used for exploratory biomarker research including, but not limited to, evaluation of EGFRvIII expression by immunohistochemistry or real-time Polymerase Chain Reaction. An appropriate definition and cutoff for EGFRvIII^pos tumors will be established, and outcome in this subpopulation will be evaluated in addition to the overall study population.
To characterize the safety and tolerability profile of tesevatinib, patients will be monitored throughout the study for adverse events (all grades), serious adverse events, and any adverse events requiring drug interruption or discontinuation. Patients will undergo safety evaluations, including physical examinations, Karnofsky Performance Status (KPS), vital sign measurements, hematology, serum chemistry, urinalysis and electrocardiogram.
Magnetic resonance imaging (MRI) will be used to evaluate the tumor at baseline. All MRIs taken on study patients will be submitted to the sponsor for possible retrospective analysis.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| Glioblastoma | Experimental | The single arm design assessing progression-free survival at 6 months (PFS-6) in the overall population with the ability to detect a rate of 25% is appropriate as a preliminary test of activity in patients with glioblastoma. The sample size of this study is also designed to permit the comparison of results with EGFR amplified and non-amplified tumors, as well as EGFRvIII mutated versus wild-type. The sample size is adequate to characterize the safety profile in patients with glioblastoma. |
|
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| Tesevatinib | Drug |
|
|
| Measure | Description | Time Frame |
|---|---|---|
| Efficacy: Median Progression-free Survival (PFS) Rate at 6 Months (PFS-6) | Proportion (%) of subjects who did not have progressive disease after treatment with tesevatinib at 6 months (PFS-6) after baseline | 6 months |
| Measure | Description | Time Frame |
|---|---|---|
| Efficacy: Median PFS | Median duration (months) of subjects who were progression-free of disease from baseline | Until disease progression, unacceptable toxicity, subject or clinician decision to discontinue, death, or up to 3 years, whichever occurred first |
| Efficacy: Median Overall Survival Rate at 9 Months (OS-9) |
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Inclusion Criteria:
Willingness and ability to provide written informed consent and to comply with the study protocol as judged by the investigator
Age ≥ 18 years old
Kamofsky performance status ≥70%
Stable or decreasing dose of corticosteroids within 5 days prior to study 5. enrollment.
For women who are not postmenopausal (i.e., < 12 months after last menstruation) or surgically sterile (absence of ovaries and/or uterus) and who are sexually active: agreement to use an adequate method of contraception (oral contraceptives, intrauterine contraceptive device, barrier method of contraception in conjunction with spermicidal jelly) during the treatment period and for at least 6 months after the last dose of study drug.
For male patients who are sexually active and who are partners of premenopausal women: agreement to use a barrier method of contraception during the treatment period and for at least 6 months after the last dose of study drug.
Histologically confirmed glioblastoma. A local pathology report constitutes adequate documentation of histology for study inclusion. Patients with an initial diagnosis of a lower-grade glioma are eligible if a subsequent biopsy was determined to be glioblastoma.
First recurrence after concurrent or adjuvant chemoradiotherapy. Imaging confirmation of first tumor progression or regrowth as defined by the RANO criteria . A minimum of 12 weeks must have elapsed from the completion of radiotherapy to study entry to minimize the potential for MRI changes related to radiation necrosis that might be misdiagnosed as progression of disease, unless there is a new lesion outside the radiation field or unequivocal evidence of viable tumor on histopathological sampling.
Prior treatment with TMZ for low grade glioma or glioblastoma.
No more than one prior line of systemic treatment for glioblastoma. Concurrent and adjuvant TMZ-based chemotherapy, including the combination of TMZ with an investigational agent, is considered one line of therapy.
Prior therapy with gamma knife or other focal high-dose radiotherapy is allowed, but the patient must have subsequent histologic documentation of recurrence, unless the recurrence is a new lesion outside the irradiated field.
Recovery from the toxic effects of prior therapy, with a minimum time of:
Patients who have undergone recent surgery for recurrent or progressive tumor are eligible provided that:
Availability of formalin-fixed paraffin-embedded tumor tissue diagnostic of glioblastoma.
Exclusion Criteria:
Concurrent therapeutic intervention (including radiation therapy and NovoTTF).
Prior exposure to EGFR inhibitors.
Prior exposure to bevacizumab or other VEGF- or VEGF-receptor-targeted agent within 8 weeks of study start.
Prior treatment with prolifeprospan 20 with carmustine wafer.
Prior intracerebral agent.
Evidence of recent hemorrhage on baseline MRI of the brain. However, patients with clinically asymptomatic presence of hemosiderin, resolving hemorrhagic changes related to surgery, or presence of punctuate hemorrhage in the tumor are eligible.
Need for urgent palliative intervention for primary disease (e.g., rapidly increasing intracranial pressure, impending herniation, uncontrolled seizures).
Hematology:
ANC < 1.5 x109/L; Plt < 100 x109/L Hgb < 9.0 g/dL within 7 days prior to enrollment. The use of transfusion or other intervention to achieve Hb ≥ 9 g/dL is acceptable.
T.Bili. ≥ 1.5 x ULN (except in patients diagnosed with Gilbert's disease).
AST(SGOT), ALT(SGPT), or alkaline phosphatase (ALP) ≥ 2.5 x ULN.
S. Creat. > 1.5 x ULN.
K+ or Mg+ < LLN.
In the absence of therapeutic intent to anticoagulate the patient: INR > 1.5 or PT > 1.5 xULN or aPTT > 1.5 xULN Therapeutic anticoagulation.
Known contraindication to MRI, such as cardiac pacemaker, shrapnel or ocular foreign body.
Used any prescription medication during the prior 2 weeks that the investigator judges is likely to interfere with the study or to pose an additional risk to the patient in participating, specifically inhibitors or inducers of cytochrome P450 (CYP)3A4 (refer to Appendix 5). A stable regimen (≥ 4 weeks) of antidepressants of the selective serotonin re-uptake inhibitor (SSRI) class is allowed (common SSRIs include escitalopram oxalate, citalopram, fluvoxamine, paroxetine, sertraline, and fluoxetine).
Taking any drugs associated with torsades de pointes or known to moderately or severely prolong the QTc(F) interval
History of torsades de pointes, ventricular tachycardia or fibrillation, pathologic sinus bradycardia (< 50 bpm), heart block (excluding first degree block, being PR interval only), or congenital long QT syndrome. Patients with a history of atrial arrhythmias should be discussed with the Medical Monitor.
Uncontrolled diabetes, as evidenced by fasting serum glucose level >200 mg/dL
New York Heart Association (NYHA) Grade II or greater congestive cardiac failure.
Has marked prolongation of QTc(F) interval at screening or baseline (QTc[F] interval > 470 msec) using the Fridericia method of correction for heart rate.
History of myocardial infarction (within 12 months) or unstable angina (within 6 months) prior to study enrolment.
History of stroke or transient ischemic attacks within 6 months prior to study enrolment.
Significant vascular disease (e.g., aortic aneurysm requiring surgical repair or recent peripheral arterial thrombosis) within 6 months prior to study enrolment.
Evidence of bleeding diathesis or coagulopathy (in the absence of therapeutic anticoagulation).
History of intracranial abscess within 6 months prior to study enrolment.
History of another malignancy in the previous 3 years, with a disease-free interval of < 3 years. Patients with prior history of in situ cancer or basal or squamous cell skin cancer are eligible.
Evidence of any active infection requiring hospitalization or IV antibiotics within 2 weeks prior to study enrolment.
Known hypersensitivity to any excipients of tesevatinib.
Inability to swallow or absorb orally-administered medication.
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| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Center for Neurosciences | Tucson | Arizona | 85718 | United States | ||
| City of Hope |
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A total of 40 subjects with recurrent glioblastoma were enrolled. Tumor samples were evaluated for the presence or absence of EGFR gene-amplification, designated Sub-population A, and/or the EGFR variant III mutation (EGFRvIII^pos), designated Sub-population B, or neither EGFR gene-amplification nor EGFRvIII^pos variant mutation.
Note: EGFR = epidermal growth factor receptor; EGFR vIII^pos = EGFR variant 3 mutation; VEGF = vascular endothelial growth factor
Subjects at least 18 years of age with recurrent glioblastoma and no concurrent therapeutic intervention including prior exposure to EGFR inhibitors, VEGF, carmustine wafer, or intracerebral agent
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| ID | Title | Description |
|---|---|---|
| FG000 | Total | Subjects with recurrent glioblastoma who had or did not have EGFR gene-amplified and/or EGFRvIII^pos glioblastoma |
| Title | Milestones | Reasons Not Completed | |||||
|---|---|---|---|---|---|---|---|
| Overall Study |
|
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| Type | Includes Protocol | Includes SAP | Includes ICF | Document Label | Document Date | Document Uploaded Date | Document File Name |
|---|---|---|---|---|---|---|---|
| Prot | Yes | No | No | Study Protocol | Apr 3, 2019 | Jun 2, 2021 |
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Median proportion (%) of subjects who survived 9 months after baseline |
| 9 months |
| Efficacy: Median OS | Median duration (months) subjects survived from baseline until death | Until unacceptable toxicity, subject or investigator decision to discontinue, death, or up to 3 years, whichever occurred first |
| Efficacy: Best Overall Response | Best overall response that subjects had to treatment with tesevatinib: complete response (CR), partial response (PR), stable disease (SD), or non-response/progressive disease (PD) | Until disease progression, unacceptable toxicity, subject or investigator decision to discontinue, death, or up to 3 years, whichever occurred first |
| Efficacy: Objective Response Rate (ORR) | Proportion (%) of subjects who had either a complete response (CR) or a partial response (PR) to treatment with tesevatinib | Until disease progression, unacceptable toxicity, subject or investigator decision to discontinue, death, or 3 years, whichever occurred first |
| Exposure to Tesevatinib: Overall Mean | Mean total amount of tesevatinib (mg) subjects received during the study | Until disease progression, unacceptable toxicity, subject or investigator decision, death, or up to 3 years, whichever occurred first |
| Exposure to Tesevatinib: Overall Median | Median amount of tesevatinib (mg) subjects received during the study | Until disease progression, unacceptable toxicity, subject or investigator decision, death, or up to 3 years, whichever occurred first |
| Exposure to Tesevatinib: Mean Number of Cycles | Mean number of 28-day cycles of treatment with tesevatinib subjects received during the study | Until disease progression, unacceptable toxicity, subject or investigator decision, death, or up to 3 years, whichever occurred first. |
| Exposure to Tesevatinib: Median Number of Cycles | Median number of 28-day cycles of treatment with tesevatinib subjects received during the study | Until disease progression, unacceptable toxicity, subject or investigator decision, death, or up to 3 years, whichever occurred first |
| Duarte |
| California |
| 91010 |
| United States |
| University of California, San Francisco (UCSF) | San Francisco | California | 94143 | United States |
| University of Colorado Cancer Center | Aurora | Colorado | 80045 | United States |
| Massachusetts General Hospital | Boston | Massachusetts | 02114 | United States |
| Dana Farber Cancer Institute | Boston | Massachusetts | 02215 | United States |
| Henry Ford Hospital | Detroit | Michigan | 48202 | United States |
| Columbia University, Herbert Irving Comprehensive Cancer Center | New York | New York | 10032 | United States |
| Cleveland Clinic | Cleveland | Ohio | 44195 | United States |
| UT MD Anderson Cancer Center | Houston | Texas | 77030 | United States |
| Huntsman Cancer Institute | Salt Lake City | Utah | 84112 | United States |
| Subpopulation A (EGFR Gene Amplified Glioblastoma) |
|
| Subpopulation B (EGFRvIII^Pos Glioblastoma) |
|
| COMPLETED |
|
| NOT COMPLETED |
|
|
All Subjects: With or without EGFR gene-amplified and/or EGFRvIII^pos variant Sub-population A: With EGFR gene-amplified only Sub-population B: With EGFR gene-amplified + EGFRvIII^pos variant (Subset of Sub-population A) Note: EGFR = epidermal growth factor receptor
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| ID | Title | Description |
|---|---|---|
| BG000 | Total: All Subjects | Subjects with recurrent glioblastoma who had or did not have EGFR gene-amplified glioblastoma and/or EGFRvIII^pos variant |
| Units | Counts |
|---|---|
| Participants |
|
| Title | Description | Population Description | Parameter Type | Dispersion Type | Unit of Measure | Calculate Percentage | Denominator Units Selected | Denominators | Classes | ||||||||||||
|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|
| Age, Continuous | All Subjects: With or without EGFR gene-amplified and/or EGFRvIII^pos variant. Sub-population A: EGFR gene-amplified. Sub-population B: EGFRvIII^pos variant (Subset of Sub-population A). | Mean | Standard Deviation | Years |
| ||||||||||||||||
| Age, Customized | All Subjects: With or without EGFR gene-amplified and/or EGFRvIII^pos variant. Sub-population A: EGFR gene-amplified. Sub-population B: EGFRvIII^pos variant (Subset of Sub-population A). | Median | Full Range | Years |
| ||||||||||||||||
| Sex: Female, Male | All Subjects: With or without EGFR gene-amplified and/or EGFRvIII^pos variant. Sub-population A: EGFR gene-amplified. Sub-population B: EGFRvIII^pos variant (Subset of Sub-population A). | Count of Participants | Participants |
| |||||||||||||||||
| Ethnicity (NIH/OMB) | All Subjects: With or without EGFR gene-amplified and/or EGFRvIII^pos variant. Sub-population A: EGFR gene-amplified. Sub-population B: EGFRvIII^pos variant (Subset of Sub-population A). | Count of Participants | Participants |
| |||||||||||||||||
| Race (NIH/OMB) | All Subjects: With or without EGFR gene-amplified and/or EGFRvIII^pos variant. Sub-population A: EGFR gene-amplified. Sub-population B: EGFRvIII^pos variant (Subset of Sub-population A). | Count of Participants | Participants |
| |||||||||||||||||
| Karnofsky Performance Status (KPS) | Karnofsky Performance Score: 50 = requires considerable assistance and frequent medical care; 60 - requires occasional assistance, but is able to care for most of his personal needs; 70 = cares for self but is unable to carry on normal activity or to do active work; 80 = normal activity with effort and some signs or symptoms of disease; 90 - able to carry on normal activity and minor signs of symptoms of disease; 100 = normal no complaints with no evidence of disease | Count of Participants | Participants |
| |||||||||||||||||
| Prior Low Grade Astrocytoma Diagnosis | Low-grade astrocytoma (diffuse astrocytoma): usually an infiltrating tumor that grows relatively slowly and usually does not have well-defined borders | Count of Participants | Participants |
| |||||||||||||||||
| Months Since First Diagnosis of Glioblastoma: Mean | All Subjects: With or without EGFR gene-amplified and/or EGFRvIII^pos variant. Sub-population A: EGFR gene-amplified. Sub-population B: EGFRvIII^pos variant (Subset of Sub-population A). | Mean | Standard Deviation | Months |
| ||||||||||||||||
| Months Since First Diagnosis of Glioblastoma: Median | All Subjects: With or without EGFR gene-amplified and/or EGFRvIII^pos variant. Sub-population A: EGFR gene-amplified. Sub-population B: EGFRvIII^pos variant (Subset of Sub-population A). | Median | Full Range | Months |
| ||||||||||||||||
| Months Since Recurrent Diagnosis of Glioblastoma: Mean | All Subjects: With or without EGFR gene-amplified and/or EGFRvIII^pos variant. Sub-population A: EGFR gene-amplified. Sub-population B: EGFRvIII^pos variant (Subset of Sub-population A). | Mean | Standard Deviation | Months |
| ||||||||||||||||
| Months Since Recurrent Diagnosis of Glioblastoma: Median | All Subjects: With or without EGFR gene-amplified and/or EGFRvIII^pos variant. Sub-population A: EGFR gene-amplified. Sub-population B: EGFRvIII^pos variant (Subset of Sub-population A). | Median | Full Range | Months |
| ||||||||||||||||
| Number of Prior Systemic Therapy Regimens | Data were not available for all subjects | Count of Participants | Participants |
| |||||||||||||||||
| Prior Surgery | All Subjects: With or without EGFR gene-amplified and/or EGFRvIII^pos variant. Sub-population A: EGFR gene-amplified. Sub-population B: EGFRvIII^pos variant (Subset of Sub-population A). | Count of Participants | Participants |
| |||||||||||||||||
| Prior Radiotherapy--Site Irradiated | Analysis is for Sub-populations A and B, and for total which includes subjects in both Sub-populations A and B, and neither sub-population. | Count of Participants | Participants |
| |||||||||||||||||
| Best Overall Response | Best overall response to previous therapy | Response Criteria in Solid Tumors (RECIST): CR = complete response; PR = partial response; SD = stable disease; PD = progressive disease; | Count of Participants | Participants |
| ||||||||||||||||
| Reason Therapy Ended | Analysis is for Sub-populations A and B, and for total which includes subjects in both Sub-populations A and B, and neither sub-population. | Count of Participants | Participants |
| |||||||||||||||||
| Corticosteroid Used at Baseline | Data only available for 4 subjects | Count of Participants | Participants |
|
| Type | Title | Description | Population Description | Reporting Status | Anticipated Posting Date | Parameter Type | Dispersion Type | Unit of Measure | Calculate Percentage | Time Frame | Units Analyzed | Denominator Units Selected | Arm/Group Information | Denominators | Classes | Analyses | ||||||||||||||||||||||||||
|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|
| Primary | Efficacy: Median Progression-free Survival (PFS) Rate at 6 Months (PFS-6) | Proportion (%) of subjects who did not have progressive disease after treatment with tesevatinib at 6 months (PFS-6) after baseline | Posted | Number | 95% Confidence Interval | Percentage (%) of subjects | 6 months |
|
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| Secondary | Efficacy: Median PFS | Median duration (months) of subjects who were progression-free of disease from baseline | Posted | Median | 95% Confidence Interval | Months | Until disease progression, unacceptable toxicity, subject or clinician decision to discontinue, death, or up to 3 years, whichever occurred first |
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| Secondary | Efficacy: Median Overall Survival Rate at 9 Months (OS-9) | Median proportion (%) of subjects who survived 9 months after baseline | Posted | Number | 95% Confidence Interval | Percentage (%) of subjects | 9 months |
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| Secondary | Efficacy: Median OS | Median duration (months) subjects survived from baseline until death | Posted | Median | 95% Confidence Interval | Months | Until unacceptable toxicity, subject or investigator decision to discontinue, death, or up to 3 years, whichever occurred first |
|
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| Secondary | Efficacy: Best Overall Response | Best overall response that subjects had to treatment with tesevatinib: complete response (CR), partial response (PR), stable disease (SD), or non-response/progressive disease (PD) | Note: NA = data not available; NE = not evaluable | Posted | Count of Participants | Participants | Until disease progression, unacceptable toxicity, subject or investigator decision to discontinue, death, or up to 3 years, whichever occurred first |
|
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| Secondary | Efficacy: Objective Response Rate (ORR) | Proportion (%) of subjects who had either a complete response (CR) or a partial response (PR) to treatment with tesevatinib | Posted | Number | 95% Confidence Interval | Percentage (%) of participants | Until disease progression, unacceptable toxicity, subject or investigator decision to discontinue, death, or 3 years, whichever occurred first |
|
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| Secondary | Exposure to Tesevatinib: Overall Mean | Mean total amount of tesevatinib (mg) subjects received during the study | Posted | Mean | Standard Deviation | mg (tesevatinib) | Until disease progression, unacceptable toxicity, subject or investigator decision, death, or up to 3 years, whichever occurred first |
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| Secondary | Exposure to Tesevatinib: Overall Median | Median amount of tesevatinib (mg) subjects received during the study | Posted | Median | Full Range | mg (tesevatinib) | Until disease progression, unacceptable toxicity, subject or investigator decision, death, or up to 3 years, whichever occurred first |
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| Secondary | Exposure to Tesevatinib: Mean Number of Cycles | Mean number of 28-day cycles of treatment with tesevatinib subjects received during the study | Posted | Mean | Standard Deviation | Number of cycles | Until disease progression, unacceptable toxicity, subject or investigator decision, death, or up to 3 years, whichever occurred first. |
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| Secondary | Exposure to Tesevatinib: Median Number of Cycles | Median number of 28-day cycles of treatment with tesevatinib subjects received during the study | Posted | Median | Full Range | Number of cycles | Until disease progression, unacceptable toxicity, subject or investigator decision, death, or up to 3 years, whichever occurred first |
|
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Subjects were followed for treatment-emergent adverse events and other safety assessments from screening through 30-day follow-up.
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| ID | Title | Description | Deaths (Affected) | Deaths (At Risk) | Serious Events (Affected) | Serious Events (At Risk) | Other Events (Affected) | Other Events (At Risk) |
|---|---|---|---|---|---|---|---|---|
| EG000 | Total | Subjects with recurrent glioblastoma who had or did not have EGFR gene-amplified and/or EGFRvIII^pos variant glioblastoma. Includes 24 subjects who had EGFR gene-amplified (Sub-population A, 11 subjects who had EGFRvIII^pos and EGFR gene-amplified (Sub-population B which is a subset of Sub-population A) and 16 subjects who were in neither sub-population | 28 | 40 | 12 | 40 | 40 | 40 |
| EG001 | Sub-population A | Subjects with EGFR gene-amplified glioblastoma | 19 | 24 | 7 | 24 | 24 | 24 |
| EG002 | Sub-population B | Subjects with EGFRvIII^pos variant glioblastoma (Subset of Sub-population A) | 9 | 11 | 2 | 11 | 11 | 11 |
| Term | Organ System | Source Vocabulary | Assessment Type | Notes | Statistical Information |
|---|---|---|---|---|---|
| Hemiparesis | Nervous system disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Brain edema | Nervous system disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Cerebrovascular accident | Nervous system disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Aphasia | Nervous system disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Cerebral hemorrhage | Nervous system disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Facial paralysis | Nervous system disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Seizure | Nervous system disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Mental status changes | Psychiatric disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Confusional state | Psychiatric disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Abdominal abscess | Infections and infestations | MedDRA (18.1) | Systematic Assessment |
| |
| Appendicitis | Infections and infestations | MedDRA (18.1) | Systematic Assessment |
| |
| Pelvic abscess | Infections and infestations | MedDRA (18.1) | Systematic Assessment |
| |
| Wound infection | Infections and infestations | MedDRA (18.1) | Systematic Assessment |
| |
| Pancreatitis | Gastrointestinal disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Pancreatitis acute | Gastrointestinal disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Wound dehiscene | Injury, poisoning and procedural complications | MedDRA (18.1) | Systematic Assessment |
| |
| Muscular weakness | Musculoskeletal and connective tissue disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Glioblastoma | Neoplasms benign, malignant and unspecified (incl cysts and polyps) | MedDRA (18.1) | Systematic Assessment |
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| Acute kidney injury | Renal and urinary disorders | MedDRA (18.1) | Systematic Assessment |
|
| Term | Organ System | Source Vocabulary | Assessment Type | Notes | Statistical Information |
|---|---|---|---|---|---|
| Diarrhea | Gastrointestinal disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Nausea | Gastrointestinal disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Abdominal pain | Gastrointestinal disorders | MedDRA (18.1) | Systematic Assessment |
| |
| GERD | Gastrointestinal disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Anal incontinence | Gastrointestinal disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Constipation | Gastrointestinal disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Mouth ulceration | Gastrointestinal disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Dermatitis acneiform | Skin and subcutaneous tissue disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Rash | Skin and subcutaneous tissue disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Rash papular | Skin and subcutaneous tissue disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Pruritus | Skin and subcutaneous tissue disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Aphasia | Nervous system disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Hemiparesis | Nervous system disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Headache | Nervous system disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Dizziness | Nervous system disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Seizure | Nervous system disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Paresthia | Nervous system disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Brain edema | Nervous system disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Cerebrovascular accident | Nervous system disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Cognitive disorder | Nervous system disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Facial paresis | Nervous system disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Memory impairment | Nervous system disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Fatigue | General disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Gait disturbance | General disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Asthenia | General disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Peripheral edema | General disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Pain | General disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Alanine aminotransferase increased | Investigations | MedDRA (18.1) | Systematic Assessment |
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| Aspartate aminotransferase increased | Investigations | MedDRA (18.1) | Systematic Assessment |
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| QT interval prolongation | Investigations | MedDRA (18.1) | Systematic Assessment |
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| Weight decreased | Investigations | MedDRA (18.1) | Systematic Assessment |
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| Hemoglobin decreased | Investigations | MedDRA (18.1) | Systematic Assessment |
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| Lymphocyte count decreased | Investigations | MedDRA (18.1) | Systematic Assessment |
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| Platelet count decreased | Investigations | MedDRA (18.1) | Systematic Assessment |
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| Weight increased | Investigations | MedDRA (18.1) | Systematic Assessment |
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| Decreased appetite | Metabolism and nutrition disorders | MedDRA (18.1) | Systematic Assessment |
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| Hypokalemia | Metabolism and nutrition disorders | MedDRA (18.1) | Systematic Assessment |
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| Hyperglycemia | Metabolism and nutrition disorders | MedDRA (18.1) | Systematic Assessment |
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| Hypomagnesemia | Metabolism and nutrition disorders | MedDRA (18.1) | Systematic Assessment |
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| Hypophosphatemia | Metabolism and nutrition disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Dehydration | Metabolism and nutrition disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Urinary tract infection | Infections and infestations | MedDRA (18.1) | Systematic Assessment |
| |
| Confusional state | Psychiatric disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Insomnia | Psychiatric disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Mental status changes | Psychiatric disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Cough | Respiratory, thoracic and mediastinal disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Dysphonia | Respiratory, thoracic and mediastinal disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Muscular weakness | Musculoskeletal and connective tissue disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Muscle spasms | Musculoskeletal and connective tissue disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Vision blurred | Eye disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Fall | Injury, poisoning and procedural complications | MedDRA (18.1) | Systematic Assessment |
| |
| Hypertension | Vascular disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Deep vein thrombosis | Vascular disorders | MedDRA (18.1) | Systematic Assessment |
| |
| Cushingoid | Endocrine disorders | MedDRA (18.1) | Systematic Assessment |
|
Not provided
Not provided
| Title | Organization | Phone | Extension | |
|---|---|---|---|---|
| Miranda Ross | Kadmon Corporation | 724-778-6170 | Miranda.Ross@kadmon.com |
| Prot_000.pdf |
| SAP | No | Yes | No | Statistical Analysis Plan | Jun 30, 2020 | Jun 2, 2021 | SAP_001.pdf |
| ID | Term |
|---|---|
| D005909 | Glioblastoma |
| D001932 | Brain Neoplasms |
| ID | Term |
|---|---|
| D001254 | Astrocytoma |
| D005910 | Glioma |
| D018302 | Neoplasms, Neuroepithelial |
| D017599 | Neuroectodermal Tumors |
| D009373 | Neoplasms, Germ Cell and Embryonal |
| D009370 | Neoplasms by Histologic Type |
| D009369 | Neoplasms |
| D009375 | Neoplasms, Glandular and Epithelial |
| D009380 | Neoplasms, Nerve Tissue |
| D016543 | Central Nervous System Neoplasms |
| D009423 | Nervous System Neoplasms |
| D009371 | Neoplasms by Site |
| D001927 | Brain Diseases |
| D002493 | Central Nervous System Diseases |
| D009422 | Nervous System Diseases |
Not provided
Not provided
| ID | Term |
|---|---|
| C571826 | XL647 |
Not provided
Not provided
Not provided
|
| Sub-population B |
|
|
| Sub-population A |
|
|
| Sub-population B |
|
|
| Male |
|
| Sub-population A |
|
|
| Sub-population B |
|
|
| Not Hispanic or Latino |
|
| Unknown or Not Reported |
|
| Sub-population A (EGFRvIII^pos glioblastoma) |
|
|
| Sub-population B |
|
|
| Asian |
|
| Native Hawaiian or Other Pacific Islander |
|
| Black or African American |
|
| White |
|
| More than one race |
|
| Unknown or Not Reported |
|
| Sub-population A |
|
|
| Sub-population B |
|
|
| 60 (Score) |
|
| 70 (Score) |
|
| 80 (Score) |
|
| 90 (Score) |
|
| 100 (Score) |
|
| Sub-population A (EGFRvIII^pos glioblastoma) |
|
|
| Sub-population |
|
|
| No |
|
| Sub-population A |
|
|
| Sub-population B |
|
|
| Sub-population A |
|
|
| Sub-population B |
|
|
| Sub-population A |
|
|
| Sub-population B |
|
|
| Sub-population A |
|
|
| Sub-population B |
|
|
| Sub-population A (EGFRvIII^pos glioblastoma) |
|
|
| Sub-population B |
|
|
| 2 Regimens |
|
| > 2 Regimens |
|
| No Prior Systemic Therapy |
|
| Sub-population A |
|
|
| Sub-population B |
|
|
| No |
|
| Unknown |
|
| Sub-population A |
|
|
| Sub-population B |
|
|
| Other |
|
| Sub-population A |
|
|
| Sub-population |
|
|
| PR |
|
| SD |
|
| PD |
|
| Unknown |
|
| Sub-population A |
|
|
| Sub-population B |
|
|
| Progressive Disease |
|
| Study Drug Toxicity |
|
| Other |
|
| Sub-population A |
|
|
| Sub-population B |
|
|
| Dose increased |
|
| Dose decreased |
|
| Dose stable |
|
| Unknown |
|
| Sub-population A |
|
|
| Sub-population B |
|
|
|
|
|
|
|
|
|
|
|
|