Blinatumomab and Combination Chemotherapy or Dasatinib, Prednisone, and Blinatumomab in Treating Older Patients With Acute Lymphoblastic Leukemia
Official Title
A Phase 2 Study of Blinatumomab and POMP (Prednisone, Vincristine, Methotrexate, 6-Mercaptopurine) for Patients >/= 65 Years of Age With Newly Diagnosed Philadelphia-Chromosome Negative (Ph-) Acute Lymphoblastic Leukemia (ALL) and of Dasatinib, Prednisone and Blinatumomab for Patients >/= 65 Years of Age With Newly Diagnosed Philadelphia-Chromosome Positive (Ph+) ALL, Relapsed/Refractory Ph+ ALL, and Philadelphia-Chromosome-Like Signature (Ph-Like) ALL (Newly Diagnosed or Relapsed/Refractory) With Known or Presumed Activating Dasatinib-Sensitive Mutations or Kinase Fusions (DSMKF)
Acronym
Not provided
Organization
National Cancer Institute (NCI)NIH
Status Module
Record Verification Date
Feb 2026
Overall Recruitment Status or Expanded Access Status
Active, not recruiting
Last Known Status
Not provided
Delayed Posting
Not provided
Why Stopped
Not provided
Expanded Access Info
No
Start Date
Jun 30, 2015Actual
Primary Completion Date
Jun 1, 2022Actual
Completion Date
Jan 26, 2027Estimated
First Submitted Date
May 19, 2014
First Submission Date that Met QC Criteria
May 19, 2014
First Posted Date
May 21, 2014Estimated
Results Waived
Not provided
Results First Submitted Date
Nov 17, 2022
Results First Submitted that Met QC Criteria
Jan 3, 2023
Results First Posted Date
Jan 25, 2023Actual
Certification/Extension (aka Delayed Results) First Submitted Date
Not provided
Certification/Extension First Submitted that Passed QC Review
Not provided
Certification/Extension First Posted Date
Not provided
Last Update Submitted Date
May 12, 2026
Last Update Posted Date
May 28, 2026Actual
Sponsor/Collaborators Module
Responsible Party, by Official Title
Sponsor
Lead Sponsor
National Cancer Institute (NCI)NIH
Collaborators
Not provided
Oversight Module
Has Data Monitoring Committee (DMC)
No
Is FDA Regulated Drug
Not provided
Is FDA Regulated Device
Not provided
Is Unapproved Device
Not provided
Pediatric Postmarket Surveillance of a Device Product
Not provided
Product Exported from US
Not provided
FDAAA801 Violation
Not provided
Description Module
Brief Summary
This phase II trial studies the side effects and how well blinatumomab and combination chemotherapy or dasatinib, prednisone, and blinatumomab work in treating older patients with acute lymphoblastic leukemia. Immunotherapy with monoclonal antibodies, such as blinatumomab, may help the body's immune system attack the cancer, and may interfere with the ability of tumor cells to grow and spread. Chemotherapy drugs, such as prednisone, vincristine sulfate, methotrexate, and mercaptopurine, work in different ways to stop the growth of cancer cells, either by killing the cells, by stopping them from dividing, or by stopping them from spreading. Dasatinib may stop the growth of cancer cells by blocking some of the enzymes needed for cell growth. Giving blinatumomab with combination chemotherapy or dasatinib and prednisone may kill more cancer cells.
Detailed Description
PRIMARY OBJECTIVES:
I. To evaluate the 3-year survival rate in elderly patients with newly diagnosed Philadelphia (Ph)-negative acute lymphoblastic leukemia (ALL) treated with blinatumomab followed by POMP (prednisone, vincristine sulfate, methotrexate, and mercaptopurine) maintenance.
II. To evaluate in a preliminary manner (feasibility study) the safety of dasatinib-steroid based induction followed by blinatumomab treatment in combination with dasatinib followed by dasatinib-based maintenance in patients with newly diagnosed Ph-positive ALL, relapsed/refractory Ph-positive ALL, and Ph-like dasatinib-sensitive mutations or kinase fusions (DSMKF) ALL (newly-diagnosed relapsed or refractory).
SECONDARY OBJECTIVES:
I. To evaluate toxicities in these patient populations treated with these regimens.
II. To estimate the rates of complete response (CR), complete remission with incomplete count recovery (CRi) and disease-free survival in Ph-negative patients.
III. To estimate disease-free and overall survival in Ph-positive ALL and Ph-like DSMKF ALL.
IV. To estimate in each cohort the rate of minimal residual disease (MRD) negativity, and the time to achieve MRD negativity (exploratory analysis).
V. To determine whether anti-idiotype antibodies directed against blinatumomab develop with blinatumomab treatment in this study.
ADDITIONAL TRANSLATIONAL MEDICINE OBJECTIVES:
I. To estimate the incidence of the Ph-like signature in elderly patients (>= 65 years of age) with newly diagnosed Philadelphia-chromosome negative ALL.
II. To estimate the incidence of the various tyrosine-kinase fusions, making up the Ph-like signature in elderly patients with newly diagnosed Philadelphia-chromosome negative ALL.
III. To evaluate outcomes (event free survival [EFS] and overall survival [OS]) in patients with the Ph-like signature versus those without the Ph-like signature in Ph-negative ALL.
IV. To describe via single cell transcriptomics the clonal diversity in gene expression of participants on the trial.
V. To describe the methylation status of the overall genome as well as key driver genes of all participants in the trial.
OUTLINE: Patients are assigned to 1 of 2 treatment cohorts according to Philadelphia chromosome status.
COHORT I (PHILADELPHIA CHROMOSOME NEGATIVE PATIENTS):
INDUCTION: Patients receive blinatumomab intravenously (IV) continuously over 24 hours on days 1-28 in the absence of disease progression or unacceptable toxicity. Patients undergo an x-ray and echocardiography (ECHO) during screening and a computed tomography (CT) scan and/or magnetic resonance imaging (MRI) as well as blood sample collection and bone marrow aspiration and biopsy throughout the trial. Patients undergo a lumbar puncture during screening and on study. Patients may also undergo a biopsy during screening. (Closed to accrual 06/29/17)
RE-INDUCTION: Patients not achieving CR or CRi after Induction, receive blinatumomab IV continuously over 24 hours on days 1-28 in the absence of disease progression or unacceptable toxicity. Patients undergo an x-ray and ECHO during screening and a CT scan and/or MRI as well as blood sample collection and bone marrow aspiration and biopsy throughout the trial. Patients undergo a lumbar puncture during screening and on study. Patients may also undergo a biopsy during screening.
POST-REMISSION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28. Treatment repeats every 42 days for 3 cycles in the absence of disease progression or unacceptable toxicity. Patients undergo a CT scan and/or MRI on study and during follow-up. Patients also undergo blood sample collection, lumbar puncture, and bone marrow aspiration and biopsy on study.
MAINTENANCE: Patients receive prednisone orally (PO) on days 1-5, vincristine sulfate IV on day 1, mercaptopurine PO on days 1-28, and methotrexate PO on days 1, 8, 15, and 22. Treatment repeats every 28 days for 18 cycles in the absence of disease progression or unacceptable toxicity. Patients undergo a CT scan and/or MRI on study and during follow-up. Patients also undergo a lumbar puncture and bone marrow aspiration and biopsy on study.
COHORT II (PHILADELPHIA CHROMOSOME POSITIVE PATIENTS):
INDUCTION: Patients receive dasatinib PO on days 1-84 and prednisone PO on days 1-24 with tapering on days 25-32 in the absence of disease progression or unacceptable toxicity. Patients undergo an x-ray and ECHO during screening and a CT scan and/or MRI throughout the trial. Patients undergo a lumbar puncture and bone marrow aspiration and biopsy during screening and on study. Patients may also undergo a biopsy during screening.
RE-INDUCTION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28. Treatment repeats every 42 days for 2 cycles in the absence of disease progression or unacceptable toxicity. Patients undergo a CT scan and/or MRI on study and during follow-up. Patients also undergo blood sample collection, a lumbar puncture, and bone marrow aspiration and biopsy on study.
POST-REMISSION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28 and dasatinib PO on days 1-42. Treatment repeats every 42 days for 3 cycles in the absence of disease progression or unacceptable toxicity. Patients undergo a CT scan and/or MRI on study and during follow-up. Patients also undergo blood sample collection, lumbar puncture, and bone marrow aspiration and biopsy on study.
MAINTENANCE: Patients receive dasatinib PO on days 1-28. Cycles repeat every 28 days in the absence of disease progression or unacceptable toxicity. Patients also receive prednisone PO on days 1-5. Treatment repeats every 28 days for 18 cycles in the absence of disease progression or unacceptable toxicity. Patients undergo a CT scan and/or MRI as well as a lumbar puncture and bone marrow aspiration and biopsy on study.
After completion of study treatment, patients are followed up every 3 months for 2 years, every 6 months for 2 years, and then annually until 10 years from initial registration.
Conditions Module
Conditions
Acute Lymphoblastic Leukemia
B Acute Lymphoblastic Leukemia
B Acute Lymphoblastic Leukemia With t(9;22)(q34.1;q11.2); BCR-ABL1
Recurrent Acute Lymphoblastic Leukemia
Refractory Acute Lymphoblastic Leukemia
Keywords
Not provided
Design Module
Study Type
Interventional
Number of References to an Expanded Access Study
Not provided
Expanded Access Types
Not provided
Patient Registry
Not provided
Target Follow-Up Duration
Not provided
Phases
Phase 2
Interventional Study Design
Allocation
Biospecimen
No data available
No data is available for this block.
Enrollment
53Actual
Arms/Interventions Module
Arm Groups
Label
Type
Description
Intervention Names
Cohort I (blinatumomab, POMP)
Experimental
See Detailed Description
Procedure: Biopsy Procedure
Procedure: Biospecimen Collection
Biological: Blinatumomab
Procedure: Bone Marrow Aspiration and Biopsy
Procedure: Computed Tomography
Procedure: Echocardiography Test
Procedure: Lumbar Puncture
Procedure: Magnetic Resonance Imaging
Drug: Mercaptopurine
Drug: Methotrexate
Drug: Methotrexate Sodium
Drug: Prednisone
Drug: Vincristine
Drug: Vincristine Sulfate
Procedure: X-Ray Imaging
Cohort II (dasatinib, prednisone, blinatumomab)
Experimental
See Detailed Description
Procedure: Biopsy Procedure
Procedure: Biospecimen Collection
Biological: Blinatumomab
Procedure: Bone Marrow Aspiration and Biopsy
Procedure: Computed Tomography
Drug: Dasatinib
Procedure: Echocardiography Test
Procedure: Lumbar Puncture
Procedure: Magnetic Resonance Imaging
Drug: Prednisone
Procedure: X-Ray Imaging
Interventions
Name
Type
Description
Arm Group Labels
Other Names
Biopsy Procedure
Procedure
Undergo a biopsy
Cohort I (blinatumomab, POMP)
Cohort II (dasatinib, prednisone, blinatumomab)
Outcomes Module
Primary Outcomes
Measure
Description
Time Frame
Overall Survival Rate (Cohort I)
To evaluate the 3-year overall survival rate in elderly participants with newly diagnosed Ph-negative ALL treated with blinatumomab followed by POMP maintenance. Overall
From the day of registration on study until death from any cause, assessed at 3 years
Incidence of Dose-limiting Toxicity (Cohort II)
Defined as any grade 4 or higher treatment-related, non-hematologic toxicity in the first cycle of post-remission therapy (blinatumomab/dasatinib) graded by National Cancer Institute (NCI) Common Terminology Criteria for Adverse Events (CTCAE) version 4.0. Only participants with Ph-positive ALL or Ph-like DSMKF ALL were evaluated.
Up to day 42 of post-remission therapy
Secondary Outcomes
Measure
Description
Time Frame
Number of Participants With Grade 3 Through 5 Adverse Events That Are Related to Study Drugs
Number of participants with Grade 3-5 adverse events that are possibly, probably or definitely related to study drug are reported by given type of adverse event. Adverse Events reported using CTCAE v 4.0, whereas Serious Adverse Events were reported with CTCAE v 5.0.
Duration of treatment and follow up until death or date of primary analysis (about 7.5 years)
Other Outcomes
Not provided
Eligibility Module
Eligibility Criteria
Inclusion Criteria:
Registration Step 1 - Induction/Re-Induction:
Patients must have a new morphologic diagnosis of precursor B cell acute lymphoblastic leukemia (ALL) (non T cell) based on World Health Organization (WHO) criteria; patients with Burkitt's (L3) are excluded; patients with Ph-positive or Ph-like ALL with dasatinib-sensitive mutations or kinase fusions may have relapsed or refractory diagnoses
NOTE: Relapsed/refractory Ph-positive patients or Ph-like patients with dasatinib-sensitive mutations or kinase fusions who have previous exposure to either dasatinib or another 2nd or 3rd generation tyrosine kinase inhibitor (TKI) will begin protocol therapy with Cohort 2: re-induction cycle 1
Patients must have a diagnosis of Philadelphia chromosome negative ALL or Ph chromosome positive ALL by cytogenetics, fluorescence in situ hybridization (FISH) or polymerase chain reaction (PCR); patients will be registered to receive treatment in either Cohort 1 (Ph-) or Cohort 2 (Ph+ or Ph-like DSMKF) based on these results; diagnostic specimens must be submitted to the site's local Clinical Laboratory Improvement Amendments (CLIA)-approved cytogenetics laboratory and results of tests (cytogenetics, FISH or PCR) must confirm Ph status prior to registration; if not already known, breakpoint cluster region- abelson murine leukemia viral oncogene homolog 1 (BCR-ABL) status (p190 or p210) must be evaluated in Ph-positive patients by PCR
For Cohort 2, Ph-like testing is not required specifically for this study; however, to be registered to Cohort 2 under the Ph-like DSMKF criterion, the patient must have a known or presumed activating Ph-like signature and dasatinib-sensitive mutation or kinase fusion, such as: ABL1, ABL2, colony stimulating factor 1 receptor (CSF1R), platelet derived growth factor receptor beta (PDGFRB), platelet derived growth factor receptor alpha (PDGFRA), or fibroblast growth factor receptor (FGFR)s that was otherwise identified as part of normal standard of care; prior to registering any patients with a known or presumed activating Ph-like signature and dasatinib-sensitive mutations or kinase fusions (DSMKF) treating physicians must confirm eligibility with the study chairs via email; the study chairs must respond via email with confirmation of patient eligibility prior to patient registration
All newly diagnosed patients must have evidence of ALL in their marrow or peripheral blood with at least 20% lymphoblasts present in blood or bone marrow collected within 28 days prior to registration; all relapsed/refractory patients (Cohort 2) must have at least 5% lymphoblasts present in blood or bone marrow collected within 28 days prior to registration; for relapsed/refractory patients, pathology and cytogenetics reports (both from time of original diagnosis) must be submitted at time of registration; if a bone marrow aspirate cannot be obtained despite an attempt (dry tap), appropriate immunohistochemistry (IHC) testing, including cluster of differentiation (CD)19, must be performed on the bone marrow biopsy to determine lineage; for ALL in marrow or peripheral blood, immunophenotyping of the blood or marrow lymphoblasts must be performed to determine lineage (B cell, T cell or mixed B/T cell); appropriate marker studies including CD19 (B cell), must be performed; co-expression of myeloid antigens (CD13 and CD33) will not exclude patients; if possible, the lineage specific markers (myeloid cells) should be determined; the blood/bone marrow sample for these assays must be obtained within 28 days prior to registration; patients with only extramedullary disease in the absence of bone marrow or blood involvement are not eligible
Patient must not have a history or presence of clinically relevant central nervous system (CNS) pathology such as epilepsy, seizure, paresis, aphasia, stroke, severe brain injuries, dementia, Parkinson's disease, cerebellar disease, organic brain syndrome, psychosis, active ALL in the CNS confirmed by cerebrospinal fluid (CSF) analysis, or other significant CNS abnormalities
Patients must have a lumbar puncture to determine CNS involvement of ALL within 14 days prior to registration; patients with CNS3 are excluded from the trial; patients with CNS1 or CNS2 will be eligible, but will be monitored for CNS involvement; note that intrathecal methotrexate administered during the pre-study lumbar puncture may count as the first dose of intrathecal therapy required as part of the study
Cohort I, Ph-negative Patients Only: Patients must not have received any prior chemotherapy, radiation therapy, or other therapy for the treatment of ALL (other than those noted below) and must not be receiving any immunosuppressive therapy; patients may not have received any prior investigational therapy within 28 days prior to registration; patients must not have received any monoclonal antibody therapy within 42 days of registration; patients may have received the following within any time prior to registration: low dose chemotherapy-including: cyclophosphamide 1 g/m^2, oral 6-mercaptopurine, or oral methotrexate (other low dose chemotherapy may be allowable, however any other options not listed here should be confirmed with the study chairs), TKI therapy, steroids, hydroxyurea, leukapheresis, intrathecal chemotherapy or vincristine
Cohort I, Ph-negative Patients Only: In the event that the patient's bone marrow blast count is >= 50% blasts, patients may be registered but should receive steroids for 3-5 days in order to reduce tumor burden prior to blinatumomab administration, as follows
Prephase treatment with dexamethasone (10-20 mg/m^2) for 3-5 days is required for patients with bone marrow blasts >= 50%, peripheral blood blasts 15,000/uL or higher, or elevated lactate dehydrogenase (LDH) suggesting rapidly progressive disease per investigator opinion
Pre-treatment should conclude at least 24 hours prior to the first dose of blinatumomab (although additional dexamethasone is automatically given as a pre-med prior to the first dose); at the time of first infusion of blinatumomab, the absolute peripheral blast count should be < 25,000/uL
Note: For the purposes of the study, day 1 of the cycle will be the first day of blinatumomab administration
Cohort I, Ph-negative Patients Only: It is preferred, but not required, that corticosteroids and hydroxyurea should start only after all diagnostic samples have been obtained; however, if the patient was previously on corticosteroids and/or hydroxyurea, this is allowable provided that the patient still has measurable disease at time of the bone marrow aspirate
Corticosteroids and/or hydroxyurea, as well as any of the other therapies mentioned (with the exception of IV cyclophosphamide), may continue to be administered, at physician discretion, until 1 day prior to blinatumomab administration
IV cyclophosphamide must be discontinued at least 7 days prior to blinatumomab administration
Cohort 2, Ph-positive and Ph-like DSMKF Patients Only: Patients must NOT have received a prior autologous or allogeneic hematopoietic stem cell transplant at any time. Patients must NOT have received any chemotherapy, investigational agents, or undergone major surgery within 14 days prior to registration, with the following exceptions:
Monoclonal antibodies must not have been received for 1 week prior to registration
Chimeric antigen receptor (CAR) T-cells must not have been received for 28 days prior to registration
Steroids, hydroxyurea, vincristine, 6-mercaptopurine, methotrexate, thioguanine and intrathecal chemotherapy are permitted within any timeframe prior to registration; Food and Drug Administration (FDA)-approved TKIs may also be administered until 1 day prior to start of study therapy (C1, D1); IV cyclophosphamide may be administered at doses of 1 g/m^2 or less until up to 7 days prior to registration
Patients must be >= 65 years of age; for patients 65-69 years of age, patient must be deemed not suitable for standard intensive induction chemotherapy at the discretion of the local investigator, or must have refused standard intensive chemotherapy
Cohort I, Ph-negative Patients Only: Patients must not be candidates for allogeneic hematopoietic stem cell transplant; NOTE: Subjects up to age 70 years who are considered fit for allogeneic hematopoietic stem cell transplant, should be considered for enrollment on E1910, in order to avoid competing with that study; if a patient is considered unfit for intensive chemotherapy at the time of initial diagnosis, but subsequently achieves a complete remission (CR), then it will be left to the treating physician's discretion to consider hematopoietic stem cell transplant (HSCT)
Cohort I, Ph-negative Patients Only: Patients must have complete history and physical examination within 28 days prior to registration
Cohort I, Ph-negative Patients Only: Patients must have a Zubrod performance status of 0-2
Cohort I, Ph-negative Patients Only: Patients must have serum creatinine =< 1.5 mg/dl within 14 days prior to registration
Cohort I, Ph-negative Patients Only: Patients must have aspartate aminotransferase (AST) and alanine aminotransferase (ALT) =< 3.0 x institutional upper limit of normal (IULN) within 14 days prior to registration
Cohort I, Ph-negative Patients Only: Patients must have total bilirubin =< 2.0 x IULN within 14 days prior to registration
Cohort I, Ph-negative Patients Only: Patients must have alkaline phosphatase =< 2.5 x IULN within 14 days prior to registration
Cohort I, Ph-negative Patients Only: Patients must not have systemic fungal, bacterial, viral or other infection that is not controlled (defined as exhibiting ongoing signs/symptoms related to the infection and without improvement, despite appropriate antibiotics or other treatment)
Cohort I, Ph-negative Patients Only: Patients must not have Common Terminology Criteria for Adverse Events (CTCAE) >= grade 2 neuropathy (cranial, motor or sensory) within 14 days prior to registration
Cohort I, Ph-negative Patients Only: Patients known to be positive for HIV (the human immunodeficiency virus) may be eligible, providing they meet the following additional criteria within 28 days prior to registration:
No history of acquired immune deficiency syndrome (AIDS)-defining conditions
CD4 cells > 350 cells/mm^3
If on antiretroviral agents, must not include zidovudine or stavudine
Viral load =< 50 copies HIV messenger ribonucleic acid (mRNA)/mm^3 if on combination antiretroviral therapy (cART) or =< 25,000 copies HIV mRNA/mm^3 if not on cART
Highly active antiretroviral therapy (HAART) regimens are acceptable providing they have only weak P450A4 interactions
Cohort I, Ph-negative Patients Only: Patients must not have any known autoimmune disease
Cohort I, Ph-negative Patients Only: Patients must not have testicular involvement; if clinical or ultrasound findings are equivocal, biopsy must be performed; all tests for establishing testicular involvement must be completed within 14 days prior to registration
Cohort I, Ph-negative Patients Only: Patients with evidence of extramedullary disease at diagnosis will have computed tomography (CT) scan or magnetic resonance imaging (MRI) of the chest, abdomen and pelvis to obtain baseline values within 28 days prior to registration
Cohort I, Ph-negative Patients Only: No other prior malignancy is allowed except for the following: adequately treated basal cell or squamous cell skin cancer, in situ cervical cancer, adequately treated stage I or II cancer from which the patient is currently in complete remission, or any other cancer from which the patient has been disease free for five years
Cohort I, Ph-negative Patients Only: Patients must have the following tests within 28 days prior to registration to obtain baseline measurements:
Prothrombin time (PT)/partial thromboplastin time (PTT)/international normalized ratio (INR)/fibrinogen (all patients)
Cohort 2, Ph+ and Ph-like DSMKF Patients Only: Patients must not have active pericardial effusion, ascites or pleural effusion of any grade based on chest x-ray and echocardiogram within 28 days prior to registration; exception: if the effusion is suspected to be related to the leukemia, the patient may have pericardial effusion =< grade 2 or pleural effusion =< grade 1
Cohort 2, Ph+ and Ph-like DSMKF Patients Only: Patients must have ejection fraction >= 45% based on echocardiogram performed within 28 days prior to registration
Cohort 2, Ph+ and Ph-like DSMKF Patients Only: Patients must have QTcF (by Fridericia calculation) < 480/msec based on electrocardiogram (EKG) performed within 28 days prior to registration
Cohort 2, Ph+ and Ph-like DSMKF Patients Only: Patients must not be receiving any proton pump inhibitors at the time of registration
Pretreatment cytogenetics must be performed on all patients; collection of pretreatment specimens must be completed within 28 days prior to registration to S1318; specimens must be submitted to the site's preferred CLIA-approved cytogenetics laboratory; BCR-ABL status must be verified in Ph-positive patients by FISH, cytogenetics, and/or PCR prior to enrollment; if a patient is Ph-positive, PCR for both p190 and p210 must be sent
Patients must be offered participation in specimen submission for future research; with patient's consent, specimens must be submitted as outlined
Cohort 1, Ph-negative Patients Only: Patients must have specimens submitted for blinatumomab immunogenicity assessment; collection of pretreatment specimens must be completed within 28 days prior to registration to S1318; specimens must be submitted to LabConnect
Cohort 2, Ph-positive and Ph-like DSMKF Patients Only: Patients must agree to have specimens submitted for blinatumomab immunogenicity testing if subsequently moved to a blinatumomab containing treatment regimen on protocol
Patients or their legally authorized representative must be informed of the investigational nature of this study and must sign and give written informed consent in accordance with institutional and federal guidelines
As a part of the Oncology Patient Enrollment Network (OPEN) registration process the treating institution's identity is provided in order to ensure that the current (within 365 days) date of institutional review board approval for this study has been entered in the system
Registration Step 2 - Post-Remission Therapy:
Cohort 1, Ph-negative Patients Only: Patients must have achieved CR or CRi within 2 cycles of induction/re-induction with blinatumomab
NOTE: day 1 of post-remission = day 43 of the preceding cycle (+/- 3 days)
Cohort 2, Ph-positive and Ph-like DSMKF Patients Only: Newly diagnosed Ph+, newly-diagnosed Ph-like DSMKF, and relapsed/refractory Ph+ patients without prior dasatinib or other 2nd or 3rd generation TKI therapy, must have achieved CR or CRi within 1 cycle of induction with dasatinib/prednisone, or within 2 cycles of re-induction with blinatumomab; relapsed/refractory Ph+ or Ph-like DSMKF patients with prior dasatinib or other 2nd or 3rd generation TKI therapy must have achieved CR or CRi within 2 cycles of re-induction therapy with blinatumomab
NOTE: day 1 of post-remission = day 85 of the preceding induction cycle (+/- 3 days), or day 43 of the preceding re-induction cycle (+/- 3 days) as applicable
Serum creatinine =< 1.5 mg/dl within 14 days prior to registration
AST and ALT =< 3.0 x institutional upper limit of normal (IULN) within 14 days prior to registration
Total bilirubin =< 2.0 x IULN within 14 days prior to registration
Absolute neutrophil count (ANC) >= 750/mcL within 28 days prior to registration
Platelets >= 50,000/mcL within 28 days prior to registration
Patients must be registered to Step 2 within 28 days after count recovery; (Note: there is no maximum allotted time period for count recovery, providing patient remains in CR or CRi)
All non-hematologic treatment related toxicities that are deemed clinically significant by the treating investigator must have resolved to =< grade 2
Registration Step 3 - Maintenance: Patients must have documented CR or CRi within 28 days prior to registration; note that bone marrow examination is only required if there are clinical signs/symptoms of progression; if progression is a concern due to the length of the time for count recovery, a bone marrow examination is recommended
Registration Step 3 - Maintenance: Patients must have serum creatinine =< 1.5 mg/dl within 14 days prior to registration
Registration Step 3 - Maintenance: Patients must have AST and ALT =< 3.0 x institutional upper limit of normal (IULN) within 14 days prior to registration
Registration Step 3 - Maintenance: Patients must have total bilirubin < 2.0 x institutional upper limit of normal (IULN) within 14 days prior to registration
Registration Step 3 - Maintenance: Patients must have adequate marrow function as evidenced by ANC >= 750/mcL within 28 days prior to registration
Registration Step 3 - Maintenance: Patients must have adequate marrow function as evidenced by platelets >= 75,000/mcL within 28 days prior to registration
Registration Step 3 - Maintenance: All non-hematologic treatment related toxicities that are deemed clinically significant by the treating investigator must have resolved to =< grade 2
Advani AS, Moseley A, O'Dwyer KM, Wood BL, Park J, Wieduwilt M, Jeyakumar D, Yaghmour G, Atallah EL, Gerds AT, O'Brien SM, Liesveld JL, Othus M, Litzow M, Stone RM, Sharon E, Erba HP. Dasatinib/prednisone induction followed by blinatumomab/dasatinib in Ph+ acute lymphoblastic leukemia. Blood Adv. 2023 Apr 11;7(7):1279-1285. doi: 10.1182/bloodadvances.2022008216.
See Also Links
Not provided
Available IPD Information
Not provided
IPD Sharing Statement Module
No data available
No data is available for this block.
Results Section
Participant Flow Module
Pre-assignment Details
Not provided
Recruitment Details
There were 57 total participants registered to the study; 31 in Cohort I and 26 in Cohort II. Four participants, two from each cohort, were deemed ineligible at the start of the study and never received protocol treatment. This left 53 eligible participants; 29 in Cohort II and 24 in Cohort II.
Type of Units Analyzed
Not provided
Arm/Group Information
ID
Title
Description
FG000
Cohort I (Ph-)
INDUCTION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28 in the absence of disease progression or unacceptable toxicity.
RE-INDUCTION: Patients not achieving CR or CRi after Induction, receive blinatumomab IV continuously over 24 hours on days 1-28 in the absence of disease progression or unacceptable toxicity.
POST-REMISSION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28. Treatment repeats every 42 days for 3 cycles in the absence of disease progression or unacceptable toxicity.
MAINTENANCE: Patients receive prednisone PO on days 1-5, vincristine sulfate IV on day 1, mercaptopurine PO on days 1-28, and methotrexate PO on days 1, 8, 15, and 22. Treatment repeats every 28 days for 18 cycles in the absence of disease progression or unacceptable toxicity. (Closed to accrual 06/29/17)
Medical Imaging, Magnetic Resonance / Nuclear Magnetic Resonance
MR
MR Imaging
MRI
MRI Scan
MRIs
NMR Imaging
NMRI
Nuclear Magnetic Resonance Imaging
sMRI
Structural MRI
Mercaptopurine
Drug
Given PO
Cohort I (blinatumomab, POMP)
3H-Purine-6-thiol
6 MP
6 Thiohypoxanthine
6 Thiopurine
6-Mercaptopurine
6-Mercaptopurine Monohydrate
6-MP
6-Purinethiol
6-Thiopurine
6-Thioxopurine
6H-Purine-6-thione, 1,7-dihydro- (9CI)
7-Mercapto-1,3,4,6-tetrazaindene
Alti-Mercaptopurine
Azathiopurine
Bw 57-323H
Flocofil
Ismipur
Leukerin
Leupurin
Mercaleukim
Mercaleukin
Mercaptina
Mercaptopurinum
Mercapurin
Mern
NCI-C04886
Puri-Nethol
Purimethol
Purine, 6-mercapto-
Purine-6-thiol (8CI)
Purine-6-thiol, monohydrate
Purinethiol
Purinethol
U-4748
WR-2785
Methotrexate
Drug
Given PO
Cohort I (blinatumomab, POMP)
Abitrexate
Alpha-Methopterin
Amethopterin
Brimexate
CL 14377
CL-14377
Emtexate
Emthexat
Emthexate
Farmitrexat
Fauldexato
Folex
Folex PFS
Jylamvo
Lantarel
Ledertrexate
Lumexon
Maxtrex
Medsatrexate
Metex
Methoblastin
Methotrexate LPF
Methotrexate Methylaminopterin
Methotrexatum
Metotrexato
Metrotex
Mexate
Mexate-AQ
MTX
Novatrex
Rheumatrex
Texate
Tremetex
Trexeron
Trixilem
WR-19039
Methotrexate Sodium
Drug
Given PO
Cohort I (blinatumomab, POMP)
Sodium Methotrexate
Trexall
Xatmep
Prednisone
Drug
Given PO
Cohort I (blinatumomab, POMP)
Cohort II (dasatinib, prednisone, blinatumomab)
.delta.1-Cortisone
1, 2-Dehydrocortisone
Adasone
Cortancyl
Dacortin
DeCortin
Decortisyl
Decorton
Delta 1-Cortisone
Delta-Dome
Deltacortene
Deltacortisone
Deltadehydrocortisone
Deltasone
Deltison
Deltra
Econosone
Lisacort
Meprosona-F
Metacortandracin
Meticorten
Ofisolona
Orasone
Panafcort
Panasol-S
Paracort
Perrigo Prednisone
PRED
Predicor
Predicorten
Prednicen-M
Prednicort
Prednidib
Prednilonga
Predniment
Prednisone Intensol
Prednisonum
Prednitone
Promifen
Rayos
Servisone
SK-Prednisone
Vincristine
Drug
Given IV
Cohort I (blinatumomab, POMP)
LCR
Leurocristine
VCR
Vincrystine
Vincristine Sulfate
Drug
Given IV
Cohort I (blinatumomab, POMP)
Kyocristine
Leurocristine Sulfate
Leurocristine, sulfate
Oncovin
Vincasar
Vincosid
Vincrex
Vincristine, sulfate
X-Ray Imaging
Procedure
Undergo an x-ray
Cohort I (blinatumomab, POMP)
Cohort II (dasatinib, prednisone, blinatumomab)
Conventional X-Ray
Diagnostic Radiology
Medical Imaging, X-Ray
Plain film radiographs
Radiographic Imaging
Radiographic imaging procedure (procedure)
Radiography
RG
Static X-Ray
X-Ray
Complete Response Rate (Cohort I)
Complete response rate is measured by the number of participants achieving complete remission (CR) or complete remission with incomplete platelet recovery (CRi) rate. CR is defined as having <5% marrow aspirate blasts, ANC >1,000/mcL, platelets > 100,000/mcL, no blasts in peripheral blood, and C1 extramedullary disease status. CRi is the same as CR but platelet count may be <= 100,000/mcL and/or ANC <=1,000/mcL.
Participants are assessed after induction treatment and again after re-induction treatment, if re-induction treatment is received (i.e. up to 85 days after registration)
Disease-free Survival (Cohort II)
An estimate of disease free survival in Ph-positive ALL and Ph-like DSMKF ALL (Cohort II). Disease free survival is measured by the number of years between the date the patient first achieves complete remission (CR) or complete remission with incomplete platelet recovery (CRi) until relapse from CR/CRi or death from any cause. CR is defined as having <5% marrow aspirate blasts, ANC >1,000/mcL, platelets > 100,000/mcL, no blasts in peripheral blood, and C1 extramedullary disease status. CRi is the same as CR but platelet count may be <= 100,000/mcL and/or ANC <=1,000/mcL.
Duration of treatment and follow up until death or date of primary analysis (about 7.5 years)
Overall Survival (Cohort II)
Estimated using the method of Kaplan-Meier.
Up to 10 years
Minimal Residual Disease Negativity
To estimate in each cohort the rate of minimal residual disease (MRD) negativity.
Participants are assessed after induction treatment and again after re-induction treatment, if re-induction treatment is received (i.e. up to 85 days after registration)
Time to Achieve Minimal Residual Disease Negativity
Will be examined separately in descriptive analyses within each cohort.
Up to 10 years
Anti-idiotype Antibody Development
To determine whether anti-idiotype antibodies directed against blinatumomab develop with blinatumomab treatment in this study.
Up to 10 years
Tucson
Arizona
85719
United States
University of Arizona Cancer Center-North Campus
Tucson
Arizona
85719
United States
John L McClellan Memorial Veterans Hospital
Little Rock
Arkansas
72205
United States
City of Hope Comprehensive Cancer Center
Duarte
California
91010
United States
UC San Diego Moores Cancer Center
La Jolla
California
92093
United States
Loma Linda University Medical Center
Loma Linda
California
92354
United States
Los Angeles General Medical Center
Los Angeles
California
90033
United States
USC / Norris Comprehensive Cancer Center
Los Angeles
California
90033
United States
USC Norris Oncology/Hematology-Newport Beach
Newport Beach
California
92663
United States
UC Irvine Health/Chao Family Comprehensive Cancer Center
Orange
California
92868
United States
Keck Medical Center of USC Pasadena
Pasadena
California
91105
United States
Smilow Cancer Center/Yale-New Haven Hospital
New Haven
Connecticut
06510
United States
Yale University
New Haven
Connecticut
06520
United States
Orlando Health Cancer Institute
Orlando
Florida
32806
United States
Northside Hospital
Atlanta
Georgia
30342
United States
Augusta University Medical Center
Augusta
Georgia
30912
United States
Rush-Copley Medical Center
Aurora
Illinois
60504
United States
OSF Saint Joseph Medical Center
Bloomington
Illinois
61701
United States
Illinois CancerCare-Bloomington
Bloomington
Illinois
61704
United States
Illinois CancerCare-Canton
Canton
Illinois
61520
United States
Memorial Hospital of Carbondale
Carbondale
Illinois
62902
United States
Illinois CancerCare-Carthage
Carthage
Illinois
62321
United States
Centralia Oncology Clinic
Centralia
Illinois
62801
United States
University of Illinois
Chicago
Illinois
60612
United States
University of Chicago Comprehensive Cancer Center
Chicago
Illinois
60637
United States
Carle at The Riverfront
Danville
Illinois
61832
United States
Cancer Care Specialists of Illinois - Decatur
Decatur
Illinois
62526
United States
Decatur Memorial Hospital
Decatur
Illinois
62526
United States
Carle Physician Group-Effingham
Effingham
Illinois
62401
United States
Crossroads Cancer Center
Effingham
Illinois
62401
United States
Illinois CancerCare-Eureka
Eureka
Illinois
61530
United States
Illinois CancerCare-Galesburg
Galesburg
Illinois
61401
United States
Western Illinois Cancer Treatment Center
Galesburg
Illinois
61401
United States
Illinois CancerCare-Kewanee Clinic
Kewanee
Illinois
61443
United States
Illinois CancerCare-Macomb
Macomb
Illinois
61455
United States
Carle Physician Group-Mattoon/Charleston
Mattoon
Illinois
61938
United States
SSM Health Good Samaritan
Mount Vernon
Illinois
62864
United States
UC Comprehensive Cancer Center at Silver Cross
New Lenox
Illinois
60451
United States
Cancer Care Center of O'Fallon
O'Fallon
Illinois
62269
United States
Illinois CancerCare-Ottawa Clinic
Ottawa
Illinois
61350
United States
Radiation Oncology of Northern Illinois
Ottawa
Illinois
61350
United States
Illinois CancerCare-Pekin
Pekin
Illinois
61554
United States
OSF Saint Francis Radiation Oncology at Pekin
Pekin
Illinois
61554
United States
Illinois CancerCare-Peoria
Peoria
Illinois
61615
United States
OSF Saint Francis Radiation Oncology at Peoria Cancer Center
Peoria
Illinois
61615
United States
Methodist Medical Center of Illinois
Peoria
Illinois
61636
United States
OSF Saint Francis Medical Center
Peoria
Illinois
61637
United States
Illinois CancerCare-Peru
Peru
Illinois
61354
United States
Valley Radiation Oncology
Peru
Illinois
61354
United States
Illinois CancerCare-Princeton
Princeton
Illinois
61356
United States
Central Illinois Hematology Oncology Center
Springfield
Illinois
62702
United States
Southern Illinois University School of Medicine
Springfield
Illinois
62702
United States
Springfield Clinic
Springfield
Illinois
62702
United States
Springfield Memorial Hospital
Springfield
Illinois
62781
United States
Carle Cancer Center
Urbana
Illinois
61801
United States
The Carle Foundation Hospital
Urbana
Illinois
61801
United States
Rush-Copley Healthcare Center
Yorkville
Illinois
60560
United States
Franciscan Health Indianapolis
Indianapolis
Indiana
46237
United States
Franciscan Saint Anthony Health-Michigan City
Michigan City
Indiana
46360
United States
Woodland Cancer Care Center
Michigan City
Indiana
46360
United States
Reid Health
Richmond
Indiana
47374
United States
McFarland Clinic - Ames
Ames
Iowa
50010
United States
McFarland Clinic - Boone
Boone
Iowa
50036
United States
McFarland Clinic - Trinity Cancer Center
Fort Dodge
Iowa
50501
United States
McFarland Clinic - Jefferson
Jefferson
Iowa
50129
United States
McFarland Clinic - Marshalltown
Marshalltown
Iowa
50158
United States
Siouxland Regional Cancer Center
Sioux City
Iowa
51101
United States
Cancer Center of Kansas - Chanute
Chanute
Kansas
66720
United States
Cancer Center of Kansas - Dodge City
Dodge City
Kansas
67801
United States
Cancer Center of Kansas - El Dorado
El Dorado
Kansas
67042
United States
Cancer Center of Kansas - Fort Scott
Fort Scott
Kansas
66701
United States
Cancer Center of Kansas-Independence
Independence
Kansas
67301
United States
University of Kansas Cancer Center
Kansas City
Kansas
66160
United States
Cancer Center of Kansas-Kingman
Kingman
Kansas
67068
United States
Lawrence Memorial Hospital
Lawrence
Kansas
66044
United States
Cancer Center of Kansas-Liberal
Liberal
Kansas
67905
United States
Cancer Center of Kansas - McPherson
McPherson
Kansas
67460
United States
Cancer Center of Kansas - Newton
Newton
Kansas
67114
United States
Cancer Center of Kansas - Parsons
Parsons
Kansas
67357
United States
Cancer Center of Kansas - Pratt
Pratt
Kansas
67124
United States
Cancer Center of Kansas - Salina
Salina
Kansas
67401
United States
Cancer Center of Kansas - Wellington
Wellington
Kansas
67152
United States
University of Kansas Hospital-Westwood Cancer Center
Westwood
Kansas
66205
United States
Associates In Womens Health
Wichita
Kansas
67208
United States
Cancer Center of Kansas-Wichita Medical Arts Tower
Wichita
Kansas
67208
United States
Ascension Via Christi Hospitals Wichita
Wichita
Kansas
67214
United States
Cancer Center of Kansas - Wichita
Wichita
Kansas
67214
United States
Wesley Medical Center
Wichita
Kansas
67214
United States
Cancer Center of Kansas - Winfield
Winfield
Kansas
67156
United States
Oncology Hematology Care Inc-Crestview
Crestview Hills
Kentucky
41017
United States
LSU Health Sciences Center at Shreveport
Shreveport
Louisiana
71103
United States
University of Maryland/Greenebaum Cancer Center
Baltimore
Maryland
21201
United States
Hickman Cancer Center
Adrian
Michigan
49221
United States
University of Michigan Rogel Cancer Center
Ann Arbor
Michigan
48109
United States
Bronson Battle Creek
Battle Creek
Michigan
49017
United States
Wayne State University/Karmanos Cancer Institute
Detroit
Michigan
48201
United States
Weisberg Cancer Treatment Center
Farmington Hills
Michigan
48334
United States
Corewell Health Farmington Hills Hospital
Farmington Hills
Michigan
48336
United States
Corewell Health Grand Rapids Hospitals - Butterworth Hospital
Grand Rapids
Michigan
49503
United States
Trinity Health Grand Rapids Hospital
Grand Rapids
Michigan
49503
United States
William Beaumont Hospital-Grosse Pointe
Grosse Pointe
Michigan
48230
United States
Bronson Methodist Hospital
Kalamazoo
Michigan
49007
United States
West Michigan Cancer Center
Kalamazoo
Michigan
49007
United States
Beacon Kalamazoo
Kalamazoo
Michigan
49048
United States
Toledo Clinic Cancer Centers-Monroe
Monroe
Michigan
48162
United States
Trinity Health Muskegon Hospital
Muskegon
Michigan
49444
United States
Corewell Health Lakeland Hospitals - Niles Hospital
Niles
Michigan
49120
United States
Corewell Health Reed City Hospital
Reed City
Michigan
49677
United States
Corewell Health William Beaumont University Hospital
Royal Oak
Michigan
48073
United States
Corewell Health Lakeland Hospitals - Marie Yeager Cancer Center
Saint Joseph
Michigan
49085
United States
Corewell Health Lakeland Hospitals - Saint Joseph Hospital
Saint Joseph
Michigan
49085
United States
Munson Medical Center
Traverse City
Michigan
49684
United States
Corewell Health Beaumont Troy Hospital
Troy
Michigan
48085
United States
Sanford Joe Lueken Cancer Center
Bemidji
Minnesota
56601
United States
Mayo Clinic in Rochester
Rochester
Minnesota
55905
United States
University of Mississippi Medical Center
Jackson
Mississippi
39216
United States
Central Care Cancer Center - Bolivar
Bolivar
Missouri
65613
United States
Parkland Health Center-Bonne Terre
Bonne Terre
Missouri
63628
United States
Cox Cancer Center Branson
Branson
Missouri
65616
United States
Mercy Cancer Center - Cape Girardeau
Cape Girardeau
Missouri
63703
United States
Saint Francis Medical Center
Cape Girardeau
Missouri
63703
United States
MU Health Care Goldschmidt Cancer Center
Jefferson City
Missouri
65109
United States
Freeman Health System
Joplin
Missouri
64804
United States
Mercy Hospital Joplin
Joplin
Missouri
64804
United States
Mercy Clinic-Rolla-Cancer and Hematology
Rolla
Missouri
65401
United States
Phelps Health Delbert Day Cancer Institute
Rolla
Missouri
65401
United States
Sainte Genevieve County Memorial Hospital
Sainte Genevieve
Missouri
63670
United States
Mercy Hospital Springfield
Springfield
Missouri
65804
United States
CoxHealth South Hospital
Springfield
Missouri
65807
United States
Mercy Infusion Center - Chippewa
St Louis
Missouri
63109
United States
Missouri Baptist Medical Center
St Louis
Missouri
63131
United States
Mercy Hospital Saint Louis
St Louis
Missouri
63141
United States
Missouri Baptist Sullivan Hospital
Sullivan
Missouri
63080
United States
BJC Outpatient Center at Sunset Hills
Sunset Hills
Missouri
63127
United States
Nebraska Medicine-Bellevue
Bellevue
Nebraska
68123
United States
Nebraska Medicine-Village Pointe
Omaha
Nebraska
68118
United States
University of Nebraska Medical Center
Omaha
Nebraska
68198
United States
University of New Mexico Cancer Center
Albuquerque
New Mexico
87106
United States
Roswell Park Cancer Institute
Buffalo
New York
14263
United States
Northwell Health/Center for Advanced Medicine
Lake Success
New York
11042
United States
North Shore University Hospital
Manhasset
New York
11030
United States
Long Island Jewish Medical Center
New Hyde Park
New York
11040
United States
University of Rochester
Rochester
New York
14642
United States
Duke University Medical Center
Durham
North Carolina
27710
United States
ECU Health Oncology Kenansville
Kenansville
North Carolina
28349
United States
ECU Health Oncology Kinston
Kinston
North Carolina
28501
United States
ECU Health Oncology Richlands
Richlands
North Carolina
28574
United States
Wake Forest University Health Sciences
Winston-Salem
North Carolina
27157
United States
Sanford Bismarck Medical Center
Bismarck
North Dakota
58501
United States
Sanford Broadway Medical Center
Fargo
North Dakota
58122
United States
Sanford Roger Maris Cancer Center
Fargo
North Dakota
58122
United States
Miami Valley Hospital South
Centerville
Ohio
45459
United States
Oncology Hematology Care Inc-Eden Park
Cincinnati
Ohio
45202
United States
Oncology Hematology Care Inc-Mercy West
Cincinnati
Ohio
45211
United States
Oncology Hematology Care Inc-Anderson
Cincinnati
Ohio
45230
United States
Oncology Hematology Care Inc-Kenwood
Cincinnati
Ohio
45236
United States
Oncology Hematology Care Inc-Blue Ash
Cincinnati
Ohio
45242
United States
Case Western Reserve University
Cleveland
Ohio
44106
United States
Cleveland Clinic Foundation
Cleveland
Ohio
44195
United States
Ohio State University Comprehensive Cancer Center
Columbus
Ohio
43210
United States
Good Samaritan Hospital - Dayton
Dayton
Ohio
45406
United States
Miami Valley Hospital
Dayton
Ohio
45409
United States
Miami Valley Hospital North
Dayton
Ohio
45415
United States
Oncology Hematology Care Inc-Healthplex
Fairfield
Ohio
45014
United States
Blanchard Valley Hospital
Findlay
Ohio
45840
United States
Atrium Medical Center-Middletown Regional Hospital
Franklin
Ohio
45005-1066
United States
Wayne Hospital
Greenville
Ohio
45331
United States
Kettering Medical Center
Kettering
Ohio
45429
United States
Toledo Clinic Cancer Centers-Maumee
Maumee
Ohio
43537
United States
Toledo Radiation Oncology at Northwest Ohio Onocolgy Center
Maumee
Ohio
43537
United States
Saint Charles Hospital
Oregon
Ohio
43616
United States
Springfield Regional Cancer Center
Springfield
Ohio
45504
United States
Springfield Regional Medical Center
Springfield
Ohio
45504
United States
Mercy Health - Saint Anne Hospital
Toledo
Ohio
43623
United States
Toledo Clinic Cancer Centers-Toledo
Toledo
Ohio
43623
United States
Upper Valley Medical Center
Troy
Ohio
45373
United States
Wright-Patterson Medical Center
Wright-Patterson Air Force Base
Ohio
45433
United States
University of Oklahoma Health Sciences Center
Oklahoma City
Oklahoma
73104
United States
Providence Portland Medical Center
Portland
Oregon
97213
United States
Providence Saint Vincent Medical Center
Portland
Oregon
97225
United States
University of Pennsylvania/Abramson Cancer Center
Philadelphia
Pennsylvania
19104
United States
Thomas Jefferson University Hospital
Philadelphia
Pennsylvania
19107
United States
Prisma Health Cancer Institute - Spartanburg
Boiling Springs
South Carolina
29316
United States
Prisma Health Cancer Institute - Easley
Easley
South Carolina
29640
United States
Greenville Health System Cancer Institute-Andrews
Greenville
South Carolina
29601
United States
Prisma Health Cancer Institute - Butternut
Greenville
South Carolina
29605
United States
Prisma Health Cancer Institute - Faris
Greenville
South Carolina
29605
United States
Prisma Health Greenville Memorial Hospital
Greenville
South Carolina
29605
United States
Prisma Health Cancer Institute - Eastside
Greenville
South Carolina
29615
United States
Prisma Health Cancer Institute - Greer
Greer
South Carolina
29650
United States
Prisma Health Cancer Institute - Seneca
Seneca
South Carolina
29672
United States
Baylor University Medical Center
Dallas
Texas
75246
United States
Saint Vincent Hospital Cancer Center Green Bay
Green Bay
Wisconsin
54301
United States
Saint Vincent Hospital Cancer Center at Saint Mary's
Green Bay
Wisconsin
54303
United States
Medical College of Wisconsin
Milwaukee
Wisconsin
53226
United States
FG001
Cohort II (Ph+/Ph-like)
INDUCTION: Patients receive dasatinib PO BID on days 1-84 and prednisone PO on days 1-24 with tapering on days 25-32 in the absence of disease progression or unacceptable toxicity.
RE-INDUCTION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28. Treatment repeats every 42 days for 2 cycles in the absence of disease progression or unacceptable toxicity.
POST-REMISSION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28 and dasatinib PO QD on days 1-42. Treatment repeats every 42 days for 3 cycles in the absence of disease progression or unacceptable toxicity.
MAINTENANCE: Patients receive dasatinib PO BID on days 1-28. Cycles repeat every 28 days in the absence of disease progression or unacceptable toxicity. Patients also receive prednisone PO on days 1-5. Treatment repeats every 28 days for 18 cycles in the absence of disease progression or unacceptable toxicity.
INDUCTION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28 in the absence of disease progression or unacceptable toxicity.
RE-INDUCTION: Patients not achieving CR or CRi after Induction, receive blinatumomab IV continuously over 24 hours on days 1-28 in the absence of disease progression or unacceptable toxicity.
POST-REMISSION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28. Treatment repeats every 42 days for 3 cycles in the absence of disease progression or unacceptable toxicity.
MAINTENANCE: Patients receive prednisone PO on days 1-5, vincristine sulfate IV on day 1, mercaptopurine PO on days 1-28, and methotrexate PO on days 1, 8, 15, and 22. Treatment repeats every 28 days for 18 cycles in the absence of disease progression or unacceptable toxicity. (Closed to accrual 06/29/17)
INDUCTION: Patients receive dasatinib PO BID on days 1-84 and prednisone PO on days 1-24 with tapering on days 25-32 in the absence of disease progression or unacceptable toxicity.
RE-INDUCTION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28. Treatment repeats every 42 days for 2 cycles in the absence of disease progression or unacceptable toxicity.
POST-REMISSION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28 and dasatinib PO QD on days 1-42. Treatment repeats every 42 days for 3 cycles in the absence of disease progression or unacceptable toxicity.
MAINTENANCE: Patients receive dasatinib PO BID on days 1-28. Cycles repeat every 28 days in the absence of disease progression or unacceptable toxicity. Patients also receive prednisone PO on days 1-5. Treatment repeats every 28 days for 18 cycles in the absence of disease progression or unacceptable toxicity.
To evaluate the 3-year overall survival rate in elderly participants with newly diagnosed Ph-negative ALL treated with blinatumomab followed by POMP maintenance. Overall
Only participants in Cohort I were evaluated
Posted
Number
95% Confidence Interval
percentage of participants
From the day of registration on study until death from any cause, assessed at 3 years
ID
Title
Description
OG000
Cohort I (Ph-)
INDUCTION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28 in the absence of disease progression or unacceptable toxicity.
RE-INDUCTION: Patients not achieving CR or CRi after Induction, receive blinatumomab IV continuously over 24 hours on days 1-28 in the absence of disease progression or unacceptable toxicity.
POST-REMISSION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28. Treatment repeats every 42 days for 3 cycles in the absence of disease progression or unacceptable toxicity.
MAINTENANCE: Patients receive prednisone PO on days 1-5, vincristine sulfate IV on day 1, mercaptopurine PO on days 1-28, and methotrexate PO on days 1, 8, 15, and 22. Treatment repeats every 28 days for 18 cycles in the absence of disease progression or unacceptable toxicity. (Closed to accrual 06/29/17)
Defined as any grade 4 or higher treatment-related, non-hematologic toxicity in the first cycle of post-remission therapy (blinatumomab/dasatinib) graded by National Cancer Institute (NCI) Common Terminology Criteria for Adverse Events (CTCAE) version 4.0. Only participants with Ph-positive ALL or Ph-like DSMKF ALL were evaluated.
Only participants in Cohort II that registered to post-remission were analyzed for dose-limiting toxicities.
Posted
Count of Participants
Participants
Up to day 42 of post-remission therapy
ID
Title
Description
OG000
Cohort II (Ph+/Ph-like)
INDUCTION: Patients receive dasatinib PO BID on days 1-84 and prednisone PO on days 1-24 with tapering on days 25-32 in the absence of disease progression or unacceptable toxicity.
RE-INDUCTION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28. Treatment repeats every 42 days for 2 cycles in the absence of disease progression or unacceptable toxicity.
POST-REMISSION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28 and dasatinib PO QD on days 1-42. Treatment repeats every 42 days for 3 cycles in the absence of disease progression or unacceptable toxicity.
MAINTENANCE: Patients receive dasatinib PO BID on days 1-28. Cycles repeat every 28 days in the absence of disease progression or unacceptable toxicity. Patients also receive prednisone PO on days 1-5. Treatment repeats every 28 days for 18 cycles in the absence of disease progression or unacceptable toxicity.
Number of Participants With Grade 3 Through 5 Adverse Events That Are Related to Study Drugs
Number of participants with Grade 3-5 adverse events that are possibly, probably or definitely related to study drug are reported by given type of adverse event. Adverse Events reported using CTCAE v 4.0, whereas Serious Adverse Events were reported with CTCAE v 5.0.
Eligible participants who received at least one dose of protocol treatment.
Posted
Number
Participants
Duration of treatment and follow up until death or date of primary analysis (about 7.5 years)
ID
Title
Description
OG000
Induction: Cohort I (Ph-)
INDUCTION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28 in the absence of disease progression or unacceptable toxicity.
RE-INDUCTION: Patients not achieving CR or CRi after Induction, receive blinatumomab IV continuously over 24 hours on days 1-28 in the absence of disease progression or unacceptable toxicity.
Blinatumomab: Given IV
OG001
Induction: Cohort II (Ph+/Ph-like)
INDUCTION: Patients receive dasatinib PO BID on days 1-84 and prednisone PO on days 1-24 with tapering on days 25-32 in the absence of disease progression or unacceptable toxicity.
RE-INDUCTION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28. Treatment repeats every 42 days for 2 cycles in the absence of disease progression or unacceptable toxicity.
Blinatumomab: Given IV
Dasatinib: Given PO
Prednisone: Given PO
Secondary
Complete Response Rate (Cohort I)
Complete response rate is measured by the number of participants achieving complete remission (CR) or complete remission with incomplete platelet recovery (CRi) rate. CR is defined as having <5% marrow aspirate blasts, ANC >1,000/mcL, platelets > 100,000/mcL, no blasts in peripheral blood, and C1 extramedullary disease status. CRi is the same as CR but platelet count may be <= 100,000/mcL and/or ANC <=1,000/mcL.
Only participants in Cohort I were evaluated.
Posted
Count of Participants
Participants
Participants are assessed after induction treatment and again after re-induction treatment, if re-induction treatment is received (i.e. up to 85 days after registration)
ID
Title
Description
OG000
Cohort I (Ph-)
INDUCTION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28 in the absence of disease progression or unacceptable toxicity.
RE-INDUCTION: Patients not achieving CR or CRi after Induction, receive blinatumomab IV continuously over 24 hours on days 1-28 in the absence of disease progression or unacceptable toxicity.
POST-REMISSION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28. Treatment repeats every 42 days for 3 cycles in the absence of disease progression or unacceptable toxicity.
MAINTENANCE: Patients receive prednisone PO on days 1-5, vincristine sulfate IV on day 1, mercaptopurine PO on days 1-28, and methotrexate PO on days 1, 8, 15, and 22. Treatment repeats every 28 days for 18 cycles in the absence of disease progression or unacceptable toxicity. (Closed to accrual 06/29/17)
An estimate of disease free survival in Ph-positive ALL and Ph-like DSMKF ALL (Cohort II). Disease free survival is measured by the number of years between the date the patient first achieves complete remission (CR) or complete remission with incomplete platelet recovery (CRi) until relapse from CR/CRi or death from any cause. CR is defined as having <5% marrow aspirate blasts, ANC >1,000/mcL, platelets > 100,000/mcL, no blasts in peripheral blood, and C1 extramedullary disease status. CRi is the same as CR but platelet count may be <= 100,000/mcL and/or ANC <=1,000/mcL.
Only participants in Cohort II that achieved complete remission were analyzable.
Posted
Median
95% Confidence Interval
years
Duration of treatment and follow up until death or date of primary analysis (about 7.5 years)
ID
Title
Description
OG000
Cohort II (Ph+/Ph-like)
INDUCTION: Patients receive dasatinib PO BID on days 1-84 and prednisone PO on days 1-24 with tapering on days 25-32 in the absence of disease progression or unacceptable toxicity.
RE-INDUCTION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28. Treatment repeats every 42 days for 2 cycles in the absence of disease progression or unacceptable toxicity.
POST-REMISSION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28 and dasatinib PO QD on days 1-42. Treatment repeats every 42 days for 3 cycles in the absence of disease progression or unacceptable toxicity.
MAINTENANCE: Patients receive dasatinib PO BID on days 1-28. Cycles repeat every 28 days in the absence of disease progression or unacceptable toxicity. Patients also receive prednisone PO on days 1-5. Treatment repeats every 28 days for 18 cycles in the absence of disease progression or unacceptable toxicity.
To estimate in each cohort the rate of minimal residual disease (MRD) negativity.
Only participants that had achieved CR or CRi and had available MRD data post-treatment were evaluated.
Posted
Count of Participants
Participants
Participants are assessed after induction treatment and again after re-induction treatment, if re-induction treatment is received (i.e. up to 85 days after registration)
ID
Title
Description
OG000
Cohort I (Ph-)
INDUCTION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28 in the absence of disease progression or unacceptable toxicity.
RE-INDUCTION: Patients not achieving CR or CRi after Induction, receive blinatumomab IV continuously over 24 hours on days 1-28 in the absence of disease progression or unacceptable toxicity.
POST-REMISSION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28. Treatment repeats every 42 days for 3 cycles in the absence of disease progression or unacceptable toxicity.
MAINTENANCE: Patients receive prednisone PO on days 1-5, vincristine sulfate IV on day 1, mercaptopurine PO on days 1-28, and methotrexate PO on days 1, 8, 15, and 22. Treatment repeats every 28 days for 18 cycles in the absence of disease progression or unacceptable toxicity. (Closed to accrual 06/29/17)
Time to Achieve Minimal Residual Disease Negativity
Will be examined separately in descriptive analyses within each cohort.
Not Posted
Up to 10 years
Participants
Secondary
Anti-idiotype Antibody Development
To determine whether anti-idiotype antibodies directed against blinatumomab develop with blinatumomab treatment in this study.
Not Posted
Up to 10 years
Participants
Time Frame
Duration of treatment and follow up until death or date of primary analysis (about 7.5 years)
Description
AEs and SAEs were reported using CTCAE v 4.0 and CTCAE v 5.0, respectively. The analysis populations for Adverse Events and All-Cause Mortality only differ for the Maintenance: Cohort I. The AE population includes participants that received maintenance treatment and thus does not include one participant which relapsed prior to receiving maintenance treatment. Whereas, the All-Cause Mortality population includes all participants registered to receive maintenance treatment.
All-Cause Mortality Comment
Not provided
Arm/Groups
ID
Title
Description
Deaths (Affected)
Deaths (At Risk)
Serious Events (Affected)
Serious Events (At Risk)
Other Events (Affected)
Other Events (At Risk)
EG000
Induction: Cohort I (Ph-)
INDUCTION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28 in the absence of disease progression or unacceptable toxicity.
RE-INDUCTION: Patients not achieving CR or CRi after Induction, receive blinatumomab IV continuously over 24 hours on days 1-28 in the absence of disease progression or unacceptable toxicity.
Blinatumomab: Given IV
1
29
13
29
28
29
EG001
Induction: Cohort II (Ph+/Ph-like)
INDUCTION: Patients receive dasatinib PO BID on days 1-84 and prednisone PO on days 1-24 with tapering on days 25-32 in the absence of disease progression or unacceptable toxicity.
RE-INDUCTION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28. Treatment repeats every 42 days for 2 cycles in the absence of disease progression or unacceptable toxicity.
Blinatumomab: Given IV
Dasatinib: Given PO
Prednisone: Given PO
2
24
14
24
24
24
EG002
Post-remission: Cohort I (Ph-)
POST-REMISSION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28. Treatment repeats every 42 days for 3 cycles in the absence of disease progression or unacceptable toxicity.
Blinatumomab: Given IV
0
19
5
19
19
19
EG003
Post-remission: Cohort II (Ph+/Ph-like)
POST-REMISSION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28 and dasatinib PO QD on days 1-42. Treatment repeats every 42 days for 3 cycles in the absence of disease progression or unacceptable toxicity.
Blinatumomab: Given IV
Dasatinib: Given PO
0
18
10
18
18
18
EG004
Maintenance: Cohort I (Ph-)
MAINTENANCE: Patients receive prednisone PO on days 1-5, vincristine sulfate IV on day 1, mercaptopurine PO on days 1-28, and methotrexate PO on days 1, 8, 15, and 22. Treatment repeats every 28 days for 18 cycles in the absence of disease progression or unacceptable toxicity. (Closed to accrual 06/29/17)
Mercaptopurine: Given PO
Methotrexate: Given PO
Methotrexate Sodium: Given PO
Prednisone: Given PO
Vincristine: Given IV
Vincristine Sulfate: Given IV
0
14
6
13
13
13
EG005
Maintenance: Cohort II (Ph+/Ph-like)
MAINTENANCE: Patients receive dasatinib PO BID on days 1-28. Cycles repeat every 28 days in the absence of disease progression or unacceptable toxicity. Patients also receive prednisone PO on days 1-5. Treatment repeats every 28 days for 18 cycles in the absence of disease progression or unacceptable toxicity.
Dasatinib: Given PO
Prednisone: Given PO
1
16
12
16
15
16
Serious Adverse Events
Term
Organ System
Source Vocabulary
Assessment Type
Notes
Statistical Information
Anemia
Blood and lymphatic system disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG0030 affected18 at risk
EG0042 affected13 at risk
EG0050 affected16 at risk
Febrile neutropenia
Blood and lymphatic system disorders
Systematic Assessment
EG0001 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Leukocytosis
Blood and lymphatic system disorders
Systematic Assessment
EG0001 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Atrial fibrillation
Cardiac disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Atrial flutter
Cardiac disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Chest pain - cardiac
Cardiac disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Heart failure
Cardiac disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Myocardial infarction
Cardiac disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Pericardial effusion
Cardiac disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Sinus tachycardia
Cardiac disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Supraventricular tachycardia
Cardiac disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Eye disorders-Other
Eye disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Abdominal pain
Gastrointestinal disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Colitis
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Diarrhea
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0013 affected24 at risk
EG0020 affected19 at risk
EG003
Enterocolitis
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Gastrointestinal pain
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Ileus
Gastrointestinal disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Lower gastrointestinal hemorrhage
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Mucositis oral
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Nausea
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Vomiting
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Chills
General disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Death NOS
General disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Edema limbs
General disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Fever
General disorders
Systematic Assessment
EG0001 affected29 at risk
EG0013 affected24 at risk
EG0022 affected19 at risk
EG003
General disorders and admin site conditions - Other
General disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Infusion related reaction
General disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Non-cardiac chest pain
General disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Cytokine release syndrome
Immune system disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Catheter related infection
Infections and infestations
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Infections and infestations-Other
Infections and infestations
Systematic Assessment
EG0001 affected29 at risk
EG0013 affected24 at risk
EG0022 affected19 at risk
EG003
Lung infection
Infections and infestations
Systematic Assessment
EG0002 affected29 at risk
EG0011 affected24 at risk
EG0021 affected19 at risk
EG003
Sepsis
Infections and infestations
Systematic Assessment
EG0002 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Upper respiratory infection
Infections and infestations
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Urinary tract infection
Infections and infestations
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Fall
Injury, poisoning and procedural complications
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Fracture
Injury, poisoning and procedural complications
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Injury, poison and procedural complications - Other
Injury, poisoning and procedural complications
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Vascular access complication
Injury, poisoning and procedural complications
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Alanine aminotransferase increased
Investigations
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Aspartate aminotransferase increased
Investigations
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Creatinine increased
Investigations
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Lymphocyte count decreased
Investigations
Systematic Assessment
EG0002 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Neutrophil count decreased
Investigations
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0022 affected19 at risk
EG003
Platelet count decreased
Investigations
Systematic Assessment
EG0002 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Weight loss
Investigations
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
White blood cell decreased
Investigations
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Dehydration
Metabolism and nutrition disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Hyperglycemia
Metabolism and nutrition disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Generalized muscle weakness
Musculoskeletal and connective tissue disorders
Systematic Assessment
EG0001 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Musculoskeletal and connective tiss disorder - Other
Musculoskeletal and connective tissue disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Neoplasms benign, malignant and unspecified - Other
Neoplasms benign, malignant and unspecified (incl cysts and polyps)
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Dysarthria
Nervous system disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Encephalopathy
Nervous system disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Nervous system disorders-Other
Nervous system disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Peripheral sensory neuropathy
Nervous system disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Syncope
Nervous system disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Agitation
Psychiatric disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Confusion
Psychiatric disorders
Systematic Assessment
EG0001 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Delirium
Psychiatric disorders
Systematic Assessment
EG0001 affected29 at risk
EG0012 affected24 at risk
EG0020 affected19 at risk
EG003
Hallucinations
Psychiatric disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Acute kidney injury
Renal and urinary disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Adult respiratory distress syndrome
Respiratory, thoracic and mediastinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Cough
Respiratory, thoracic and mediastinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Dyspnea
Respiratory, thoracic and mediastinal disorders
Systematic Assessment
EG0003 affected29 at risk
EG0012 affected24 at risk
EG0020 affected19 at risk
EG003
Hypoxia
Respiratory, thoracic and mediastinal disorders
Systematic Assessment
EG0001 affected29 at risk
EG0012 affected24 at risk
EG0021 affected19 at risk
EG003
Pleural effusion
Respiratory, thoracic and mediastinal disorders
Systematic Assessment
EG0001 affected29 at risk
EG0012 affected24 at risk
EG0020 affected19 at risk
EG003
Pneumonitis
Respiratory, thoracic and mediastinal disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Pneumothorax
Respiratory, thoracic and mediastinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Pulmonary hypertension
Respiratory, thoracic and mediastinal disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Respiratory failure
Respiratory, thoracic and mediastinal disorders
Systematic Assessment
EG0002 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Hematoma
Vascular disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Hypertension
Vascular disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Hypotension
Vascular disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Thromboembolic event
Vascular disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Other Adverse Events
Term
Organ System
Source Vocabulary
Assessment Type
Notes
Statistical Information
Anemia
Blood and lymphatic system disorders
Systematic Assessment
EG00017 affected29 at risk
EG00113 affected24 at risk
EG0029 affected19 at risk
EG00312 affected18 at risk
EG0049 affected13 at risk
EG0059 affected16 at risk
Blood and lymphatic system disorders - Other
Blood and lymphatic system disorders
Systematic Assessment
EG0001 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Disseminated intravascular coagulation
Blood and lymphatic system disorders
Systematic Assessment
EG0002 affected29 at risk
EG0011 affected24 at risk
EG0021 affected19 at risk
EG003
Febrile neutropenia
Blood and lymphatic system disorders
Systematic Assessment
EG0006 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Leukocytosis
Blood and lymphatic system disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Atrial fibrillation
Cardiac disorders
Systematic Assessment
EG0003 affected29 at risk
EG0012 affected24 at risk
EG0022 affected19 at risk
EG003
Atrial flutter
Cardiac disorders
Systematic Assessment
EG0002 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Atrioventricular block first degree
Cardiac disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Cardiac disorders-Other
Cardiac disorders
Systematic Assessment
EG0001 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Chest pain - cardiac
Cardiac disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Heart failure
Cardiac disorders
Systematic Assessment
EG0001 affected29 at risk
EG0012 affected24 at risk
EG0021 affected19 at risk
EG003
Palpitations
Cardiac disorders
Systematic Assessment
EG0000 affected29 at risk
EG0012 affected24 at risk
EG0020 affected19 at risk
EG003
Pericardial effusion
Cardiac disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Sinus bradycardia
Cardiac disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Sinus tachycardia
Cardiac disorders
Systematic Assessment
EG0004 affected29 at risk
EG0012 affected24 at risk
EG0024 affected19 at risk
EG003
Supraventricular tachycardia
Cardiac disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Ear and labyrinth disorders-Other
Ear and labyrinth disorders
Systematic Assessment
EG0002 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Ear pain
Ear and labyrinth disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Hearing impaired
Ear and labyrinth disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Vertigo
Ear and labyrinth disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Endocrine disorders-Other
Endocrine disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Hyperthyroidism
Endocrine disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Hypothyroidism
Endocrine disorders
Systematic Assessment
EG0001 affected29 at risk
EG0011 affected24 at risk
EG0021 affected19 at risk
EG003
Blurred vision
Eye disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0023 affected19 at risk
EG003
Cataract
Eye disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Dry eye
Eye disorders
Systematic Assessment
EG0002 affected29 at risk
EG0010 affected24 at risk
EG0022 affected19 at risk
EG003
Eye disorders-Other
Eye disorders
Systematic Assessment
EG0001 affected29 at risk
EG0012 affected24 at risk
EG0022 affected19 at risk
EG003
Eye pain
Eye disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Photophobia
Eye disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Retinopathy
Eye disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Watering eyes
Eye disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Abdominal distension
Gastrointestinal disorders
Systematic Assessment
EG0002 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Abdominal pain
Gastrointestinal disorders
Systematic Assessment
EG0003 affected29 at risk
EG0013 affected24 at risk
EG0023 affected19 at risk
EG003
Anal hemorrhage
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Bloating
Gastrointestinal disorders
Systematic Assessment
EG0004 affected29 at risk
EG0011 affected24 at risk
EG0021 affected19 at risk
EG003
Cheilitis
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Colitis
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Constipation
Gastrointestinal disorders
Systematic Assessment
EG00010 affected29 at risk
EG0014 affected24 at risk
EG0022 affected19 at risk
EG003
Dental caries
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Diarrhea
Gastrointestinal disorders
Systematic Assessment
EG0005 affected29 at risk
EG0018 affected24 at risk
EG0022 affected19 at risk
EG003
Dry mouth
Gastrointestinal disorders
Systematic Assessment
EG0002 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Dyspepsia
Gastrointestinal disorders
Systematic Assessment
EG0001 affected29 at risk
EG0012 affected24 at risk
EG0020 affected19 at risk
EG003
Dysphagia
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Enterocolitis
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0021 affected19 at risk
EG003
Esophageal pain
Gastrointestinal disorders
Systematic Assessment
EG0002 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Esophagitis
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Fecal incontinence
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Flatulence
Gastrointestinal disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Gastritis
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Gastroesophageal reflux disease
Gastrointestinal disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Gastrointestinal disorders-Other
Gastrointestinal disorders
Systematic Assessment
EG0002 affected29 at risk
EG0013 affected24 at risk
EG0020 affected19 at risk
EG003
Hemorrhoids
Gastrointestinal disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Lower gastrointestinal hemorrhage
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Mucositis oral
Gastrointestinal disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Nausea
Gastrointestinal disorders
Systematic Assessment
EG0008 affected29 at risk
EG0016 affected24 at risk
EG0025 affected19 at risk
EG003
Oral hemorrhage
Gastrointestinal disorders
Systematic Assessment
EG0001 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Oral pain
Gastrointestinal disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Rectal ulcer
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Stomach pain
Gastrointestinal disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Toothache
Gastrointestinal disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Vomiting
Gastrointestinal disorders
Systematic Assessment
EG0002 affected29 at risk
EG0012 affected24 at risk
EG0022 affected19 at risk
EG003
Chills
General disorders
Systematic Assessment
EG0006 affected29 at risk
EG0012 affected24 at risk
EG0020 affected19 at risk
EG003
Edema face
General disorders
Systematic Assessment
EG0000 affected29 at risk
EG0012 affected24 at risk
EG0020 affected19 at risk
EG003
Edema limbs
General disorders
Systematic Assessment
EG00012 affected29 at risk
EG00110 affected24 at risk
EG0026 affected19 at risk
EG003
Edema trunk
General disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Fatigue
General disorders
Systematic Assessment
EG00012 affected29 at risk
EG00113 affected24 at risk
EG0025 affected19 at risk
EG003
Fever
General disorders
Systematic Assessment
EG0008 affected29 at risk
EG0014 affected24 at risk
EG0023 affected19 at risk
EG003
Flu like symptoms
General disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Gait disturbance
General disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
General disorders and admin site conditions - Other
General disorders
Systematic Assessment
EG0003 affected29 at risk
EG0011 affected24 at risk
EG0021 affected19 at risk
EG003
Infusion related reaction
General disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Infusion site extravasation
General disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Injection site reaction
General disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Irritability
General disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Localized edema
General disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Malaise
General disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Non-cardiac chest pain
General disorders
Systematic Assessment
EG0003 affected29 at risk
EG0013 affected24 at risk
EG0022 affected19 at risk
EG003
Pain
General disorders
Systematic Assessment
EG0001 affected29 at risk
EG0014 affected24 at risk
EG0024 affected19 at risk
EG003
Cholecystitis
Hepatobiliary disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Hepatobiliary disorders-Other
Hepatobiliary disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Allergic reaction
Immune system disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Cytokine release syndrome
Immune system disorders
Systematic Assessment
EG0002 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Immune system disorders-Other
Immune system disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Conjunctivitis infective
Infections and infestations
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Infections and infestations-Other
Infections and infestations
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Lung infection
Infections and infestations
Systematic Assessment
EG0001 affected29 at risk
EG0012 affected24 at risk
EG0021 affected19 at risk
EG003
Mucosal infection
Infections and infestations
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Nail infection
Infections and infestations
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Pharyngitis
Infections and infestations
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Rash pustular
Infections and infestations
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Sinusitis
Infections and infestations
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Skin infection
Infections and infestations
Systematic Assessment
EG0001 affected29 at risk
EG0011 affected24 at risk
EG0021 affected19 at risk
EG003
Soft tissue infection
Infections and infestations
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Upper respiratory infection
Infections and infestations
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0022 affected19 at risk
EG003
Urinary tract infection
Infections and infestations
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Bruising
Injury, poisoning and procedural complications
Systematic Assessment
EG0003 affected29 at risk
EG0013 affected24 at risk
EG0020 affected19 at risk
EG003
Burn
Injury, poisoning and procedural complications
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Fall
Injury, poisoning and procedural complications
Systematic Assessment
EG0002 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Activated partial thromboplastin time prolonged
Investigations
Systematic Assessment
EG0003 affected29 at risk
EG0011 affected24 at risk
EG0022 affected19 at risk
EG003
Alanine aminotransferase increased
Investigations
Systematic Assessment
EG00010 affected29 at risk
EG0015 affected24 at risk
EG0024 affected19 at risk
EG003
Alkaline phosphatase increased
Investigations
Systematic Assessment
EG0004 affected29 at risk
EG0015 affected24 at risk
EG0023 affected19 at risk
EG003
Aspartate aminotransferase increased
Investigations
Systematic Assessment
EG0009 affected29 at risk
EG0014 affected24 at risk
EG0023 affected19 at risk
EG003
Blood bilirubin increased
Investigations
Systematic Assessment
EG0007 affected29 at risk
EG0011 affected24 at risk
EG0021 affected19 at risk
EG003
Cardiac troponin T increased
Investigations
Systematic Assessment
EG0000 affected29 at risk
EG0012 affected24 at risk
EG0020 affected19 at risk
EG003
Cholesterol high
Investigations
Systematic Assessment
EG0001 affected29 at risk
EG0011 affected24 at risk
EG0021 affected19 at risk
EG003
Creatinine increased
Investigations
Systematic Assessment
EG0006 affected29 at risk
EG0014 affected24 at risk
EG0022 affected19 at risk
EG003
Electrocardiogram QT corrected interval prolonged
Investigations
Systematic Assessment
EG0002 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Fibrinogen decreased
Investigations
Systematic Assessment
EG0002 affected29 at risk
EG0012 affected24 at risk
EG0020 affected19 at risk
EG003
INR increased
Investigations
Systematic Assessment
EG0004 affected29 at risk
EG0012 affected24 at risk
EG0021 affected19 at risk
EG003
Investigations-Other
Investigations
Systematic Assessment
EG0003 affected29 at risk
EG0012 affected24 at risk
EG0024 affected19 at risk
EG003
Lymphocyte count decreased
Investigations
Systematic Assessment
EG0008 affected29 at risk
EG0018 affected24 at risk
EG0026 affected19 at risk
EG003
Lymphocyte count increased
Investigations
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Neutrophil count decreased
Investigations
Systematic Assessment
EG00013 affected29 at risk
EG00114 affected24 at risk
EG0026 affected19 at risk
EG003
Platelet count decreased
Investigations
Systematic Assessment
EG00015 affected29 at risk
EG00116 affected24 at risk
EG0027 affected19 at risk
EG003
Weight gain
Investigations
Systematic Assessment
EG0002 affected29 at risk
EG0011 affected24 at risk
EG0021 affected19 at risk
EG003
Weight loss
Investigations
Systematic Assessment
EG0001 affected29 at risk
EG0011 affected24 at risk
EG0023 affected19 at risk
EG003
White blood cell decreased
Investigations
Systematic Assessment
EG00015 affected29 at risk
EG00112 affected24 at risk
EG0027 affected19 at risk
EG003
Acidosis
Metabolism and nutrition disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Anorexia
Metabolism and nutrition disorders
Systematic Assessment
EG0004 affected29 at risk
EG0019 affected24 at risk
EG0022 affected19 at risk
EG003
Dehydration
Metabolism and nutrition disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Hypercalcemia
Metabolism and nutrition disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0021 affected19 at risk
EG003
Hyperglycemia
Metabolism and nutrition disorders
Systematic Assessment
EG00013 affected29 at risk
EG0019 affected24 at risk
EG0026 affected19 at risk
EG003
Hyperkalemia
Metabolism and nutrition disorders
Systematic Assessment
EG0002 affected29 at risk
EG0013 affected24 at risk
EG0021 affected19 at risk
EG003
Hypermagnesemia
Metabolism and nutrition disorders
Systematic Assessment
EG0001 affected29 at risk
EG0012 affected24 at risk
EG0020 affected19 at risk
EG003
Hypernatremia
Metabolism and nutrition disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Hypertriglyceridemia
Metabolism and nutrition disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Hypoalbuminemia
Metabolism and nutrition disorders
Systematic Assessment
EG00013 affected29 at risk
EG00113 affected24 at risk
EG0027 affected19 at risk
EG003
Hypocalcemia
Metabolism and nutrition disorders
Systematic Assessment
EG0007 affected29 at risk
EG0019 affected24 at risk
EG0022 affected19 at risk
EG003
Hypoglycemia
Metabolism and nutrition disorders
Systematic Assessment
EG0004 affected29 at risk
EG0011 affected24 at risk
EG0023 affected19 at risk
EG003
Hypokalemia
Metabolism and nutrition disorders
Systematic Assessment
EG0006 affected29 at risk
EG0015 affected24 at risk
EG0021 affected19 at risk
EG003
Hypomagnesemia
Metabolism and nutrition disorders
Systematic Assessment
EG0005 affected29 at risk
EG0013 affected24 at risk
EG0023 affected19 at risk
EG003
Hyponatremia
Metabolism and nutrition disorders
Systematic Assessment
EG00013 affected29 at risk
EG0013 affected24 at risk
EG0024 affected19 at risk
EG003
Hypophosphatemia
Metabolism and nutrition disorders
Systematic Assessment
EG0003 affected29 at risk
EG0018 affected24 at risk
EG0021 affected19 at risk
EG003
Metabolism and nutrition disorders - Other, specify
Metabolism and nutrition disorders
Systematic Assessment
EG0002 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Arthralgia
Musculoskeletal and connective tissue disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Arthritis
Musculoskeletal and connective tissue disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Back pain
Musculoskeletal and connective tissue disorders
Systematic Assessment
EG0007 affected29 at risk
EG0013 affected24 at risk
EG0027 affected19 at risk
EG003
Bone pain
Musculoskeletal and connective tissue disorders
Systematic Assessment
EG0003 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Chest wall pain
Musculoskeletal and connective tissue disorders
Systematic Assessment
EG0000 affected29 at risk
EG0011 affected24 at risk
EG0020 affected19 at risk
EG003
Flank pain
Musculoskeletal and connective tissue disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Generalized muscle weakness
Musculoskeletal and connective tissue disorders
Systematic Assessment
EG0003 affected29 at risk
EG0015 affected24 at risk
EG0022 affected19 at risk
EG003
Joint range of motion decreased
Musculoskeletal and connective tissue disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Muscle weakness lower limb
Musculoskeletal and connective tissue disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Musculoskeletal and connective tiss disorder - Other
Musculoskeletal and connective tissue disorders
Systematic Assessment
EG0001 affected29 at risk
EG0010 affected24 at risk
EG0021 affected19 at risk
EG003
Myalgia
Musculoskeletal and connective tissue disorders
Systematic Assessment
EG0003 affected29 at risk
EG0010 affected24 at risk
EG0022 affected19 at risk
EG003
Neck pain
Musculoskeletal and connective tissue disorders
Systematic Assessment
EG0000 affected29 at risk
EG0012 affected24 at risk
EG0021 affected19 at risk
EG003
Osteoporosis
Musculoskeletal and connective tissue disorders
Systematic Assessment
EG0000 affected29 at risk
EG0010 affected24 at risk
EG0020 affected19 at risk
EG003
Pain in extremity
Musculoskeletal and connective tissue disorders
Systematic Assessment
EG0005 affected29 at risk
EG0012 affected24 at risk
EG0022 affected19 at risk
EG003
Neoplasms benign, malignant and unspecified - Other
Neoplasms benign, malignant and unspecified (incl cysts and polyps)
POST-REMISSION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28. Treatment repeats every 42 days for 3 cycles in the absence of disease progression or unacceptable toxicity.
Blinatumomab: Given IV
OG003
Post-remission: Cohort II (Ph+/Ph-like)
POST-REMISSION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28 and dasatinib PO QD on days 1-42. Treatment repeats every 42 days for 3 cycles in the absence of disease progression or unacceptable toxicity.
Blinatumomab: Given IV
Dasatinib: Given PO
OG004
Maintenance: Cohort I (Ph-)
MAINTENANCE: Patients receive prednisone PO on days 1-5, vincristine sulfate IV on day 1, mercaptopurine PO on days 1-28, and methotrexate PO on days 1, 8, 15, and 22. Treatment repeats every 28 days for 18 cycles in the absence of disease progression or unacceptable toxicity. (Closed to accrual 06/29/17)
Mercaptopurine: Given PO
Methotrexate: Given PO
Methotrexate Sodium: Given PO
Prednisone: Given PO
Vincristine: Given IV
Vincristine Sulfate: Given IV
OG005
Maintenance: Cohort II (Ph+/Ph-like)
MAINTENANCE: Patients receive dasatinib PO BID on days 1-28. Cycles repeat every 28 days in the absence of disease progression or unacceptable toxicity. Patients also receive prednisone PO on days 1-5. Treatment repeats every 28 days for 18 cycles in the absence of disease progression or unacceptable toxicity.
Dasatinib: Given PO
Prednisone: Given PO
Units
Counts
Participants
OG00029
OG00124
OG00219
OG00318
OG00413
OG00516
Title
Denominators
Categories
Abdominal pain
Title
Measurements
OG0000
OG0010
OG0020
OG0030
OG0041
OG0050
Adult respiratory distress syndrome
Title
Measurements
OG0000
OG0010
OG0020
OG003
Agitation
Title
Measurements
OG0000
OG0010
OG0020
OG003
Alanine aminotransferase increased
Title
Measurements
OG0001
OG0011
OG0020
OG003
Alkaline phosphatase increased
Title
Measurements
OG0000
OG0010
OG0020
OG003
Anemia
Title
Measurements
OG00010
OG0018
OG0022
OG003
Anorexia
Title
Measurements
OG0000
OG0010
OG0020
OG003
Aspartate aminotransferase increased
Title
Measurements
OG0000
OG0010
OG0020
OG003
Atrial flutter
Title
Measurements
OG0000
OG0010
OG0020
OG003
Blood bilirubin increased
Title
Measurements
OG0000
OG0010
OG0020
OG003
Cataract
Title
Measurements
OG0000
OG0010
OG0020
OG003
Catheter related infection
Title
Measurements
OG0000
OG0011
OG0020
OG003
Colitis
Title
Measurements
OG0000
OG0010
OG0020
OG003
Confusion
Title
Measurements
OG0001
OG0010
OG0020
OG003
Cytokine release syndrome
Title
Measurements
OG0001
OG0010
OG0020
OG003
Dehydration
Title
Measurements
OG0000
OG0011
OG0020
OG003
Diarrhea
Title
Measurements
OG0001
OG0011
OG0020
OG003
Dizziness
Title
Measurements
OG0000
OG0011
OG0020
OG003
Dysarthria
Title
Measurements
OG0001
OG0010
OG0020
OG003
Dyspnea
Title
Measurements
OG0003
OG0011
OG0020
OG003
Edema limbs
Title
Measurements
OG0000
OG0012
OG0020
OG003
Encephalopathy
Title
Measurements
OG0000
OG0010
OG0020
OG003
Fatigue
Title
Measurements
OG0001
OG0010
OG0021
OG003
Febrile neutropenia
Title
Measurements
OG0003
OG0011
OG0020
OG003
Fever
Title
Measurements
OG0001
OG0010
OG0020
OG003
Gastrointestinal pain
Title
Measurements
OG0000
OG0010
OG0020
OG003
General disorders and admin site conditions - Other
Title
Measurements
OG0000
OG0011
OG0020
OG003
Generalized muscle weakness
Title
Measurements
OG0000
OG0011
OG0020
OG003
Heart failure
Title
Measurements
OG0000
OG0011
OG0020
OG003
Hematoma
Title
Measurements
OG0000
OG0011
OG0020
OG003
Hyperglycemia
Title
Measurements
OG0004
OG0011
OG0021
OG003
Hypertension
Title
Measurements
OG0003
OG0010
OG0021
OG003
Hypoalbuminemia
Title
Measurements
OG0000
OG0010
OG0020
OG003
Hypocalcemia
Title
Measurements
OG0001
OG0010
OG0020
OG003
Hypokalemia
Title
Measurements
OG0000
OG0011
OG0021
OG003
Hypophosphatemia
Title
Measurements
OG0001
OG0010
OG0020
OG003
Hypotension
Title
Measurements
OG0001
OG0011
OG0020
OG003
Hypoxia
Title
Measurements
OG0001
OG0011
OG0020
OG003
Infections and infestations - Other, specify
Title
Measurements
OG0001
OG0011
OG0020
OG003
Infusion related reaction
Title
Measurements
OG0001
OG0010
OG0020
OG003
Lung infection
Title
Measurements
OG0002
OG0012
OG0020
OG003
Lymphocyte count decreased
Title
Measurements
OG0008
OG0016
OG0022
OG003
Metabolism and nutrition disorders - Other, specify
Title
Measurements
OG0000
OG0010
OG0020
OG003
Mucositis oral
Title
Measurements
OG0000
OG0010
OG0020
OG003
Nausea
Title
Measurements
OG0000
OG0011
OG0020
OG003
Nervous system disorders - Other, specify
Title
Measurements
OG0001
OG0010
OG0020
OG003
Neutrophil count decreased
Title
Measurements
OG00010
OG0019
OG0025
OG003
Non-cardiac chest pain
Title
Measurements
OG0000
OG0010
OG0020
OG003
Pericardial effusion
Title
Measurements
OG0000
OG0010
OG0020
OG003
Platelet count decreased
Title
Measurements
OG00013
OG0018
OG0020
OG003
Pleural effusion
Title
Measurements
OG0000
OG0010
OG0020
OG003
Pneumonitis
Title
Measurements
OG0001
OG0010
OG0020
OG003
Pulmonary hypertension
Title
Measurements
OG0000
OG0010
OG0020
OG003
Rash maculo-papular
Title
Measurements
OG0000
OG0011
OG0020
OG003
Respiratory failure
Title
Measurements
OG0001
OG0010
OG0020
OG003
Sepsis
Title
Measurements
OG0000
OG0011
OG0020
OG003
Soft tissue infection
Title
Measurements
OG0000
OG0010
OG0020
OG003
Thrombotic thrombocytopenic purpura
Title
Measurements
OG0001
OG0010
OG0020
OG003
Urinary tract infection
Title
Measurements
OG0000
OG0011
OG0020
OG003
Vascular access complication
Title
Measurements
OG0000
OG0010
OG0020
OG003
Weight loss
Title
Measurements
OG0000
OG0010
OG0020
OG003
White blood cell decreased
Title
Measurements
OG00011
OG0016
OG0022
OG003
Units
Counts
Participants
OG00029
Title
Denominators
Categories
CR or CRi
Title
Measurements
OG00019
No CR or CRi
Title
Measurements
OG00010
Units
Counts
Participants
OG00022
Title
Denominators
Categories
Title
Measurements
OG0005.3(3.0 to NA)There have not been enough events occurring after the median was reached to estimate the upper limit of the confidence interval.
Cohort II (Ph+/Ph-like)
INDUCTION: Patients receive dasatinib PO BID on days 1-84 and prednisone PO on days 1-24 with tapering on days 25-32 in the absence of disease progression or unacceptable toxicity.
RE-INDUCTION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28. Treatment repeats every 42 days for 2 cycles in the absence of disease progression or unacceptable toxicity.
POST-REMISSION: Patients receive blinatumomab IV continuously over 24 hours on days 1-28 and dasatinib PO QD on days 1-42. Treatment repeats every 42 days for 3 cycles in the absence of disease progression or unacceptable toxicity.
MAINTENANCE: Patients receive dasatinib PO BID on days 1-28. Cycles repeat every 28 days in the absence of disease progression or unacceptable toxicity. Patients also receive prednisone PO on days 1-5. Treatment repeats every 28 days for 18 cycles in the absence of disease progression or unacceptable toxicity.