 |
|
Phase II Pilot Study of Intensified Chemotherapy With or Without Allogeneic Hematopoietic Stem Cell Transplantation in Children With Very High-Risk Acute Lymphoblastic Leukemia
Alternate Title
Basic Trial Information
Objectives
Entry Criteria
Expected Enrollment
Outcomes
Outline
Published Results
Trial Contact Information
Registry Information
Alternate Title
Combination Chemotherapy With or Without Peripheral Stem Cell Transplant in Treating Children With Acute Lymphoblastic Leukemia
Basic Trial Information
|
Phase
|
|
|
|
Type
|
|
|
|
Status
|
|
|
|
Age
|
|
|
|
Sponsor
|
|
|
|
Protocol IDs
|
|
|
|
Phase II
|
|
|
|
Treatment
|
|
|
|
Closed
|
|
|
|
1 to 21
|
|
|
|
NCI
|
|
|
|
COG-AALL0031
NCT00022737, AALL0031
|
|
|
Objectives - Determine the feasibility of treatment with intensified chemotherapy, in terms of toxicity and patient accrual, in children with very high-risk acute lymphoblastic leukemia.
- Determine the feasibility and efficacy of following intensified chemotherapy with allogeneic hematopoietic stem cell transplantation in patients with HLA-matched related donors.
- Determine the toxicity of imatinib mesylate in combination with intensified chemotherapy in Philadelphia chromosome-positive patients.
- Determine the event-free survival of patients treated with this regimen.
- Determine whether minimal residual disease (MDR) after induction therapy and prior to intensification therapy can predict relapse in these patients.
- Determine whether MDR after intensification is prognostically significant.
- Determine whether gene expression patterns predict disease recurrence or response to imatinib mesylate.
Entry Criteria Disease Characteristics:
- Diagnosis of acute lymphoblastic leukemia
- Received prior front-line therapy on a Pediatric Oncology Group (POG),
Children's Cancer Group (CCG), or Central Oncology Group (COG) study
OR
- Received induction therapy comprising vincristine, asparaginase,
prednisone/dexamethasone, and daunorubicin as in CCG, POG, or COG
protocols
- M1 or M2 bone marrow status after front-line induction therapy and presenting with at
least 1
of the following:
- Philadelphia chromosome positive (Ph+) with
t(9;22)(q34;q11) by cytogenetics
or fluorescence in situ hybridization
-
bcr-abl fusion transcript by reverse transcription
polymerase chain reaction
- Hypodiploid with less than 44 chromosomes and/or
DNA index less than
0.81
- MLL translocation (11q23) by cytogenetics and a slow early response (SER) to induction therapy, defined as at least 5% blasts at day 15 of induction and/or at least .1% minimal residual disease (MRD) after induction therapy
OR
- Failed to achieve remission after front-line induction therapy
- M3 bone marrow status (greater than 25% blasts) after
induction therapy
OR - M2 bone marrow status (5-25% blasts) or at least 1% MRD after induction
therapy and M2 or M3
or at least 1% MRD after consolidation therapy (CCG studies) or
extended induction therapy (POG or COG
studies)
Prior/Concurrent Therapy:
Biologic therapy: Chemotherapy: - See Disease Characteristics
Endocrine therapy: - See Disease Characteristics
Radiotherapy: - No concurrent prophylactic cranial radiotherapy
Surgery: Patient Characteristics:
Age: Performance status: Life expectancy: Hematopoietic: - See Disease Characteristics
Hepatic: Renal: Other: - Not pregnant or nursing
- Negative pregnancy test
- Fertile patients must use effective contraception
Expected Enrollment 220Approximately 220 patients (116 Philadelphia chromosome-positive) will be
accrued for this study within 4.2 years. Outcomes Primary Outcome(s)Feasibility, in terms of toxicity and patient accrual
Safety
Secondary Outcome(s)Event-free survival
Feasibility of administering hematopoietic stem cell transplantation after the second consolidation block of chemotherapy
Prognostic effect of minimal residual disease assays
Outline This is a multicenter study. This is also a dose-escalation study of
imatinib mesylate in Philadelphia chromosome-positive (Ph+) patients. Patients are
stratified according to Philadelphia chromosome (Ph) status (Ph-positive vs Ph-negative or indeterminate), hypodiploidy (yes vs no), MLL translocation (11q23) AND slow early response to prior induction therapy (yes vs no), and
failed prior induction therapy (yes vs no). Cohorts of 8-12 Ph+ patients receive escalating doses of imatinib mesylate,
according to the guidelines for each treatment block of this study, until the
maximum tolerated dose (MTD) for each treatment combination is determined.
The MTD is defined as the dose preceding that at which 2 of 6 patients
experience dose-limiting toxicity. An additional 35 patients are treated at the MTD. - Consolidation block 1: Patients receive etoposide IV over 1 hour
followed by ifosfamide IV over 1.5 hours on days 1-5. Patients also receive methotrexate intrathecally on day 1 and filgrastim (G-CSF) subcutaneously
(SC) on days 6-15 or until blood counts recover. Patients with CNS 2/3 at diagnosis also receive intrathecal triple therapy comprising methotrexate, hydrocortisone, and cytarabine (ITT) on days 8 and 15. Ph+ patients in cohorts 3,
4, and 5 receive oral imatinib mesylate on days 1-21. Within 4 days of starting
consolidation therapy, patients with biopsy-proven testicular leukemia undergo
radiotherapy daily for 12 days.
- Consolidation block 2: Patients receive high-dose methotrexate IV over 24 hours
and ITT on day 1 followed by high-dose cytarabine IV over 3 hours, every 12 hours on days
2 and 3. Patients also receive leucovorin calcium IV or orally every 6 hours for 3 doses
beginning on day 2, and G-CSF SC on days 4-13 or until blood counts
recover. Ph+ patients in cohorts 2, 3,
4, and 5 receive oral imatinib mesylate as in consolidation block 1.
Patients undergoing allogeneic hematopoietic stem cell transplantation
(HSCT) proceed to preparative chemotherapy. All other patients proceed to
reinduction block 1. - Reinduction block 1: Patients receive vincristine IV on days 1, 8, and
15; daunorubicin IV on days 1 and 2; cyclophosphamide IV over 30 minutes,
every 12 hours on days 3 and 4; pegaspargase intramuscularly (IM) on day 4;
and ITT on days 1 and 15. Patients also receive oral
dexamethasone twice daily on days 1-7 and 15-21 and G-CSF SC on days 5-14 or
until blood counts recover. Ph+ patients in cohorts 2, 4, and 5 receive
imatinib mesylate as in consolidation block 1.
- Intensification block 1: Patients receive high-dose methotrexate IV over 24 hours
on days 1 and 15 and ITT on days 1 and 22. Patients also receive
leucovorin calcium IV or orally every 6 hours for 3 doses beginning on days 2 and 16.
Patients receive etoposide IV over 2 hours followed by cyclophosphamide IV
over 30 minutes on days 22-24; G-CSF SC on days 27-36 or until blood counts
recover; high-dose cytarabine IV over 3 hours, every 12 hours on days 43 and 44; and
asparaginase IM on day 44. Ph+ patients in cohorts 1 and 4 receive
oral imatinib mesylate on days 43-63, and patients in cohort 5 receive oral imatinib mesylate on days 1-56.
- Reinduction block 2: Patients receive vincristine, daunorubicin,
cyclophosphamide, pegaspargase, dexamethasone, and G-CSF as in reinduction
block 1. Patients also receive ITT on days 1 and 15. Ph+ patients
receive imatinib mesylate as in reinduction block 1.
- Intensification block 2: Patients receive methotrexate, leucovorin
calcium, etoposide, cyclophosphamide, filgrastim, cytarabine, and asparaginase
as in intensification block 1. Ph+ patients receive imatinib mesylate as in
intensification block 1.
- Maintenance 1: Patients receive high-dose methotrexate IV and leucovorin calcium
as in consolidation block 2. Patients also receive ITT and
vincristine IV on days 1 and 29; oral dexamethasone twice daily on days 1-5
and 29-33; oral methotrexate on days 8, 15, and 22; oral mercaptopurine on
days 8-28; etoposide IV over 2 hours followed by cyclophosphamide IV over 30
minutes on days 29-33; and G-CSF SC on days 34-43. Ph+ patients in cohorts 1-4 receive oral imatinib mesylate on days 29-49 and patients in cohort 5 receive oral imatinib mesylate on days 1-56. Treatment repeats every 8 weeks
for 4 courses in the absence of disease progression or unacceptable
toxicity.
- Maintenance 2: Patients receive vincristine and dexamethasone as in maintenance 1. Beginning on day 1, patients undergo cranial radiotherapy once daily, 5 days a week, for approximately 2 weeks. Patients also receive oral methotrexate on days 8, 15, 22, 29, 36, 43, and 50 and oral mercaptopurine on days 11-56. Ph+
patients in cohorts 1-4 receive oral imatinib mesylate on days 1-21 and 29-49, and patients in cohort 5 receive oral imatinib mesylate on days 1-56.
- Maintenance 3: Patients receive vincristine and dexamethasone as in
maintenance 2. Patients also receive oral methotrexate on days 1, 8, 15, 22, 29, 36, 43, and 50; and oral mercaptopurine on days 1-56. Ph+ patients receive imatinib mesylate as in maintenance 2. Treatment repeats every 8 weeks for 7 courses (12 course total in maintenance 1, 2, and 3) in the absence of disease
progression or unacceptable toxicity.
Patients may undergo allogeneic HSCT after consolidation block 2 if
there is an available HLA-DR matched or HLA-A or -B matched or 1 antigen mismatched relative donor. Patients with CNS leukemia undergo cranial radiotherapy 3 times daily on
days -10 to -8. All patients undergo radiotherapy twice daily on days -7 to
-5 and receive etoposide IV on day -4 and cyclophosphamide IV on days -3 and
-2. Patients undergo allogeneic bone marrow, peripheral blood stem cell, or
umbilical cord blood transplantation on day 0. Patients receive cyclosporine
IV beginning on day -1 and continuing every 12 hours, switching to oral
administration when possible, until day 60 and tapering thereafter. Patients
also receive methotrexate on days 1, 3, and 6. Beginning 16-24 weeks after transplantation, Ph+ patients receive oral
imatinib mesylate once daily for 24 weeks. Patients are followed every 4-8 weeks for 1 year, every 3 months for 1
year, every 6 months for 1 year, and then annually thereafter. Patients
undergoing HSCT are followed weekly for the first year. Published ResultsSchultz KR, Aledo A, Bowman WP, et al.: Minimal toxicity of imatinib mesylate in combination with intensive chemotherapy for Philadelphia chromosome positive (Ph+) acute lymphoblastic leukemia (ALL) in children: a report of the Childrens Oncology Group (COG) AALL0031 protocol for very high risk ALL. [Abstract] Blood 108 (11): A-283, 2006.
Trial Contact Information
Trial Lead Organizations Children's Oncology Group | | | | Kirk Schultz, MD, Protocol chair | | | |
| Registry Information | | | Official Title | | A Children's Oncology Group Pilot Study for the Treatment of Very High Risk Acute Lymphoblastic Leukemia in Children and Adolescents (STI571 NSC#716051/IND#55666) | | | Trial Start Date | | 2002-10-14 | | | Trial Completion Date | | 2007-10-01 (estimated) | | | Registered in ClinicalTrials.gov | | NCT00022737 | | | Date Submitted to PDQ | | 2001-07-02 | | | Information Last Verified | | 2006-10-21 | | | NCI Grant/Contract Number | | CA30969 |
Note: The purpose of most clinical trials listed in this database is to test new cancer treatments, or new methods of diagnosing, screening, or preventing cancer. Because all potentially harmful side effects are not known before a trial is conducted, dose and schedule modifications may be required for participants if they develop side effects from the treatment or test. The therapy or test described in this clinical trial is intended for use by clinical oncologists in carefully structured settings, and may not prove to be more effective than standard treatment. A responsible investigator associated with this clinical trial should be consulted before using this protocol.  Back to Top |
 |
