TITLE:Less Intensive Therapy for Children With Non-Hodgkin's Lymphoma
NCT ID: NCT00002757
Last Updated: 2014-07-24
Study Results
Results pending
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
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Recruitment Status
COMPLETED
Clinical Phase
PHASE3
Total Enrollment
1148 participants
Study Classification
INTERVENTIONAL
Study Start Date
2001-06-30
Study Completion Date
2009-10-31
Brief Summary
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RATIONALE: Less intensive therapy may attain in the same results as intensive therapy in children with non-Hodgkin's lymphoma.
PURPOSE: Randomized phase III trial to study the effectiveness of less intensive therapy for children who have non-Hodgkin's lymphoma.
PURPOSE: Randomized phase III trial to study the effectiveness of less intensive therapy for children who have non-Hodgkin's lymphoma.
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Detailed Description
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OBJECTIVES:
* Confirm the previously found excellent survival for low-risk patients (Group A) with B-cell lymphoma/leukemia treated with the LMB 89 regimen.
* Verify that good event-free survival is retained in intermediate-risk patients (Group B) when the dose of cyclophosphamide (CTX) or the number of CTX-containing regimens is reduced.
* Verify that good event-free survival is retained in high-risk patients (Group C) despite reduction in doses during consolidation therapy and a reduced number of maintenance courses, and, for patients with CNS involvement, additional intravenous and intrathecal methotrexate in place of cranial irradiation.
* Monitor survival and event-free survival of all patients registered prior to the first chemotherapy course.
* Compare the survival and event-free survival of Group C patients with CNS involvement against results from those treated on the LMB 89 study.
* Compare event-free survival and survival of patients with large cell and Burkitt's and Burkitt's-like lymphoma.
* Monitor the long-term toxicity in patients treated on this study, including fertility, cardiotoxicity, and secondary malignancy.
* Characterize further the biology of childhood small non-cleaved cell lymphoma with respect to drug resistance (i.e., topoisomerase II and MDR activity), viral association (i.e., Epstein-Barr virus, human immunodeficiency virus, human herpesvirus 6), and specific breakpoint translocations (i.e., IgH and C-myc) per companion study CCG-B944.
* Characterize further the biology of childhood mature B-cell lymphoma per UKCCSG studies.
OUTLINE: This is a randomized study. Patients are stratified according to participating group (UKCCSG vs SFOP vs CCG), histology (large cell vs small non-cleaved cell), risk group (Group A vs Group B vs Group C). Stage III Group B patients are further stratified according to Murphy stage (stages I/II vs III vs III/IV) and by LDH (less than twice normal vs twice normal or higher). Group C patients are further stratified based on presence of CNS disease (yes vs no).
Patients with resected stage I and resected abdominal-only stage II disease are treated on the Group A Regimen. Patients with unresected stage I/II, stage III, or CNS-negative stage IV disease with fewer than 25% blasts in bone marrow are treated on the Group B Regimen. Patients with 25% or more blasts in bone marrow or with CNS involvement (i.e., L3 blasts in CSF, cranial nerve palsy, clinical spinal cord compression, isolated intracerebral mass, or parameningeal cranial or spinal extension) are treated on the Group C Regimen.
The following acronyms are used:
* ARA-C Cytarabine, NSC-63878
* CF Leucovorin calcium, NSC-3590
* COP CTX/VCR/PRED (or PRDL)
* COPAD CTX/VCR/PRED (or PRDL)/DOX
* COPADM CTX/VCR/PRED (or PRDL)/DOX/MTX
* CTX Cyclophosphamide, NSC-26271
* CYM ARA- C/MTX
* CYVE ARA-C/VP-16
* DOX Doxorubicin, NSC-123127
* G-CSF Granulocyte Colony-Stimulating Factor (Amgen), NSC-614629
* HC Hydrocortisone, NSC-10483
* HD High Dose
* MTX Methotrexate, NSC-740
* PRDL Prednisolone, NSC-9900
* PRED Prednisone, NSC-10023
* TIT Triple Intrathecal Chemotherapy (IT MTX/IT HC/IT ARA-C)
* VCR Vincristine, NSC-67574
* VP-16 Etoposide, NSC-141540
Group A Regimen (Low-Risk Patients)
* Induction: Patients receive COPAD: VCR IV on days 1 and 6, oral PRED (or IV) twice daily on days 1-5, then tapered over 3 days, CTX IV over 15 minutes every 12 hours on days 1-3, and DOX IV over 6 hours on day 1 starting after the first CTX dose. G-CSF SC is administered until hematopoietic recovery beginning on day 7. Patients receive a second course beginning on day 21.
Group B Regimen (Intermediate-Risk Patients)
* Induction 1: Patients receive CTX IV over 15 minutes on day 1, VCR IV on day 1, and oral PRED on days 1-7, and MTX IT and HC IT on day 1. Patients with responding disease proceed with COPADM. Patients with no response proceed to treatment on arm I of the Group C Regimen.
* COPADM 1: Patients receive VCR IV on day 8, oral PRED twice daily on days 8-12, then tapered over 3 days, MTX IV over 3 hours on day 8, oral CF every 6 hours for 12 doses beginning 24 hours after start of MTX, CTX IV over 15 minutes every 12 hours on days 9-11, and DOX IV over 6 hours on day 9 beginning after the first CTX dose. G-CSF is administered as in the Group A Regimen. MTX IT and HC IT are given on days 9 and 13.
* Group B patients are randomized to 1 of 4 treatments following recovery and disease assessment:
Arm I:
* Induction 2 (begins no sooner than 16 days after start of COPADM 1): Patients receive COPADM 2 according to the same schedule as in COPADM 1 in Induction 1 except CTX is increased. G-CSF is administered as in the Group A Regimen. Patients receive MTX IT and HC IT on days 2 and 6.
* Consolidation: Patients receive CYM: MTX IV over 3 hours on day 1, oral CF every 6 hours for a maximum of 12 doses beginning 24 hours after the start of MTX, and ARA-C IV over 24 hours on days 2-6. Patients receive TIT: MTX IT on day 2, HC IT on days 2 and 7, and ARA-C IT on day 7.
* Response is assessed upon recovery with resection of residual masses. If histology is negative patients proceed to a second course of CYM. If histology is positive patients proceed to CYVE on arm I of the Group C Regimen.
* Maintenance: Patients receive COPADM 3 as in COPADM 1 in Induction 1, except CTX IV is administered over 30 minutes on days 2 and 3, and MTX IT and HC IT are administered on day 2.
Arm II:
* Induction 2: Patients receive COPADM 2 as in arm I of the Group B Regimen. G-CSF is administered as in the Group A Regimen. MTX IT and HC IT are administered as in Induction 1.
* Consolidation: Patients receive CYM, TIT, and response assessment as in arm I of the Group B Regimen.
* Maintenance: Patients receive no maintenance therapy.
Arm III:
* Induction 2: Patients receive COPADM 2 as in COPADM 1 in Induction 1. G-CSF is administered as in the Group A Regimen. Patients receive MTX IT and HC IT as in Induction 1.
* Consolidation: Patients receive CYM, TIT, and response assessment as in arm I of the Group B Regimen.
* Maintenance: Patients receive COPADM 3 as in arm I of the Group B Regimen. Patients receive MTX IT and HC IT on day 2.
Arm IV:
* Induction 2: Patients receive COPADM 2 as in COPADM 1 in Induction 1. G-CSF is administered as in the Group A Regimen. Patients receive MTX IT and HC IT as in Induction 1.
* Consolidation: Patients receive CYM, TIT, and response assessment as in arm I of the Group B Regimen.
* Maintenance: Patients receive no maintenance therapy.
Group C Regimen (High-Risk Patients)
* Induction: Patients receive COP as in Induction 1 of the Group B Regimen, TIT on days 1, 3, and 5, and oral CF every 12 hours on days 2 and 4. Tumor response is evaluated on day 7 and treatment decisions are made as in Induction 1 of the Group B Regimen. Patients receive COPADM 1 as in COPADM 1 in Induction 1 of the Group B Regimen except HD MTX IV is given over 4 hours on day 1. G-CSF is administered as in the Group A Regimen. TIT is given on days 2, 4, and 6. Patients receive COPADM 2 as in COPADM 2 in arm I of the Group B Regimen, Induction 2 except HD MTX IV is given over 4 hours on day 1. G-CSF is administered as in the Group A Regimen. Patients receive TIT on days 2, 4, and 6.
* Patients are randomized to 1 of 2 treatment arms upon recovery and disease assessment:
Arm I:
* Consolidation: Patients receive CYVE: ARA-C IV on days 1-5, and VP-16 IV over 2 hours on days 2-5. G-CSF is administered as in the Group A Regimen. For patients with CNS disease: MTX IT and HC IT on day 1, 6 hours prior to initiation of ARA-C, HD MTX IV over 4 hours, about day 18, oral CF every 6 hours for a maximum of 12 doses, beginning 24 hours after starting MTX, and TIT prior to beginning CF.
* Response is assessed upon recovery with resection of residual masses. Patients with a complete response receive a second course of CYVE (no HD MTX/CF), beginning 1 week after HD MTX.
* Maintenance (28 days between courses):
* Course 1: Patients receive COPADM as in arm I Maintenance in the Group B Regimen, except HD MTX is administered as in Group C Induction, and TIT is given on day 2 replacing MTX IT and HC.
* Course 2: Patients receive CYVE: ARA-C IV every 12 hours on days 1-5, and VP-16 IV over 90 minutes on days 1-3.
* Course 3: Patients receive COPAD as in Group B Induction 1, except CTX IV is administered over 30 minutes on days 1 and 2.
* Course 4: Patients receive treatment identical to Course 2.
Arm II:
* Consolidation: Patients receive Mini-CYVE: ARA-C IV on days 1-5, and VP-16 IV over 1 hour on days 2-5. G-CSF is administered as in the Group A Regimen. For patients with CNS disease: MTX IT and HC IT as in arm I in the Group C Regimen, and HD MTX, CF, and TIT as in arm I in the Group C Regimen.
* Response is assessed upon recovery with resection of residual masses. Patients with a complete response receive a second course of CYVE (no HD MTX and CF) beginning 1 week after HD MTX.
* Maintenance: Patients receive COPADM and TIT as in arm I of the Group C Regimen in Course 1 for 1 course only.
Patients are followed every 3 months for 6 months, every 6 months for 2.5 years, and then annually thereafter.
PROJECTED ACCRUAL: A total of 900 patients will be accrued for this study within 5 years. Yearly accrual is expected to be 20 Group A patients, 115 Group B patients, and 45 Group C patients.
* Confirm the previously found excellent survival for low-risk patients (Group A) with B-cell lymphoma/leukemia treated with the LMB 89 regimen.
* Verify that good event-free survival is retained in intermediate-risk patients (Group B) when the dose of cyclophosphamide (CTX) or the number of CTX-containing regimens is reduced.
* Verify that good event-free survival is retained in high-risk patients (Group C) despite reduction in doses during consolidation therapy and a reduced number of maintenance courses, and, for patients with CNS involvement, additional intravenous and intrathecal methotrexate in place of cranial irradiation.
* Monitor survival and event-free survival of all patients registered prior to the first chemotherapy course.
* Compare the survival and event-free survival of Group C patients with CNS involvement against results from those treated on the LMB 89 study.
* Compare event-free survival and survival of patients with large cell and Burkitt's and Burkitt's-like lymphoma.
* Monitor the long-term toxicity in patients treated on this study, including fertility, cardiotoxicity, and secondary malignancy.
* Characterize further the biology of childhood small non-cleaved cell lymphoma with respect to drug resistance (i.e., topoisomerase II and MDR activity), viral association (i.e., Epstein-Barr virus, human immunodeficiency virus, human herpesvirus 6), and specific breakpoint translocations (i.e., IgH and C-myc) per companion study CCG-B944.
* Characterize further the biology of childhood mature B-cell lymphoma per UKCCSG studies.
OUTLINE: This is a randomized study. Patients are stratified according to participating group (UKCCSG vs SFOP vs CCG), histology (large cell vs small non-cleaved cell), risk group (Group A vs Group B vs Group C). Stage III Group B patients are further stratified according to Murphy stage (stages I/II vs III vs III/IV) and by LDH (less than twice normal vs twice normal or higher). Group C patients are further stratified based on presence of CNS disease (yes vs no).
Patients with resected stage I and resected abdominal-only stage II disease are treated on the Group A Regimen. Patients with unresected stage I/II, stage III, or CNS-negative stage IV disease with fewer than 25% blasts in bone marrow are treated on the Group B Regimen. Patients with 25% or more blasts in bone marrow or with CNS involvement (i.e., L3 blasts in CSF, cranial nerve palsy, clinical spinal cord compression, isolated intracerebral mass, or parameningeal cranial or spinal extension) are treated on the Group C Regimen.
The following acronyms are used:
* ARA-C Cytarabine, NSC-63878
* CF Leucovorin calcium, NSC-3590
* COP CTX/VCR/PRED (or PRDL)
* COPAD CTX/VCR/PRED (or PRDL)/DOX
* COPADM CTX/VCR/PRED (or PRDL)/DOX/MTX
* CTX Cyclophosphamide, NSC-26271
* CYM ARA- C/MTX
* CYVE ARA-C/VP-16
* DOX Doxorubicin, NSC-123127
* G-CSF Granulocyte Colony-Stimulating Factor (Amgen), NSC-614629
* HC Hydrocortisone, NSC-10483
* HD High Dose
* MTX Methotrexate, NSC-740
* PRDL Prednisolone, NSC-9900
* PRED Prednisone, NSC-10023
* TIT Triple Intrathecal Chemotherapy (IT MTX/IT HC/IT ARA-C)
* VCR Vincristine, NSC-67574
* VP-16 Etoposide, NSC-141540
Group A Regimen (Low-Risk Patients)
* Induction: Patients receive COPAD: VCR IV on days 1 and 6, oral PRED (or IV) twice daily on days 1-5, then tapered over 3 days, CTX IV over 15 minutes every 12 hours on days 1-3, and DOX IV over 6 hours on day 1 starting after the first CTX dose. G-CSF SC is administered until hematopoietic recovery beginning on day 7. Patients receive a second course beginning on day 21.
Group B Regimen (Intermediate-Risk Patients)
* Induction 1: Patients receive CTX IV over 15 minutes on day 1, VCR IV on day 1, and oral PRED on days 1-7, and MTX IT and HC IT on day 1. Patients with responding disease proceed with COPADM. Patients with no response proceed to treatment on arm I of the Group C Regimen.
* COPADM 1: Patients receive VCR IV on day 8, oral PRED twice daily on days 8-12, then tapered over 3 days, MTX IV over 3 hours on day 8, oral CF every 6 hours for 12 doses beginning 24 hours after start of MTX, CTX IV over 15 minutes every 12 hours on days 9-11, and DOX IV over 6 hours on day 9 beginning after the first CTX dose. G-CSF is administered as in the Group A Regimen. MTX IT and HC IT are given on days 9 and 13.
* Group B patients are randomized to 1 of 4 treatments following recovery and disease assessment:
Arm I:
* Induction 2 (begins no sooner than 16 days after start of COPADM 1): Patients receive COPADM 2 according to the same schedule as in COPADM 1 in Induction 1 except CTX is increased. G-CSF is administered as in the Group A Regimen. Patients receive MTX IT and HC IT on days 2 and 6.
* Consolidation: Patients receive CYM: MTX IV over 3 hours on day 1, oral CF every 6 hours for a maximum of 12 doses beginning 24 hours after the start of MTX, and ARA-C IV over 24 hours on days 2-6. Patients receive TIT: MTX IT on day 2, HC IT on days 2 and 7, and ARA-C IT on day 7.
* Response is assessed upon recovery with resection of residual masses. If histology is negative patients proceed to a second course of CYM. If histology is positive patients proceed to CYVE on arm I of the Group C Regimen.
* Maintenance: Patients receive COPADM 3 as in COPADM 1 in Induction 1, except CTX IV is administered over 30 minutes on days 2 and 3, and MTX IT and HC IT are administered on day 2.
Arm II:
* Induction 2: Patients receive COPADM 2 as in arm I of the Group B Regimen. G-CSF is administered as in the Group A Regimen. MTX IT and HC IT are administered as in Induction 1.
* Consolidation: Patients receive CYM, TIT, and response assessment as in arm I of the Group B Regimen.
* Maintenance: Patients receive no maintenance therapy.
Arm III:
* Induction 2: Patients receive COPADM 2 as in COPADM 1 in Induction 1. G-CSF is administered as in the Group A Regimen. Patients receive MTX IT and HC IT as in Induction 1.
* Consolidation: Patients receive CYM, TIT, and response assessment as in arm I of the Group B Regimen.
* Maintenance: Patients receive COPADM 3 as in arm I of the Group B Regimen. Patients receive MTX IT and HC IT on day 2.
Arm IV:
* Induction 2: Patients receive COPADM 2 as in COPADM 1 in Induction 1. G-CSF is administered as in the Group A Regimen. Patients receive MTX IT and HC IT as in Induction 1.
* Consolidation: Patients receive CYM, TIT, and response assessment as in arm I of the Group B Regimen.
* Maintenance: Patients receive no maintenance therapy.
Group C Regimen (High-Risk Patients)
* Induction: Patients receive COP as in Induction 1 of the Group B Regimen, TIT on days 1, 3, and 5, and oral CF every 12 hours on days 2 and 4. Tumor response is evaluated on day 7 and treatment decisions are made as in Induction 1 of the Group B Regimen. Patients receive COPADM 1 as in COPADM 1 in Induction 1 of the Group B Regimen except HD MTX IV is given over 4 hours on day 1. G-CSF is administered as in the Group A Regimen. TIT is given on days 2, 4, and 6. Patients receive COPADM 2 as in COPADM 2 in arm I of the Group B Regimen, Induction 2 except HD MTX IV is given over 4 hours on day 1. G-CSF is administered as in the Group A Regimen. Patients receive TIT on days 2, 4, and 6.
* Patients are randomized to 1 of 2 treatment arms upon recovery and disease assessment:
Arm I:
* Consolidation: Patients receive CYVE: ARA-C IV on days 1-5, and VP-16 IV over 2 hours on days 2-5. G-CSF is administered as in the Group A Regimen. For patients with CNS disease: MTX IT and HC IT on day 1, 6 hours prior to initiation of ARA-C, HD MTX IV over 4 hours, about day 18, oral CF every 6 hours for a maximum of 12 doses, beginning 24 hours after starting MTX, and TIT prior to beginning CF.
* Response is assessed upon recovery with resection of residual masses. Patients with a complete response receive a second course of CYVE (no HD MTX/CF), beginning 1 week after HD MTX.
* Maintenance (28 days between courses):
* Course 1: Patients receive COPADM as in arm I Maintenance in the Group B Regimen, except HD MTX is administered as in Group C Induction, and TIT is given on day 2 replacing MTX IT and HC.
* Course 2: Patients receive CYVE: ARA-C IV every 12 hours on days 1-5, and VP-16 IV over 90 minutes on days 1-3.
* Course 3: Patients receive COPAD as in Group B Induction 1, except CTX IV is administered over 30 minutes on days 1 and 2.
* Course 4: Patients receive treatment identical to Course 2.
Arm II:
* Consolidation: Patients receive Mini-CYVE: ARA-C IV on days 1-5, and VP-16 IV over 1 hour on days 2-5. G-CSF is administered as in the Group A Regimen. For patients with CNS disease: MTX IT and HC IT as in arm I in the Group C Regimen, and HD MTX, CF, and TIT as in arm I in the Group C Regimen.
* Response is assessed upon recovery with resection of residual masses. Patients with a complete response receive a second course of CYVE (no HD MTX and CF) beginning 1 week after HD MTX.
* Maintenance: Patients receive COPADM and TIT as in arm I of the Group C Regimen in Course 1 for 1 course only.
Patients are followed every 3 months for 6 months, every 6 months for 2.5 years, and then annually thereafter.
PROJECTED ACCRUAL: A total of 900 patients will be accrued for this study within 5 years. Yearly accrual is expected to be 20 Group A patients, 115 Group B patients, and 45 Group C patients.
Conditions
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Leukemia
Lymphoma
Study Design
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Allocation Method
RANDOMIZED
Primary Study Purpose
TREATMENT
Study Groups
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Group A
All resected stage I and Abdominal stage II only. All Group A patients will be treated with two cycles of COPAD and will be followed in a confirmatory study of the current result of nearly 100% cure rate.
Group Type
ACTIVE_COMPARATOR
filgrastim
Intervention Type
BIOLOGICAL
cyclophosphamide
Intervention Type
DRUG
doxorubicin hydrochloride
Intervention Type
DRUG
prednisone
Intervention Type
DRUG
vincristine sulfate
Intervention Type
DRUG
Group B
Non resected stage I \& II, stage III \& st IV (CNS - ve, BM \< 25%). Patients with bulky disease are at risk from metabolic complications secondary to tumor lysis syndrome. Vigorous measures should be taken to minimise the risk of this. Prior to any chemotherapy being administered intravenous hydration fluids should be given run at a rate of 3000 mls/m2/day. Alkalinisation may be necessary Pay close attention to fluid balance and continue hydration fluids after the administration of COP for as long as the risk of tumour lysis persists.
Group Type
ACTIVE_COMPARATOR
filgrastim
Intervention Type
BIOLOGICAL
cyclophosphamide
Intervention Type
DRUG
doxorubicin hydrochloride
Intervention Type
DRUG
methotrexate
Intervention Type
DRUG
prednisolone
Intervention Type
DRUG
prednisone
Intervention Type
DRUG
therapeutic hydrocortisone
Intervention Type
DRUG
vincristine sulfate
Intervention Type
DRUG
Group C
Bone marrow \> 25% but CNS negative Patients with bulky disease are at risk from metabolic complications secondary to tumor lysis syndrome. Vigorous measures should be taken to minimize the risk of this. Intravenous hydration fluids should be given prior to chemotherapy. Alkalinisation may be necessary. Monitor fluid balance and continue hydration fluids after the administration of COP for as long as the risk of tumor lysis persists
Group Type
ACTIVE_COMPARATOR
filgrastim
Intervention Type
BIOLOGICAL
cyclophosphamide
Intervention Type
DRUG
cytarabine
Intervention Type
DRUG
doxorubicin hydrochloride
Intervention Type
DRUG
etoposide
Intervention Type
DRUG
methotrexate
Intervention Type
DRUG
prednisolone
Intervention Type
DRUG
therapeutic hydrocortisone
Intervention Type
DRUG
vincristine sulfate
Intervention Type
DRUG
Interventions
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filgrastim
Intervention Type
BIOLOGICAL
cyclophosphamide
Intervention Type
DRUG
cytarabine
Intervention Type
DRUG
doxorubicin hydrochloride
Intervention Type
DRUG
etoposide
Intervention Type
DRUG
methotrexate
Intervention Type
DRUG
prednisolone
Intervention Type
DRUG
prednisone
Intervention Type
DRUG
therapeutic hydrocortisone
Intervention Type
DRUG
vincristine sulfate
Intervention Type
DRUG
Other Intervention Names
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G-CSF
Neupogen
NSC-614629
NSC-26271
NSC-63878
NSC-123127
VP16
NSC-141540
NSC-740
NSC-10023
NSC-10023
HYDROCORTISONE SODIUM SUCCINATE
NSC-10483
VCR
NSC-675574
Eligibility Criteria
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Inclusion Criteria
DISEASE CHARACTERISTICS:
* One of the following diagnoses:
* Newly diagnosed B-cell non-Hodgkin's lymphoma in Revised European-American Lymphoma (REAL) categories II 9, 10, and 11, i.e.:
* Diffuse large cell
* Burkitt's
* High-grade B-cell, Burkitt's-like
* L3 leukemia with greater than 5% blasts in bone marrow
* No anaplastic large cell Ki1-positive lymphomas
* Immunophenotype and Murphy stage required prior to randomization
PATIENT CHARACTERISTICS:
Age:
* Over 6 months to under 21 years
* Maximum age 18 years in France and the United Kingdom
Other:
* No congenital immunodeficiency
* No prior organ transplantation
* No prior malignancy
* Not HIV positive
* Available for at least 36 months of follow-up
PRIOR CONCURRENT THERAPY:
Biologic therapy:
* Not specified
Chemotherapy:
* No prior chemotherapy
Endocrine therapy:
* Steroids initiated no more than 72 hours prior to entry allowed
* Bone marrow and cerebrospinal fluid examination required prior to steroids
Radiotherapy:
* Emergency radiotherapy initiated no more than 72 hours prior to entry allowed
Surgery:
* Not specified
* One of the following diagnoses:
* Newly diagnosed B-cell non-Hodgkin's lymphoma in Revised European-American Lymphoma (REAL) categories II 9, 10, and 11, i.e.:
* Diffuse large cell
* Burkitt's
* High-grade B-cell, Burkitt's-like
* L3 leukemia with greater than 5% blasts in bone marrow
* No anaplastic large cell Ki1-positive lymphomas
* Immunophenotype and Murphy stage required prior to randomization
PATIENT CHARACTERISTICS:
Age:
* Over 6 months to under 21 years
* Maximum age 18 years in France and the United Kingdom
Other:
* No congenital immunodeficiency
* No prior organ transplantation
* No prior malignancy
* Not HIV positive
* Available for at least 36 months of follow-up
PRIOR CONCURRENT THERAPY:
Biologic therapy:
* Not specified
Chemotherapy:
* No prior chemotherapy
Endocrine therapy:
* Steroids initiated no more than 72 hours prior to entry allowed
* Bone marrow and cerebrospinal fluid examination required prior to steroids
Radiotherapy:
* Emergency radiotherapy initiated no more than 72 hours prior to entry allowed
Surgery:
* Not specified
Maximum Eligible Age
20 Years
Eligible Sex
ALL
Accepts Healthy Volunteers
No
Sponsors
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National Cancer Institute (NCI)
NIH
Sponsor Role
collaborator
Societe Francaise Oncologie Pediatrique
OTHER
Sponsor Role
collaborator
Children's Cancer and Leukaemia Group
OTHER
Sponsor Role
collaborator
Children's Oncology Group
NETWORK
Sponsor Role
lead
Responsible Party
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Responsibility Role
SPONSOR
Principal Investigators
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Mitchell S. Cairo, MD
Role: STUDY_CHAIR
Herbert Irving Comprehensive Cancer Center
Catherine Patte, MD
Role: STUDY_CHAIR
Gustave Roussy, Cancer Campus, Grand Paris
Mary P. Gerrard, MBChB, FRCP, FRCPCH
Role: STUDY_CHAIR
Children's Hospital - Sheffield
Locations
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Institut Gustave Roussy
Villejuif, , France
Site Status
Children's Hospital - Sheffield
Sheffield, England, United Kingdom
Site Status
Countries
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France
United Kingdom
References
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Lones MA, Raphael M, Perkins SL, Wotherspoon A, Auperin A, Terrier-Lacombe MJ, Sposto R, Weston C, Gerrard M, Patte C, Cairo MS, McCarthy K. Mature B-cell lymphoma in children and adolescents: International group pathologist consensus correlates with histology technical quality. J Pediatr Hematol Oncol. 2006 Sep;28(9):568-74. doi: 10.1097/01.mph.0000212980.67114.a5.
Reference Type
BACKGROUND
Cairo MS, Sposto R, Gerrard M, Auperin A, Goldman SC, Harrison L, Pinkerton R, Raphael M, McCarthy K, Perkins SL, Patte C. Advanced stage, increased lactate dehydrogenase, and primary site, but not adolescent age (>/= 15 years), are associated with an increased risk of treatment failure in children and adolescents with mature B-cell non-Hodgkin's lymphoma: results of the FAB LMB 96 study. J Clin Oncol. 2012 Feb 1;30(4):387-93. doi: 10.1200/JCO.2010.33.3369. Epub 2012 Jan 3.
Reference Type
RESULT
Shiramizu B, Goldman S, Kusao I, Agsalda M, Lynch J, Smith L, Harrison L, Morris E, Gross TG, Sanger W, Perkins S, Cairo MS. Minimal disease assessment in the treatment of children and adolescents with intermediate-risk (Stage III/IV) B-cell non-Hodgkin lymphoma: a children's oncology group report. Br J Haematol. 2011 Jun;153(6):758-63. doi: 10.1111/j.1365-2141.2011.08681.x. Epub 2011 Apr 18.
Reference Type
RESULT
Nelson M, Perkins SL, Dave BJ, Coccia PF, Bridge JA, Lyden ER, Heerema NA, Lones MA, Harrison L, Cairo MS, Sanger WG. An increased frequency of 13q deletions detected by fluorescence in situ hybridization and its impact on survival in children and adolescents with Burkitt lymphoma: results from the Children's Oncology Group study CCG-5961. Br J Haematol. 2010 Feb;148(4):600-10. doi: 10.1111/j.1365-2141.2009.07967.x. Epub 2009 Nov 4.
Reference Type
RESULT
Poirel HA, Cairo MS, Heerema NA, Swansbury J, Auperin A, Launay E, Sanger WG, Talley P, Perkins SL, Raphael M, McCarthy K, Sposto R, Gerrard M, Bernheim A, Patte C; FAB/LMB 96 International Study Committee. Specific cytogenetic abnormalities are associated with a significantly inferior outcome in children and adolescents with mature B-cell non-Hodgkin's lymphoma: results of the FAB/LMB 96 international study. Leukemia. 2009 Feb;23(2):323-31. doi: 10.1038/leu.2008.312. Epub 2008 Nov 20.
Reference Type
RESULT
Gerrard M, Cairo MS, Weston C, Auperin A, Pinkerton R, Lambilliote A, Sposto R, McCarthy K, Lacombe MJ, Perkins SL, Patte C; FAB LMB96 International Study Committee. Excellent survival following two courses of COPAD chemotherapy in children and adolescents with resected localized B-cell non-Hodgkin's lymphoma: results of the FAB/LMB 96 international study. Br J Haematol. 2008 Jun;141(6):840-7. doi: 10.1111/j.1365-2141.2008.07144.x. Epub 2008 Mar 26.
Reference Type
RESULT
Miles RR, Raphael M, McCarthy K, Wotherspoon A, Lones MA, Terrier-Lacombe MJ, Patte C, Gerrard M, Auperin A, Sposto R, Davenport V, Cairo MS, Perkins SL; SFOP/LMB96/CCG5961/UKCCSG/NHL 9600 Study Group. Pediatric diffuse large B-cell lymphoma demonstrates a high proliferation index, frequent c-Myc protein expression, and a high incidence of germinal center subtype: Report of the French-American-British (FAB) international study group. Pediatr Blood Cancer. 2008 Sep;51(3):369-74. doi: 10.1002/pbc.21619.
Reference Type
RESULT
Cairo MS, Gerrard M, Sposto R, Auperin A, Pinkerton CR, Michon J, Weston C, Perkins SL, Raphael M, McCarthy K, Patte C; FAB LMB96 International Study Committee. Results of a randomized international study of high-risk central nervous system B non-Hodgkin lymphoma and B acute lymphoblastic leukemia in children and adolescents. Blood. 2007 Apr 1;109(7):2736-43. doi: 10.1182/blood-2006-07-036665.
Reference Type
RESULT
Patte C, Auperin A, Gerrard M, Michon J, Pinkerton R, Sposto R, Weston C, Raphael M, Perkins SL, McCarthy K, Cairo MS; FAB/LMB96 International Study Committee. Results of the randomized international FAB/LMB96 trial for intermediate risk B-cell non-Hodgkin lymphoma in children and adolescents: it is possible to reduce treatment for the early responding patients. Blood. 2007 Apr 1;109(7):2773-80. doi: 10.1182/blood-2006-07-036673.
Reference Type
RESULT
Goldman S, Gerrard M, Sposto R, et al.: Excellent results in children and adolescents with isolated mature B-acute lymphoblastic leukemia (B-ALL) (Burkitt): report from the French-American-British (FAB) international LMB study FAB/LMB96. [Abstract] Blood 106 (11): A-234, 2005.
Reference Type
RESULT
Poirel HA, Heerema NA, Swansbury J, et al.: In pediatric mature B-cell non Hodgkin's lymphoma (NHL), complex karyotype or del(13q) are linked prognostic factors in Burkitt lymphoma (BL) while 8q24/c-myc rearrangement is associated with a strong adverse effect in diffuse large B-cell lymphoma (DLBCL). [Abstract] Blood 106 (11): A-1905, 2005.
Reference Type
RESULT
Lones M, Perkins S, Sposto R, et al.: T-cell-rich large B-cell lymphoma (TCRLBCL) in children and adolescents treated on a B-large cell lymphoma trial: a report from the Children's Cancer Group (CCG) study CCG-5961. [Abstract] Ann Oncol 13(suppl 2): A-137, 45, 2002.
Reference Type
RESULT
Perkins S, Lones M, Sposto R, et al.: B-cell non-Hodgkin lymphoma (NHL) in children and adolescents: central phenotype results from Children's Cancer Group (CCG) study CCG-5961 and implications for future targeted bio-immune therapy (TBIT). [Abstract] Ann Oncol 13(suppl 2): A-136, 45, 2002.
Reference Type
RESULT
Sanger W, Lones M, Perkins S, et al.: Chromosome abnormalities in B-cell non-Hodgkin lymphoma (NHL) of children and adolescents: a report from Children's Cancer Group (CCG)study CCG-5961. [Abstract] Ann Oncol 13(suppl 2): A-138, 45, 2002.
Reference Type
RESULT
Perkins SL, Lones MA, Cairo MS, et al.: B-cell lymphoma/leukemia in children and adolescents: central phenotype results from Children's Cancer Group study (CCG)-5961 and implications for future Targeted Bio-Immune Therapy (TBIT). [Abstract] Proceedings of the American Society of Clinical Oncology 20: A-1520, 2001.
Reference Type
RESULT
Lones MA, Cairo MS, Perkins SL. T-cell-rich large B-cell lymphoma in children and adolescents: a clinicopathologic report of six cases from the Children's Cancer Group Study CCG-5961. Cancer. 2000 May 15;88(10):2378-86. doi: 10.1002/(sici)1097-0142(20000515)88:103.0.co;2-q.
Reference Type
RESULT
Other Identifiers
Review additional registry numbers or institutional identifiers associated with this trial.
COG-C5961
Identifier Type: OTHER
Identifier Source: secondary_id
CCG-5961
Identifier Type: OTHER
Identifier Source: secondary_id
SFOP-LMB-96
Identifier Type: -
Identifier Source: secondary_id
CCLG-NHL-9600
Identifier Type: -
Identifier Source: secondary_id
EU-96048
Identifier Type: -
Identifier Source: secondary_id
CDR0000064702
Identifier Type: OTHER
Identifier Source: secondary_id
5961
Identifier Type: -
Identifier Source: org_study_id
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