Fludarabine, Total-Body Irradiation, and Donor Stem Cell Transplant Followed By Cyclosporine and Mycophenolate Mofetil in Treating Patients With Chronic Myelogenous Leukemia
NCT ID: NCT00119340
Last Updated: 2010-09-21
Study Results
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Basic Information
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COMPLETED
PHASE1/PHASE2
75 participants
INTERVENTIONAL
2005-04-30
2007-11-30
Brief Summary
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PURPOSE: This phase I/II trial is studying the side effects and best dose of fludarabine, total-body irradiation, and donor stem cell transplant followed by cyclosporine and mycophenolate mofetil and to see how well they work in treating patients with chronic myelogenous leukemia.
Detailed Description
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Primary
* Determine whether increasing the intensity of a nonmyeloablative conditioning regimen comprising fludarabine and total body irradiation allows achievement of a donor T-cell chimerism level of \> 40% on day 28 post-transplantation in 90% or more of patients with chronic myelogenous leukemia undergoing allogeneic peripheral blood stem cell transplantation and immunosuppression comprising cyclosporine and mycophenolate mofetil.
* Determine the feasibility of reducing the day 84 graft rejection rate/graft failure to \< 10% in patients treated with this regimen.
* Determine the feasibility of maintaining the incidence of grade 4 acute graft-versus-host disease at \< 10% in patients treated with this regimen.
* Determine the feasibility of maintaining the day 200 nonrelapse mortality rate at \< 15% in patients treated with this regimen.
Secondary
* Determine the rate of complete cytogenetic remission in patients treated with this regimen.
* Determine the probability of actuarial disease-free survival of patients treated with this regimen.
* Determine the pharmacokinetics of mycophenolate mofetil and fludarabine in these patients.
OUTLINE: This is a multicenter, dose-escalation study of fludarabine and total-body irradiation (TBI).
* Nonmyeloablative conditioning regimen: Patients receive fludarabine IV on days -4 to -2 OR days -6 to -2. Patients undergo TBI on day 0.
* Allogeneic peripheral blood stem cell transplantation (PBSCT): After the completion of TBI, patients undergo allogeneic PBSCT on day 0.
* Immunosuppression: Patients receive oral cyclosporine twice daily on days -3 to 100 followed by a taper to day 177 in the absence of graft-versus-host disease (GVHD). Beginning within 4-6 hours after the completion of PBSCT, patients receive oral mycophenolate mofetil 2-3 times daily on days 0-40 followed by a taper to day 96 in the absence of GVHD.
Cohorts of 5-25 patients receive cumulative doses of fludarabine and escalating doses of TBI until 2 of 5, 3 of 10-15, 4 of 20, or 5 of 25 patients experience a day 28 post-transplant T-cell chimerism level ≤ 40% and/or a day 84 post-transplant graft rejection rate of \> 10%.
After completion of study transplantation, patients are followed 3 times weekly for 3 months, at 6, 12, and 18 months, annually for 5 years, and then periodically thereafter.
PROJECTED ACCRUAL: A total of 5-75 patients will be accrued for this study.
Conditions
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Study Design
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TREATMENT
Interventions
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cyclosporine
fludarabine phosphate
mycophenolate mofetil
peripheral blood stem cell transplantation
radiation therapy
Eligibility Criteria
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Inclusion Criteria
* Diagnosis of chronic myelogenous leukemia (CML), meeting 1 of the following criteria:
* First or second chronic phase
* Philadelphia chromosome-positive (Ph+) disease by cytogenetics or fluorescent in situ hybridization (FISH)
* First accelerated phase, meeting any of the following criteria:
* More than 10% but \< 30% myeloblasts and promyelocytes in bone marrow or peripheral blood
* Any additional clonal cytogenetic abnormalities
* Increasing splenomegally
* Extramedullary tumor
* WBC, platelet count, or hematocrit pertubations not controlled by therapy with hydroxyurea, interferon, or imatininb mesylate
* Persistent unexplained fever or bone pain
* Less than 5% blasts in marrow at time of transplant
* No blast crisis
* No other curative therapy exists
* Received prior imatinib mesylate AND meets ≥ 1 of the following criteria:
* Hematologic evidence of disease progression
* Lack of complete hematologic response after 3 months of treatment with imatinib mesylate
* Cytogenetic evidence of disease progression, defined as an increase in Ph+ cells or BCR/ABL-positive (BCR/ABL+) cells of \> 25%
* Lack of complete cytogenetic remission (no Ph+ cells by cytogenetic analysis or BCR/ABL+ cells by FISH) after 1 year of treatment with imatinib mesylate
* At least 65% Ph+ cells by cytogenetic analysis or BCR/ABL+ cells by FISH after 6 months of treatment with imatinib mesylate
* Less than 3-log reduction in BCR/ABL mRNA levels by quantitative polymerase chain reaction (Q-PCR) compared to a standard baseline level after 1 year of treatment with imatinib mesylate
* Molecular evidence of disease progression, defined as \> 1 log increase in BCR/ABL mRNA levels by Q-PCR, detected in 2 samples
* Experienced adverse events with imatinib mesylate treatment that would preclude further administration of the drug
* Patient refused further treatment with imatinib mesylate despite lack of disease progression
* Refused conventional myeloablative allogeneic stem cell transplantation OR at high risk for regimen-related toxicity due to pre-existing medical conditions (for patients \< 50 years of age)
* Unrelated donor available
* Matched at HLA-A, -B, -C, -DRB1, and -DQB1 by high-resolution typing
* A single allele\* disparity for HLA-A, -B, or -C allowed
* Negative anti-donor cytotoxic crossmatch
* Not a marrow donor NOTE: \*Patient and donor pairs homozygous at a mismatched allele (e.g., the patient is A\*0101 and the donor is A\*0201) are considered a two-allele mismatch and are not allowed
* No CNS involvement with disease that is refractory to intrathecal chemotherapy
PATIENT CHARACTERISTICS:
Age
* Any age
Performance status
* Karnofsky 70-100%
* Lanksy 50-100% (for pediatric patients)
Life expectancy
* Not specified
Hematopoietic
* See Disease Characteristics
Hepatic
* No fulminant liver failure
* No cirrhosis of the liver with evidence of portal hypertension
* No alcoholic hepatitis
* No esophageal varices
* No history of bleeding esophageal varices
* No hepatic encephalopathy
* No uncorrectable hepatic synthetic dysfunction evidenced by prolongation of PT
* No ascites related to portal hypertension
* No bacterial or fungal liver abscess
* No biliary obstruction
* No chronic viral hepatitis AND bilirubin \> 3 mg/dL
* No symptomatic biliary disease
Renal
* Not specified
Cardiovascular
* Ejection fraction ≥ 40%
* No cardiac failure requiring therapy
* No poorly controlled hypertension (i.e., blood pressure ≥ 150/90 mm Hg despite standard medication)
Pulmonary
* DLCO ≥ 35% (corrected)
* No requirement for supplementary continuous oxygen
* Pulmonary nodules allowed at the discretion of the principal investigator
Immunologic
* HIV negative
* No uncontrolled systemic infection
* No fungal infection with radiological progression after treatment with amphotericin B or active triazole for \> 1 month
Other
* Not pregnant or nursing
* Fertile patients must use effective contraception during and for 12 months after completion of study treatment
* No other active malignancy except nonmelanoma skin cancer
* No prior localized malignancy at high risk (≥ 20%) of recurrence
PRIOR CONCURRENT THERAPY:
Biologic therapy
* See Disease Characteristics
* See Chemotherapy
Chemotherapy
* See Disease Characteristics
* More than 3 weeks since prior cytotoxic chemotherapy
* Imatinib mesylate and interferon are not considered cytotoxic chemotherapy
Endocrine therapy
* Not specified
Radiotherapy
* Not specified
Surgery
* Not specified
ALL
No
Sponsors
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National Cancer Institute (NCI)
NIH
Fred Hutchinson Cancer Center
OTHER
Responsible Party
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Fred Hutchinson Cancer Research Center
Principal Investigators
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Brenda Sandmaier, MD
Role: PRINCIPAL_INVESTIGATOR
Fred Hutchinson Cancer Center
Locations
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Veterans Affairs Medical Center - Seattle
Seattle, Washington, United States
Seattle Cancer Care Alliance
Seattle, Washington, United States
Fred Hutchinson Cancer Research Center
Seattle, Washington, United States
Countries
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Other Identifiers
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FHCRC-1939.00
Identifier Type: -
Identifier Source: secondary_id
CDR0000432959
Identifier Type: REGISTRY
Identifier Source: secondary_id
1939.00
Identifier Type: -
Identifier Source: org_study_id