A Pilot Study to Evaluate the Co-Infusion of Ex Vivo Expanded Cord Blood Cells With an Unmanipulated Cord Blood Unit in Patients Undergoing Cord Blood Transplant for Hematologic Malignancies
NCT ID: NCT00343798
Last Updated: 2015-02-11
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
PHASE1
Total Enrollment
23 participants
Study Classification
INTERVENTIONAL
Study Start Date
2006-04-30
Brief Summary
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This phase I multicenter feasibility trial is studying the safety and potential efficacy of infusing ex vivo expanded cord blood progenitors with one unmanipulated umbilical cord blood unit for transplantation following conditioning with fludarabine, cyclophosphamide and total body irradiation (TBI), and immunosuppression with cyclosporine and mycophenolate mofetil (MMF) for patients with hematologic malignancies. Chemotherapy, such as fludarabine and cyclophosphamide, and TBI given before an umbilical cord blood transplant stops the growth of leukemia cells and works to prevent the patient's immune system from rejecting the donor's stem cells. The healthy stem cells from the donor's umbilical cord blood help the patient's bone marrow make new red blood cells, white blood cells, and platelets. It may take several weeks for these new blood cells to grow. During that period of time, patients are at increased risk for bleeding and infection. Faster recovery of white blood cells may decrease the number and severity of infections. Studies have shown that counts are more likely to recover more quickly if increased numbers of cord blood cells are given with the transplant. We have developed a way of growing or "expanding" the number of cord blood cells in the lab so that there are more cells available for transplant. We are doing this study to find out whether or not giving these expanded cells along with one unexpanded cord blood unit is safe and if use of expanded cells can decrease the time it takes for white blood cells to recover after transplant. We will study the time it takes for blood counts to recover, which of the two cord blood units makes up the patient's new blood system, and how quickly immune system cells return
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Detailed Description
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PRIMARY OBJECTIVES:
I. Examine the safety and toxicity when ex vivo expanded cord blood cells are co-infused with a second non-human leukocyte antigen (HLA)-identical cord blood graft following myeloablative therapy in patients with hematologic malignancies.
II. Examine the in vivo persistence of the ex vivo expanded cord blood cells. The kinetics and durability of hematopoietic reconstitution (time to engraftment defined as the first of 2 consecutive days in which the absolute neutrophil count \[ANC\] \> 500) will be determined and the relative contribution to engraftment of the expanded cord blood cells and the unmanipulated cord blood cells in early and long-term engraftment will be determined by donor chimerisms.
SECONDARY OBJECTIVES:
I. Estimate the incidence and severity of acute and chronic graft-versus-host disease (GVHD) in patients receiving Notch-expanded cord blood cells.
II. Estimate the incidence of transplant related mortality at day 100.
III. Estimate the incidence of malignant relapse and probabilities of overall and event-free survival at 1 and 2 years post transplant.
IV. Obtain preliminary data on the phenotype and function of immune cells recovering in patients receiving expanded and unmanipulated cord blood grafts.
V. Obtain feasibility data on overnight shipment of ex vivo expanded progenitor cells for infusion in patients are distant sites.
OUTLINE:
MYELOABLATIVE CONDITIONING REGIMEN: Patients receive fludarabine intravenously (IV) over 1 hour on days -8 to -6 and cyclophosphamide IV on days -7 and -6. Patients undergo TBI twice daily (BID) on days -4 to -1.
TRANSPLANTATION : On Day 0, patients undergo double-unit umbilical cord blood transplantation which includes the infusion of one unmanipulated (not expanded) cord blood unit followed 4 hours later by infusion of one ex vivo-expanded cord blood unit.
GRAFT-VERSUS-HOST-DISEASE PROPHYLAXIS: Patients initially receive cyclosporine IV beginning on day -3. Cyclosporine may be given orally when the patient can tolerate oral medications and has a normal gastrointestinal transit time. Cyclosporine is given until day 100, and may taper on day 101 if there is no graft versus host disease. Patients also receive MMF IV on days -3 to 5 and then may receive oral MMF beginning day 6 to 30. MMF is stopped at Day 30 or 7 days after engraftment, whichever day is later, if no acute GVHD.
After completion of study treatment, patients are followed up periodically for 2 years.
I. Examine the safety and toxicity when ex vivo expanded cord blood cells are co-infused with a second non-human leukocyte antigen (HLA)-identical cord blood graft following myeloablative therapy in patients with hematologic malignancies.
II. Examine the in vivo persistence of the ex vivo expanded cord blood cells. The kinetics and durability of hematopoietic reconstitution (time to engraftment defined as the first of 2 consecutive days in which the absolute neutrophil count \[ANC\] \> 500) will be determined and the relative contribution to engraftment of the expanded cord blood cells and the unmanipulated cord blood cells in early and long-term engraftment will be determined by donor chimerisms.
SECONDARY OBJECTIVES:
I. Estimate the incidence and severity of acute and chronic graft-versus-host disease (GVHD) in patients receiving Notch-expanded cord blood cells.
II. Estimate the incidence of transplant related mortality at day 100.
III. Estimate the incidence of malignant relapse and probabilities of overall and event-free survival at 1 and 2 years post transplant.
IV. Obtain preliminary data on the phenotype and function of immune cells recovering in patients receiving expanded and unmanipulated cord blood grafts.
V. Obtain feasibility data on overnight shipment of ex vivo expanded progenitor cells for infusion in patients are distant sites.
OUTLINE:
MYELOABLATIVE CONDITIONING REGIMEN: Patients receive fludarabine intravenously (IV) over 1 hour on days -8 to -6 and cyclophosphamide IV on days -7 and -6. Patients undergo TBI twice daily (BID) on days -4 to -1.
TRANSPLANTATION : On Day 0, patients undergo double-unit umbilical cord blood transplantation which includes the infusion of one unmanipulated (not expanded) cord blood unit followed 4 hours later by infusion of one ex vivo-expanded cord blood unit.
GRAFT-VERSUS-HOST-DISEASE PROPHYLAXIS: Patients initially receive cyclosporine IV beginning on day -3. Cyclosporine may be given orally when the patient can tolerate oral medications and has a normal gastrointestinal transit time. Cyclosporine is given until day 100, and may taper on day 101 if there is no graft versus host disease. Patients also receive MMF IV on days -3 to 5 and then may receive oral MMF beginning day 6 to 30. MMF is stopped at Day 30 or 7 days after engraftment, whichever day is later, if no acute GVHD.
After completion of study treatment, patients are followed up periodically for 2 years.
Conditions
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Accelerated Phase Chronic Myelogenous Leukemia
Acute Myeloid Leukemia With Multilineage Dysplasia Following Myelodysplastic Syndrome
Adult Acute Lymphoblastic Leukemia in Remission
Adult Acute Myeloid Leukemia in Remission
Adult Acute Myeloid Leukemia With 11q23 (MLL) Abnormalities
Adult Acute Myeloid Leukemia With Del(5q)
Adult Acute Myeloid Leukemia With Inv(16)(p13;q22)
Adult Acute Myeloid Leukemia With t(15;17)(q22;q12)
Adult Acute Myeloid Leukemia With t(16;16)(p13;q22)
Adult Acute Myeloid Leukemia With t(8;21)(q22;q22)
Adult Nasal Type Extranodal NK/T-cell Lymphoma
Anaplastic Large Cell Lymphoma
Childhood Acute Lymphoblastic Leukemia in Remission
Childhood Acute Myeloid Leukemia in Remission
Childhood Burkitt Lymphoma
Childhood Chronic Myelogenous Leukemia
Childhood Diffuse Large Cell Lymphoma
Childhood Immunoblastic Large Cell Lymphoma
Childhood Myelodysplastic Syndromes
Childhood Nasal Type Extranodal NK/T-cell Lymphoma
Chronic Phase Chronic Myelogenous Leukemia
Contiguous Stage II Adult Burkitt Lymphoma
Contiguous Stage II Adult Diffuse Large Cell Lymphoma
Contiguous Stage II Adult Diffuse Mixed Cell Lymphoma
Contiguous Stage II Adult Immunoblastic Large Cell Lymphoma
Contiguous Stage II Adult Lymphoblastic Lymphoma
Contiguous Stage II Grade 3 Follicular Lymphoma
Contiguous Stage II Mantle Cell Lymphoma
de Novo Myelodysplastic Syndromes
Extranodal Marginal Zone B-cell Lymphoma of Mucosa-associated Lymphoid Tissue
Nodal Marginal Zone B-cell Lymphoma
Noncontiguous Stage II Adult Burkitt Lymphoma
Noncontiguous Stage II Adult Diffuse Large Cell Lymphoma
Noncontiguous Stage II Adult Diffuse Mixed Cell Lymphoma
Noncontiguous Stage II Adult Immunoblastic Large Cell Lymphoma
Noncontiguous Stage II Adult Lymphoblastic Lymphoma
Noncontiguous Stage II Grade 3 Follicular Lymphoma
Noncontiguous Stage II Mantle Cell Lymphoma
Previously Treated Myelodysplastic Syndromes
Prolymphocytic Leukemia
Recurrent Adult Burkitt Lymphoma
Recurrent Adult Diffuse Large Cell Lymphoma
Recurrent Adult Diffuse Mixed Cell Lymphoma
Recurrent Adult Grade III Lymphomatoid Granulomatosis
Recurrent Adult Immunoblastic Large Cell Lymphoma
Recurrent Adult Lymphoblastic Lymphoma
Recurrent Childhood Anaplastic Large Cell Lymphoma
Recurrent Childhood Grade III Lymphomatoid Granulomatosis
Recurrent Childhood Large Cell Lymphoma
Recurrent Childhood Lymphoblastic Lymphoma
Recurrent Grade 1 Follicular Lymphoma
Recurrent Grade 2 Follicular Lymphoma
Recurrent Grade 3 Follicular Lymphoma
Recurrent Mantle Cell Lymphoma
Recurrent Marginal Zone Lymphoma
Recurrent Small Lymphocytic Lymphoma
Refractory Anemia
Refractory Anemia With Excess Blasts
Refractory Anemia With Excess Blasts in Transformation
Refractory Chronic Lymphocytic Leukemia
Refractory Multiple Myeloma
Secondary Acute Myeloid Leukemia
Secondary Myelodysplastic Syndromes
Splenic Marginal Zone Lymphoma
Stage I Adult Burkitt Lymphoma
Stage I Adult Diffuse Large Cell Lymphoma
Stage I Adult Diffuse Mixed Cell Lymphoma
Stage I Adult Immunoblastic Large Cell Lymphoma
Stage I Adult Lymphoblastic Lymphoma
Stage I Childhood Lymphoblastic Lymphoma
Stage I Grade 3 Follicular Lymphoma
Stage I Mantle Cell Lymphoma
Stage II Childhood Lymphoblastic Lymphoma
Stage III Adult Burkitt Lymphoma
Stage III Adult Diffuse Large Cell Lymphoma
Stage III Adult Diffuse Mixed Cell Lymphoma
Stage III Adult Immunoblastic Large Cell Lymphoma
Stage III Adult Lymphoblastic Lymphoma
Stage III Childhood Lymphoblastic Lymphoma
Stage III Grade 3 Follicular Lymphoma
Stage III Mantle Cell Lymphoma
Stage IV Adult Burkitt Lymphoma
Stage IV Adult Diffuse Large Cell Lymphoma
Stage IV Adult Diffuse Mixed Cell Lymphoma
Stage IV Adult Immunoblastic Large Cell Lymphoma
Stage IV Adult Lymphoblastic Lymphoma
Stage IV Childhood Lymphoblastic Lymphoma
Stage IV Grade 3 Follicular Lymphoma
Stage IV Mantle Cell Lymphoma
Study Design
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Allocation Method
NA
Intervention Model
SINGLE_GROUP
Primary Study Purpose
TREATMENT
Blinding Strategy
NONE
Study Groups
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Treatment (umbilical cord blood transplant)
MYELOABLATIVE CONDITIONING REGIMEN: Patients receive fludarabine phosphate IV over 1 hour on days -8 to -6 and cyclophosphamide IV on days -7 and -6. Patients undergo TBI BID on days -4 to -1.
TRANSPLANTATION : Patients undergo double-unit umbilical cord blood transplantation comprising unmanipulated umbilical cord blood unit IV over 20-30 minutes, and 4-6 hours later patients receive ex vivo-expanded umbilical cord blood cells IV over 30 minutes on day 0.
GRAFT-VERSUS-HOST-DISEASE PROPHYLAXIS: Patients receive cyclosporine IV every 8 or 12 hours on days -3 to 100, followed by a taper to at least day 180. Patients also receive MMF IV every 8 hours on days -3 to 5 and then PO, if tolerated, on days 6-30.
Group Type
EXPERIMENTAL
cyclophosphamide
Intervention Type
DRUG
Given IV
fludarabine phosphate
Intervention Type
DRUG
Given IV
cyclosporine
Intervention Type
DRUG
Given IV
mycophenolate mofetil
Intervention Type
DRUG
Given IV or PO
ex-vivo umbilical cord blood expansion
Intervention Type
OTHER
Undergo double-unit umbilical cord blood transplantation
double-unit umbilical cord blood transplantation
Intervention Type
PROCEDURE
Undergo double-unit umbilical cord blood transplantation
biopsy
Intervention Type
PROCEDURE
Optional correlative studies
immunologic technique
Intervention Type
OTHER
Correlative studies
diagnostic laboratory biomarker analysis
Intervention Type
OTHER
Correlative studies
Interventions
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cyclophosphamide
Given IV
Intervention Type
DRUG
fludarabine phosphate
Given IV
Intervention Type
DRUG
cyclosporine
Given IV
Intervention Type
DRUG
mycophenolate mofetil
Given IV or PO
Intervention Type
DRUG
ex-vivo umbilical cord blood expansion
Undergo double-unit umbilical cord blood transplantation
Intervention Type
OTHER
double-unit umbilical cord blood transplantation
Undergo double-unit umbilical cord blood transplantation
Intervention Type
PROCEDURE
biopsy
Optional correlative studies
Intervention Type
PROCEDURE
immunologic technique
Correlative studies
Intervention Type
OTHER
diagnostic laboratory biomarker analysis
Correlative studies
Intervention Type
OTHER
Other Intervention Names
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CPM
CTX
Cytoxan
Endoxan
Endoxana
2-F-ara-AMP
Beneflur
Fludara
ciclosporin
cyclosporin
cyclosporin A
CYSP
Sandimmune
Cellcept
MMF
biopsies
immunological laboratory methods
laboratory methods, immunological
Eligibility Criteria
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Inclusion Criteria
* Patient has no existing 0-1 HLA-A, B, C, DRB1 and DQB1 matched related donor
* Acute Myeloid Leukemia:
* High risk first complete remission (CR1) as evidenced by preceding myelodysplastic syndromes (MDS), high risk cytogenetics (for example, monosomy 5 or 7, or HR as defined by referring institution treatment protocol), \>= 2 cycles to obtain complete remission (CR), erythroblastic or megakaryocytic leukemia; \>= second complete remission (CR2);
* All patients must be in CR as defined by hematologic recovery and \< 5% blasts by morphology within the bone marrow and a cellularity of \>= 15%;
* Patients in which adequate marrow/biopsy specimens cannot be obtained to determine remission status by morphologic assessment, but have fulfilled criteria of remission by flow cytometry (\< 5% blasts) and, recovery of peripheral blood counts with no circulating blasts, may still be eligible; reasonable attempts must be made to obtain an adequate specimen for morphologic assessment, including possible repeat procedures
* Acute lymphoblastic leukemia:
* High risk CR1 (for example, but not limited to: t(9;22), t(1;19), t(4;11) or other mixed-lineage leukemia (MLL) rearrangements, hypodiploid);
* \> 1 cycle to obtain CR;
* \>= CR2;
* All patients must be in CR as defined by hematologic recovery and \< 5% blasts by morphology within the bone marrow and a cellularity of \>= 15%;
* Patients in which adequate marrow/biopsy specimens can not be obtained to determine remission status by morphologic assessment, but have fulfilled criteria of remission by flow cytometry (\< 5% blasts) and, recovery of peripheral blood counts with no circulating blasts, may still be eligible; reasonable attempts must be made to obtain an adequate specimen for morphologic assessment, including possible repeat procedures
* Chronic Myelogenous Leukemia:
* Patients in blast crisis (BC) must receive therapy and must achieve accelerated phase (AP)/chronic phase (CP) in order to be eligible (patients who remain in BC are not eligible);
* If in first chronic phase, patient must have failed or be intolerant to imatinib mesylate
* Myelodysplasia (MDS):
* International Prognostic Scoring System (IPSS) Int-2 or high risk (Refractory anemia with excess blasts \[RAEB\], refractory anemia with excess blasts in transformation \[RAEBt\]) or refractory anemia with severe pancytopenia or high risk cytogenetics;
* Blasts must be \< 10% morphologically in representative bone marrow aspirate (obtained \< 2 weeks from enrollment)
* Lymphoblastic lymphoma, Burkitt's lymphoma, and other high-grade non-Hodgkin lymphoma (NHL) after initial therapy if stage III/IV in first partial remission (PR1) or after progression if stage I/II \< 1 year; Stage III/IV patients are eligible after progression in complete response (CR)/partial response (PR)
* Chronic lymphocytic leukemia/small lymphocytic lymphoma (CLL/SLL), marginal zone B-cell lymphoma, lymphoplasmacytic lymphoma or follicular lymphoma that have progressed after at least two different prior therapies; patients with bulky disease (nodal mass greater than 5 cm) should be considered for debulking chemotherapy before transplant (these patients must be presented at Patient Care Conference \[PCC\] prior to enrollment given potential competing eligibility on autotransplant protocols)
* Mantle-cell lymphoma, prolymphocytic leukemia: Eligible after initial therapy in \>= CR1 or \>= PR1
* Large cell NHL \> CR2/ \> PR2:
* Patients in CR2/PR2 with initial short remission (\< 6 months) are eligible;
* These patients must be presented at PCC prior to enrollment given potential competing eligibility on autotransplant protocols
* Multiple myeloma beyond PR2: Patients with chromosome 13 abnormalities, first response lasting less than 6 months, or beta-2 microglobulin \> 3 mg/L, may be considered for this protocol after initial therapy
* Serum creatinine =\< 2.0 mg/dL (adults) and creatinine clearance \> 60 ml/min (pediatrics)
* Patients with clinical or laboratory evidence of liver disease will be evaluated for the cause of liver disease, its clinical severity in terms of liver function, histology, and the degree of portal hypertension; patients with fulminant liver failure, cirrhosis with evidence of portal hypertension or bridging fibrosis, alcoholic hepatitis, esophageal varices, a history of bleeding esophageal varices, hepatic encephalopathy, or correctable hepatic synthetic dysfunction evidenced by prolongation of the prothrombin time, ascites related to portal hypertension, bacterial or fungal abscess, biliary obstruction, chronic viral hepatitis with total serum bilirubin \> 3 mg/dL and symptomatic biliary disease will be excluded
* Diffusing capacity of the lung for carbon monoxide corrected (DLCOcorr) \> 50% normal
* Left ventricular ejection fraction \>= 45% or shortening fraction \> 26%
* Karnofsky score \>= 70% (adults) or Lansky score \>= 50% (pediatrics)
* Acute Myeloid Leukemia:
* High risk first complete remission (CR1) as evidenced by preceding myelodysplastic syndromes (MDS), high risk cytogenetics (for example, monosomy 5 or 7, or HR as defined by referring institution treatment protocol), \>= 2 cycles to obtain complete remission (CR), erythroblastic or megakaryocytic leukemia; \>= second complete remission (CR2);
* All patients must be in CR as defined by hematologic recovery and \< 5% blasts by morphology within the bone marrow and a cellularity of \>= 15%;
* Patients in which adequate marrow/biopsy specimens cannot be obtained to determine remission status by morphologic assessment, but have fulfilled criteria of remission by flow cytometry (\< 5% blasts) and, recovery of peripheral blood counts with no circulating blasts, may still be eligible; reasonable attempts must be made to obtain an adequate specimen for morphologic assessment, including possible repeat procedures
* Acute lymphoblastic leukemia:
* High risk CR1 (for example, but not limited to: t(9;22), t(1;19), t(4;11) or other mixed-lineage leukemia (MLL) rearrangements, hypodiploid);
* \> 1 cycle to obtain CR;
* \>= CR2;
* All patients must be in CR as defined by hematologic recovery and \< 5% blasts by morphology within the bone marrow and a cellularity of \>= 15%;
* Patients in which adequate marrow/biopsy specimens can not be obtained to determine remission status by morphologic assessment, but have fulfilled criteria of remission by flow cytometry (\< 5% blasts) and, recovery of peripheral blood counts with no circulating blasts, may still be eligible; reasonable attempts must be made to obtain an adequate specimen for morphologic assessment, including possible repeat procedures
* Chronic Myelogenous Leukemia:
* Patients in blast crisis (BC) must receive therapy and must achieve accelerated phase (AP)/chronic phase (CP) in order to be eligible (patients who remain in BC are not eligible);
* If in first chronic phase, patient must have failed or be intolerant to imatinib mesylate
* Myelodysplasia (MDS):
* International Prognostic Scoring System (IPSS) Int-2 or high risk (Refractory anemia with excess blasts \[RAEB\], refractory anemia with excess blasts in transformation \[RAEBt\]) or refractory anemia with severe pancytopenia or high risk cytogenetics;
* Blasts must be \< 10% morphologically in representative bone marrow aspirate (obtained \< 2 weeks from enrollment)
* Lymphoblastic lymphoma, Burkitt's lymphoma, and other high-grade non-Hodgkin lymphoma (NHL) after initial therapy if stage III/IV in first partial remission (PR1) or after progression if stage I/II \< 1 year; Stage III/IV patients are eligible after progression in complete response (CR)/partial response (PR)
* Chronic lymphocytic leukemia/small lymphocytic lymphoma (CLL/SLL), marginal zone B-cell lymphoma, lymphoplasmacytic lymphoma or follicular lymphoma that have progressed after at least two different prior therapies; patients with bulky disease (nodal mass greater than 5 cm) should be considered for debulking chemotherapy before transplant (these patients must be presented at Patient Care Conference \[PCC\] prior to enrollment given potential competing eligibility on autotransplant protocols)
* Mantle-cell lymphoma, prolymphocytic leukemia: Eligible after initial therapy in \>= CR1 or \>= PR1
* Large cell NHL \> CR2/ \> PR2:
* Patients in CR2/PR2 with initial short remission (\< 6 months) are eligible;
* These patients must be presented at PCC prior to enrollment given potential competing eligibility on autotransplant protocols
* Multiple myeloma beyond PR2: Patients with chromosome 13 abnormalities, first response lasting less than 6 months, or beta-2 microglobulin \> 3 mg/L, may be considered for this protocol after initial therapy
* Serum creatinine =\< 2.0 mg/dL (adults) and creatinine clearance \> 60 ml/min (pediatrics)
* Patients with clinical or laboratory evidence of liver disease will be evaluated for the cause of liver disease, its clinical severity in terms of liver function, histology, and the degree of portal hypertension; patients with fulminant liver failure, cirrhosis with evidence of portal hypertension or bridging fibrosis, alcoholic hepatitis, esophageal varices, a history of bleeding esophageal varices, hepatic encephalopathy, or correctable hepatic synthetic dysfunction evidenced by prolongation of the prothrombin time, ascites related to portal hypertension, bacterial or fungal abscess, biliary obstruction, chronic viral hepatitis with total serum bilirubin \> 3 mg/dL and symptomatic biliary disease will be excluded
* Diffusing capacity of the lung for carbon monoxide corrected (DLCOcorr) \> 50% normal
* Left ventricular ejection fraction \>= 45% or shortening fraction \> 26%
* Karnofsky score \>= 70% (adults) or Lansky score \>= 50% (pediatrics)
Exclusion Criteria
* Acute leukemia in relapse (\>= 5% marrow blasts by morphology)
* Active central nervous system (CNS) leukemia involvement at the time of study enrollment (cerebrospinal fluid with \> 5 white blood cells (WBC)/mm\^3 AND malignant cells on cytospin)
* Chemotherapy refractory large cell lymphoma and high grade NHL (progressive disease after \> 2 salvage regimens)
* Female patients who are pregnant or breastfeeding
* Karnofsky performance status \< 70% (adults) or Lanksy score \< 50% (pediatrics)
* Prior autologous or allogeneic stem cell transplant with myeloablative preparative regimen (If =\< 18 years old, prior myeloablative transplant within the last 6 months)
* Uncontrolled viral, or bacterial infection at the time of study enrollment
* Active or recent (prior 6 months) invasive fungal infection without ID consult and approval
* Seropositive for human immunodeficiency virus (HIV)
* Consenting 5 of 6 or 6 of 6 HLA-matched related donor available
* Unable to provide informed consent
* Use of any other experimental drug within 28 days of baseline
* Active central nervous system (CNS) leukemia involvement at the time of study enrollment (cerebrospinal fluid with \> 5 white blood cells (WBC)/mm\^3 AND malignant cells on cytospin)
* Chemotherapy refractory large cell lymphoma and high grade NHL (progressive disease after \> 2 salvage regimens)
* Female patients who are pregnant or breastfeeding
* Karnofsky performance status \< 70% (adults) or Lanksy score \< 50% (pediatrics)
* Prior autologous or allogeneic stem cell transplant with myeloablative preparative regimen (If =\< 18 years old, prior myeloablative transplant within the last 6 months)
* Uncontrolled viral, or bacterial infection at the time of study enrollment
* Active or recent (prior 6 months) invasive fungal infection without ID consult and approval
* Seropositive for human immunodeficiency virus (HIV)
* Consenting 5 of 6 or 6 of 6 HLA-matched related donor available
* Unable to provide informed consent
* Use of any other experimental drug within 28 days of baseline
Minimum Eligible Age
6 Months
Maximum Eligible Age
45 Years
Eligible Sex
ALL
Accepts Healthy Volunteers
No
Sponsors
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National Heart, Lung, and Blood Institute (NHLBI)
NIH
Sponsor Role
collaborator
National Cancer Institute (NCI)
NIH
Sponsor Role
collaborator
Damon Runyon Cancer Research Foundation
OTHER
Sponsor Role
collaborator
Fred Hutchinson Cancer Center
OTHER
Sponsor Role
lead
Responsible Party
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Responsibility Role
SPONSOR
Principal Investigators
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Colleen Delaney
Role: PRINCIPAL_INVESTIGATOR
Fred Hutchinson Cancer Research Center/University of Washington Cancer Consortium
Locations
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City of Hope Medical Center
Duarte, California, United States
Site Status
University of Colorado Cancer Center - Anschutz Cancer Pavilion
Aurora, Colorado, United States
Site Status
University of Colorado
Denver, Colorado, United States
Site Status
Fred Hutchinson Cancer Research Center/University of Washington Cancer Consortium
Seattle, Washington, United States
Site Status
Countries
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United States
Other Identifiers
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NCI-2010-00236
Identifier Type: REGISTRY
Identifier Source: secondary_id
2044.00
Identifier Type: -
Identifier Source: org_study_id
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RECRUITING
NA
Low-Dose Fludarabine, Busulfan, and Anti-Thymocyte Globulin Followed By Donor Umbilical Cord Blood Transplant in Treating Patients With Advanced Hematologic Cancer
NCT00301951
COMPLETED
PHASE1
Donor Umbilical Cord Blood Transplant After Fludarabine Phosphate, Cyclophosphamide, and Total-Body Irradiation in Treating Patients With High-Risk Hematologic Cancer
NCT00963872
TERMINATED
PHASE1/PHASE2
Donor Umbilical Cord Blood Transplant in Treating Patients With Advanced Hematologic Cancer
NCT00304018
COMPLETED
PHASE1
Fludarabine Phosphate, Low-Dose Total Body Irradiation, and Donor Stem Cell Transplant in Treating Patients With Hematologic Malignancies or Kidney Cancer
NCT00005799
COMPLETED
NA
T-Regulatory Cell Infusion Post Umbilical Cord Blood Transplant in Patients With Advanced Hematologic Cancer
NCT00602693
COMPLETED
PHASE1
Non-Myeloablative Conditioning for Unrelated Donor Umbilical Cord Blood Transplant
NCT00305682
COMPLETED
PHASE2
Umbilical Cord Blood Stem Cell Transplant in Treating Patients With Hematologic Cancer or Other Disease
NCT00423826
NO_LONGER_AVAILABLE
Single vs Double Umbilical Cord Blood Transplants in Children With High Risk Leukemia and Myelodysplasia (BMT CTN 0501)
NCT00412360
COMPLETED
PHASE3
Reduced Intensity Donor Peripheral Blood Stem Cell Transplant in Treating Patients With De Novo or Secondary Acute Myeloid Leukemia in Remission
NCT00045435
COMPLETED
PHASE2
Donor Umbilical Cord Blood Natural Killer Cells, Aldesleukin and Umbilical Cord Blood Transplant in Patients With Refractory Hematologic Cancers.
NCT00354172
TERMINATED
PHASE2
Fludarabine Phosphate and Total Body Irradiation Followed by a Donor Peripheral Stem Cell Transplant in Treating Patients With Myelodysplastic Syndromes or Myeloproliferative Disorders
NCT00397813
COMPLETED
PHASE2
Donor Umbilical Cord Blood Transplant in Treating Patients With Advanced Hematological Cancer or Other Disease
NCT00719849
TERMINATED
PHASE2