A Trial Comparing Unrelated Donor BMT With IST for Pediatric and Young Adult Patients With Severe Aplastic Anemia (TransIT, BMT CTN 2202)

Study Description

Brief Summary

Severe Aplastic Anemia (SAA) is a rare condition in which the body stops producing enough new blood cells. SAA can be cured with immune suppressive therapy or a bone marrow transplant. Regular treatment for patients with aplastic anemia who have a matched sibling (brother or sister), or family donor is a bone marrow transplant. Patients without a matched family donor normally are treated with immune suppressive therapy (IST). Match unrelated donor (URD) bone marrow transplant (BMT) is used as a secondary treatment in patients who did not get better with IST, had their disease come back, or a new worse disease replaced it (like leukemia).

This trial will compare time from randomization to failure of treatment or death from any cause of IST versus URD BMT when used as initial therapy to treat SAA.

The trial will also assess whether health-related quality of life and early markers of fertility differ between those randomized to URD BMT or IST, as well as assess the presence of marrow failure-related genes and presence of gene mutations associated with MDS or leukemia and the change in gene signatures after treatment in both study arms.

This study treatment does not include any investigational drugs. The medicines and procedures in this study are standard for treatment of SAA.

Detailed Description

This study is a multi-center randomized phase III trial to compare the failure free survival between those randomized to IST vs 9-10/10 HLA matched URD BMT. The study will also address patient-reported outcomes and gonadal function in each arm and explore critical biological correlates including assessing germline genetic mutations associated with pediatric SAA that may lead to a predisposition to the disease and the risk of development of clonal hematopoiesis following IST vs BMT in pediatric and young adult SAA.

This clinical trial will randomize 234 children/AYA over 3.3-4.7 years at a 1:1 ratio between initial treatment with immune suppression therapy (IST) with horse ATG (hATG)/cyclosporine (CsA) versus well- matched (9-10/10 allele) unrelated donor (URD) bone marrow transplantation (BMT) using a regimen of rabbit ATG (rATG)/fludarabine/cyclophosphamide and 200 cGy TBI. Duration of subject participation for all study procedures in this study will be up to 2 years after treatment; a single later timepoint between 3 and 5 years will be collected to follow patients for specific protocol defined late effects and survival.

Study Design

Outcome Measures

Primary Outcome Measures

1. The primary endpoint of this trial is time from randomization to treatment failure or death from any cause. [Randomization to 2 years post-randomization]

   The median time to failure or death will be compared on the two arms using the log-rank test. Failure of IST is defined as initiation of a second definitive therapy (BMT, second course of ATG) and failure of BMT defined as initiation of a second definitive therapy (second BMT, course of ATG).

Secondary Outcome Measures

1. Comparison of subjects with failure of IST or BMT before or at 2 years [Randomization to 2 years post-randomization]

   The proportion of subjects with failure of IST or BMT before or at 2 years. Failure of IST is defined as initiation of a second definitive therapy (BMT, second course of ATG) and failure of BMT defined as initiation of a second definitive therapy (second BMT, course of ATG).

2. Comparison of subjects with inadequate counts at 2 years among those who have not died or failed treatment. [Randomization to 2 years post-randomization]

   The proportion of subjects with inadequate counts at 2 years among those who have not failed therapy or died. Adequate counts are defined as: Absolute Neutrophil Count (ANC) >1 x 10^9/L, Hemoglobin >10g/dL, and Platelets >50 x10^9/L.

3. Comparison of subjects on immune suppression therapy at 2 years among those who have not died or failed treatment. [Randomization to 2 years post-randomization]

   The proportion of subjects on immune suppression therapy at 2 years among those who have not failed therapy or died. Immune suppression is defined as systemic therapies necessary to treat SAA or GVHD (cyclosporine, tacrolimus, etc.). Isolated treatment with topical agents will not be considered as immune suppression therapy.

4. Estimate the time from randomization to initiation of IST or BMT. [Randomization through Day 100]

   The median time in days from randomization to initiation of IST or BMT will be estimated. Initiation of therapy is first day of ATG for IST subjects, or day 0 (infusion day) for bone marrow transplant subjects.

5. Comparison of the frequency of failure to receive primary assigned therapy (IST or BMT) and reasons for the failure. [Randomization through Day 100]

   The proportion of subjects who fail to receive randomized therapy and the frequency of reasons for failure.

6. Comparison of the incidence of bacteremia, viremia, and invasive fungal infection in the first two years after randomization in the IST and BMT arms. [Randomization through two years post randomization]

   Proportion of subjects from the time of randomization in the first 2 years with each of the following: Documented bacteremia Documented viremia Documented invasive fungal infection (defined as confirmed or suspected fungal infection based upon imaging)

7. Estimate the median time to T- and B-cell immune reconstitution the first year for the URD BMT Arm [Initiation of therapy (Day 0) to 100 days, 180 days, 1 year and 2 years]

   Absolute CD3, CD4, CD8, CD19, and CD56 (NK cell) numbers will be tracked at 100 days, 180 days, 1 year and 2 years post initiation of therapy in URT BMT arm. IgG levels free of IVIG replacement will be collected at the same timepoints. The median time to T- and B-cell reconstitution will be estimated.

8. Comparison of overall survival at 1 and 2 years from randomization in both arms. [Randomization to one year, randomization to two years]

   Proportion of subjects who have died at 1 year and 2 years after randomization for any reason.

9. Comparison of treatment-related mortality (TRM) at 1 and 2 years from randomization in both arms. [Randomization to 1 year, randomization to 2 years]

   Proportion of subjects who have died at 1 year and 2 years after randomization due to treatment-related reasons. TRM is defined as death in recipients without relapse or progression of their disease. Non-medical, accidental causes of death, e.g., natural disasters, are not considered TRM.

10. Comparison of the median time from randomization to and rates of neutrophil recovery on both arms [Randomization to 100 days, 180 days, 1 year and 2 years]

    The time from randomization to neutrophil recovery. Neutrophil recovery is defined as ANC 0.5 x109/L for 3 consecutive measures for neutrophils (recovery date is the first date).

11. Comparison of the median time from randomization to and rate of platelet recovery on both arms [Randomization to 100 days, 180 days, 1 year and 2 years]

    The time from randomization to platelet recovery. Platelet recovery is defined as platelet levels >= 20 x10^9/L for 3 consecutive measures (recovery is the first date) with no transfusions for 1 full week.

12. Comparison of the median time from randomization to and rates of red blood cell recovery on both arms [Randomization to 100 days, 180 days, 1 year and 2 years]

    The time from randomization to red blood cell recovery. Red blood cell recovery is defined as RBC hemoglobin level >= 8g/dL and 10g/dL with no transfusions for 4 weeks.

13. Comparison of the median time from initiation of therapy to and rates of neutrophil recovery on both arms [Initiation of therapy to 100 days, 180 days, 1 year and 2 years]

    The time from initiation of therapy (defined as Day 1 for patients randomized to IST and Day 0 for patients randomized to URD BMT) to neutrophil recovery. Neutrophil recovery is defined as ANC 0.5 x109/L for 3 consecutive measures for neutrophils (recovery date is the first date).

14. Comparison of the median time from initiation of therapy to and rate of platelet recovery on both arms [Initiation of therapy to 100 days, 180 days, 1 year and 2 years]

    The time from initiation of therapy (defined as Day 1 for patients randomized to IST and Day 0 for patients randomized to URD BMT) to platelet recovery. Platelet recovery is defined as platelet levels >= 20 x10^9/L for 3 consecutive measures (recovery is the first date) with no transfusions for 1 full week.

15. Comparison of the median time from initiation of therapy to and rates of red blood cell recovery on both arms. [Randomization to 100 days, 180 days, 1 year and 2 years]

    The time from initiation of therapy (defined as Day 1 for patients randomized to IST and Day 0 for patients randomized to URD BMT) to red blood cell recovery. Red blood cell recovery is defined as RBC hemoglobin level >= 8g/dL and 10g/dL with no transfusions for 4 weeks.

16. Estimate the rates of engraftment in patients who are randomized to URD BMT. [Randomization to 3-5 years]

    Proportion of subjects with engraftment in patients who receive URD BMT.

17. Estimate the rates of primary graft failure in patients who are randomized to URD BMT . [Randomization to 3-5 years]

    Proportion of subjects with primary graft failure in patients who receive URD BMT. Primary graft failure is defined as failure to achieve neutrophil recovery by Day +28 following a conditioning regimen induced neutrophil nadir < 0.5 x10^9/L.

18. Estimate the rates of secondary graft failure in patients who are randomized to URD BMT . [Randomization to 3-5 years]

    Proportion of subjects with secondary graft failure in patients who receive URD BMT. Secondary graft failure will be defined as a fall in the neutrophil count after documented primary engraftment to < 0.5 x10^9/L sustained for more than three days that cannot be attributed to other causes such as drugs, infection, GVHD, etc., and is not responsive to G-CSF or GM-CSF.

19. Estimate the rates of grade II-IV acute GVHD in patients who are randomized to URD BMT . [Randomization to 3-5 years]

    Proportion of subjects with grade II-IV in patients who receive URD BMT.

20. Estimate the rates of grade III-IV acute GVHD in patients who are randomized to URD BMT. [Randomization to 3-5 years]

    Proportion of subjects with grade III-IV acute GVHD in patients who receive URD BMT.

21. Estimate the rates of extensive chronic GVHD in patients who are randomized to URD BMT. [Randomization to 3-5 years]

    Proportion of subjects with extensive chronic GVHD in patients who receive URD BMT.

22. Estimate the rates of response of patients randomized to IST [Randomization to 100 days, 180 days, 1 year and 2 years]

    Proportion of subjects with IST response. IST response criteria is: Complete Remission: Hemoglobin ≥10 g/dL and ANC ≥1x10^9/L and Platelets ≥100x10^9/L Very Good Partial Response: Hemoglobin ≥8 g/dL and ANC ≥0.5x10^9/L and Platelets ≥50x10^9/L Partial Response: Hemoglobin ≥8 g/dL and ANC ≥0.5x10^9/L and Platelets ≥20x10^9/L and transfusion independent No Response (failure): Hemoglobin <8 g/dL or ANC <0.5x10^9/L or Platelets <20x10^9/L

23. Estimate the rates of failure of patients randomized to IST [Randomization to 100 days, 180 days, 1 year and 2 years]

    Proportion of subjects with IST failure at 6 months (defined as Hemoglobin <8 g/dL or ANC <0.5x10^9/L or Platelets <20x10^9/L).

24. Describe the secondary therapies given and outcomes achieved for patients failing initial therapy [Randomization to 3-5 years]

    Collect secondary therapies given for failure of primary randomized therapy (BMT after IST, second course of IST, second BMT). For the outcome after subsequent therapy, the median survival time will be estimated.

25. Comparison of rates of secondary MDS, AML, other subsequent neoplasms, and development of Paroxysmal Nocturnal Hemoglobinuria in both treatment arms for the duration of the trial. [Randomization to 3-5 years]

    Proportion of subjects in each treatment arm with i) subsequent neoplasms, ii) presence of a PNH clone at time of randomization who go on to develop symptomatic PNH through the duration of the protocol.

26. Comparison of HR-QoL score between patients randomized to both arms [Randomization to 2 years post-randomization, randomization to up to 5 years post-randomization]

    Change in score between baseline and two years and the trajectory of change over all timepoints.

27. Comparison of gonadal function values between patients randomized to both arms [Randomization to 1 year post-randomization, randomization to 2 years post-randomization, and randomization to up to 5 years post-randomization]

    Proportion of subjects with gonadal function values outside the expected percentile for that age.

Eligibility Criteria

Criteria

Inclusion Criteria:

To be eligible to participate in the randomized trial, an individual must meet all the following criteria:

1. Provision of signed and dated informed consent form for the randomized trial by patient and/or legal guardian.

2. Age ≤25 years old at time of randomized trial consent.

3. Confirmed diagnosis of idiopathic SAA, defined as:

4. Bone marrow cellularity <25%, or <30% hematopoietic cells.

5. Two of three of the following (in peripheral blood): neutrophils <0.5 x 10^{9/L, platelets <20 x 10}9/L, absolute reticulocyte count <60 x 10^9/L or hemoglobin <8 g/dL.

6. No suitable fully matched related donor available (minimum 6/6 match for HLA-A and B at intermediate or high resolution and DRB1 at high resolution using DNA based typing).

7. At least 2 unrelated donors noted on NMDP search who are well matched (9/10 or 10/10 for HLA-A, B, C, DRB1, and DQB1 using high resolution).

8. In the treating physician's opinion, no obvious contraindications precluding them from BMT or IST.

Exclusion Criteria:

1. Presence of Inherited bone marrow failure syndromes (IBMFS). The diagnosis of Fanconi anemia must be excluded by diepoxybutane (DEB) or equivalent testing on peripheral blood or marrow. Telomere length testing should be sent on all patients to exclude Dyskeratosis Congenita (DC), but if results are delayed or unavailable and there are no clinical manifestations of DC, patients may enroll. If patients have clinical characteristics suspicious for Shwachman-Diamond syndrome, this disorder should be excluded by pancreatic isoamylase testing or gene mutation analysis (note: pancreatic isoamylase testing is not useful in children <3). Other testing per center may be performed to exclude IBMFS.

2. Clonal cytogenetic abnormalities or Fluorescence In-Situ Hybridization (FISH) pattern consistent with pre- myelodysplastic syndrome (pre-MDS) or MDS on marrow examination.

3. Known severe allergy to ATG.

4. Prior allogeneic or autologous stem cell transplant.

5. Prior solid organ transplant.

6. Infection with human immunodeficiency virus (HIV).

7. Active Hepatitis B or C. This only needs to be excluded in patients where there is clinical suspicion of hepatitis (e.g., elevated LFTs).

8. Female patients who are pregnant or breast-feeding.

9. Prior malignancies except resected basal cell carcinoma or treated cervical carcinoma in situ.

10. Disease modifying treatment prior to study enrollment, including but not limited to use of androgens, eltrombopag, romiplostim, or immune suppression. Note: Supportive care measures such as G-CSF, blood transfusion support and antibiotics are allowable

Contacts and Locations

Locations

Sponsors and Collaborators

• Boston Children's Hospital
• Center for International Blood and Marrow Transplant Research
• National Institutes of Health (NIH)
• National Heart, Lung, and Blood Institute (NHLBI)
• North American Pediatric Aplastic Anemia Consortium
• Pediatric Transplantation and Cellular Therapy Consortium
• Blood and Marrow Transplant Clinical Trials Network

Investigators

• Principal Investigator: David Williams, MD, Boston Children's Hospital
• Principal Investigator: Michael Pulsipher, MD, University of Utah
• Principal Investigator: Bronwen Shaw, MD, CIBMTR/Medical College of Wisconsin (MCW)

Study Documents (Full-Text)

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