Sickle Cell Disease Clinical Trial
Official title:
A Pilot Study of Allogeneic Hematopoietic Stem Cell Transplantation for Patients With High Risk Hemoglobinopathy Using a Non-Myeloablative Preparative Regimen to Achieve Stable Mixed Chimerism
Hypothesis 1: A novel nonmyeloablative condition regimen will be safe and efficacious in
producing stable donor chimerism and cure of severe hemoglobinopathy.
Hypothesis 2: Stable donor chimerism will result in amelioration of cerebral vasculopathy,
improved cerebral perfusion and neurocognitive function.
Specific Aim 1: Study the safety and efficacy of a novel non-toxic conditioning regimen for
HSCT for patients with severe hemoglobinopathies and the kinetics of lineage specific
chimerism after HSCT
We will test our hypothesis that a novel nonmyeloablative condition regimen will be safe and
efficacious in producing stable donor chimerism and cure of severe hemoglobinopathy:
Specific Aim 2: Optimize the immunosuppressive regimen for HSCT patients through a thorough
understanding of the pharmacokinetics of Busulfan (BU) and mycophenolate mofetil (MMF) in
the patient population. This will involve:
1. Determine the pharmacokinetics of intravenously and orally administered MMF and
intravenous BU in patients receiving HSCT.
2. Determine the relationship of Area under the curve (AUC) of BU and mean trough
concentrations of mycophenolic acid (MPA) to engraftment and graft versus host disease
(GVHD).
3. Determine the relationship of Area under the curve (AUC) and steady state concentration
of BU to engraftment at day 30 and 1 year post HSCT.
Specific Aim 3: Study the effect of complete or partial donor chimerism on silent and overt
cerebral vasculopathy, and neurocognitive functioning in patients with SCD undergoing HSCT.
We will test our hypothesis that stable donor chimerism will result in improvement in
cerebral vasculopathy and neurocognitive function. This will include.
1. Determine effect of transplantation silent and overt cerebral vasculopathy by
comparison MRA and TCD 1 year after HSCT to pre-HSCT studies.
2. Determine effect on HSCT on neurocognitive function. Specific Aim 4: To determine the
rate of T cell immune reconstitution in children with sickle cell disease following
myeloablative compared to nonmyeloablative stem cell transplantation, using
immunophenotyping assays, CDR3 spectratyping TREC analysis, and measurement of T cell
specific donor engraftment.
| Status | Recruiting |
| Enrollment | 20 |
| Est. completion date | December 2012 |
| Est. primary completion date | June 2012 |
| Accepts healthy volunteers | No |
| Gender | Both |
| Age group | 3 Years to 35 Years |
| Eligibility |
Inclusion Criteria: - Patients with SCD 0-35 years of age with an HLA-identical or 1 HLA antigen mismatched bone marrow or up to 2 HLA antigen mismatched umbilical cord blood (UCB) donor with one or more of the following: - Stroke, CNS hemorrhage or a neurologic event lasting longer than 24 hours, or abnormal cerebral MRI or cerebral arteriogram or MRI angiographic study and impaired neuropsychological testing, - Acute chest syndrome with a history of recurrent hospitalizations or exchange transfusions, - Recurrent vaso-occlusive pain 3 or more episodes per year for 3 years or more years or recurrent priapism, - Impaired neuropsychological function and abnormal cerebral MRI scan, - Stage I or II sickle lung disease, - Sickle nephropathy (moderate or severe proteinuria or a glomerular filtration rate [GFR] 30-50% of the predicted normal value), - Bilateral proliferative retinopathy and major visual impairment in at least one eye, - Osteonecrosis of multiple joints with documented destructive changes, - Requirement for chronic transfusions but with RBC alloimmunization >2 antibodies during long term transfusion therapy. - Patients with transfusion dependent Thalassemia 0-35 years of age with an HLA-identical or 1 HLA antigen mismatched bone marrow or up to 2 HLA antigen mismatched UCB donor. - Second Transplants - Patients with sickle cell disease or Thalassemia who have failed to engraft or have autologous recovery are eligible for this protocol. - Patients must meet above criteria. - If first transplant was a non-myeloablative regimen, the second transplant can occur at any time. - If the first transplant was a myeloablative regimen, then the second transplant must be > 6 months from the first transplant. Exclusion Criteria: - Patients with one or more of the following: - Karnofsky or Lansky performance score <70, - Acute hepatitis or evidence of moderate or severe portal fibrosis or cirrhosis on biopsy, - Stage III-IV lung disease, - GFR<30% predicted normal values. - Pregnant or lactating females. - Active serious infection whereby patient has been on intravenous antibiotics for one week prior to study entry. Any patient with AIDS or ARC or HIV seropositivity. Any patient with invasive aspergillums infection within one year of study entry. - Psychologically incapable of undergoing BMT with associated strict isolation or documented history of medical non-compliance. - Patients not able to receive TLI due to prior radiation therapy. Donor Inclusion Criteria - Donor must be in good health based on review of systems and results of physical examination. - Donor must have a normal hemoglobin, white count, platelet count and PTT. - Female donors of childbearing potential must have a negative pregnancy test. Donor Exclusion Criteria - Donor has active infection (including HIV, hepatitis). - Donor is a lactating female. Donor Selection In the case where more than one donor meets the eligibility criteria, donor selection will be guided by the following considerations: - HLA A, B, DRB1 identical sibling donor is preferable to an unrelated donor - Homozygous normal donor is preferable to heterozygote (carrier) - ABO-compatible donor is preferable to ABO-incompatible donor - Younger donor is preferable to older - Cytomegalovirus seronegative donor is preferable to CMV seropositive donor, if the patient is CMV negative |
Allocation: Non-Randomized, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
| Country | Name | City | State |
|---|---|---|---|
| United States | Children's Hospital of Pittsburgh | Pittsburgh | Pennsylvania |
| Lead Sponsor | Collaborator |
|---|---|
| University of Pittsburgh | Children's Hospital of Pittsburgh |
United States,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | GVHD at 100 days, 6 months and 1 year will be tabulated by grade. | 100 days, 6 months and 1 year | Yes | |
| Primary | The incidence of =5% chimerism at 100 days, 6 months and 1 year will be estimated, and reported with 95% confidence bounds. | 100 days, 6 months and 1 year | No | |
| Primary | The association between % donor chimerism of lymphocytes and erythroid precursors at day 30 to % donor chimerism in the bone marrow at 1 year will be assessed via the Spearman correlation coefficient. | day 30 and 1 year | No | |
| Primary | In addition, the Wilcoxon test will be used to assess association of the % chimerism on day 30 to successful transplantation, which is defined as = 5% donor chimerism in the bone marrow at 1 year. | Day 30, 1 year | No |
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