Sickle Cell Disease Clinical Trial
Official title:
HLA-Identical Sibling Donor Bone Marrow Transplantation for Individuals With Severe Sickle Cell Disease Using a Reduced Intensity Conditioning Regimen
Sickle cell disease (SCD) is the most common inherited blood disorder in Saudi Arabia . Its
clinical severity is widely heterogeneous among patients who share the same genetic mutation
. Severe frequent pain crisis, recurrent acute chest syndrome and stroke are features of
severe SCD. Hydroxyurea is an effective treatment of SCD as it ameliorates the severity and
frequency of pain crisis and acute chest syndrome and decreases mortality, however, it is
less effective in the prevention and treatment of stroke and other end organ dysfunctions .
The only readily available cure of SCD is by hematopoietic stem cell transplantation (HSCT)
. Most children with SCD who are treated by HSCT receive myeloablative conditioning with
excellent results. The application of reduced intensity (RIC) and non-myeloablative (NMA)
conditioning regimens are reserved for patients older than 16 years of age because of the
increased risks of morbidity and mortality after HSCT6. However, infertility and gonadal
failure after myeloablative conditioning are important barriers to the willingness of
patients and their families to undergo HSCT . The development of an effective RIC HSCT in
SCD that might spare the fertility of SCD patients would have obvious merit.
With the ultimate goal of expanding this curative therapy to SCD patients, we propose to
investigate HSCT with a RIC conditioning regimen. We will carry out a pilot study of HSCT
from HLA matched sibling donors using thymoglobulin/fludarabine/melphalan conditioning and
sirolimus and mycophenolate mofetil (MMF) as GVHD prophylaxis in SCD patients with severe
complications such as stroke and other severe complications. We hypothesize that HSCT from
HLA matched sibling using thymoglobulin/fludarabine/melphalan conditioning in SCD will
maintain a level of stable donor chimerism that is sufficient to cure SCD with minimal
toxicity.
Busulfan-based myeloablative allogeneic HSCT from an HLA-matched related donor in children
is associated with high cure rate ranging from 80-90% in different trials, reviewed in 6.
Lessons learned from these trials include; rabbit ATG significantly contributes to a lower
graft rejection rate, the presence of stable mixed chimerism is sufficient to cure SCD, and
the risk of neurological toxicities was minimized by maintaining platelet count greater than
50,000/uL and hemoglobin level between 9-11g/dL, adding phenytoin prophylaxis, and
preventing hypertension and hypomagnesemia . We will not present results of these trials
here, as the focus of this proposal is to investigate the use of NMA/RIC HSCT in SCD.
2.1 RIC/NMA HSCT in SCD:
1. Van Besien et al 8 reported transplant results in two adults with SCD who underwent
allogeneic transplantation from an HLA-identical sibling donor after conditioning with
fludarabine/melphalan and ATG. One patient was a 40-year-old female who had significant
end-organ dysfunction related to SCD (renal failure treated by dialysis, pulmonary
diffusion capacity was reduced by 25% and ischemic stroke) and was heavily transfused
prior to transplant. She also had RBC alloantibodies and was receiving hydroxyurea and
erythropoietin. She was conditioned with ATG 30 mg/kg for 4 consecutive days (day -5 to
day -2), fludarabine 30 mg/m2 i.v. for 4 consecutive days (day -5 to day -2) and
melphalan 140 mg/m2 i.v. on day -1. The patient had hemodialysis performed on day -5,
day -3 and day -1 after chemotherapy was administered. On day 0, the patient received
an infusion of cryopreserved G-CSF-mobilized peripheral blood stem cells (PBSC). GVHD
prophylaxis consisted of daily tacrolimus and mini methotrexate regimen (5 mg/m2 given
on days 1, 3 and 6). There was successful neutrophil and platelet engraftment and 100%
stable chimerism. She developed interstitial pneumonia, possibly secondary to GVHD, 140
days after transplantation and progressed to respiratory failure leading to her death
on day 355. The second patient was a 56 year old with SC disease who was heavily
pretransfused and had multiple SCD complications. She received the same conditioning,
GVHD prophylaxis, and PBSC source as the first patient. She had 100% donor chimerism
but died on day 142 secondary to TTP and severe gut GVHD with CNS infection.
2. Iannone et al 9 described 6 pediatric patients with SCD who underwent bone marrow
transplant from their HLA matched siblings after conditioning with fludarabine
50mg/m2/day for 3-5 days and 200 cGy TBI in addition to horse ATG in one patient. GVHD
prophylaxis included MMF and tacrolimus or cyclosporine with various taper schedules.
There was minimal toxicity, however, all patients developed graft rejection upon taper
of immunosuppressive medications.
3. Horan et al 10 described three SCD patients who were heavily transfused prior to
transplant and underwent HLA matched sibling transplant after conditioning with
fludarabine 25mg/m2 on 5 consecutive days before transplantation (days -6 to -2),
rabbit ATG (Thymoglobulin) on 4 consecutive days before transplantation (days -6 to -2)
with age adjusted dose, and single dose TBI 200 cGy. GVHD prophylaxis included MMF in
the first three months and CSA for at least six months. All had graft rejection except
one when the immunosuppression was tapered. There was no GVHD.
4. Horwitz et al 11 reported the outcome in two adult SCD patients who underwent HLA
matched sibling transplant and PBSC was the source of graft in both cases. Conditioning
was TBI 200 cGy followed by fludrabine 24-30 mg/m2 for 4 days and cyclophosphamide 500
mg/m2 for four days and alemtuzumab 100mg for five days. MMF was given in the first 100
days post transplant. Both engrafted successfully with no GVHD and a follow up of 20
months.
5. Krishnamurti et al described the use of RIC in seven SCD patients, age range 6-16
years. The conditioning was busulfan 3.2 mg/kg on day -8 and -7, fludarabine 35mg/m2 on
days -6 to -2, equine ATG 30mg/kg on days -5 to -1, and total lymphoid irradiation.
GVHD prophylaxis was CSA and MMF. CSA was tapered starting day +180 and MMF taper
varied from +45 to +220 day. Six patients had stable mixed chimerism after stopping CSA
and MMF. One patient had late graft failure. There was a low rate of GVHD.
6. Hsieh et al reported the use of non-myeloablative conditioning in SCD patients older
than 16 years of age. Graft source was GCSF mobilized PBSC from HLA matched siblings
with at least 10 X106 CD34/kg of recipient weight. Conditioning was alemtuzumab (total
1mg/kg divided on days -7 to -3) and single dose TBI 300 cGy on day -2. Presence of
major ABO incompatibility was one of the exclusion criteria for this study. Sirolimus
was used as GVHD prophylaxis and to prevent graft rejection. Nine of 10 patients
engrafted successfully and had stable chimerism, however, all patients continue to be
on sirolimus. None of patients had GVHD. They recently updated these promising results
in a total of 30 patients and were able to taper off sirolimus in 15 patients.
2.2 Rationale for using thymoglobulin/fludarabine/melphalan conditioning RIC is a feasible
option for patients with SCD and can successfully cure the disease. A pre-transplant
backbone regimen consisting of Alemtuzumab or ATG, fludarabine, and melphalan has been
applied successfully in SCD patients as described above. We anticipate that the toxicity
risk is lower than the full myeloablative conditioning using busulfan and cyclophosphamide
(BU/CY). Melphalan was reported to cause infertility, mostly when we used with other
chemotherapy agents. The use of melphalan alone in the conditioning regimen was reported
before to potentially preserve fertility in women. So our regimen could potentially preserve
fertility at higher rate compared to BU/CY.
2.3 Rationale for pre-transplant immunosuppression therapy with hydroxyurea Individuals with
hemoglobinopathies have in general adequate T cell function and active bone marrow that can
lead to higher risk of graft rejection especially among patients who are heavily transfused.
Experience with class 3 thalassemia patients showed that pretreatment with hydroxyurea,
azathioprine, and fludarabine decreased the risk of graft rejection and allowed the use of
lower dose cyclophosphamide . So we will use hydroxyurea prior to transplant to minimize the
risk of graft rejection associated with RIC in sickle cell anemia.
2.4 Rationale for using sirolimus and MMF as GVHD prophylaxis: Post-grafting
immunosuppression appears crucial to ensuring stable engraftment; an early taper appears to
contribute to late graft rejection in several of the series. Sirolimus is an inhibitor of
the mammalian target of rapamycin (mTOR) and it induces immune tolerance and was used
successfully as GVHD prophylaxis in adult SCA patients who underwent RIC/ NMA. Sirolimus in
combination with calcineurin inhibitors or MMF was utilized effectively in pediatric
patients 19-21. However, studies showed increased risk of veno-occlusive disease with the
combination of sirolimus and MMF and increased risk of transplant-associated thrombotic
microangiopathy when combined with tacrolimus especially among patients who received
busulfan-based conditioning 22-24. We will be using a RIC regimen so we do not anticipate
that the combination of sirolimus and MMF will cause excess toxicity.
;
Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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