Hematopoietic stem cell transplant (HSCT) is the only cure for sickle cell disease (SCD). HSCT using an HLA-identical sibling donor is currently an acceptable treatment option for children with severe SCD, with expected HSCT survival >95% and event-free survival >85%. HSCT for children with less severe SCD (children who have not yet suffered overt disease complications or only had mild problems) is controversial. It is important to consider the ethical issues of a proposed study comparing HLA-identical sibling HSCT to best supportive care for children with less severe SCD. In evaluating the principles of nonmaleficence, respect for individual autonomy, and justice, we conclude that a study of HLA-identical sibling HSCT for all children with SCD, particularly hemoglobin SS and Sβ0-thalassemia disease, is ethically sound. Future work should explore the implementation of a large trial to help determine whether HSCT is a beneficial treatment of children with less severe SCD.

Subjects:
Pediatric Hematology, Perspectives, Red Cells, Iron, and Erythropoiesis, Sickle Cell Disease, Transplantation
Topics:
child, ethics, hematopoietic stem cell transplantation, sickle cell anemia, human leukocyte antigens, supportive care, hemoglobin, thalassemia

Transplant to cure sickle cell disease

Sickle cell disease (SCD) is an inherited disorder of the hemoglobin protein in red blood cells that causes serious acute and chronic complications affecting multiple organs. In the early 1980s, a child with SCD who also developed acute myeloid leukemia at age 8 became the first person cured of SCD when she underwent allogeneic hematopoietic stem cell transplant (HSCT) to treat her leukemia.1  Although this initial case demonstrated the curative potential of HSCT for SCD, at that time, transplant was not considered a treatment option for SCD given the significant morbidity and mortality associated with HSCT. However, as transplant care improved, a few years later, a small group of patients in Belgium was successfully transplanted explicitly for SCD.2  This work helped lead in the 1990s to an international trial of HLA-identical sibling HSCT for SCD.3  This study was limited to patients with severe SCD who had suffered certain complications like a stroke (Table 1). The results of the study were encouraging, with >93% of patients surviving the transplant and 85% successfully cured of SCD.4  Similar results involving other centers,5-7  as well as long-term follow-up studies of transplanted patients, have demonstrated that HSCT definitively cures SCD, preventing further, and in some cases even reversing, SCD-mediated organ damage.8-10  More recent studies of HLA-identical sibling HSCT for SCD have reported even better results, with overall survival approaching 100% and SCD cure rates of ∼90%.11-18 

Table 1

Eligibility criteria used to define severe SCD by the Collaborative Group Study of Marrow Transplantation for Sickle Cell Anemia

One or more of the following3 :
Stroke or central nervous system event lasting longer than 24 hours 
Acute chest syndrome with recurrent hospitalizations or previous exchange transfusions 
Recurrent vaso-occlusive pain (≥2 episodes per year for several 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 30% to 50% of the predicted normal value) 
Bilateral proliferative retinopathy and major visual impairment in at least one eye 
Osteonecrosis of multiple joints 
Red cell alloimmunization (≥2 antibodies) during long-term transfusion therapy 
One or more of the following3 :
Stroke or central nervous system event lasting longer than 24 hours 
Acute chest syndrome with recurrent hospitalizations or previous exchange transfusions 
Recurrent vaso-occlusive pain (≥2 episodes per year for several 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 30% to 50% of the predicted normal value) 
Bilateral proliferative retinopathy and major visual impairment in at least one eye 
Osteonecrosis of multiple joints 
Red cell alloimmunization (≥2 antibodies) during long-term transfusion therapy 
View Large

Because HSCT is associated with serious toxicities, its initial use was limited to treating patients with severe SCD in research settings. These patients with severe SCD had a high risk of further SCD-related complications and death at a young age. The risk/benefit ratio of a curative treatment—even one associated with its own risk of death—was reasonable for them. Now, given the existing research on HSCT for SCD, many experts currently agree that HSCT is a good treatment option for these SCD patients with severe disease who have HLA-identical siblings.14,19,20  The concept of promoting HSCT for children with less severe SCD, however, is controversial, given that their disease is not as predictably life shortening to the degree of severe SCD, and it is less clear that the benefits of transplant outweigh the risks. Is it ethical to conduct a trial of HLA-identical sibling HSCT vs supportive care for children with less severe SCD?

What is less severe sickle cell disease?

It is first necessary to define our concept of less severe SCD. We do not use this term to refer to patients who have had serious SCD complications that fall just short of restrictive established transplant eligibility criteria (Table 1). We also do not use this term to refer to patients started on chronic transfusion therapy for primary stroke prevention due to an elevated transcranial Doppler velocity, as these patients are at high risk of serious clinical events even if they have not yet had any problems.21  Although still not viewed as first-line therapy by some hematologists,22  an HLA-identical sibling transplant is less controversial for these types of patients. We instead define less severe SCD to refer to children who have had only minor or no overt SCD complications. Some have used the term mild SCD or asymptomatic SCD to refer to this group of patients. We believe this language is misleading because a child with initially mild SCD may suffer life-threatening SCD complications as a young adult. The term asymptomatic SCD is especially problematic as it wrongly implies that some children with SCD are not affected by the condition, when, in reality, most will typically suffer at least some pain, and their hemoglobinopathy will cause progressive multiorgan damage. Even at the very young age of 12 months, the overwhelming majority of infants with hemoglobin SS and Sβ0-thalassemia disease have evidence of splenic dysfunction,23  and most show signs of renal dysfunction.24  Especially concerning is the finding that >25% of young (age < 6 years) neurologically asymptomatic children with hemoglobin SS disease have evidence of ischemia on screening brain magnetic resonance images,25  and these “silent strokes” are associated with poor school performance26  and a global loss of intellectual function.27 

In our defined group of children with less severe SCD, if we could predict which patients would later develop serious SCD-related problems and which patients would instead continue to enjoy mostly good health as adults, then it may be prudent to only consider HSCT in those children who would later develop significant problems. Unfortunately, despite research in this area,28-30  clinical markers have failed to reliably predict later SCD severity,31  and, given advances in our care, historic predictive models have limited applicability to patients with SCD today.32  Although some laboratory tests in early childhood may prove to be helpful in forecasting later SCD severity,33  a hallmark of SCD is its unpredictable clinical course, so accurately predicting the extent of an individual child’s future SCD complications is likely impossible.

We use the general term SCD to refer to all SCD genotypes (hemoglobin SS, Sβ0-thalassemia, Sβ+-thalassemia, SC disease); however, we recognize that the prognosis of patients with Sβ+-thalassemia and SC disease is typically much better than patients with hemoglobin SS and Sβ0-thalassemia disease. The risk of SCD-related death and stroke in children with hemoglobin Sβ+-thalassemia and SC disease is extremely low,34  and overall life expectancy of individuals with these genotypes is significantly greater than individuals with hemoglobin SS and Sβ0-thalassemia disease.35,36  Thus, when considering transplant for children with SCD who have not yet suffered any overt disease-related complications (asymptomatic patients), it seems prudent to initially consider transplant only for individuals with hemoglobin SS and Sβ0-thalassemia disease. However, we feel that there is a role for HSCT for some children with hemoglobin Sβ+-thalassemia and SC disease, as some individuals with these genotypes experience major SCD complications,37  suffer with pain,38  and report reduced quality of life,39  similar to patients with hemoglobin SS and Sβ0-thalassemia disease.

Is there clinical equipoise?

A basic ethical requirement of any proposed clinical study involving different interventions is that there must be “clinical equipoise” regarding the interventions. In other words, experts must be uncertain if intervention A or intervention B is superior. In this case, the research question is as follows: is an HLA-identical sibling HSCT or current supportive care the best treatment approach for less severe SCD? We believe that there is definite clinical equipoise in this setting, as recent reviews have opposing conclusions. Kassim and DeBaun,32  especially noting further improvement in SCD supportive care with hydroxyurea therapy, are “hesitant” to recommend HSCT for asymptomatic children. In contrast, Sheth et al14  assert that HSCT “should be considered a first-line therapy for all children with a matched sibling.”

The principle primum non nocere (first, do no harm) is revered as fundamental to medical ethics. Some have cited this concept of nonmaleficence as a reason to potentially not perform HSCT in children with less severe SCD.40  First, although the risk of transplant-related mortality is low for HLA-identical sibling HSCT (<5%, possibly lower for children with less severe SCD5 ), it is almost certainly higher than the short-term mortality risk of less severe SCD, as we now expect virtually all children with SCD in developed countries to survive childhood with current supportive care practices.41,42  This small but important risk of death is, however, not the only potential harm of transplant. Importantly, HSCT is also associated with a risk (10-20%)43  of graft-versus-host disease (GVHD). Although most GVHD can be managed well (and even eliminated), transplant may rarely cause extensive GVHD that may be comparable to or even worse than SCD in its impact on health and quality of life. Another important potential harm of HSCT involves long-term side effects including gonadal dysfunction and infertility,8,44  although this risk will likely decrease in the future with the increased use of less gonadotoxic conditioning regimens. Additional long-term follow-up is also needed on patients transplanted for SCD to determine if they are at an increased risk of malignancy years after HSCT. Finally, transplant would likely harm the short-term psycho-social well-being of the apparently asymptomatic child and family by requiring them to miss school and work, to endure a long hospitalization possibly far from home, and to follow a strict regimen of medicines, restrictions, and medical appointments for months.

Although the potential harms of HSCT are significant, especially for a child with less severe SCD, it is important to consider these potential harms relative to the risks of having SCD (Table 2). Although childhood mortality in SCD has been dramatically reduced and some individuals even with hemoglobin SS disease are living past age 60,45  many people with SCD die before age 40.46-49  In addition to this >20-year reduction in life expectancy, many adults with SCD experience pain most days,38  have high rates of disability,50  and report poor overall quality of life.39,51  Although the long-term prognosis of children with initially less severe SCD may be better (especially in the future with continued improvements in supportive care), an individual patient’s disease course is likely to involve significant problems. The specific risk of infertility secondary to HSCT also has to be balanced with the risk of reproductive problems related to SCD complications (impotence from priapism for men,52-54  increased pregnancy complications for women55-57 ) and also weighed against hydroxyurea therapy toxicity.44,58,59  Thus, given the serious problems caused by SCD, some have questioned: Is the medical community actually harming patients with SCD by not offering them a curative therapy (HSCT) early and forcing these patients to live with a disease that causes high morbidity and premature mortality?60 

Table 2

Summary of key potential harms of HLA-identical sibling HSCT and SCD

HarmHSCTSCD
Death Low risk of dying from transplant complication Very low risk of dying as a child with current supportive care, high risk of dying prematurely as an adult 
Infection Severely immunocompromised for weeks post-transplant Defective or absent splenic function 
Acute complication Mucositis, hair loss, veno-occlusive disease, cerebral hemorrhage, posterior reversible encephalopathy syndrome Vaso-occlusive crisis, acute chest syndrome, cholecystitis, priapism, splenic sequestration, aplastic crisis, stroke 
Chronic complication Graft-versus-host disease Chronic pain, avascular necrosis, progressive multi-organ damage (retinopathy, kidney dysfunction, pulmonary hypertension) 
Reproductive problems Possible secondary to gonadotoxic conditioning Possible secondary to organ damage (men: erectile dysfunction; women: pregnancy complications) or hydroxyurea therapy 
Social Intense short-term burden due to transplant hospitalization and care post-transplant Life-long burden of chronic disease 
HarmHSCTSCD
Death Low risk of dying from transplant complication Very low risk of dying as a child with current supportive care, high risk of dying prematurely as an adult 
Infection Severely immunocompromised for weeks post-transplant Defective or absent splenic function 
Acute complication Mucositis, hair loss, veno-occlusive disease, cerebral hemorrhage, posterior reversible encephalopathy syndrome Vaso-occlusive crisis, acute chest syndrome, cholecystitis, priapism, splenic sequestration, aplastic crisis, stroke 
Chronic complication Graft-versus-host disease Chronic pain, avascular necrosis, progressive multi-organ damage (retinopathy, kidney dysfunction, pulmonary hypertension) 
Reproductive problems Possible secondary to gonadotoxic conditioning Possible secondary to organ damage (men: erectile dysfunction; women: pregnancy complications) or hydroxyurea therapy 
Social Intense short-term burden due to transplant hospitalization and care post-transplant Life-long burden of chronic disease 
View Large

We believe that currently we do not have sufficient evidence to answer the above question when considering HLA-identical sibling HSCT for SCD. While the potential harms of HSCT are significant, so are the potential harms of SCD (even SCD that is viewed initially as less severe). Given this uncertainty, a trial studying HLA-identical sibling HSCT in less severe SCD does not violate the principle of nonmaleficence. However, it is important to clarify that the transplants being discussed herein are all from HLA-identical sibling donors. At present, we believe it is appropriate to restrict HSCT using alternative donor sources (unrelated cord blood units, unrelated bone marrow donors, haplo-identical family members) to patients with more severe SCD. Currently alternative donor HSCTs for SCD are much more likely to cause harm (higher risk of death, GVHD, graft rejection)61-64  than are HSCTs from matched sibling donors. Thus, until the potential harms of alternative donor HSCTs can be decreased, they cannot ethically be used to treat children with “less severe” SCD.

Our society has rejected the notion that a doctor should unilaterally dictate the treatment of a specific patient as medical paternalism. Instead we now embrace the principle of respect for autonomy—an individual patient is honored as the person who makes the final medical decisions regarding his or her treatment. In the research setting, respect for autonomy requires that we obtain the informed consent of the research participant. However, here we are considering a study on young children who cannot consent to participate. Can parents of a child with less severe SCD ethically permit a study of HSCT on their child?

Some may argue that HSCT for young children with less severe SCD violates that child’s autonomy. An informed adult with SCD may view HSCT as too dangerous and be unwilling to accept the risks of such an intervention—so why should a young child with less severe SCD be subjected to such a risky intervention (with potential long-term side effects) even if his or her parents give full, informed consent? It would be ethically preferable to wait until the child becomes an adult (or at least an adolescent) who can make his or her own autonomous choice regarding this very difficult decision.

If there was no potential downside in waiting until a child with SCD could consent and make his or her own decision regarding HSCT as an adult, then it would be unethical to transplant children with less severe SCD. However, from a medical perspective, it is likely better to transplant an individual with SCD as a child rather than as an adult. Initially patients with SCD over the age of 16 years were not even considered eligible for transplant because of legitimate concerns that older patients who had already suffered SCD-related organ damage would not tolerate myeloablative conditioning.3  Even when solely considering pediatric patients, evidence exists that younger children with other conditions have better HSCT outcomes65  and in particular less GVHD66-68  possibly due to better pretransplant thymic function compared with older patients.69  Regarding SCD specifically, Vermylen et al5  reported that a group of young (median age, 2.0 years) children transplanted for less severe SCD had an impressive 100% overall survival and 93% event-free survival with no severe GVHD, outcomes significantly better than their older group of patients (median age, 8.6 years) transplanted because of SCD severity. Additional research is needed to confirm this finding that children with SCD transplanted at a younger age and for less severe disease have better HSCT outcomes. In addition to having less organ damage before HSCT that would likely decrease transplant toxicity, younger and less severe patients also have received fewer blood transfusions. Blood transfusions cause alloantibody formation in many SCD patients, and transfusion-related alloimmunization may complicate future HSCT.70-73  Finally, although a recent study using reduced intensity conditioning was successful in curing adults with SCD with acceptable toxicity (suggesting it is possible to wait until children with SCD become adults to pursue HSCT), these patients required long-term immunosuppression to prevent graft rejection.12  Even if HSCT as an adult is feasible, it seems desirable to transplant individuals with SCD before they suffer permanent organ damage and other complications of SCD, which, as detailed above, unfortunately begin in infancy.

It is also prudent to consider the idea that restricting a child with less severe SCD from undergoing HSCT violates that child’s theoretical future autonomous choice to have wanted to pursue HSCT as a child instead of as an adult. As part of this consideration, it should be noted that adult SCD patients’ desire to pursue HSCT and to accept the risk of transplant-related mortality does not appear to be associated with their disease severity or health care providers’ assessment of risk.74  Patients with SCD thus appear to have different perceptions about the acceptability of HSCT risk than physicians and are often willing to accept more risk to achieve cure. Rather than maintaining a paternalistic system in which physicians only consider patients with severe SCD eligible for HSCT, to promote the principle of autonomy, informed patients should be allowed to make their own decision regarding HSCT. Because children are not capable of making such a decision, we believe that, like in other difficult medical decisions and research involving children, parents should decide what is best for their child and thus can ethically consent for the proposed study. Although some may worry that this decision may burden parents or that parents are not capable of properly weighing the risks and benefits of participation for their child (Tables 2 and 3), parents are likely the best agents to represent their child. Of note, parents’ willingness to accept hypothetical varying risks of transplant-related mortality for SCD is very similar to the risks that adult patients with SCD would accept,74,75  supporting the concept that parents make reasonable decisions on behalf of their children.

Table 3

Potential reasons for early transplant vs reasons to wait for transplant in children with less severe SCD

Transplant early to:Wait to consider transplant because:
Prevent early organ damage secondary to SCD Advances in HSCT technology may further improve HSCT outcomes in the future 
Avoid SCD complications in childhood Other curative therapy (gene therapy) may be developed in future with less risks than HSCT 
Achieve better HSCT outcomes secondary to less pre-HSCT organ damage and alloimmunization Further improvement in SCD supportive care (new medications other than hydroxyurea) may make curative therapy less important 
Transplant early to:Wait to consider transplant because:
Prevent early organ damage secondary to SCD Advances in HSCT technology may further improve HSCT outcomes in the future 
Avoid SCD complications in childhood Other curative therapy (gene therapy) may be developed in future with less risks than HSCT 
Achieve better HSCT outcomes secondary to less pre-HSCT organ damage and alloimmunization Further improvement in SCD supportive care (new medications other than hydroxyurea) may make curative therapy less important 
View Large

It is worth noting that SCD disproportionately affects minority groups traditionally viewed as vulnerable research populations. Although people of many different races have SCD worldwide, in the United States, SCD primarily affects African Americans, a group that historically has suffered serious injustice in medical research as demonstrated by the infamous Tuskegee syphilis study. Given this background, the proposed study of an intervention with serious potential risks on seemingly asymptomatic children for a genetic condition that primarily affects a historically disadvantaged racial group could raise concerns that this group is unfairly being subject to experimentation. However, because the proposed research is seeking to benefit the vulnerable group (and no other group), we argue the opposite idea: justice, with its goal to distribute the benefits of research to all groups, demands that we pursue research like the proposed study on children with SCD to ensure this group receives the best treatment. It unfortunately appears that SCD has not received a fair distribution of research funding compared with conditions like cystic fibrosis that do not primarily affect minorities.76 

We conclude that a study of HLA-identical sibling HSCT for children with less severe SCD is ethically sound. Such a study must be conducted with strict safeguards in place to monitor safety and to ensure informed parental permission, and patients with certain justified contraindications to HSCT should be excluded. Whereas actual design and feasibility are critical issues for the proposed study comparing HSCT to supportive care, these challenges should not prevent the medical community from conducting this important research. We believe such a trial would be pivotal in advancing the pursuit of optimal treatment options for children with SCD.

Contribution: R.S.N. wrote the paper; and J.E.H. and A.E.H. critically reviewed and edited the manuscript.

Conflict-of-interest disclosure: The authors declare no competing financial interests.

Correspondence: Robert Sheppard Nickel, 2015 Uppergate Dr, Atlanta, GA 30322; e-mail: robert.nickel@choa.org.

1
Johnson
 
FL
Look
 
AT
Gockerman
 
J
Ruggiero
 
MR
Dalla-Pozza
 
L
Billings
 
FT
Bone-marrow transplantation in a patient with sickle-cell anemia.
N Engl J Med
1984
, vol. 
311
 
12
(pg. 
780
-
783
)
Google Scholar
Crossref
Search ADS
PubMed
 
2
Vermylen
 
C
Fernandez Robles
 
E
Ninane
 
J
Cornu
 
G
Bone marrow transplantation in five children with sickle cell anaemia.
Lancet
1988
, vol. 
1
 
8600
(pg. 
1427
-
1428
)
Google Scholar
Crossref
Search ADS
PubMed
 
3
Walters
 
MC
Patience
 
M
Leisenring
 
W
et al. 
Bone marrow transplantation for sickle cell disease.
N Engl J Med
1996
, vol. 
335
 
6
(pg. 
369
-
376
)
Google Scholar
Crossref
Search ADS
PubMed
 
4
Walters
 
MC
Patience
 
M
Leisenring
 
W
et al. 
Multicenter Investigation of Bone Marrow Transplantation for Sickle Cell Disease
Stable mixed hematopoietic chimerism after bone marrow transplantation for sickle cell anemia.
Biol Blood Marrow Transplant
2001
, vol. 
7
 
12
(pg. 
665
-
673
)
Google Scholar
Crossref
Search ADS
PubMed
 
5
Vermylen
 
C
Cornu
 
G
Ferster
 
A
et al. 
Haematopoietic stem cell transplantation for sickle cell anaemia: the first 50 patients transplanted in Belgium.
Bone Marrow Transplant
1998
, vol. 
22
 
1
(pg. 
1
-
6
)
Google Scholar
Crossref
Search ADS
PubMed
 
6
Bernaudin
 
F
Socie
 
G
Kuentz
 
M
et al. 
SFGM-TC
Long-term results of related myeloablative stem-cell transplantation to cure sickle cell disease.
Blood
2007
, vol. 
110
 
7
(pg. 
2749
-
2756
)
Google Scholar
Crossref
Search ADS
PubMed
 
7
Panepinto
 
JA
Walters
 
MC
Carreras
 
J
et al. 
Non-Malignant Marrow Disorders Working Committee, Center for International Blood and Marrow Transplant Research
Matched-related donor transplantation for sickle cell disease: report from the Center for International Blood and Transplant Research.
Br J Haematol
2007
, vol. 
137
 
5
(pg. 
479
-
485
)
Google Scholar
Crossref
Search ADS
PubMed
 
8
Walters
 
MC
Hardy
 
K
Edwards
 
S
et al. 
Multicenter Study of Bone Marrow Transplantation for Sickle Cell Disease
Pulmonary, gonadal, and central nervous system status after bone marrow transplantation for sickle cell disease.
Biol Blood Marrow Transplant
2010
, vol. 
16
 
2
(pg. 
263
-
272
)
Google Scholar
Crossref
Search ADS
PubMed
 
9
Mynarek
 
M
Bettoni da Cunha Riehm
 
C
Brinkmann
 
F
et al. 
Normalized transcranial Doppler velocities, stroke prevention and improved pulmonary function after stem cell transplantation in children with sickle cell anemia.
Klin Padiatr
2013
, vol. 
225
 
3
(pg. 
127
-
132
)
Google Scholar
Crossref
Search ADS
PubMed
 
10
Bockenmeyer
 
J
Chamboredon
 
E
Missud
 
F
et al. 
[Development of psychological and intellectual performance in transplanted sickle cell disease patients: a prospective study from pretransplant period to 5 years after HSCT].
Arch Pediatr
2013
, vol. 
20
 
7
(pg. 
723
-
730
)
Google Scholar
Crossref
Search ADS
PubMed
 
11
Krishnamurti
 
L
Kharbanda
 
S
Biernacki
 
MA
et al. 
Stable long-term donor engraftment following reduced-intensity hematopoietic cell transplantation for sickle cell disease.
Biol Blood Marrow Transplant
2008
, vol. 
14
 
11
(pg. 
1270
-
1278
)
Google Scholar
Crossref
Search ADS
PubMed
 
12
Hsieh
 
MM
Kang
 
EM
Fitzhugh
 
CD
et al. 
Allogeneic hematopoietic stem-cell transplantation for sickle cell disease.
N Engl J Med
2009
, vol. 
361
 
24
(pg. 
2309
-
2317
)
Google Scholar
Crossref
Search ADS
PubMed
 
13
Majumdar
 
S
Robertson
 
Z
Robinson
 
A
Starnes
 
S
Iyer
 
R
Megason
 
G
Outcome of hematopoietic cell transplantation in children with sickle cell disease, a single center’s experience.
Bone Marrow Transplant
2010
, vol. 
45
 
5
(pg. 
895
-
900
)
Google Scholar
Crossref
Search ADS
PubMed
 
14
Sheth
 
S
Licursi
 
M
Bhatia
 
M
Sickle cell disease: time for a closer look at treatment options?
Br J Haematol
2013
, vol. 
162
 
4
(pg. 
455
-
464
)
Google Scholar
Crossref
Search ADS
PubMed
 
15
Locatelli
 
F
Kabbara
 
N
Ruggeri
 
A
et al. 
Eurocord and European Blood and Marrow Transplantation (EBMT) group
Outcome of patients with hemoglobinopathies given either cord blood or bone marrow transplantation from an HLA-identical sibling.
Blood
2013
, vol. 
122
 
6
(pg. 
1072
-
1078
)
Google Scholar
Crossref
Search ADS
PubMed
 
16
Dedeken
 
L
 
PQ
Azzi
 
N
et al. 
Haematopoietic stem cell transplantation for severe sickle cell disease in childhood: a single centre experience of 50 patients.
Br J Haematol
2014
, vol. 
165
 
3
(pg. 
402
-
408
)
Google Scholar
Crossref
Search ADS
PubMed
 
17
Soni
 
S
Gross
 
TG
Rangarajan
 
H
Baker
 
KS
Sturm
 
M
Rhodes
 
M
Outcomes of matched sibling donor hematopoietic stem cell transplantation for severe sickle cell disease with myeloablative conditioning and intermediate-dose of rabbit anti-thymocyte globulin [published online ahead of print April 17, 2014].
Pediatr Blood Cancer
18
Soni
 
S
Boulad
 
F
Cowan
 
MJ
et al. 
Combined umbilical cord blood and bone marrow from HLA-identical sibling donors for hematopoietic stem cell transplantation in children with hemoglobinopathies [published online ahead of print May 7, 2014].
Pediatr Blood Cancer
doi:10.1002/pbc.25085
Google Scholar
 
19
Hsieh
 
MM
Fitzhugh
 
CD
Tisdale
 
JF
Allogeneic hematopoietic stem cell transplantation for sickle cell disease: the time is now.
Blood
2011
, vol. 
118
 
5
(pg. 
1197
-
1207
)
Google Scholar
Crossref
Search ADS
PubMed
 
20
King
 
A
Shenoy
 
S
Evidence-based focused review of the status of hematopoietic stem cell transplantation as treatment of sickle cell disease and thalassemia.
Blood
2014
, vol. 
123
 
20
(pg. 
3089
-
3094, quiz 3210
)
Google Scholar
Crossref
Search ADS
PubMed
 
21
Adams
 
RJ
McKie
 
VC
Carl
 
EM
et al. 
Long-term stroke risk in children with sickle cell disease screened with transcranial Doppler.
Ann Neurol
1997
, vol. 
42
 
5
(pg. 
699
-
704
)
Google Scholar
Crossref
Search ADS
PubMed
 
22
Mikles
 
B
Bhatia
 
M
Oyeku
 
SO
Jin
 
Z
Green
 
NS
Pediatric hematology providers on referral for transplant evaluation for sickle cell disease: a regional perspective [published online ahead of print March 13, 2014].
J Pediatr Hematol Oncol
23
Rogers
 
ZR
Wang
 
WC
Luo
 
Z
et al. 
BABY HUG
Biomarkers of splenic function in infants with sickle cell anemia: baseline data from the BABY HUG Trial.
Blood
2011
, vol. 
117
 
9
(pg. 
2614
-
2617
)
Google Scholar
Crossref
Search ADS
PubMed
 
24
Ware
 
RE
Rees
 
RC
Sarnaik
 
SA
et al.  
Renal function in infants with sickle cell anemia: baseline data from the BABY HUG trial. J Pediatr. 2010;156(1):66-70
25
Kwiatkowski
 
JL
Zimmerman
 
RA
Pollock
 
AN
et al. 
Silent infarcts in young children with sickle cell disease.
Br J Haematol
2009
, vol. 
146
 
3
(pg. 
300
-
305
)
Google Scholar
Crossref
Search ADS
PubMed
 
26
Schatz
 
J
Brown
 
RT
Pascual
 
JM
Hsu
 
L
DeBaun
 
MR
Poor school and cognitive functioning with silent cerebral infarcts and sickle cell disease.
Neurology
2001
, vol. 
56
 
8
(pg. 
1109
-
1111
)
Google Scholar
Crossref
Search ADS
PubMed
 
27
DeBaun
 
MR
Armstrong
 
FD
McKinstry
 
RC
Ware
 
RE
Vichinsky
 
E
Kirkham
 
FJ
Silent cerebral infarcts: a review on a prevalent and progressive cause of neurologic injury in sickle cell anemia.
Blood
2012
, vol. 
119
 
20
(pg. 
4587
-
4596
)
Google Scholar
Crossref
Search ADS
PubMed
 
28
Miller
 
ST
Sleeper
 
LA
Pegelow
 
CH
et al. 
Prediction of adverse outcomes in children with sickle cell disease.
N Engl J Med
2000
, vol. 
342
 
2
(pg. 
83
-
89
)
Google Scholar
Crossref
Search ADS
PubMed
 
29
Quinn
 
CT
Shull
 
EP
Ahmad
 
N
Lee
 
NJ
Rogers
 
ZR
Buchanan
 
GR
Prognostic significance of early vaso-occlusive complications in children with sickle cell anemia.
Blood
2007
, vol. 
109
 
1
(pg. 
40
-
45
)
Google Scholar
Crossref
Search ADS
PubMed
 
30
Sebastiani
 
P
Nolan
 
VG
Baldwin
 
CT
et al. 
A network model to predict the risk of death in sickle cell disease.
Blood
2007
, vol. 
110
 
7
(pg. 
2727
-
2735
)
Google Scholar
Crossref
Search ADS
PubMed
 
31
Quinn
 
CT
Lee
 
NJ
Shull
 
EP
Ahmad
 
N
Rogers
 
ZR
Buchanan
 
GR
Prediction of adverse outcomes in children with sickle cell anemia: a study of the Dallas Newborn Cohort.
Blood
2008
, vol. 
111
 
2
(pg. 
544
-
548
)
Google Scholar
Crossref
Search ADS
PubMed
 
32
Kassim
 
AA
DeBaun
 
MR
The case for and against initiating either hydroxyurea therapy, blood transfusion therapy or hematopoietic stem cell transplant in asymptomatic children with sickle cell disease.
Expert Opin Pharmacother
2014
, vol. 
15
 
3
(pg. 
325
-
336
)
Google Scholar
Crossref
Search ADS
PubMed
 
33
Meier
 
ER
Byrnes
 
C
Lee
 
YT
et al. 
Increased reticulocytosis during infancy is associated with increased hospitalizations in sickle cell anemia patients during the first three years of life.
PLoS ONE
2013
, vol. 
8
 
8
pg. 
e70794
 
Google Scholar
Crossref
Search ADS
PubMed
 
34
Quinn
 
CT
Rogers
 
ZR
Buchanan
 
GR
Survival of children with sickle cell disease.
Blood
2004
, vol. 
103
 
11
(pg. 
4023
-
4027
)
Google Scholar
Crossref
Search ADS
PubMed
 
35
Platt
 
OS
Brambilla
 
DJ
Rosse
 
WF
et al. 
Mortality in sickle cell disease. Life expectancy and risk factors for early death.
N Engl J Med
1994
, vol. 
330
 
23
(pg. 
1639
-
1644
)
Google Scholar
Crossref
Search ADS
PubMed
 
36
Elmariah
 
H
Garrett
 
ME
De Castro
 
LM
et al. 
Factors associated with survival in a contemporary adult sickle cell disease cohort.
Am J Hematol
2014
, vol. 
89
 
5
(pg. 
530
-
535
)
Google Scholar
Crossref
Search ADS
PubMed
 
37
Powars
 
DR
Hiti
 
A
Ramicone
 
E
Johnson
 
C
Chan
 
L
Outcome in hemoglobin SC disease: a four-decade observational study of clinical, hematologic, and genetic factors.
Am J Hematol
2002
, vol. 
70
 
3
(pg. 
206
-
215
)
Google Scholar
Crossref
Search ADS
PubMed
 
38
Smith
 
WR
Penberthy
 
LT
Bovbjerg
 
VE
et al. 
Daily assessment of pain in adults with sickle cell disease.
Ann Intern Med
2008
, vol. 
148
 
2
(pg. 
94
-
101
)
Google Scholar
Crossref
Search ADS
PubMed
 
39
McClish
 
DK
Penberthy
 
LT
Bovbjerg
 
VE
et al. 
Health related quality of life in sickle cell patients: the PiSCES project.
Health Qual Life Outcomes
2005
, vol. 
3
 pg. 
50
 
Google Scholar
Crossref
Search ADS
PubMed
 
40
de Montalembert
 
M
Roberts
 
I
Sickle cell disease: primum non nocere (first do no harm).
Haematologica
2010
, vol. 
95
 
1
(pg. 
4
-
5
)
Google Scholar
Crossref
Search ADS
PubMed
 
41
Telfer
 
P
Coen
 
P
Chakravorty
 
S
et al. 
Clinical outcomes in children with sickle cell disease living in England: a neonatal cohort in East London.
Haematologica
2007
, vol. 
92
 
7
(pg. 
905
-
912
)
Google Scholar
Crossref
Search ADS
PubMed
 
42
Quinn
 
CT
Rogers
 
ZR
McCavit
 
TL
Buchanan
 
GR
Improved survival of children and adolescents with sickle cell disease.
Blood
2010
, vol. 
115
 
17
(pg. 
3447
-
3452
)
Google Scholar
Crossref
Search ADS
PubMed
 
43
Gluckman
 
E
 
Allogeneic transplantation strategies including haploidentical transplantation in sickle cell disease. Hematology Am Soc Hematol Educ Program. 2013;370-376
44
Lukusa
 
AK
Vermylen
 
C
Vanabelle
 
B
et al. 
Bone marrow transplantation or hydroxyurea for sickle cell anemia: long-term effects on semen variables and hormone profiles.
Pediatr Hematol Oncol
2009
, vol. 
26
 
4
(pg. 
186
-
194
)
Google Scholar
Crossref
Search ADS
PubMed
 
45
Serjeant
 
GR
Serjeant
 
BE
Mason
 
KP
Hambleton
 
IR
Fisher
 
C
Higgs
 
DR
The changing face of homozygous sickle cell disease: 102 patients over 60 years.
Int J Lab Hematol
2009
, vol. 
31
 
6
(pg. 
585
-
596
)
Google Scholar
Crossref
Search ADS
PubMed
 
46
Lanzkron
 
S
Carroll
 
CP
Haywood
 
C
Mortality rates and age at death from sickle cell disease: U.S., 1979-2005.
Public Health Rep
2013
, vol. 
128
 
2
(pg. 
110
-
116
)
Google Scholar
Crossref
Search ADS
PubMed
 
47
Hassell
 
KL
Population estimates of sickle cell disease in the U.S.
Am J Prev Med
2010
, vol. 
38
 
4 Suppl
(pg. 
S512
-
S521
)
Google Scholar
Crossref
Search ADS
PubMed
 
48
Hamideh
 
D
Alvarez
 
O
Sickle cell disease related mortality in the United States (1999-2009).
Pediatr Blood Cancer
2013
, vol. 
60
 
9
(pg. 
1482
-
1486
)
Google Scholar
Crossref
Search ADS
PubMed
 
49
Wierenga
 
KJJ
Hambleton
 
IR
Lewis
 
NA
Unit
 
SC
Survival estimates for patients with homozygous sickle-cell disease in Jamaica: a clinic-based population study.
Lancet
2001
, vol. 
357
 
9257
(pg. 
680
-
683
)
Google Scholar
Crossref
Search ADS
PubMed
 
50
Swanson
 
ME
Grosse
 
SD
Kulkarni
 
R
Disability among individuals with sickle cell disease: literature review from a public health perspective.
Am J Prev Med
2011
, vol. 
41
 
6 Suppl 4
(pg. 
S390
-
S397
)
Google Scholar
Crossref
Search ADS
PubMed
 
51
Dampier
 
C
LeBeau
 
P
Rhee
 
S
et al. 
Comprehensive Sickle Cell Centers (CSCC) Clinical Trial Consortium (CTC) Site Investigators
Health-related quality of life in adults with sickle cell disease (SCD): a report from the comprehensive sickle cell centers clinical trial consortium.
Am J Hematol
2011
, vol. 
86
 
2
(pg. 
203
-
205
)
Google Scholar
Crossref
Search ADS
PubMed
 
52
Emond
 
AM
Holman
 
R
Hayes
 
RJ
Serjeant
 
GR
Priapism and impotence in homozygous sickle cell disease.
Arch Intern Med
1980
, vol. 
140
 
11
(pg. 
1434
-
1437
)
Google Scholar
Crossref
Search ADS
PubMed
 
53
Madu
 
AJ
Ubesie
 
A
Ocheni
 
S
et al. 
Priapism in homozygous sickle cell patients: important clinical and laboratory associations.
Med Princ Pract
2014
, vol. 
23
 
3
(pg. 
259
-
263
)
Google Scholar
Crossref
Search ADS
PubMed
 
54
Broderick
 
GA
Priapism and sickle-cell anemia: diagnosis and nonsurgical therapy.
J Sex Med
2012
, vol. 
9
 
1
(pg. 
88
-
103
)
Google Scholar
Crossref
Search ADS
PubMed
 
55
Serjeant
 
GR
Loy
 
LL
Crowther
 
M
Hambleton
 
IR
Thame
 
M
Outcome of pregnancy in homozygous sickle cell disease.
Obstet Gynecol
2004
, vol. 
103
 
6
(pg. 
1278
-
1285
)
Google Scholar
Crossref
Search ADS
PubMed
 
56
Fenelon
 
VM
Viana
 
MB
Aguiar
 
RA
Pregnancy in patients with sickle cell disease: maternal and perinatal outcomes [published online ahead of print May 28, 2014].
J Matern Fetal Neonatal Med
57
Boulet
 
SL
Okoroh
 
EM
Azonobi
 
I
Grant
 
A
Craig Hooper
 
W
Sickle cell disease in pregnancy: maternal complications in a Medicaid-enrolled population.
Matern Child Health J
2013
, vol. 
17
 
2
(pg. 
200
-
207
)
Google Scholar
Crossref
Search ADS
PubMed
 
58
Berthaut
 
I
Guignedoux
 
G
Kirsch-Noir
 
F
et al. 
Influence of sickle cell disease and treatment with hydroxyurea on sperm parameters and fertility of human males.
Haematologica
2008
, vol. 
93
 
7
(pg. 
988
-
993
)
Google Scholar
Crossref
Search ADS
PubMed
 
59
Lukusa
 
AK
Vermylen
 
C
 
Use of hydroxyurea from childhood to adult age in sickle cell disease: semen analysis. Haematologica. 2008;93(11):e67
60
Kamani
 
N
Lantos
 
JD
Myers
 
D
Kahn
 
JP
Ethical considerations in pediatric BMT donors and recipients.
Biol Blood Marrow Transplant
2011
, vol. 
17
 
1 Suppl
(pg. 
S132
-
S136
)
Google Scholar
Crossref
Search ADS
PubMed
 
61
Kamani
 
NR
Walters
 
MC
Carter
 
S
et al. 
Unrelated donor cord blood transplantation for children with severe sickle cell disease: results of one cohort from the phase II study from the Blood and Marrow Transplant Clinical Trials Network (BMT CTN).
Biol Blood Marrow Transplant
2012
, vol. 
18
 
8
(pg. 
1265
-
1272
)
Google Scholar
Crossref
Search ADS
PubMed
 
62
Bolaños-Meade
 
J
Fuchs
 
EJ
Luznik
 
L
et al. 
HLA-haploidentical bone marrow transplantation with posttransplant cyclophosphamide expands the donor pool for patients with sickle cell disease.
Blood
2012
, vol. 
120
 
22
(pg. 
4285
-
4291
)
Google Scholar
Crossref
Search ADS
PubMed
 
63
Dallas
 
MH
Triplett
 
B
Shook
 
DR
et al. 
Long-term outcome and evaluation of organ function in pediatric patients undergoing haploidentical and matched related hematopoietic cell transplantation for sickle cell disease.
Biol Blood Marrow Transplant
2013
, vol. 
19
 
5
(pg. 
820
-
830
)
Google Scholar
Crossref
Search ADS
PubMed
 
64
Kharbanda
 
S
Smith
 
AR
Hutchinson
 
SK
et al. 
Unrelated donor allogeneic hematopoietic stem cell transplantation for patients with hemoglobinopathies using a reduced-intensity conditioning regimen and third-party mesenchymal stromal cells.
Biol Blood Marrow Transplant
2014
, vol. 
20
 
4
(pg. 
581
-
586
)
Google Scholar
Crossref
Search ADS
PubMed
 
65
Railey
 
MD
Lokhnygina
 
Y
Buckley
 
RH
 
Long-term clinical outcome of patients with severe combined immunodeficiency who received related donor bone marrow transplants without pretransplant chemotherapy or post-transplant GVHD prophylaxis. J Pediatr. 2009;155(6):834-840
66
Eisner
 
MD
August
 
CS
Impact of donor and recipient characteristics on the development of acute and chronic graft-versus-host disease following pediatric bone marrow transplantation.
Bone Marrow Transplant
1995
, vol. 
15
 
5
(pg. 
663
-
668
)
Google Scholar
PubMed
 
67
Kondo
 
M
Kojima
 
S
Horibe
 
K
Kato
 
K
Matsuyama
 
T
Risk factors for chronic graft-versus-host disease after allogeneic stem cell transplantation in children.
Bone Marrow Transplant
2001
, vol. 
27
 
7
(pg. 
727
-
730
)
Google Scholar
Crossref
Search ADS
PubMed
 
68
Zecca
 
M
Prete
 
A
Rondelli
 
R
et al. 
AIEOP-BMT Group. Italian Association for Pediatric Hematology and Oncology-Bone Marrow Transplant
Chronic graft-versus-host disease in children: incidence, risk factors, and impact on outcome.
Blood
2002
, vol. 
100
 
4
(pg. 
1192
-
1200
)
Google Scholar
Crossref
Search ADS
PubMed
 
69
Toubert
 
A
Glauzy
 
S
Douay
 
C
Clave
 
E
Thymus and immune reconstitution after allogeneic hematopoietic stem cell transplantation in humans: never say never again.
Tissue Antigens
2012
, vol. 
79
 
2
(pg. 
83
-
89
)
Google Scholar
Crossref
Search ADS
PubMed
 
70
Chou
 
ST
Jackson
 
T
Vege
 
S
Smith-Whitley
 
K
Friedman
 
DF
Westhoff
 
CM
High prevalence of red blood cell alloimmunization in sickle cell disease despite transfusion from Rh-matched minority donors.
Blood
2013
, vol. 
122
 
6
(pg. 
1062
-
1071
)
Google Scholar
Crossref
Search ADS
PubMed
 
71
McPherson
 
ME
Anderson
 
AR
Castillejo
 
MI
et al. 
HLA alloimmunization is associated with RBC antibodies in multiply transfused patients with sickle cell disease.
Pediatr Blood Cancer
2010
, vol. 
54
 
4
(pg. 
552
-
558
)
Google Scholar
PubMed
 
72
Desmarets
 
M
Cadwell
 
CM
Peterson
 
KR
Neades
 
R
Zimring
 
JC
Minor histocompatibility antigens on transfused leukoreduced units of red blood cells induce bone marrow transplant rejection in a mouse model.
Blood
2009
, vol. 
114
 
11
(pg. 
2315
-
2322
)
Google Scholar
Crossref
Search ADS
PubMed
 
73
Champlin
 
RE
Horowitz
 
MM
van Bekkum
 
DW
et al. 
Graft failure following bone marrow transplantation for severe aplastic anemia: risk factors and treatment results.
Blood
1989
, vol. 
73
 
2
(pg. 
606
-
613
)
Google Scholar
Crossref
Search ADS
PubMed
 
74
van Besien
 
K
Koshy
 
M
Anderson-Shaw
 
L
et al. 
Allogeneic stem cell transplantation for sickle cell disease. A study of patients’ decisions.
Bone Marrow Transplant
2001
, vol. 
28
 
6
(pg. 
545
-
549
)
Google Scholar
Crossref
Search ADS
PubMed
 
75
Kodish
 
E
Lantos
 
J
Stocking
 
C
Singer
 
PA
Siegler
 
M
Johnson
 
FL
Bone marrow transplantation for sickle cell disease. A study of parents’ decisions.
N Engl J Med
1991
, vol. 
325
 
19
(pg. 
1349
-
1353
)
Google Scholar
Crossref
Search ADS
PubMed
 
76
Smith
 
LA
Oyeku
 
SO
Homer
 
C
Zuckerman
 
B
Sickle cell disease: a question of equity and quality.
Pediatrics
2006
, vol. 
117
 
5
(pg. 
1763
-
1770
)
Google Scholar
Crossref
Search ADS
PubMed
 
© 2014 by The American Society of Hematology
2014
Sign in via your Institution