Sickle Cell Disease Clinical Trial
Official title:
Abciximab (ReoPro) as a Therapeutic Intervention for Sickle Cell Vaso-Occlusive Pain Crisis
The purpose of this study is to determine whether giving abciximab (ReoPro) to children with sickle cell disease who are hospitalized for acute pain crisis will improve their pain and shorten the time spent in the hospital, when compared with standard supportive care.
Sickle cell disease (SCD) is one of the more common genetic diseases worldwide, affecting
approximately 1 in 500 African-Americans and 1 in 1000 Hispanic-Americans. A single amino
acid substitution decreases the solubility of deoxygenated hemoglobin, leading to polymer
formation and subsequent distortion of erythrocyte shape from the normal biconcave disc into
a relatively rigid crescent or sickle shape. Initially reversible, the polymer formation and
shape distortion eventually becomes permanent. Clinical manifestations of sickle cell
disease relate both to increased clearance of these misshapen erythrocytes (causing a
chronic hemolytic anemia) as well as occlusion of small (and sometimes large) blood vessels.
Vaso-occlusive phenomena are responsible for much of the acute morbidity of sickle cell
disease, including episodes of pain resulting from bone infarcts, splenic infarction with a
secondary increased risk of infection, and a relatively high incidence of ischemic stroke
(~10% in the first 2 decades of life). In addition, chronic and cumulative ischemic episodes
contribute to long-term morbidity (including avascular necrosis of bone, retinopathy, renal
insufficiency, and pulmonary hypertension) and a significantly shortened life span.
Vaso-occlusive pain crises often require hospitalization for the administration of
parenteral narcotics; the average duration of hospitalization is 4-5 days, and a significant
proportion of patients experience multiple crises per year. In most episodes, pain continues
to intensify over the first 2-3 days before beginning to abate, suggesting that there is
ongoing extension of tissue damage for some time following initiation of the episode; also,
many patients will develop additional foci of pain even during the course of
hospitalization.
While direct mechanical blockage of small vessels by sickled erythrocytes is undoubtedly an
important factor in vaso-occlusion, there are other secondary phenomena that are likely to
contribute to these episodes, including increased erythrocyte adhesion to the endothelium of
post-capillary venules. SCD patients also exhibit chronic pro-coagulation changes in soluble
clotting factors, as well as increased platelet number and activation. The relative
contribution of these various changes to the pathophysiology of vaso-occlusive crises is
unclear. One published study showed that the antiplatelet drug ticlopidine decreased
frequency, duration, and severity of pain crises in SCD patients, suggesting that the
increase in platelet activation does indeed contribute to vaso-occlusion.
Current therapy for vaso-occlusive pain crises is mostly supportive (maintaining adequate
hydration and oxygenation and administering pain medication). With the possible exception of
exchange transfusion—a procedure with significant potential morbidity—there is no therapy
that directly targets the vaso-occlusion.
Abciximab (ReoPro) is the Fab fragment of the chimeric human-mouse monoclonal antibody 7E3.
It avidly binds to both glycoprotein IIb/IIIa and to integrin αvβ3, and so would potentially
inhibit both erythrocyte binding to vascular endothelial as well as platelet adhesion, thus
targeting two separate mechanisms that are felt to be components of the vaso-occlusive
phenomenon in SCD.
The relatively prolonged course of most pain crises—which typically involves increasing
intensity of pain and often development of new areas of pain over the first few
days—suggests that treatment during the early phases of a crisis might be effective in
ameliorating the course of the episode, resulting not only in decreased acute morbidity but
possibly also in less long-term tissue damage. The study hypothesis is that administration
of abciximab early in the course of a vaso-occlusive sickle cell pain crisis will reduce the
median length of hospitalization without an accompanying increase in bleeding or other
serious complications.
Participants will be randomized in a double blind fashion to receive either abciximab
(ReoPro) or placebo intravenously over 12 hours. Randomization will be stratified by sickle
cell genotype: Sickle Cell Anemia (SS) vs. Sickle-Hemoglobin C Disease (SC). All patients
will receive standard supportive care, including hydration, supplemental oxygen as needed to
maintain oxygen saturation >92%, scheduled use of NSAIDS, and narcotics titrated to effect.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator), Primary Purpose: Treatment
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