Sickle Cell Disease Clinical Trial
Official title:
Spectralis HRA+OCT Imaging of the Retina With Autofluorescence in Sickle Cell Disease
To determine the retinal and choroidal thickness in patients with sickle cell disease compared to age, race matched population without sickle cell disease to allow a better understanding of the clinical manifestations of sickle cell retinopathy. The purpose of this research study is to evaluate the relationship between sickle cell disease and the eye. The research study is recruiting African American population with or without Sickle Cell Disease. The investigator in charge of this study is Dr E. Bowie. Approximately 60 subjects of both sexes will be enrolled at the Medical University of South Carolina.
About 10% of African Americans have an abnormal hemoglobin gene. About 8% of African
Americans are heterozygous for Hb S. In the United States, sickle cell anemia primarily
occurs in the black population, with approximately 0.2% of African American children
afflicted by this disease. The prevalence in adults is lower because of the decrease in life
expectancy. The Storm Eye Institute at the Medical University of South Carolina (MUSC) is
uniquely situated geographically and epidemiologically to study the interaction between
sickle cell disease and the retina. The frequency of sickle cell trait (Hb AS) in
African-Americans of Charleston County is 16%, twice the national average of 8% in
African-Americans. This is thought to be due to the autosomal recessive inheritance of
sickle cell disease, and the genetic roots and relative isolation of the Sea Island Gullah
population (Pollitzer 1999).
Variations in the alteration of the amino acid sequence on the globin chain produce
variations in the disease's expression. The four forms of the disease are often referred to
by their genotype: sickle cell trait (AS), sickle cell anemia (SS), sickle cell disease (SC)
and sickle cell thalassemia (SThal).
Systemically, the sickle cell anemia variation (SS) produces the most symptoms. With respect
to the eye, the sickle cell disease mutation (SC) produces the most effects.
The widely accepted pathogenesis for sickle cell retinopathy is vasoocclusion that leads to
retinal hypoxia, ischemia, infarction, neovascularization, and fibrovascularization. In
sickle cell anemia, the amino acid substitution valine for glutamate occurs on the beta
chain at the sixth position. This substitution, combined with conditions that may promote
sickling (ie, acidosis, hypoxia), triggers the deoxygenated Hb S to polymerize, making the
erythrocyte rigid. This rigidity is partially responsible for the vasoocclusion.
Vasoocclusion also is in part due to the interaction between sickled cells and the vascular
endothelium. The adherence of sickled cells to the endothelium triggers an inflammatory
process with the release of inflammatory agents. The result of this cascade is vascular
stasis, hemolysis, and vasoocclusion of the capillary beds.
Classically, posterior segment changes are classified by either nonproliferative sickle
retinopathy (NPSR) or proliferative sickle retinopathy (PSR). In NPSR, the retinal changes
do not involve neovascularization as they do in PSR. The use of Spectralis HRA+OCT gives us
visualization of the individual layers of the retina to determine if there are underlying
changes not seen clinically in the gross ophthalmic posterior segment exam. This knowledge
will aid the care of African-Americans with sickle cell disease to enable greater
understanding of the ocular disease progression leading to earlier eye screenings, possible
novel treatments and ultimately visual loss prevention.
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Observational Model: Case Control, Time Perspective: Prospective
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