Anemia, Sickle Cell Clinical Trial
To continue to follow the newborn cohort and the over-35 years of age cohort from the Cooperative Study of Sickle Cell Disease (CSSCD), a study of the natural history of sickle cell disease.
BACKGROUND:
The Cooperative Study of Sickle Cell Disease was initiated in 1977 to determine the natural
history of sickle cell disease from birth to death in order to identify those factors
contributing to the morbidity and mortality of the disease. Patients in the study had been
followed previously in CSSCD.
Follow-up of the newborn cohort provided data demonstrating that life-threatening septicemia
can occur as early as four months of age, and that the incidence of septicemia in children
with sickle cell disease is higher than previously reported. Serial measurements of pocked
or vesiculated red blood cells determined the onset of splenic dysfunction. The loss of
splenic function has been characterized by genotype and the observed patterns of loss of
splenic function were different developmentally depending on the sickle hemoglobinopathy
syndrome.
Growth retardation, which becomes obvious around seven years of age, has no relationship to
reported family income. Prophylactic oral penicillin can decrease morbidity and mortality
associate with pneumococcal septicemia. The newborn infant cohort was unique in determining
issues related to the natural history of the disease because the information was prospective
and has been captured in the database. The complex database permitted an opportunity to
determine outcomes, risk factors, and the application of the severity index to determine the
spectrum of severity.
Follow-up of the over-35 cohort is important because it was not so long ago that it was
estimated that 50 percent of patients with sickle cell anemia in the United States died
before their twentieth birthday. However, data accumulated over the past eight years by the
CSSCD demonstrates that this is incorrect. Survival beyond the age of forty suggests that
surviving patients are somehow different from other patients with a high mortality in the
earlier years. Therefore, they constitute a cohort of special interest, and the reasons for
prolonged survival in this disease remain to be well documented prospectively. Technology is
now available to identify genetic differences which may influence survival.
Based on the findings of the earlier CSSCD, the Blood Diseases and Resources Advisory
Committee Red Cell Working Group recommended this initiative which was approved by the May
1987 National Heart, Lung, and Blood Advisory Council. The Request for Proposals was
released in February 1988 and awards made in October 1988.
DESIGN NARRATIVE:
Follow-up of the newborn cohort continued in order to better understand the severity, onset
of early organ damage, and risk factors. Patients were given an entry evaluation consisting
of interim history, complete physical examination, complete blood count, urinalysis, blood
drawn for haplotype determination and for the serum bank, magnetic resonance imaging of the
brain, pulmonary function tests with arterial blood gas, and psychomotor tests. Patients had
interim assessments at six months and annual assessments as well as an exit assessment in
the fourth or fifth years. The exit assessment was the same as the entry assessment.
Follow-up of the over-35 cohort continued in order to better understand factors that
contribute to longevity. Entry evaluation consisted of interim history, complete physical
examination, complete blood count, urinalysis, blood drawn for haplotype determination and
for the serum bank, cardiac MUGA, and renal and pulmonary function tests. Follow-up was
yearly with an exit evaluation in the fourth or fifth years.
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