Diabetic Retinopathy Clinical Trial
To evaluate the effectiveness of both argon laser photocoagulation and aspirin therapy in
delaying or preventing progression of early diabetic retinopathy to more severe stages of
visual loss and blindness.
To help determine the best time to initiate photocoagulation treatment in diabetic
retinopathy.
To monitor closely the effects of diabetes mellitus and of photocoagulation on visual
function.
To produce natural history data that can be used to identify risk factors and test etiologic
hypotheses in diabetic retinopathy.
ETDRS was a multicenter, randomized clinical trial designed to evaluate argon laser
photocoagulation and aspirin treatment in the management of patients with nonproliferative
or early proliferative diabetic retinopathy. A total of 3,711 patients were recruited to be
followed for a minimum of 4 years to provide long-term information on the risks and benefits
of the treatments under study.
The eligibility criteria for the ETDRS were designed to include a broad range of macular
edema severity, from a few small hard exudates within a disc diameter of the fovea with
normal visual acuity to extensive cystoid spaces with a visual acuity of 20/200. All study
patients had one eye randomly assigned to immediate photocoagulation and the other eye to
deferral of photocoagulation until high-risk proliferative retinopathy developed. During
followup, additional photocoagulation was allowed for any degree of macular edema within the
eligibility range, but additional photocoagulation was required only for edema involving or
threatening the center of the macula. The term "clinically significant macular edema" was
coined to designate this level of severity.
The trial use of aspirin therapy was based on clinical observation and on aspirin's possible
mechanisms of action. Previous observations of diabetic patients who were taking large doses
of aspirin for rheumatoid arthritis showed that the prevalence of retinopathy in this group
was lower than the prevalence that would be expected in the diabetic population at large.
Evidence suggested that diabetic patients have altered platelet aggregation and
disaggregation, which may contribute to the capillary closure seen in retinopathy. This
abnormality is reversed by aspirin in vitro . However, because of aspirin's other possible
mechanisms of action and its well-known side effects, such as allergic, idiosyncratic, and
intolerance reactions, the use of this therapy in the ETDRS was carefully controlled and
monitored.
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Allocation: Randomized, Primary Purpose: Treatment
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