ORLANDO — Treatment with fenofibrate led to a substantial drop in the need for laser treatments for retinopathy in a controlled trial of nearly 10,000 patients with type 2 diabetes.
Physicians should “consider using fenofibrate on all patients with diabetes, even patients already on a statin and at their target lipid levels, to further reduce their risk and microvascular complications,” Dr. Anthony C. Keech said at an industry-sponsored press briefing during the annual scientific sessions of the American Heart Association.
“Having a new tool to deal with [diabetic retinopathy] is very exciting. It's exciting to use it to treat patients, and it opens a whole new area of research,” commented Dr. Virgil Brown, who is professor of internal medicine at Emory University, Atlanta.
The benefits of fenofibrate for microvascular disease of diabetes appeared to extend beyond its significant effect on retinopathy. Patients treated with fenofibrate also had less progression of albuminuria, and fewer amputations, Dr. Keech and his associates reported.
“The results were very clear-cut. It's very hard to make a coherent argument not to use fenofibrate” in patients with diabetes, said Dr. Keech, professor of medicine, cardiology, and epidemiology at the University of Sydney. “This is a unique finding in a lipid-modifying drug. We don't see the effect with statin treatment.”
Dr. Frank Sachs, professor of medicine at Harvard Medical School, Boston, agreed. “It would be very easy to recommend fenofibrate for any diabetes patient with the earliest sign of retinopathy. That might be the first step in trying to translate these findings to clinical recommendations,” he commented.
The new retinopathy findings came from a prespecified, tertiary analysis in the Fenofibrate Intervention and Event Lowering in Diabetes (FIELD) trial, which involved 9,795 patients with type 2 diabetes at 63 centers in Australia, New Zealand, and Finland. The study's primary end point was the rate of cardiovascular events—cardiovascular deaths, nonfatal myocardial infarctions, strokes, and coronary revascularization procedures—during 5 years of follow-up. Treatment with 200 mg daily of micronized fenofibrate cut this rate by 11%, compared with placebo, an effect that was not statistically significant (Lancet 2005;366:1849–61).
In the analysis of retinopathy end points, the 4,895 patients on fenofibrate had a 3.4% rate of all laser eye treatments, compared with a 4.9% rate in 4,900 placebo patients, a 37% relative risk reduction that was highly significant. The relative risk of a first laser treatment was cut by about 30% in all patients, including those who developed macular edema and those with proliferative retinopathy.
The results were released by the Lancet on the same day as the briefing (Lancet 2007 [Epub doi:10.1016/S0140-6736(07)61607-9]).
The trial was initially sponsored by Laboratories Fournier; the company, which owned the rights to fenofibrate, was acquired by Solvay Pharmaceuticals in 2005. Fenofibrate (Tricor) is marketed in the United States by Abbott under license from Solvay, and it is marketed as Lipanthyl everywhere else by Solvay. Dr. Keech has served on an advisory board for Solvay and Abbott, and receives travel support from those companies to attend meetings. He is also listed on a patent application for fenofibrate.
Treatment with fenofibrate cut the rate of laser treatments in patients with no history of retinopathy and in patients who had retinopathy when they started the study, although the reduction was not statistically significant among the patients who already had retinopathy before starting treatment.
The trial also included an ophthalmologic substudy with 1,012 patients, in which serial retinal photography was used to assess patients in more detail. In this subgroup, treatment with fenofibrate slowed development of a two-step progression of retinopathy on the Early Treatment Diabetic Retinopathy Study scale among patients with pre-existing retinopathy: There was a 3% progression rate among patients treated with fenofibrate, compared with a 15% rate among patients treated with placebo, a statistically significant difference. Among patients with no retinopathy at baseline, the rate of two-step progression was virtually the same in the two treatment groups.
The primary end point for this substudy was the overall rate of two-step progression of retinopathy among all patients. The rate was 12.3% in the placebo group and 9.6% in the fenofibrate group, a difference that was not statistically significant.
The safety profiles of fenofibrate and placebo were similar during 5 years of treatment.
Several weaknesses in the study's design were noted in an editorial by Dr. Rafael Simó and Dr. Cristina Hernández, of the Diabetes Research Unit at Vall d'Hebron University Hospital, Barcelona, that accompanied the printed version of the new report. Retinal photographs were not routinely collected for all patients in the FIELD trial, which makes it impossible to confirm the retinal status of most patients (Lancet 2007 Nov. 6 [Epub doi:10.1016/S0140-6736(07)61608-0]).