Diabetic Retinopathy Clinical Trial
Official title:
Pilot Study of Peribulbar Triamcinolone Acetonide for Diabetic Macular Edema
This study will evaluate which of the three following treatment options is better for
diabetic macular edema: laser alone, steroid injection alone, or steroid injection followed
by laser. Macular edema is a swelling in the small central part of the retina - the part of
the retina that is used for sharp, straight-ahead vision. Laser treatment is the only
treatment that has been proven to be beneficial for diabetic macular edema. It reduces the
swelling and lessens the chance of further vision loss, but it does not improve vision.
Triamcinolone is a steroid drug that decreases inflammation and scarring. Injections of the
drug have decreased macular edema in some patients and improved vision. Swelling may return,
requiring repeat injections, and it is not known if the vision improvement is permanent.
This 3-year study will examine and compare the benefits and side effects of both treatments,
alone and in combination.
Patients 18 years of age and older with diabetic macular edema may be eligible for this
study. Participants undergo the following tests and procedures.
At the beginning of the study:
- Blood tests to measure HbA1C (measure of diabetes control).
- Measurement of blood pressure.
- Eye examination to assess visual acuity (eye chart test) and eye pressure, and to
examine pupils, lens, retina and eye movements. The pupils are dilated with drops for
this examination.
- Optical coherence tomography (OCT) to measure retinal thickness. This test shines a
light into the eye and produces cross-sectional pictures of the retina. These
measurements are repeated during the study to determine if retinal thickening is
getting better or worse, or staying the same.
Photographs of the retina and lens. A special camera with bright flashes is used to take
these photographs.
Treatments
Some patients will have one eye treated and some patients will have both eyes treated. The
treatment for a given individual is determined by chance:
- Triamcinolone acetonide injection alone. The steroid is injected in the tissue around
the eye. Two injection procedures are used in the study, differing in their location
and dose. Numbing drops are placed over the area to be injected and the steroid is
injected.
- Laser treatment alone. The surface of the eye is numbed with drops and a contact lens
is placed on the eye during the laser beam application. Before the treatment, patients
may have fluorescein angiography, in which pictures of the retina are taken using a
yellow dye. The dye is injected into a vein and travels to the blood vessels in the
eye. The camera flashes a blue light in the eye and takes pictures that show the amount
of dye leakage into the retina. Treatments may be repeated at several visits.
- Triamcinolone acetonide plus laser treatment. Patients who receive both the steroid
injection and laser have the steroid injection first and the laser treatment 1 month
later.
Follow-up
Patients return to the clinic for follow-up visits at 1, 2, 4, 8, 12, 24 and 36 months, or
more often if needed, after the initial treatment for an eye exam, measurement of visual
acuity, and OTC. Photographs of the retina are taken at the 4- and 8-month visits and at the
1-, 2- and 3-year visits. Fluorescein angiography may be done at 4 months. Blood pressure is
measured at the 1-, 2- and 3-year visits, and an HbA1c blood test is done at 4 and 8 months
and at the yearly visits. Participants may be asked to complete a questionnaire once a year
about their vision and medical condition. Treatment options are discussed at the 4- and
8-month visits.
Diabetic retinopathy is a major cause of visual impairment in the United States. Diabetic
macular edema (DME) is a manifestation of diabetic retinopathy that produces loss of central
vision. Data from the Wisconsin Epidemiologic Study of Diabetic Retinopathy (WESDR) estimate
that after 15 years of known diabetes, the prevalence of diabetic macular edema is
approximately 20% in patients with type 1 diabetes mellitus (DM), 25% in patients with type
2 DM who are taking insulin, and 14% in patients with type 2 DM who do not take insulin.
In a review of three early studies concerning the natural history of diabetic macular edema,
Ferris and Patz found that 53% of 135 eyes with diabetic macular edema, presumably all
involving the center of the macula, lost two or more lines of visual acuity over a two year
period. In the Early Treatment Diabetic Retinopathy Study (ETDRS), 33% of 221 untreated eyes
available for follow-up at the 3-year visit, all with edema involving the center of the
macula at baseline, had experienced a 15 or more letter decrease in visual acuity score
(equivalent to a doubling of the visual angle, e.g., 20/25 to 20/50, and termed "moderate
visual loss").
In the ETDRS, focal/grid photocoagulation of eyes with clinically significant macular edema
(CSME) reduced the risk of moderate visual loss by approximately 50% (from 24% to 12%, three
years after initiation of treatment). Therefore, 12% of treated eyes developed moderate
visual loss in spite of treatment. Furthermore, approximately 40% of treated eyes that had
retinal thickening involving the center of the macula at baseline still had thickening
involving the center at 12 months, as did 25% of treated eyes at 36 months.
Although several treatment modalities are currently under investigation, the only
demonstrated means to reduce the risk of vision loss from diabetic macular edema are laser
photocoagulation, as demonstrated by the ETDRS, and intensive glycemic control, as
demonstrated by the Diabetes Control and Complications Trial (DCCT) and the United Kingdom
Prospective Diabetes Study (UKPDS). In the DCCT, intensive glucose control reduced the risk
of onset of diabetic macular edema by 23% compared with conventional treatment. Long-term
follow-up of patients in the DCCT show a sustained effect of intensive glucose control, with
a 58% risk reduction in the development of diabetic macular edema for the DCCT patients
followed in the Epidemiology of Diabetes Interventions and Complications Study.
The frequency of an unsatisfactory outcome following laser photocoagulation in some eyes
with diabetic macular edema has prompted interest in other treatment modalities. One such
treatment is pars plana vitrectomy. These studies suggest that vitreomacular traction, or
the vitreous itself, may play a role in increased retinal vascular permeability. Removal of
the vitreous or relief of mechanical traction with vitrectomy and membrane stripping may be
followed by substantial resolution of macular edema and corresponding improvement in visual
acuity. However, this treatment may be applicable only to a specific subset of eyes with
diabetic macular edema. It also requires a complex surgical intervention with its inherent
risks, recovery time, and expense. Other treatment modalities such as pharmacologic therapy
with oral protein kinase C inhibitors and antibodies targeted at vascular endothelial growth
factor (VEGF) are under investigation.
The use of intravitreal corticosteroids is another treatment modality that has generated
recent interest. However, use of intravitreal corticosteroids generally has been reserved
for cases of DME in which there is at least moderate loss of visual acuity (e.g., worse than
20/40). This treatment generally has not been widely used for mild cases of DME due to
concerns about its potential risks, particularly glaucoma and cataract, relative to the
potential benefit.
Injection of corticosteroids around the eye (anterior subtenon's, posterior subtenon's,
retrobulbar) has been used as an alternative to intravitreal injection. Although data are
limited, it is presumed that the adverse effects on the eye are lower with an injection
around the eye compared with in the eye. There are also little data on the efficacy of this
treatment. This study is being conducted to collect pilot data on the safety and efficacy of
peribulbar corticosteroids to determine whether there is sufficient evidence of efficacy to
merit conducting a phase 3 randomized trial.
;
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