The Course of Response to Focal Photocoagulation for DME
Information source: National Eye Institute (NEI)
Information obtained from ClinicalTrials.gov on December 31, 2007
Link to the current ClinicalTrials.gov record.
Condition(s) targeted: Diabetic Retinopathy; Diabetic Macular Edema
Intervention: Laser photocoagulation (Procedure)
Phase: N/A
Status: Active, not recruiting
Sponsored by: National Eye Institute (NEI) Official(s) and/or principal investigator(s):
David Browning, M.D., Study Chair, Affiliation: Charlotte Eye, Ear, Nose and Throat Assoc., PA
Summary
The study involves the enrollment of subjects over 18 years of age with diabetic macular
edema who have not already been given maximal laser treatment. Subjects may only have one
study eye which will receive focal photocoagulation at baseline. The study objective is to
determine the course of changes in OCT measured macular thickness and visual acuity following
a single session of focal photocoagulation for center-involved DME. The response will be
evaluated separately in eyes with and without prior focal photocoagulation for DME. The
purpose is to determine the proportion of eyes that continue to improve at least 5 letters in
visual acuity or at least 10% in central retinal thickness after a session of focal
photocoagulation. In addition, the study will explore whether any baseline factors can be
identified that are predictive of the response.
All subjects will have follow-up visits 8 weeks and 16 weeks post treatment. At the 16-week
visit, study eyes are evaluated for change in retinal thickness and visual acuity from
baseline.
Treatment is to be deferred and follow up continued if visual acuity letter score has
improved by >5 or OCT central subfield thickness has decreased by >10% compared with
baseline.
If visual acuity letter score has not improved by at least 5 and OCT central subfield
thickness has not decreased by at least 10%, then the eye is classified as 'not improved'
and the investigator may provide additional treatment. Follow up ends for eyes that receive
additional treatment at this visit. However, if the investigator and participant elect to
defer additional treatment (even if deferral criteria are not met), then follow up will
continue until the study eye receives additional treatment for DME.
Eyes continuing in follow up have visits every 8 weeks (+1week) as long as there has been
continued improvement in visual acuity (letter score improved >5 ) or retinal thickness
(central subfield thickness decreased by >10%) compared with the visit 16 weeks earlier. The
longest follow-up time will be 48 weeks.
By providing information on the length of time during which clinically meaningful improvement
occurs following focal photocoagulation, clinicians will be better able to determine when
further photocoagulation or other treatments should be considered for persistent DME.
Depending on the results of this study, a future randomized clinical trial will be considered
comparing the more aggressive retreatment photocoagulation regimen currently serving as the
standard DRCR Network approach to focal photocoagulation for macular edema with the less
aggressive regimen evaluated in this protocol.
Clinical Details
Official title: The Course of Response to Focal Photocoagulation for Diabetic Macular Edema
Study design: Longitudinal, Defined Population, Prospective Study
Detailed description:
Focal photocoagulation is the only treatment that has been demonstrated to be beneficial for
diabetic macular edema. In the ETDRS, focal photocoagulation of eyes with macular edema
reduced the risk of moderate visual loss (decrease of 15 or more letters) by approximately
50% (from 24% to 12%, three years after initiation of treatment). For eyes with
center-involved DME and visual acuity worse than 20/40 that were treated with focal
photocoagulation, the 15-letter improvement rate at 1 year was 11% and at 3 years was 16%.
In the ETDRS, focal photocoagulation treatment for diabetic macular edema involved direct
treatment to discrete lesions between 500 microns and 3000 microns from the center of the
macula that were thought to be causing retinal thickening or hard exudates with or without
"grid" treatment to other macular areas of retinal thickening or non-perfusion. The lesions
treated directly included microaneurysms, identified on fluorescein angiography, that either
filled or leaked, intraretinal microvascular abnormalities (IRMA), or pruned capillaries that
leaked fluorescein. Grid treatment was applied in the ETDRS to areas of thickened retina that
showed diffuse fluorescein leakage or areas of non-perfusion identified as capillary dropout
on fluorescein angiography. Areas of non-perfusion in the macula could be treated with grid
at the discretion of the treating ophthalmologist. Areas that had both discrete lesions and
diffuse leakage or capillary dropout would receive a combination of direct and grid
treatment. Re-treatment was applied at four month intervals if clinically significant macular
edema persisted, one or more treatable lesions were identified, and the investigator believed
these lesions were responsible for the edema. The median number of focal laser treatments
applied in the ETDRS was 3. 8.
The mechanism of action of focal photocoagulation is not fully understood; however, it is
clear that the retinal pigment epithelium (RPE) absorbs the majority of the laser energy and
thermal injury occurs at the level of the RPE. Studies have shown that photocoagulation can
eventually result in retinal and apparent RPE atrophy 200-300% larger than the original laser
spot size. These areas of expanded atrophy can lead to loss of central vision, central
scotomata, and decreased color vision. Consequently, many retinal specialists today tend to
treat with lighter, less intense laser burns than originally specified in the ETDRS.
In addition to the concern regarding the spread of intense laser burns, there are a number of
other reasons that retinal specialists today have modified the treatment procedures
originally specified in the ETDRS protocol. These reasons include the advent of new lasers
and the clinical observation that different techniques, such as focal photocoagulation with
lighter burns or grid treatment alone, may be similar in beneficial effect as the original
ETDRS treatment protocol. A modified ETDRS focal photocoagulation protocol adapted from the
original ETDRS approach, has been adopted as the standard laser technique for DME used in
DRCRnet studies.
There are limited data on the course of visual acuity and central retinal thickness after a
single focal photocoagulation session for DME. In prior DRCRnet DME treatment protocols that
included a laser arm, according to the re-treatment protocol eyes received a second focal
photocoagulation session at 3. 5- 4 months (which was the first follow-up visit) unless there
was substantial improvement defined as at least a 50% decrease in retinal thickening of the
central subfield measurement on OCT. As a result, it is unknown what proportion of eyes with
lesser degrees of improvement would have continued to improve and the time course for further
improvement following the initial photocoagulation session given additional time. In one
study conducted by DRCRnet of eyes that had not been previously treated for DME, among 113
eyes in the modified ETDRS laser treatment group with baseline OCT central subfield >250
microns, a 50% or more reduction in OCT central subfield thickening was present at 3. 5 months
in only 28 (25%). The table below categorizes the 85 eyes that did not meet this measure of
improvement at 3. 5 months with regard to improvement in visual acuity of at least 5 letters
and/or reduction in central subfield thickness of at least 10%. The 5 letter reduction was
selected based on the 95% confidence interval for change determined in a study that evaluated
the validity and reliability of the electronic ETDRS visual acuity testing procedure that is
used in DRCRnet protocols. The 10% threshold was selected based on the DRCRnet OCT
reproducibility study which found that a 10% change in central subfield thickness was likely
to be real. Forty-seven (42%) eyes that met the protocol requirement for repeat
photocoagulation at the first follow-up visit had an improvement in either visual acuity (of
at least 5 letters), central subfield (of at least a 10% reduction), or both at this
follow-up visit.
Other DRCRnet protocols provide data on the course following a single photocoagulation
session through 4 months of follow up. In a pilot study designed to evaluate peribulbar
corticosteroids for mild DME (OCT central subfield thickness = 250 microns and visual acuity
20/40 or better at baseline), modified ETDRS focal photocoagulation was the treatment given
to the control group. Follow-up visits occurred after 1, 2, and 4 months before the eye was
eligible to be retreated. Twenty-one of the 37 eyes in the laser group had not been
previously treated with focal photocoagulation for DME and 17 eyes had been previously
treated with focal photocoagulation. A 50% or more reduction in OCT central subfield
thickening occurred in 11 (30%) of the 37 eyes at 17 weeks. Fourteen (38%) eyes that would
have met the criteria for re-treatment had an improvement in either visual acuity (of at
least 5 letters), central subfield (of at least 10%), or both at 17 weeks.
In another pilot study evaluating intravitreal bevacizumab for DME (OCT central subfield
thickness = 275 microns and visual acuity 20/32 or worse at baseline), modified ETDRS focal
photocoagulation was the treatment given to the control group. Follow-up visits occurred
after 3, 6, 9, and 12 weeks before the eye was eligible to be retreated. There were 7 eyes in
the laser group that had not been previously treated with focal photocoagulation for DME and
12 eyes that had been previously treated with focal photocoagulation. Among these 19 eyes, a
50% or more reduction in OCT central subfield thickening occurred in 3 (16%) at 12 weeks. Ten
(53%) eyes that would have met criteria for re-treatment had an improvement in either visual
acuity (of at least 5 letters), central subfield (of at least 10%), or both at 12 weeks.
The data from these three protocols indicate that a substantial number of eyes receiving
focal photocoagulation (either an initial course or repeat application) will show improvement
in central retinal thickness after 3-4 months that is at least 10% but is less than 50% of
the baseline thickening. It is for these eyes that further knowledge of the course of retinal
thickening and visual acuity without additional interventions is needed to assess whether the
present requirements for re-treatment are more aggressive than they need to be.
Eligibility
Minimum age: 18 Years.
Maximum age: N/A.
Gender(s): Both.
Criteria:
General Inclusion Criteria
To be eligible, the following inclusion criteria must be met:
Age >= 18 years
Diagnosis of diabetes mellitus (type 1 or type 2.
At least one eye meets the study eye criteria.
Able and willing to provide informed consent.
General Exclusion Criteria
A subject is not eligible if any of the following exclusion criteria are
present:
Significant renal disease, defined as a history of chronic renal failure requiring dialysis
or kidney transplant.
A condition that, in the opinion of the investigator, would preclude participation in the
study (e. g., unstable medical status including blood pressure, cardiovascular disease, and
glycemic control).
Blood pressure > 180/110 (systolic above 180 OR diastolic above 110).
Participation in an investigational trial within 30 days of enrollment that involved
treatment with any drug that has not received regulatory approval at the time of study
entry.
Subject is expecting to move out of the area of the clinical center to an area not covered
by another clinical center during the next 6 months.
Study Eye Inclusion Criteria
The subject must have one eye meeting all of the inclusion criteria and none of the
exclusion criteria listed below. If both eyes are eligible, the study eye is selected by
the investigator and subject.
Best corrected E-ETDRS visual acuity letter score >= 24 (i. e., 20/320 or better) within 8
days of enrollment.
On clinical exam, definite retinal thickening due to diabetic macular edema involving the
center of the macula.
OCT central subfield >=250 microns within 8 days of enrollment.
Media clarity, pupillary dilation, and subject cooperation sufficient for adequate
OCT.
Investigator believes that focal photocoagulation is the most appropriate treatment for the
DME.
Study Eye Exclusion Criteria
The following exclusions apply to the study eye only (i. e., they may be present for the
nonstudy eye):
Macular edema is considered to be due to a cause other than diabetic macular edema.
An ocular condition is present such that, in the opinion of the investigator, visual acuity
loss would not improve from resolution of macular edema (e. g., foveal atrophy, pigment
abnormalities, dense subfoveal hard exudates, significant macular ischemia, nonretinal
condition).
An ocular condition is present (other than diabetes) that, in the opinion of the
investigator, might affect macular edema or alter visual acuity during the course of the
study (e. g., vein occlusion, uveitis or other ocular inflammatory disease, neovascular
glaucoma, etc.).
Substantial cataract that, in the opinion of the investigator, is likely to be decreasing
visual acuity by 3 lines or more (i. e., cataract would be reducing acuity to 20/40 or worse
if eye was otherwise normal).
History of treatment for DME at any time in the past 4 months (such as focal/grid macular
photocoagulation, intravitreal or peribulbar corticosteroids, anti-VEGF drugs, or any other
treatment).
History of panretinal (scatter) photocoagulation (PRP) within 4 months prior to enrollment
or anticipated to be performed within next 6 months.
History of major ocular surgery (including vitrectomy, cataract extraction, scleral buckle,
any intraocular surgery, etc.) within prior 4 months or anticipated within the next 6
months.
History of YAG capsulotomy performed within 2 months prior to enrollment.
Locations and Contacts
Southern California Desert Retina Consultants, MC, Palm Springs, California 92262, United States
Central Florida Retina Institute, Lakeland, Florida 33805, United States
Retina Vitreous Consultants, Ft. Lauderdale, Florida, United States
Retina Consultants of Southwest Florida, Fort Myers, Florida 33912, United States
Southeast Retina Center, P.C., Augusta, Georgia, United States
Retina Associates of Hawaii, Inc., Honolulu, Hawaii 96813, United States
American Eye Institute, New Albany, Indiana, United States
Raj K. Maturi, M.D., P.C., Indianapolis, Indiana, United States
Paducah Retinal Center, Paducah, Kentucky, United States
Retina and Vitreous Associates of Kentucky, Lexington, Kentucky, United States
Maine Vitreoretinal Consultants, Bangor, Maine 04401, United States
Elman Retina Group, P.A., Baltimore, Maryland 21237, United States
Joslin Diabetes Center, Boston, Massachusetts 02215, United States
Ophthalmic Consultants of Boston, Boston, Massachusetts 02114, United States
Southern New England Retina Associates, Attleboro, Massachusetts 02703, United States
Vitreo-Retinal Associates, Grand Rapids, Michigan 49525, United States
Associated Retina Consultants, Williamsburg, Michigan 49690, United States
Delaware Valley Retina Associates, Lawrenceville, New Jersey 08648, United States
Retina-Vitreous Surgeons of Central New York, PC, Syracuse, New York, United States
University of Rochester, Rochester, New York 14642, United States
Charlotte Eye, Ear, Nose and Throat Assoc., PA, Charlotte, North Carolina, United States
University of North Carolina, Dept. of Ophthalmology, Chapel Hill, North Carolina 27599, United States
Retina Associates of Cleveland, Inc., Beachwood, Ohio 44122, United States
Casey Eye Institute, Portland, Oregon 97239, United States
Carolina Retina Center, Columbia, South Carolina, United States
Palmetto Retina Center, Columbia, South Carolina, United States
Retina and Vitreous of Texas, Houston, Texas, United States
Retina Research Center, Austin, Texas, United States
Texas Retina Associates, Dallas, Texas, United States
Texas Retina Associates, Lubbock, Texas, United States
Charles A. Garcia, PA & Associates, Houston, Texas 77002, United States
University of Wisconsin-Madison, Dept. of Ophthalmology, Madison, Wisconsin 53705, United States
Additional Information
NEI Clinical Studies Database Diabetic Retinopathy Clinical Research Network
Starting date: January 2007
Last updated: August 9, 2007
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