Do NSAIDs reduce the risk of progression to central
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Transcript Do NSAIDs reduce the risk of progression to central
The Diabetic Retinopathy Clinical
Research Network
A Phase II Evaluation of Topical NSAIDs in Eyes
with Non-Central Involved DME (Protocol R)
Scott Friedman MD
Protocol Chair
Sponsored by the National Eye Institute,
National Institutes of Health, U.S. Department of Health and Human Services.
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Study Question
Do topical non-steroidal anti-inflammatory
drugs (NSAIDs) have biological effects on
non-central involved DME?
Is macular volume influenced by using NSAID
drops in these eyes?
Do NSAIDs reduce the risk of progression to
central-involved DME?
Do NSAIDs reduce the risk of progression of
current non-central DME?
Do NSAIDs increase the chance of resolution of
non-central DME?
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Non-central DME
Clinical Definition - Retinal thickening due to
DME within 3000µm of, but not involving, the
center of macula
OCT definition - Retinal thickening due to DME
>2 SD beyond the normal value outside the
central subfield BUT <mean+2 SD in spectral
domain OCT machines within the central
subfield
Typical Management – observation until
center becomes thickened or until imminent
involvement of center is perceived
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Progression of
Non-center Involved DME
ETDRS
22% of study participants with non-center involved
(DME) by color fundus photographs assigned to
deferral of laser progressed to the center of the
macula by 1 year
Protein Kinase C-β DME Study Group
1/3 of eyes with non-central DME in the control
group progressed to the central subfield within 1
year
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Rationale for Use of NSAIDs on
Non-central DME
Possible role of inflammatory markers in DME
Some topical NSAID medicines reach
posterior segment of the eye
Observational studies showed some beneficial
effects of topical NSAID eye drops on DME
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Study Objectives
Primary Objective: Assess effect of topical
NSAIDs on retinal volume compared with
placebo in eyes with non-central DME
Secondary Objective: Assess effect of topical
NSAIDs on central subfield thickness, and to
compare the progression of non-central to
central DME as determined by spectral domain
OCT, and as determined by color fundus
photographs
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Nepafenac 0.1%(Nevanac®)
Converted to active metabolite, amfenac, in
ocular tissues
Nepafenac and amfenac inhibit both
cyclooxygenase (COX) I and II which catalyze the
formation of pro-inflammatory prostaglandins
that contribute to edema
FDA approved to treat pain and inflammation
associated with cataract surgery
Dosage: 1 drop, 3 times per day (TID)
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Study Design
Phase II
Multi-center
Randomized
Double-masked
Clinical Trial
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Study Design
Eligibility Criteria Met/Informed Consent
Run-In Phase/Enrollment Visit
30-60 days
Randomization Visit/Baseline
Nepafenac (TID)
Placebo (TID)
4 Months
4 Months
8 Months
8 Months
Primary outcome analysis at 1 year
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Subject Eligibility Criteria
Inclusion
• Age ≥ 18 years
• Diabetes mellitus (type 1 or type 2)
• Successful completion of the run-in
phase during which level of compliance
is more than 80%
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Subject Eligibility Criteria (cont.)
Exclusion
• Use of systemic corticosteroids or anti-VEGF
therapy
• Current use of prescription systemic NSAIDs.
• Auto-immune diseases judged to result in a
higher risk for corneal complications
• Known allergy to any component of the study
drug
• Blood pressure > 180/110 mmHg
• For women of child-bearing potential: pregnant
or lactating or intending to become pregnant
within the next 12 months
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Ocular Eligibility Criteria
Inclusion
• BCVA letter score ≥ 74 E-ETDRS (20/32 or better)
• By Clinical exam: Retinal thickening due to DME
within 3000 µm of but not involving the macular
center
• By OCT: Thickened non-central macular
subfields
• Media clarity
• If patient on other drop(s), willingness to comply
with a multi-drop regimen
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Ocular Eligibility Criteria (cont.)
CSF less than the gender-specific
mean thickness from a normal cohort
+ 2 SD, from one of the following SD
OCT machines:
Machine
Zeiss Cirrus
Optovue RTVue
Heidelberg Spectralis
Women
<290
<290
<305
Men
<305
<305
<320
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Ocular Eligibility Criteria (cont.)
Thickened non-central macular subfields
on OCT map must meet either one of the
following criteria:
• At least two subfields with thickness above
threshold* in spectral domain OCT machines
• At least one subfield with thickness of at
least 15μm above threshold in spectral
domain OCT machines
* Threshold= average normal + 2 standard deviations (SD)
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Ocular Eligibility Criteria (cont.)
Exclusion
• Focal/grid laser within the last 6 months or other treatment for DME
within the last 4 months
• Anticipated need to treat DME during the study
• NSAID eye drops use within the last 30 days or anticipated need for
such drops during the study
• History of PRP within 4 months prior to randomization
• Need for PRP in the 6 months following randomization
• Need for cataract surgery of study eye during the study
• Lipid in the fovea
• History of major ocular surgery within prior 4 months or anticipated
within the next 6 months
• An ocular condition, other than DME, that may affect VA
• YAG capsulotomy within 2 months of randomization
• Severe external ocular infection
• Aphakia
• Vitrectomy for any reason
• Cataract surgery within the prior 1 year
• Uncontrolled glaucoma
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How can investigators know if an
eye meets the protocol definition of
non-central DME?
OCT threshold grids provided by the
coordinating center for reference
Site personnel enter each subfield thickness
value directly into the study website
Computer algorithm determines if an eye meets
protocol criteria for non-central DME
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Study Eye
Both eyes may be evaluated for
eligibility, but only ONE eye will be
enrolled
If both eyes are eligible at the time of
enrollment, study eye will be
selected by investigator and study
participant
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Run-in Phase
Purpose
Filtering participants with poor compliance
Protocol
All eligibility criteria must be met before
enrollment
Artificial tears (Tears Naturale Forte®)-1
drop, 3 times per day
At least 30 days (30-60 days)
Compliance assessed at end of run-in
phase before randomization
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Randomization
All eligibility criteria, except VA and OCT,
will be reconfirmed again after run-in
phase
OCT and VA will not be reconfirmed at
randomization, provided investigator is
not planning on DME treatment
Randomization data will be the baseline
Study participants must show good
compliance with drops during the run-in
period
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Compliance Assessment and
Randomization Eligibility
Compliance will be assessed by
weighing bottles and comparing to
an expected weight
Study participants will be eligible for
randomization if compliance was
80% or more of expected
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Compliance Assessment
Digital scales are provided by the
Coordinating Center
Each bottle will be weighed prior to
dispending to study participant
Each bottle will be re-weighed at the next visit
One artificial tears bottle for run-in phase
Six drug/placebo bottles at randomization and
each follow-up visit
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Study Testing Procedures
E-ETDRS BCVA/
Eye Exam/
OCT
Enrollment
Randomization
4M
8M
12M
Run-in (30-60
days)
Baseline
±1M
±1M
±1M
X
X
X
X
X
X
Fundus Photo
Blood Pressure
X
X
X
HbA1c
Weighing
Bottles
X
X
X
X
X
X
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Guidelines for DME Treatment
Randomized eye drops
No treatment for DME is given unless
OCT CSF increases to more than gender and machine
specific mean+2 SD value, provided at least 10% increase
from baseline. Computer algorithm will calculate and
give appropriate alert.
Extenuating circumstances after protocol chair
discussion e.g. rapidly-developing cataract prior to
cataract surgery
Study participants will continue their study treatment
through 12 months regardless of whether treatment for
DME is received
Primary outcome analysis at 1 year
Outcome Measures
Primary Outcome
Mean change in macular retinal volume
(mm3) between baseline and 12 months
Secondary Outcomes
Progression of non-central involved DME
Correlation of progression of DME in OCT
and fundus photographs
Visual Acuity
Safety Outcomes
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Safety Outcome
Cornea
•
•
•
•
•
•
Irritation/burning sensation
Corneal edema
Superficial keratitis
Ulceration
Melting
Note: Corneal complications will be
expeditiously sent for review by the DSMC
Cataract/cataract surgery
Ocular infection/inflammation
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Sample Size
60 study participants per group
convenience sample size will be recruited
Total number of eyes is 120 in 120 study
participants
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Thank You on Behalf of Diabetic Retinopathy
Clinical Research Network (DRCR.net)
Dedicated to multicenter clinical research of diabetic
retinopathy, macular edema and associated disorders.
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