Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT02985619 |
| Other study ID # |
1.599.864 |
| Secondary ID |
|
| Status |
Completed |
| Phase |
Phase 2/Phase 3
|
| First received |
|
| Last updated |
|
| Start date |
July 21, 2016 |
| Est. completion date |
December 21, 2017 |
Study information
| Verified date |
May 2022 |
| Source |
University of Sao Paulo |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Background: Diabetic macular edema (DME) shows a sustained functional and morphologic
response to anti-vascular endothelial growth factor (VEGF) drugs, but the optimal approach
for persistent macular edema still in debate.
Purpose: To evaluate 24-week visual and anatomical effects of intravitreal bevacizumabe or
triamcinolone in patients who have residual edema after 24-weeks to "pro re nata"(prn)
intravitreal bevacizumabe therapy.
Methods: This study will enroll a total of 100 DME eyes. Each patient will receive "prn"
bevacizumabe therapy throughout 24 weeks. At week 24, patients who have recurrent or
persistent edema were randomized 1:1 to Group 1 (prn bevacizumane) or Group 2 (prn
triamcinolone). Patients with no recurrent or persistent edema at week 24 will comprise to
Group 3 and continue receive prn bevacizumabe. Prn treatment was administered when central
subfield thickness of the macula (CST) > 300 µm and/or there are intraretinal cystoid spaces
in the fovea. Study visits will occur every 4 weeks with the endpoint at week 48. At each
visit, patients will have an eye exam and CST, best-corrected visual acuity (BCVA), and
intraocular pressure (IOP) were assessed. Fundus photography and fluorescein angiography will
also perform at baseline, week 16, week 40, and week 48. All patients will resume standard
care after exiting.
Description:
Methods Study Design. The current study is a prospective randomized clinical trial registered
at ClinicalTrials.gov (NCT02985619). The study protocol adhered to the tenets of the
Declaration of Helsinki and was approved by the local Institutional Review Board, research
ethics committee of School of Medicine of Ribeirão Preto at University of Sao Paulo. All
patients will give inform consent signature before entering one year study and will evaluate
in the Retina Section of Department of Ophthalmology, School of Medicine of Ribeirao Preto of
the University of Sao Paulo with center-involved DME in at least 1 eye. Recruiting phase will
be consider the first 6 months. All patients with diagnostic of DME in at least 1 eye from
July 2016 to December 2016 will invite to participate in the study.
Study Population. Inclusion criteria. Inclusion criteria are as follows: (1) Eligible
participants are age 18 years old with diabetes mellitus (type 1 or 2); (2) center-involved
DME, defined as a central subfield thickness >300 µm on spectral domain optical coherence
tomography (SD-OCT), despite of macular laser photocoagulation, cataract surgery and
intraocular injection performed at least 4 months previously; (3) best-corrected ETDRS visual
acuity (BCVA) measurement between 0.3 logMAR (Snellen equivalent: 20/32) and 1.3 logMAR
(Snellen equivalent: 20/400); (4) signed informed consent. Exclusion criteria. Exclusion
criteria were: (1) vitreo-macular traction on SD-OCT; (2) proliferative diabetic retinopathy
needing panretinal photocoagulation (PRP) or anticipated to need PRP in the next 12 months;
(3) macular capillary dropout on fluorescein angiography; (4) history of glaucoma or ocular
hypertension (defined as an intraocular pressure higher than 25 mm Hg); (5) an ocular
condition (other than diabetes) that, in the opinion of the investigator, might affect
macular edema or alter visual acuity during the course of the study (eg, retinal vein
occlusion, uveitis or other ocular inflammatory disease, neovascular glaucoma, etc); (6)
systemic corticosteroid therapy; (7) any condition that, in the opinion of the investigator,
might preclude follow-up throughout the study period; (8) Recent (within 3 months)
thromboembolic events including acute myocardial infarction (MI) and cerebrovascular accident
(CVA); (9) Other Clinical trial participation in the last 30 days.
Randomization and Intervention. After eligibility phase, subjects with center-involving DME
will enroll and undergo comprehensive ophthalmologic evaluation at baseline and every 4 weeks
up to week 48. Patients will receive monthly prn 1.25 mg (0.05 cc) IVB throughout 24 weeks if
central subfield thickness (CSFT) will great than 300 µm. At week 24, patients who has
recurrent or persistent edema (CSFT>300) will randomize 1:1 to Group 1 (prn IVB therapy) or
Group 2 (quarterly IVT therapy). Randomization will be do from binomial distribution with
parameters that it enters as function arguments. Patients with no recurrent or persistent
edema (CSFT≤300µm) at 24-week will comprise to Group 3 and continue receiving prn IVB
therapy. If patient have edema in both eyes and the patient agree to treat both eyes, 1 eye
will receive the random treatment according to a computer-generate sequence and the
contralateral eye will receive the other therapy option on the next day; thus if an eye was
randomized to the IVB group I, the contralateral eye will allocate to the IVT group II and
the reverse will also true.
Examination Procedures and follow-up. Each patient will receive a detailed ophthalmologic
examination including measurement of BCVA according to the standardized ETDRS refraction
protocol using a retroilluminate Lighthouse for the Blind distance visual acuity test chart
(using modified ETDRS charts 1, 2, and R; Precision Vision, IL), as well as applanation
tonometry, slit-lamp biomicroscopic examination, indirect fundus examination, and fluorescein
angiography using high-resolution angiography (HRA; Heidelberg Engineering, Heidelberg,
Germany). SD-OCT evaluation (HRA-OCT; Heidelberg Engineering) will be performe in all
patients, and retinal thickness measurements will be acquire using a standard 20, 15-degree
raster scan protocol. CSFT values will be calculate automatically as the average thickness of
a central macular region 1000 mm in diameter centered on the patient's foveola by built-in
Heidelberg software using retinal map analysis. Patients will schedule for follow-up
examinations at monthly intervals. At these visits the BCVA will be determined after ETDRS
refraction and complete ophthalmic examination similar to baseline valuations with the
exception of fluorescein angiography schedule at baseline and week 36.
Antiglaucomatous eyedrops criteria. Intraocular pressure (IOP) ≥ 25 mmHg and/or 10mmHg
increased from baseline measurement will be adopt to initiate anti-glaucomatous eyedrops.
Intravitreal Injection. All injections will be were performed using topical proparacaine
drops under sterile conditions (eyelid speculum and povidone-iodine). Topical antibiotics
will not use before the day of injection. Before the injection are perform, the eyelids will
scrubb with 10% povidone-iodine, and 5% povidone-iodine drops will be apply to the
conjunctiva. The time between application of 5% povidone-iodine solution to the conjunctiva
and administration of the intravitreal injection will be 2 minutes. Povidone-iodine will be
was apply to the conjunctiva directly over the intended injection site. Care will be take in
all cases to insure that the needle do not touch the lids or lashes. Bevacizumab (1.25
mg/0.05 cc; F. Hoffmann- La Roche Ltd., Basel, Switzerland) or Triamcinolone (1.20 mg/ 0.03
cc; Opthaac, Ophthalmos, São Paulo, Brazil) will be inject into the vitreous cavity using a
29-gauge 0.5- inch needle insert through the superotemporal pars plana 3.0-3.5 mm posterior
to the limbus.25 After the injection, central retinal artery perfusion will be confirm with
indirect ophthalmoscopy. Patients will instruct to instill 1 drop of 0.3% ciprofloxacin into
the inject eye 4 times daily for 1 week after the procedure.
Retreatment Protocol. Retreatment with the originally assign treatment is perform monthly if
central subfield thickness is great than 300 µm.
Rescue Therapy. Before randomization, all patients will receive prn-IVB and if, after 3
consecutive visits, there will be not a reduction in CST of at least 10% or an increase in
BCVA of at least 5 ETDRS letters score when compare with baseline, the patient can continue
with the same intravitreal medication for an additional 3 consecutive visits or discontinue
treatment. After randomization, a similar strategy is used as rescue therapy for all 3
groups.
Outcomes. Primary outcome measure: Mean change in CSFT from baseline to week 48. Secondary
outcomes measures: Mean change in BCVA from baseline to week 48; mean change in IOP at any
visit; lens status changes, mean number of intravitreous injections Sample Size. Sample size
and powering is base on a previous clinical trial on bevacizumab use for diabetic macular
edema, where a mean change observed in central subfield thickness from baseline was 130 mm
with a standard deviation of 122 μm. Therefore, to have 80% power to detect a difference of
50 μm between central subfield thickness change found in both groups, the sample size require
in each group was 25 eyes. Thirty eyes per treatment group is require if one assume a 10%
dropout rate. With this sample size, there is a 20% chance for a failure to detect a true
mean difference of at least 50 μm between the treatment groups (type I error), or for an
incorrect conclusion that a difference of at least 50 μm exists between the treatment groups
(type II error).
Statistical Analysis. BCVA and central subfield thickness measured at each follow-up visit
will be compare with baseline BCVA and CSFT values for within- and between-group comparisons,
which is perform using multiple analysis of variance (MANOVA) for repeated measurements.
Proportions of eyes with central subfield thickness ≤ 300 mm is compare using the likelihood
ratio x2 test. In addition, a multivariate analysis comparing BCVA and CSFT outcomes in the
prn-IVB group and qIVT group is perform, considering number of injections, baseline BCVA, and
CSFT as effects. A statistically significant effect is define if P < .05, and a trend towards
significance is report if P < .1. Statistical analyses are performe using JMP 10.0.0 (2010;
SAS Institute Inc, Cary, North Carolina, USA) software.
