Retinal Dystrophies Clinical Trial
Official title:
Efficacy and Safety of Intravitreal Ranibizumab (Lucentis®) Injection in the Treatment of Non-leaking Macular Cysts in Patients With Retinal Dystrophy.
To evaluate the efficacy and safety of intravitreal ranibizumab (IVR) injection in the
treatment of non-leaking macular cysts in patients with retinal dystrophy.
Material and Methods:
Design - Prospective, nonrandomized, nonblinded, clinical trial. Participants - Patients >18
years diagnosed with retinal dystrophies and non-leaking macular cysts between Jan 2015 and
July 2018 in 1 center.
Methods - Phase 1: Patients with best corrected visual acuity (BCVA) < 0.5 will receive
carbonic anhydrase inhibitors (CAI) [oral acetazolamide 500mg/day or topical brinzolamide
twice daily] and followed up for three months. Phase 2: Patients who do not show an adequate
response with CAI will receive three 0.5mg IVR injection at monthly intervals.
Outcome - 1) Significant reduction (> 10%) of the central macular thickness (CMT), 2)
Improvement (> 1 line) in BCVA 3) Presence of any complication.
The treatment of cystoid macular edema (CME) in retinitis pigmentosa (RP) is well established
in medical literature. These treatments include topical and oral carbonic anhydrase
inhibitors (CAI), intravitreal triamcinolone acetonide, and laser photocoagulation. Oral
acetazolamide, a carbonic anhydrase inhibitor (CAI), was found to be effective in the
treatment of RP related CME with improvement in both visual acuity and fundus fluorescein
angiography (FFA). However, some patients may not benefit from the treatment, or do not
tolerate it, while others may develop rebound CME with prolonged use of at least 8 to 12
weeks.
An emerging treatment modality for CME in RP is the use of intravitreal injections of
anti-vascular endothelial growth factors (anti-VEGF) such as bevacizumab (Avastin®) and
ranibizumab (Lucentis®). Anti-VEGF has been used successfully for treating diabetic macular
edema, and macular edema secondary to retinal vein occlusion and choroidal
neovascularization, with limited side effects.
A subset of patients with retinal dystrophy develop non-leaking macular cysts that can be
confused with CME on ophthalmoscopy and optical coherence tomography (OCT). FFA establishes
the cavitary nature of the maculopathy, with no hyperfluorescence seen on angiography
compared with leakage seen in patients with CME and retinal dystrophy.
CAI may promote resolution of the non-leaking macular cysts. There are limited studies that
explore the effect of anti-VEGF specifically on non-leaking macular cysts in retinal
dystrophies.
Aims:
- Assess the efficacy of intravitreal ranibizumab (IVR) injection in the treatment of
non-leaking macular cystic lesions in patients with retinal dystrophy that have not responded
to therapy with oral or topical CAI.
Objectives:
- Delineate the entity of non-leaking macular cysts by OCT and FFA.
- Assess the efficacy of short-term oral and topical CAI treatment on non-leaking macular
cysts in retinal dystrophies.
- Study the visual response and structural resolution of non-leaking macular cysts in
response to IVR.
Design: Two-phase prospective, non-randomized, open-label, comparative interventional,
clinical trial.
Inclusion criteria:
1. Omani patients over 18 years old
2. Retinal dystrophy and non-leaking macular cysts confirmed by fundus examination,
electroretinography (ERG), OCT, FFA and genetic testing.
3. Capacity and cooperation to undergo visual function assessment (i.e. best-corrected
visual acuity (BCVA), as well as the above-mentioned investigations.
4. Written, informed consent to participate in the study
Exclusion Criteria:
1. Patients with pseudo-RP
2. Patients with cystic macular lesions or progressive retinal disease due to any cause
other than retinal dystrophy
3. Patients with reduced visual acuity due to media opacities (e.g. cataract).
4. Patients with any contraindication or known allergy to CAI or anti-VEGF agents
5. Patients who have undergone vitreo-retinal surgery or intravitreal injection.
Methods:
Phase 1: Patients with best corrected visual acuity (BCVA) < 0.5 will receive carbonic
anhydrase inhibitors (CAI) [oral acetazolamide 500mg/day or topical brinzolamide twice daily]
and followed up for three months. Baseline urea and electrolyte (U&E) will be tested prior to
receiving CAI, and monitored every month while on the treatment. Upon completion of the
treatment course, the patients will be assessed for response with visual function assessment
and central macular thickness (CMT) on OCT. Patients who show an adequate response (defined
as > 10% reduction of CMT) and/or improvement of BCVA by two lines or more) will continue in
the CAI arm.
Phase 2: Patients who do not show an adequate response with CAI or develop significant side
effects from CAI treatment will stop receiving CAI and will move to Phase 2 of the study and
receive three 0.5mg IVR injection at monthly intervals. Upon completion of the treatment
course, the patients will be assessed for response with visual function assessment and CMT on
OCT.
The purpose of the proposed procedures/treatment, as well as potential complications, will be
clearly explained to participants. It will be made clear to the patient that IVR treatment is
experimental and may or may not lead to improvement of vision. The patient will also be
informed that the treatment will be withheld in case of allergy or complications. It will be
emphasized that he/she may withdraw from the study at any stage.
Patients will be under regular and close follow-up. They will be monitored for the
development of any complications during the study. Any complication will be logged and
treated appropriately. Patients' personal information, clinical history, examination,
investigation results and progress with treatment, will be treated confidentially.
Institutional research ethics board approval will be obtained prior to the start of the
study.
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