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Venous Occlusive Disease
F.Fazel MD
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History
RVO patients commonly report decreased vision and blurring in one eye, but it’s typically painless with sudden onset. They may also report distortion of images, and their visual disturbances may be limited to one part of the visual field.
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Clinical exam
Classic features of branch retinal vein occlusion (BRVO) and central retinal vein occlusion (CRVO), include intraretinal hemorrhages and tortuosity and dilation of the retinal blood vessels. Macular edema, exudates and cotton wool spots may be present.
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Retinal Vein Occlusion
Retinal vein occlusion is the second most common cause of visual loss due to retinal vascular disease1-3
Two major types: Branch retinal vein occlusion (BRVO) Central retinal vein occlusion (CRVO)
BRVO is the most common3
– Five-year incidence of 0.6% (21/3558) for BRVO and 0.2% (7/3593) for CRVO3
Persistent macular edema causes VA loss
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Central Retinal Vein Occlusion
Findings Dilated and tortuous
retinal veins Swollen optic disc Intra-retinal hemorrhages Retinal edema
All four quadrants
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Central Retinal Vein Occlusion
Classification Based on amount of non-profusion on fluorescein
angiography» Ischemic
≥10 disk areas
» Non-ischemic < 10 disk areas
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Central Retinal Vein Occlusion
Pathogenesis Thrombosis of the central retinal vein
» At or posterior to the lamina cribrosa
Atherosclerotic central retinal artery » Impinges on central retinal vein
Turbulent flow → thrombus
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Central Retinal Vein Occlusion
Non-ischemic CRVO Less dilation and vascular
tortuosity Dot and flame hemorrhages
in all quadrants Less or no disk swelling
Angiogram shows» Delayed A-V transit time» Leakage» Minimal capillary dropout
Neovascularization is rare
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Central Retinal Vein Occlusion Ischemic CRVO
Extensive hemorrhage Retinal edemaMarked venous dilation Cotton-wool spots
Angiogram show» Widespread capillary nonprofusion
Visual prognosis poor» Only 10% have >20/400 vision
NVI» As high as 60% of eyes» Occurs 3-5 months post occlusion
“the three month glaucoma”
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Central Retinal Vein Occlusion
Risk Factors Eye Disease Case-Control
Study» Hypertension» Diabetes
Unlike BRVO» Glaucoma
Check and treat IOP!
CRVO in young patients requires more extensive workup for cause
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CRVO In Young Patients – Causes
Systemic vascular disease Hypertension Diabetes mellitus Cardiovascular disease
Blood dyscrasias Polycythemia vera Lymphoma Leukemia
Clotting disorders Activated protein C resistance Lupus anticoagulant Anticardiolipin antibodies Protein C Protein S Antithrombin III
Paraproteinemia and dysproteinemias Multiple myeloma Cryoglobulinemia
Vasculitis Syphilis Sarcoidosis
Autoimmune disease Systemic lupus erythematosus
Oral contraceptive use in women Other rare associations
Closed-head trauma Optic disc drusen Arteriovenous malformations of retina
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Central Retinal Vein Occlusion
Management Family medical doctor to
manage» Hypertension» Diabetes» Elevated cholesterol
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Branch Retinal Vein Occlusion
FindingsWithin one sector of the
retina» Superficial hemorrhages» Retinal edema» Cotton-wool spots» Dilated and tortuous vein» Corresponding artery narrowed
and sheathed
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Branch Retinal Vein Occlusion
Findings Superotemporal quadrant
most common» 63%
Occurs at arteriovenous crossing
» Artery and vein bound together in a common sheath
» Arterial thickening compresses vein Turbulent flow → thrombus
formation
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Branch Retinal Vein Occlusion
Risk factors Identified by the Eye Disease
Case-Control Study» Hypertension» Cardiovascular disease» Increased BMI at age 20» Glaucoma
Note : Diabetes not an independent risk factor
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Branch Retinal Vein Occlusion
Visual Loss Acute
» Macular hemorrhage» Macular edema» Capillary occlusion
Chronic» Macular ischemia» CME» Macular pigmentary changes» Epiretinal membrane formation» Subretinal fibrosis
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Reframing How We ThinkAbout Treatment for RVO
Clinically, we see the repercussions of RVO disease stages that follow the initial occlusive event — capillary permeability and leakage, edema, inflammation, vessel remodeling and recanalization, neovascularization if ischemia is present, and fibrosis.
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Fluorescein angiography
Delayed venous filling, hypofluorescence caused by hemorrhage and capillary nonperfusion, dilation and tortuosity of veins, leakage due to neovascularization and macular edema
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OCT
OCT provides us with a more efficient, less invasive and less costly way than repeat FA to evaluate and monitor RVO and associated macular edema over time.
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Clinical Trials for RVO
• Laser studies– 1980s Branch Vein Occlusion Study (BVOS)– 1990s Central Vein Occlusion Study (CVOS)
• 2009 Steroid studies– SCORE Study– Ozurdex Trials
• 2010 Anti-VEGF Ranibizumab studies– BRAVO and CRUISE
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BVOS and CVOS
BVOS: Argon MGL is preferable to observation for patients with macular edema secondary to branch retinal vein occlusion (BRVO) and vision of 20/40 or worse.
CVOS: macular grid photocoagulation is not recommended for treating macular edema due to central retinal vein occlusion (CRVO).
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Pan Retinal Photocoagulation
Management Iris neovascularization
PRP to eyes prior to NVI or NVE
» NO benefit Even if very ischemic
Once neovascularization detected
» Prompt PRP
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Primary Results: The Standard Care versus COrticosteroid for REtinal Vein Occlusion Study (The SCORE Study)
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SCORE BRVO
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SCORE BRVO Conclusion
The SCORE-BRVO trial results support grid laser as the SC treatment for macular edema secondary to BRVO because:
Similar efficacy in all 3 treatment arms up to month 12
Improved efficacy for laser beyond month 12 Superior safety profile of SC over 1-mg and
4-mg TA
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SCORE CRVO % With VA Gain of 15 letters or More
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SCORE CRVO Conclusion
Both triamcinolone groups were superior to the observation group for VA at 12 months
Visual benefit as early as 4 months Visual benefit continued to 24 months The 1-mg dose has a safety profile superior
to that of the 4-mg dose and similar to observation
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OZURDEX™ (dexamethasone intravitreal implant)
Injectable, biodegradable intravitreal implant contains 0.7 mg (700 μg) dexamethasone in the NOVADUR™ solid polymer drug delivery system (preservative-free).
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Ozurdex Mean Change BCVA BRVO(GENEVA trial)
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Ozurdex Mean Change BCVA CRVO(GENEVA trial)
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Ozurdex Trials Conclusions
DEX groups’ time to gain 15 letters was significantly shorter than sham eyes through day 90
Mean change in BCVA was statistically:Better for DEX groups for BRVO through day 180
Better for DEX groups for CRVO through day 90
Persistence of efficacy in 21% BRVO; 17% CRVO at month 12 required only 1 Rx
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Anti-VEGF Trials
Ranibizumab (Lucentis) BRAVO and CRUISE
Afilbercept (VEGF-Trap eye, Regeneron) Galileo and Copernicus
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Mean Change from Baseline BCVA (BRVO)
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Mean Change from Baseline(CRVO)
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Anti-VEGF Trials
BRAVO: Ranibizumab monthly for 6 months better than observation/laser in BRAVO. Improved VA: 61% vs 29% eyes gained 15 or more letters
CRUISE: Ranibizumab monthly for 6 months better than observation. Improved VA: 48% vs 17% eyes gained 15 or more letters
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Treatment Criteria
Treat all patients who have edema and a vision complaint, even if their Snellen visual acuity is 20/20.
One reason is that the longer we wait to treat, the less vision we can expect the patient to recover. Another reason is that Snellen acuity is not a true assessment of visual function.
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Treatment regimens for RVO now typically start with monthly injections of anti-VEGF agents before patients are switched to as-needed dosing with monthly monitoring
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Gauging Response to Treatment
First-line therapy for RVO-associated macular edema is an anti-VEGF agent
BRAVO and CRUISE studies of ranibizumab analysis showed that in patients with central retinal vein occlusion, 90% of the response to treatment occurred within the first three injections. Therefore, if I see no response after three injections, I’m confident that monotherapy will not be adequate, and I move to the next option.
Use caution in our patients who are at highest risk for ATEs, particularly patients 85 and older.
Focal laser therapy often is used adjunctively after 5–6 months of initial therapy.
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Where are we going?
Despite the advances in pharmacologic therapy, many eyes with RVO continue to lose vision. The common final pathway appears to be photoreceptor cell death.
Future research for RVO treatments may focus on neuroprotective and photoreceptor regeneration therapies to improve sight in patients who have limited vision due to RVO.
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Thank you for you attention