Age-related Macular Degeneration (ARMD)

Introduction

ARMD is a progressive loss of central vision due to drusen formation and retinal pigment epithelium changes.
Most common cause of blindness in people over 60 in the UK and Ireland.

No single cause identified; multifactorial with genetic and environmental factors.
Risk factors:
Age
Caucasian ethnicity
Family history
Smoking
Hypertension
High-fat diet
Aspirin use
Sunlight exposure
Blue eyes
Female gender
Previous cataract surgery

Type	Clinical Features
No AMD	Few small drusen (<63µm) or none
Early AMD	≥1 medium drusen (63–124µm) or mild pigment changes
Intermediate AMD	≥1 large drusen (≥125µm) or geographic atrophy not involving fovea
Advanced AMD	Geographic atrophy involving fovea or neovascular AMD

Progressive central visual loss, difficulty with detail, faces, and contrast.
Symptom variation often worse in low light.
Acute rapid vision loss indicates wet AMD (ophthalmic emergency).
Associated symptoms: visual distortions, central scotomas, metamorphopsia.
Assess risk factors: smoking, hypertension, family history, cataract surgery, aspirin use.
Impact on activities of daily living, driving status, falls risk.

Condition	Key Features
Dry AMD	Gradual central vision loss, drusen on fundoscopy
Wet AMD	Sudden vision loss, retinal hemorrhage
Open-angle glaucoma	Peripheral vision loss, optic disc cupping
Cataract	Blurred vision, glare, no central scotoma
Diabetic retinopathy	Retinal hemorrhages, microaneurysms, history of diabetes
Retinal detachment	Flashes, floaters, peripheral vision loss
Central retinal artery occlusion	Sudden vision loss, cherry-red macula
Giant cell arteritis	Headache, scalp tenderness, jaw claudication

No reliable blood biomarkers for AMD.
Community/non-specialist: Amsler grid for screening.
Specialist imaging:
Ocular Coherence Tomography (OCT): retinal layer thickness, drusen, neovascular membranes.
Fluorescein angiography: detects choroidal neovascularisation.
Indocyanine green angiography: for deeper choroidal vessel imaging in hemorrhagic cases.
Autofluorescence: assesses geographic atrophy.

No cure; focus on preserving vision and quality of life.
Lifestyle advice: smoking cessation, cardiovascular risk control, diet, sunlight protection.
Dry AMD:
Low vision aids.
AREDS2 vitamin supplements (vitamins C, E, beta-carotene, zinc, lutein, zeaxanthin).
Wet AMD:
Intravitreal anti-VEGF injections (Ranibizumab, Bevacizumab, Pegaptanib).
Initial monthly injections for 3 months, then individualized dosing.
Support:
Registration with blind services.
Occupational therapy and psychological support.
Driving advice based on visual acuity standards.

Injection complications:
Chemosis, scleral injection, grittiness.
Rare: endophthalmitis (<1%), retinal detachment (<1%), cataract formation (<1%).
Disease progression:
1.3%-18% risk of advancing over 5 years depending on stage.
43% risk of advanced disease in fellow eye if one eye affected.
Visual loss increases fall/fracture risk.

Bowling B. Kanski's Clinical Ophthalmology, 8th Ed. 2015.
Batterbury M, Murphy C. Ophthalmology, 4th Ed. 2018.
Age-Related Eye Disease Study Research Group (AREDS). 1999.
Haugsdal J, Sohn E. Age-Related Macular Degeneration Review. 2018.
Ghasemi Falavarjani K, Nguyen Q. Adverse Events with Anti-VEGF Injections, 2013.

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