Abstract
PurposeAge‐related macular degeneration (AMD) is a degenerative disease of the macula, often leading to progressive vision loss. The rate of disease progression can vary among individuals and has been associated with multiple risk factors. In this review, we provide an overview of the current literature investigating phenotypic, demographic, environmental, genetic, and molecular risk factors, and propose the most consistently identified risk factors for disease progression in AMD based on these studies. Finally, we describe the potential use of these risk factors for personalised healthcare.Recent findingsWhile phenotypic risk factors such as drusen and pigment abnormalities become more important to predict disease progression during the course of the disease, demographic, environmental, genetic and molecular risk factors are more valuable at earlier disease stages. Demographic and environmental risk factors such as age and smoking are consistently reported to be related to disease progression, while other factors such as sex, body mass index (BMI) and education are less often associated. Of all known AMD variants, variants that are most consistently reported with disease progression are rs10922109 and rs570618 in CFH, rs116503776 in C2/CFB/SKIV2L, rs3750846 in ARMS2/HTRA1 and rs2230199 in C3. However, it seems likely that other AMD variants also contribute to disease progression but to a lesser extent. Rare variants have probably a large effect on disease progression in highly affected families. Furthermore, current prediction models do not include molecular risk factors, while these factors can be measured accurately in the blood. Possible promising molecular risk factors are High‐Density Lipoprotein Cholesterol (HDL‐C), Docosahexaenoic acid (DHA), eicosapentaenoic acid (EPA), zeaxanthin and lutein.SummaryPhenotypic, demographic, environmental, genetic and molecular risk factors can be combined in prediction models to predict disease progression, but the selection of the proper risk factors for personalised risk prediction will differ among individuals and is dependent on their current disease stage. Future prediction models should include a wider set of genetic variants to determine the genetic risk more accurately, and rare variants should be taken into account in highly affected families. In addition, adding molecular factors in prediction models may lead to preventive strategies and personalised advice.
Highlights
Age-related macular degeneration (AMD) is the most important cause of irreversible severe vision loss in the elderly in the Western population
A model including demographic and environmental factors showed that age, sex, smoking status, body mass index (BMI), triglycerides and disease status were significantly associated with systemic complement activation (P
Patients should consider taking supplements and adhere a healthy lifestyle to pursue high plasma docosahexaenoic acid (DHA)/fatty acids (FA) ratio and zeaxanthin levels in order to reduce the risk of second eye progression and remain eyesight for a longer period
Summary
Age-related macular degeneration (AMD) is the most important cause of irreversible severe vision loss in the elderly in the Western population. It is estimated that 196 million people are currently (2020) affected worldwide, and due to aging of the population, this number is projected to increase to 288 million by 2040.1 The prevalence of AMD increases with age (FIGURE 1). In those aged 50-54 years, 3.5% have a non-advanced stage of AMD, and the prevalence increases to 18% in those aged 85 years and above. Due to increased ageing of the global population, AMD is becoming a considerable health care burden
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