Heterogeneous Visual Function Deficits in Intermediate Age-Related Macular Degeneration: A MACUSTAR Report

IF 3.2 Q1 OPHTHALMOLOGY

Ophthalmology science Pub Date : 2025-01-13 DOI:10.1016/j.xops.2025.100708

Hannah M.P. Dunbar PhD , David P. Crabb PhD , Charlotte Behning MSc , Alison M. Binns PhD , Amina Abdirahman , Jan H. Terheyden MD , Stephen Poor MRCOphth , Robert P. Finger MD, PhD , Sergio Leal MD , Adnan Tufail MD, FRCOphth , Frank G. Holz MD , Matthias Schmid PhD , Ulrich F.O. Luhmann PhD , MACUSTAR Consortium

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Abstract

Objective

To examine the extent to which visual function in Beckman age-related macular degeneration (AMD) disease stages differs from age-similar peers with no AMD and, using reference limits derived from those with no AMD, test the hypothesis that people with intermediate AMD (iAMD) have heterogeneous visual function deficits.

Design

Cross-sectional analyses of a range of baseline visual function measures from the MACUSTAR study—an international, multicenter (n = 20), noninterventional clinical trial.

Participants

Five hundred eighty-five participants with iAMD (67% female, mean [standard deviation] age 72 [7] years) were recruited alongside 56 with no AMD (59% female, 68 [6]), 34 with early AMD (79% female, 72 [6]), and 43 with late AMD (49% female, 75 [6]).

Methods

Participants performed best-corrected visual acuity (BCVA), low luminance visual acuity (LLVA), Moorfields acuity test (MAT), Pelli-Robson contrast sensitivity (PR-CS), small print standardized International reading speed test (SPS), mesopic and scotopic average threshold (MesAT and ScoAT; macular integrity assessment, iCare), and rod intercept time (RIT; AdaptDx, Lumithera).

Main Outcome Measures

Relationship between each visual function measure and disease classification was examined by linear regression adjusted for age, sex, and phakic status. No AMD data were used to estimate normal reference limits for each visual function test. Intermediate AMD scores were dichotomized against reference limits, and the proportion worse than each limit was calculated.

Results

Relative to no AMD, SPS was significantly worse in early AMD (P = 0.001); all measures except SPS were significantly reduced in iAMD (P < 0.02), and all measures were markedly reduced in late AMD (P < 0.0001). Thirty-one point three percent of iAMD participants breached reference limits for PR-CS, 29.4% for RIT, 24.1% for LLVA, 23.2% for MAT, 20.5% for BCVA, 19.8% for MesAT, 17.9% for ScoAT, and 12.6% for SPS. Of the iAMD participants, 69.6% and 42.7% breached ≥1 and ≥2 reference limits, respectively, whereas 33.6% and 5.7% would be expected by chance.

Conclusions

A large proportion of people with structurally defined iAMD exhibit heterogeneous visual function deficits outside normal reference limits. This observation may be relevant for the design and inclusion criteria of future interventional trials.