Contemporary Clinical Trials Communications (Dec 2020)

Baseline characteristics and age-related macular degeneration in participants of the “ASPirin in Reducing Events in the Elderly” (ASPREE)-AMD trial

  • Liubov D. Robman,
  • Le Thi Phuong Thao,
  • Robyn H. Guymer,
  • Rory Wolfe,
  • Robyn L. Woods,
  • Lauren AB. Hodgson,
  • James Phung,
  • Galina A. Makeyeva,
  • Y-Anh Le-Pham,
  • Suzanne G. Orchard,
  • Jewhara Suleiman,
  • Emily Maguire,
  • Ruth E. Trevaks,
  • Stephanie A. Ward,
  • Moeen Riaz,
  • Paul Lacaze,
  • Elsdon Storey,
  • Walter P. Abhayaratna,
  • Mark R. Nelson,
  • Michael E. Ernst,
  • Christopher M. Reid,
  • John J. McNeil

Journal volume & issue
Vol. 20
p. 100667

Abstract

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Purpose: To describe the baseline participant characteristics in the ASPREE-AMD study, investigating the effect of aspirin on AMD incidence and progression. Methods: Australian participants from the ASPirin in Reducing Events in the Elderly (ASPREE) trial, randomized to 100 mg aspirin daily or placebo, had non-mydriatic, digital color fundus images graded according to the Beckman AMD classification. Associations with AMD were determined for baseline characteristics and genetic risk variants. Results: ASPREE-AMD sub-study enrolled 4993 participants with gradable macular images. Median age was 73.4 years (IQR, 71.5, 76.6), 52% were female, 10% had diabetes mellitus, 73% had hypertension, and 44% were former/current smokers. Early, intermediate and late AMD (detected in 20.6%, 16.1%, 1.1%, respectively), significantly associated with age, were also associated with increasing HDL levels: OR = 1.52 (95%CI, 1.26, 1.84), OR = 1.43 (1.17, 1.77) and OR = 1.96 (1.02, 3.76), respectively. Female sex was associated with early [OR = 1.37 (1.16, 1.62)], and intermediate [OR = 1.35 (1.12, 1.63)] AMD, as was previous regular use of aspirin, with OR = 1.46 (1.11, 1.92) and OR = 1.37 (1.01, 1.85), respectively. Current smoking had increased odds for late AMD, OR = 4.02 (1.42, 11.36). Genetic risk variant rs3750846 (ARMS2/HTRA1) was associated with each AMD stage (p < 0.001), risk variants rs570618 and rs10922109 (CFH) with intermediate and late AMD (p < 0.001), and rare variant rs147859257 (C3) with late AMD (p < 0.001). The randomized groups were well balanced for all analyzed AMD risk factors. Conclusions: Observed associations are typical of AMD. The ASPREE-AMD clinical trial provides a unique opportunity to determine the risks and benefits of low-dose aspirin for AMD incidence and progression in elderly population. Trial registration: Australian New Zealand Clinical Trial Registry: ACTRN 12613000755730.

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