4.7 Article

Urinary Mass Spectrometry Profiles in Age-Related Macular Degeneration

Journal

JOURNAL OF CLINICAL MEDICINE
Volume 11, Issue 4, Pages -

Publisher

MDPI
DOI: 10.3390/jcm11040940

Keywords

age-related macular degeneration; metabolomics; urine

Funding

  1. Miller Retina Research Fund (Mass. Eye and Ear)
  2. Champalimaud Vision Award
  3. National Institutes of Health (NIH) [R01EY030088]
  4. Research to Prevent Blindness, Inc., New York
  5. Portuguese Foundation for Science and Technology/Harvard Medical School Portugal Program [HMSP-ICJ/006/2013]
  6. Commonwealth Unrestricted Grant for Eye Research

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This study aimed to assess urinary metabolomic profiles of patients with different stages of age-related macular degeneration (AMD) and controls. Results showed no significant differences in urine metabolites when comparing patients with AMD and controls. However, when disease severity was considered as an outcome, six urinary metabolites differed significantly, supporting previous work performed with plasma.
We and others have shown that patients with different severity stages of age-related macular degeneration (AMD) have distinct plasma metabolomic profiles compared to controls. Urine is a biofluid that can be obtained non-invasively and, in other fields, urine metabolomics has been proposed as a feasible alternative to plasma biomarkers. However, no studies have applied urinary mass spectrometry (MS) metabolomics to AMD. This study aimed to assess urinary metabolomic profiles of patients with different stages of AMD and a control group. We included two prospectively designed, multicenter, cross-sectional study cohorts: Boston, US (n = 185) and Coimbra, Portugal (n = 299). We collected fasting urine samples, which were used for metabolomic profiling (Ultrahigh Performance Liquid chromatography-Mass Spectrometry). Multivariable logistic and ordinal logistic regression models were used for analysis, accounting for gender, age, body mass index and use of AREDS supplementation. Results from both cohorts were then meta-analyzed. No significant differences in urine metabolites were seen when comparing patients with AMD and controls. When disease severity was considered as an outcome, six urinary metabolites differed significantly (p < 0.01). In particular, two of the metabolites identified have been previously shown by our group to also differ in the plasma of patients of AMD compared to controls and across severity stages. While there are fewer urinary metabolites associated with AMD than plasma metabolites, this study identified some differences across stages of disease that support previous work performed with plasma, thus highlighting the potential of these metabolites as future biomarkers for AMD.

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