PLoS Genetics (Aug 2023)

Multi-ancestry GWAS analysis identifies two novel loci associated with diabetic eye disease and highlights APOL1 as a high risk locus in patients with diabetic macular edema.

  • Amy D Stockwell,
  • Michael C Chang,
  • Anubha Mahajan,
  • William Forrest,
  • Neha Anegondi,
  • Rion K Pendergrass,
  • Suresh Selvaraj,
  • Jens Reeder,
  • Eric Wei,
  • Victor A Iglesias,
  • Natalie M Creps,
  • Laura Macri,
  • Andrea N Neeranjan,
  • Marcel P van der Brug,
  • Suzie J Scales,
  • Mark I McCarthy,
  • Brian L Yaspan

DOI
https://doi.org/10.1371/journal.pgen.1010609
Journal volume & issue
Vol. 19, no. 8
p. e1010609

Abstract

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Diabetic retinopathy (DR) is a common complication of diabetes. Approximately 20% of DR patients have diabetic macular edema (DME) characterized by fluid leakage into the retina. There is a genetic component to DR and DME risk, but few replicable loci. Because not all DR cases have DME, we focused on DME to increase power, and conducted a multi-ancestry GWAS to assess DME risk in a total of 1,502 DME patients and 5,603 non-DME controls in discovery and replication datasets. Two loci reached GWAS significance (p<5x10-8). The strongest association was rs2239785, (K150E) in APOL1. The second finding was rs10402468, which co-localized to PLVAP and ANKLE1 in vascular / endothelium tissues. We conducted multiple sensitivity analyses to establish that the associations were specific to DME status and did not reflect diabetes status or other diabetic complications. Here we report two novel loci for risk of DME which replicated in multiple clinical trial and biobank derived datasets. One of these loci, containing the gene APOL1, is a risk factor in African American DME and DKD patients, indicating that this locus plays a broader role in diabetic complications for multiple ancestries. Trial Registration: NCT00473330, NCT00473382, NCT03622580, NCT03622593, NCT04108156.