Single-cell multiome of the human retina and deep learning nominate causal variants in complex eye diseases
Genome-wide association studies (GWASs) of eye disorders have identified hundreds of genetic variants associated with ocular disease. However, the vast majority of these variants are noncoding, making it challenging to interpret their function. Here we present a joint single-cell atlas of gene expression and chromatin accessibility of the adult human retina with more than 50,000 cells, which we used to analyze single-nucleotide polymorphisms (SNPs) implicated by GWASs of age-related macular degeneration, glaucoma, diabetic retinopathy, myopia, and type 2 macular telangiectasia. We integrate this atlas with a HiChIP enhancer connectome, expression quantitative trait loci (eQTL) data, and base-resolution deep learning models to predict noncoding SNPs with causal roles in eye disease, assess SNP impact on transcription factor binding, and define their known and novel target genes. Our efforts nominate pathogenic SNP-target gene interactions for multiple vision disorders and provide a potentially powerful resource for interpreting noncoding variation in the eye.
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Atlas
Analysis Portals
Project Label
scMultiomeOfTheHumanRetinaSpecies
Homo sapiens
Sample Type
specimens
Anatomical Entity
eye
Organ Part
retina
Selected Cell Types
Unspecified
Disease Status (Specimen)
normal
Disease Status (Donor)
Development Stage
human adult stage
Library Construction Method
10x multiome
Nucleic Acid Source
Paired End
false, trueAnalysis Protocol
analysis_protocol_1File Format
Cell Count Estimate
51.6kDonor Count
4