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Retinal ganglion cell-specific genetic regulation in primary open-angle glaucoma

Authors :
Daniszewski, M
Senabouth, A
Liang, HH
Han, X
Lidgerwood, GE
Hernandez, D
Sivakumaran, P
Clarke, JE
Lim, SY
Lees, JG
Rooney, L
Gulluyan, L
Souzeau, E
Graham, SL
Chan, C-L
Nguyen, U
Farbehi, N
Gnanasambandapillai, V
Mccloy, RA
Clarke, L
Kearns, LS
Mackey, DA
Craig, JE
Macgregor, S
Powell, JE
Pebay, A
Hewitt, AW
Daniszewski, M
Senabouth, A
Liang, HH
Han, X
Lidgerwood, GE
Hernandez, D
Sivakumaran, P
Clarke, JE
Lim, SY
Lees, JG
Rooney, L
Gulluyan, L
Souzeau, E
Graham, SL
Chan, C-L
Nguyen, U
Farbehi, N
Gnanasambandapillai, V
Mccloy, RA
Clarke, L
Kearns, LS
Mackey, DA
Craig, JE
Macgregor, S
Powell, JE
Pebay, A
Hewitt, AW
Publication Year :
2022

Abstract

To assess the transcriptomic profile of disease-specific cell populations, fibroblasts from patients with primary open-angle glaucoma (POAG) were reprogrammed into induced pluripotent stem cells (iPSCs) before being differentiated into retinal organoids and compared with those from healthy individuals. We performed single-cell RNA sequencing of a total of 247,520 cells and identified cluster-specific molecular signatures. Comparing the gene expression profile between cases and controls, we identified novel genetic associations for this blinding disease. Expression quantitative trait mapping identified a total of 4,443 significant loci across all cell types, 312 of which are specific to the retinal ganglion cell subpopulations, which ultimately degenerate in POAG. Transcriptome-wide association analysis identified genes at loci previously associated with POAG, and analysis, conditional on disease status, implicated 97 statistically significant retinal ganglion cell-specific expression quantitative trait loci. This work highlights the power of large-scale iPSC studies to uncover context-specific profiles for a genetically complex disease.

Details

Database :
OAIster
Publication Type :
Electronic Resource
Accession number :
edsoai.on1397538830
Document Type :
Electronic Resource