Transcriptomic and proteomic retinal pigment epithelium signatures of age-related macular degeneration

Author:

Senabouth Anne,Daniszewski Maciej,Lidgerwood Grace E.,Liang Helena H.,Hernández Damián,Mirzaei Mehdi,Zhang Ran,Han Xikun,Neavin Drew,Rooney Louise,Sanchez Isabel Lopez,Gulluyan Lerna,Paulo Joao A,Clarke Linda,Kearns Lisa S,Gnanasambandapillai Vikkitharan,Chan Chia-Ling,Nguyen Uyen,Steinmann Angela M,Zekanovic Rachael,Farbehi Nona,Gupta Vivek K.,Mackey David A,Bylsma Guy,Verma Nitin,MacGregor Stuart,Guymer Robyn H,Powell Joseph E.,Hewitt Alex W.,Pébay AliceORCID

Abstract

AbstractInduced pluripotent stem cells generated from patients with geographic atrophy as well as healthy individuals were differentiated to retinal pigment epithelium (RPE) cells. By integrating transcriptional profiles of 127,659 RPE cells generated from 43 individuals with geographic atrophy and 36 controls with genotype data, we identified 439 expression Quantitative Trait (eQTL) loci in cis that were associated with disease status and specific to subpopulations of RPE cells. We identified loci linked to two genes with known associations with geographic atrophy - PILRB and PRPH2, in addition to 43 genes with significant genotype x disease interactions that are candidates for novel genetic associations for geographic atrophy. On a transcriptome-only level, we identified molecular pathways significantly upregulated in geographic atrophy-RPE including in extracellular cellular matrix reorganisation, neurodegeneration, and mitochondrial functions. We subsequently implemented a large-scale proteomics analysis, confirming modification in proteins associated with these pathways. We also identified six significant protein (p) QTL that regulate protein expression in the RPE cells and in geographic atrophy - two of which share variants with cis-eQTL. Transcriptome-wide association analysis identified genes at loci previously associated with age-related macular degeneration. Further analysis conditional on disease status, implicated statistically significant RPE-specific eQTL. This study uncovers important differences in RPE homeostasis associated with geographic atrophy.

Publisher

Cold Spring Harbor Laboratory

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