Transcriptomic and chromatin accessibility analysis of the human macular and peripheral retinal pigment epithelium at the single cell level

Nathaniel K Mullin; Andrew P Voigt; Erin A Boese; Xiuying Liu; Edwin M Stone; Budd A Tucker; Robert F Mullins

doi:10.1016/j.ajpath.2023.01.012

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Transcriptomic and chromatin accessibility analysis of the human macular and peripheral retinal pigment epithelium at the single cell level

Journal article

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Transcriptomic and chromatin accessibility analysis of the human macular and peripheral retinal pigment epithelium at the single cell level

Nathaniel K Mullin, Andrew P Voigt, Erin A Boese, Xiuying Liu, Edwin M Stone, Budd A Tucker and Robert F Mullins

The American journal of pathology, Vol.193(11), pp.1750-1761

11/2023

DOI: 10.1016/j.ajpath.2023.01.012

PMCID: PMC10616710

PMID: 36775060

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Abstract

Human retinal diseases are frequently characterized by pathology that is restricted to specific cell types and to specific regions of the eye. Several disease entities either selectively affect or spare the macula, the retinal region at the center of the posterior pole. Photoreceptor cells of the macula are responsible for high acuity vision and require metabolic support from non-neuronal cell types. Macular diseases often involve an epithelial cell layer known as the retinal pigment epithelium (RPE) that has several essential metabolic support functions for the overlying photoreceptors. In the current study, we probed how the RPE confers region-specific disease susceptibility by examining heterogeneity within human donor RPE. We profiled RPE nuclei from the macular and peripheral retina using joint single-cell RNA and ATAC sequencing. We found that the expression of several genes varies between macular and peripheral RPE. We further found region-specific ATAC peaks implying regulatory elements used exclusively by macular or peripheral RPE. Across anatomical regions, we identify subpopulations of RPE that appear to have differential expression levels of visual cycle genes. Finally, we examined loci connected to age related macular degeneration to better understand RPE-specific disease phenotypes. Together, these data show how gene expression regulation in the human RPE varies by region and subpopulation and provide a resource for better understanding the molecular basis of macular disease.

Details

Title: Subtitle: Transcriptomic and chromatin accessibility analysis of the human macular and peripheral retinal pigment epithelium at the single cell level
Creators: Nathaniel K Mullin
Andrew P Voigt
Erin A Boese
Xiuying Liu
Edwin M Stone
Budd A Tucker
Robert F Mullins
Resource Type: Journal article
Publication Details: The American journal of pathology, Vol.193(11), pp.1750-1761
DOI: 10.1016/j.ajpath.2023.01.012
PMID: 36775060
PMCID: PMC10616710
NLM abbreviation: Am J Pathol
ISSN: 0002-9440
eISSN: 1525-2191
Grant note: DOI: 10.13039/100000053, name: National Eye Institute; DOI: 10.13039/100000057, name: National Institute of General Medical Sciences; DOI: 10.13039/100008097, name: Edward N and Della L Thome Memorial Foundation; DOI: 10.13039/100012201, name: Elmer and Sylvia Sramek Charitable Trust
Language: English
Electronic publication date: 02/10/2023
Date published: 11/2023
Academic Unit: The University of Iowa Institute for Vision Research; Iowa Neuroscience Institute; John and Marcia Carver Nonprofit Genetic Testing Laboratory; Ophthalmology and Visual Sciences
Record Identifier: 9984366459102771

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