AI Article Synopsis

  • The study focused on the diversity of human retinal pigment epithelium (hRPE) cells, employing single-cell RNA sequencing on over 9,000 cells from three donors.
  • Two distinct subpopulations of hRPE cells were identified: one with markers specific to macular regions and another associated with peripheral regions, each showing different gene expression and functions.
  • The findings suggest that these clusters may serve as important targets for future retinal disease therapies, shedding light on the role of specific genes related to oxidative stress and metabolism in hRPE health and disease.

Article Abstract

Human retinal pigment epithelium cells are arranged in a monolayer that plays an important supporting role in the retina. Although the heterogeneity of specific retinal cells has been well studied, the diversity of hRPE cells has not been reported. Here, we performed a single-cell RNA sequencing on 9,302 hRPE cells from three donors and profiled a transcriptome atlas. Our results identified two subpopulations that exhibit substantial differences in gene expression patterns and functions. One of the clusters specifically expressed , a macular retinal pigment epithelium marker. The other cluster highly expressed , a peripheral RPE marker. Our results also showed that the genes associated with oxidative stress and endoplasmic reticulum stress were more enriched in the macular RPE. The genes related to light perception, oxidative stress and lipid metabolism were more enriched in the peripheral RPE. Additionally, we provided a map of disease-related genes in the hRPE and highlighted the importance of the macular RPE and peripheral RPE clusters P4 and P6 as potential therapeutic targets for retinal diseases. Our study provides a transcriptional landscape for the human retinal pigment epithelium that is critical to understanding retinal biology and disease.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8718768PMC
http://dx.doi.org/10.3389/fcell.2021.802457DOI Listing

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