Dynamics of microRNA secreted via extracellular vesicles during the maturation of embryonic stem cell‐derived retinal pigment epithelium

Author:

Pollalis Dimitrios12,Nair Gopa Kumar Gopinadhan12,Leung Justin13,Bloemhof Clarisa Marie145ORCID,Bailey Jeffrey K.67,Pennington Britney O.67,Kelly Kaitlin R.67,Khan Amir I.67,Yeh Ashley K.78,Sundaram Kartik S.69,Clegg Dennis O.679,Peng Chen‐Ching110,Xu Liya110ORCID,Georgescu Constantin11,Wren Jonathan D.11,Lee Sun Young1212ORCID

Affiliation:

1. USC Roski Eye Institute, Keck School of Medicine University of Southern California Los Angeles California USA

2. USC Ginsburg Institute for Biomedical Therapeutics University of Southern California Los Angeles California USA

3. USC Dornsife College of Letters, Arts and Sciences Los Angeles California USA

4. University of Southern California Los Angeles California USA

5. School of Medicine California University of Science and Medicine Colton California USA

6. Center for Stem Cell Biology and Engineering, Neuroscience Research Institute University of California Santa Barbara California USA

7. Department of Molecular Cellular and Developmental Biology University of California Santa Barbara California USA

8. College of Creative Studies, Biology University of California Santa Barbara California USA

9. Biomolecular Science and Engineering University of California Santa Barbara California USA

10. Children's Hospital Los Angeles Vision Center Los Angeles California USA

11. Genes & Human Diseases Research Program Oklahoma Medical Research Foundation Oklahoma City Oklahoma USA

12. Department of Physiology and Neuroscience, Keck School of Medicine University of Southern California Los Angeles California USA

Abstract

AbstractRetinal pigment epithelial (RPE) cells are exclusive to the retina, critically multifunctional in maintaining the visual functions and health of photoreceptors and the retina. Despite their vital functions throughout lifetime, RPE cells lack regenerative capacity, rendering them vulnerable which can lead to degenerative retinal diseases. With advancements in stem cell technology enabling the differentiation of functional cells from pluripotent stem cells and leveraging the robust autocrine and paracrine functions of RPE cells, extracellular vesicles (EVs) secreted by RPE cells hold significant therapeutic potential in supplementing RPE cell activity. While previous research has primarily focused on the trophic factors secreted by RPE cells, there is a lack of studies investigating miRNA, which serves as a master regulator of gene expression. Profiling and defining the functional role of miRNA contained within RPE‐secreted EVs is critical as it constitutes a necessary step in identifying the optimal phenotype of the EV‐secreting cell and understanding the biological cargo of EVs to develop EV‐based therapeutics. In this study, we present a comprehensive profile of miRNA in small extracellular vesicles (sEVs) secreted during RPE maturation following differentiation from human embryonic stem cells (hESCs); earlystage hESC‐RPE (20–21 days in culture), midstage hESC‐RPE (30–31 days in culture) and latestage hESC‐RPE (60–61 days in culture). This exploration is essential for ongoing efforts to develop and optimize EV‐based intraocular therapeutics utilizing RPE‐secreted EVs, which may significantly impact the function of dysfunctional RPE cells in retinal diseases.

Funder

National Eye Institute

Alcon Research Institute

National Institutes of Health

Publisher

Wiley

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