Dorgau, Birthe, Georgiou, Maria, Chaudhary, Alexander, Moya-Molina, Marina, Collin, Joseph, Queen, Rachel, Hilgen, Gerrit, Davey, Tracey, Hewitt, Philip, Schmitt, Michael, Kustermann, Stefan, Pognan, Francois, Steel, David H, Sernagor, Evelyne, Armstrong, Lyle and Lako, Majlinda (2022) Human Retinal Organoids Provide a Suitable Tool for Toxicological Investigations: a Comprehensive Validation Using Drugs and Compounds Affecting the Retina. Stem Cells Translational Medicine, 11 (2). pp. 159-177. ISSN 2157-6564
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Abstract
Retinal drug toxicity screening is essential for the development of safe treatment strategies for a large number of diseases. To this end, retinal organoids derived from human pluripotent stem cells (hPSCs) provide a suitable screening platform due to their similarity to the human retina and the ease of generation in large-scale formats. In this study, two hPSC cell lines were differentiated to retinal organoids, which comprised all key retinal cell types in multiple nuclear and synaptic layers. Single-cell RNA-Seq of retinal organoids indicated the maintenance of retinal ganglion cells and development of bipolar cells: both cell types segregated into several subtypes. Ketorolac, digoxin, thioridazine, sildenafil, ethanol, and methanol were selected as key compounds to screen on retinal organoids because of their well-known retinal toxicity profile described in the literature. Exposure of the hPSC-derived retinal organoids to digoxin, thioridazine, and sildenafil resulted in photoreceptor cell death, while digoxin and thioridazine additionally affected all other cell types, including Müller glia cells. All drug treatments caused activation of astrocytes, indicated by dendrites sprouting into neuroepithelium. The ability to respond to light was preserved in organoids although the number of responsive retinal ganglion cells decreased after drug exposure. These data indicate similar drug effects in organoids to those reported in in vivo models and/or in humans, thus providing the first robust experimental evidence of their suitability for toxicological studies.
Item Type: | Article |
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Additional Information: | Funding information: The authors are grateful for financial support from NC3Rs CRACKIT23 challenge (NC/CO16206/1). The authors would like to acknowledge the Bioimaging Unit (Newcastle University) for their support and assistance in this work. |
Uncontrolled Keywords: | human embryonic stem cells, human induced pluripotent stem cells, retina, toxicology, retinal organoids, drug screening |
Subjects: | B200 Pharmacology, Toxicology and Pharmacy B500 Ophthalmics |
Department: | Faculties > Health and Life Sciences > Applied Sciences |
Depositing User: | John Coen |
Date Deposited: | 01 Mar 2022 10:08 |
Last Modified: | 05 Apr 2022 11:30 |
URI: | http://nrl.northumbria.ac.uk/id/eprint/48574 |
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