Gene Correction Reverses Ciliopathy and Photoreceptor Loss in iPSC-Derived Retinal Organoids from Retinitis Pigmentosa Patients

Wen-Li Deng; Mei-Ling Gao; Xin-Lan Lei; Ji-Neng Lv; Huan Zhao; Kai-Wen He; Xi-Xi Xia; Ling-Yun Li; Yu-Chen Chen; Yan-Ping Li; Deng Pan; Tian Xue; Zi-Bing Jin

doi:10.1016/j.stemcr.2018.02.003

Gene Correction Reverses Ciliopathy and Photoreceptor Loss in iPSC-Derived Retinal Organoids from Retinitis Pigmentosa Patients

Stem Cell Reports. 2018 Apr 10;10(4):1267-1281. doi: 10.1016/j.stemcr.2018.02.003. Epub 2018 Mar 8.

Authors

Wen-Li Deng¹, Mei-Ling Gao¹, Xin-Lan Lei¹, Ji-Neng Lv¹, Huan Zhao², Kai-Wen He¹, Xi-Xi Xia¹, Ling-Yun Li², Yu-Chen Chen¹, Yan-Ping Li¹, Deng Pan¹, Tian Xue², Zi-Bing Jin³

Affiliations

¹ Lab for Stem Cell & Retinal Regeneration, Institute of Stem Cell Research, Division of Ophthalmic Genetics, The Eye Hospital, Wenzhou Medical University, State Key Laboratory of Ophthalmology, Optometry and Visual Science, Wenzhou 325027, China.
² Hefei National Laboratory for Physical Sciences at Microscale, CAS Key Laboratory of Brain Function and Disease, Neurodegenerative Disorder Research Center, School of Life Sciences, University of Science and Technology of China, Hefei 230026, China.
³ Lab for Stem Cell & Retinal Regeneration, Institute of Stem Cell Research, Division of Ophthalmic Genetics, The Eye Hospital, Wenzhou Medical University, State Key Laboratory of Ophthalmology, Optometry and Visual Science, Wenzhou 325027, China. Electronic address: jinzb@mail.eye.ac.cn.

Abstract

Retinitis pigmentosa (RP) is an irreversible, inherited retinopathy in which early-onset nyctalopia is observed. Despite the genetic heterogeneity of RP, RPGR mutations are the most common causes of this disease. Here, we generated induced pluripotent stem cells (iPSCs) from three RP patients with different frameshift mutations in the RPGR gene, which were then differentiated into retinal pigment epithelium (RPE) cells and well-structured retinal organoids possessing electrophysiological properties. We observed significant defects in photoreceptor in terms of morphology, localization, transcriptional profiling, and electrophysiological activity. Furthermore, shorted cilium was found in patient iPSCs, RPE cells, and three-dimensional retinal organoids. CRISPR-Cas9-mediated correction of RPGR mutation rescued photoreceptor structure and electrophysiological property, reversed the observed ciliopathy, and restored gene expression to a level in accordance with that in the control using transcriptome-based analysis. This study recapitulated the pathogenesis of RPGR using patient-specific organoids and achieved targeted gene therapy of RPGR mutations in a dish as proof-of-concept evidence.

Keywords: RPE cells; RPGR; ciliopathy; cilium; disease modeling; electrophysiology; patient-derived iPSCs; photoreceptor; retinal organoid; retinitis pigmentosa.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Cell Differentiation
Ciliopathies / pathology
Ciliopathies / physiopathology
Ciliopathies / therapy*
Eye Proteins / genetics
Genetic Therapy*
Humans
Induced Pluripotent Stem Cells / metabolism
Induced Pluripotent Stem Cells / pathology*
Mutation / genetics
Organoids / pathology*
Photoreceptor Cells / metabolism
Photoreceptor Cells / pathology*
Potassium Channels / metabolism
Retina / pathology*
Retinitis Pigmentosa / pathology*
Retinitis Pigmentosa / physiopathology
Retinitis Pigmentosa / therapy*

Substances

Eye Proteins
Potassium Channels
RPGR protein, human