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Aberrant hiPSCs-Derived from Human Keratinocytes Differentiates into 3D Retinal Organoids that Acquire Mature Photoreceptors

DOI:10.3390/cells8010036 期刊:Cells 出版年份:2019 更新时间:2025-09-23 15:22:29
摘要: Human induced pluripotent stem cell (hiPSC)-derived three-dimensional retinal organoids are a new platform for studying the organoidogenesis. However, recurrent genomic aberration, acquired during generation of hiPSCs, limit its biomedical application and/or aberrant hiPSCs has not been evaluated for generation of differentiated derivatives, such as organoids and retinal pigment epithelium (RPE). In this study, we efficiently differentiated mosaic hiPSCs into retinal organoids containing mature photoreceptors. The feeder-free hiPSCs were generated from the human epidermal keratinocytes that were rapid in process with improved efficiency over several passages and maintained pluripotency. But, hiPSCs were cytogenetically mosaic with normal and abnormal karyotypes, while copy number variation analysis revealed the loss of chromosome 8q. Despite this abnormality, the stepwise differentiation of hiPSCs to form retinal organoids was autonomous and led to neuronal lamination. Furthermore, the use of a Notch inhibitor, DAPT, at an early timepoint from days 29–42 of culture improved the specification of the retinal neuron and the use of retinoic acid at days 70–120 led to the maturation of photoreceptors. hiPSC-derived retinal organoids acquired all subtypes of photoreceptors, such as RHODOPSIN, B-OPSIN and R/G-OPSIN. Additionally, the advanced maturation of photoreceptors was observed, revealing the development of specific sensory cilia and the formation of the outer-segment disc. This report is the first to show that hiPSCs with abnormal chromosomal content are permissive to the generation of three-dimensional retinal organoids.
作者: Rupendra Shrestha,Yao-Tseng Wen,Dah-Ching Ding,Rong-Kung Tsai
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To investigate whether aberrant human induced pluripotent stem cells (hiPSCs) with genomic abnormalities can differentiate into three-dimensional retinal organoids that acquire mature photoreceptors.

Aberrant hiPSCs derived from human keratinocytes can successfully differentiate into 3D retinal organoids that recapitulate retinogenesis and acquire mature photoreceptors with sensory cilia and outer-segment discs, despite genomic abnormalities. This suggests flexibility in the genome for organoid generation and provides a model for studying retinal diseases, though further validation is needed for clinical use.

The hiPSCs acquired chromosomal abnormalities and copy number variations, which may limit clinical applications due to potential functional consequences. The study used a specific cell line and culture conditions, and the impact of genomic aberrations on organoid functionality requires further investigation. The differentiation efficiency and reproducibility might vary with different hiPSC lines.

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