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Neural stem cells derived from human midbrain organoids as a stable source for treating Parkinson’s disease

类有机物 诱导多能干细胞 神经干细胞 生物 移植 干细胞 神经科学 细胞分化 细胞生物学 中脑 细胞疗法 胚胎干细胞 中枢神经系统 医学 内科学 生物化学 基因
作者
Seung Won Kim,Hye-Ji Woo,Eun Hee Kim,Hyung Sun Kim,Han Na Suh,Soo-hyun Kim,Jae J. Song,Noviana Wulansari,Minji Kang,Se‐Young Choi,Su Jeong Choi,Won Hyuk Jang,Jungbin Lee,Ki Hean Kim,Wongyoung Lee,Sung Hyun Kim,Jinhee Yang,Jangbeen Kyung,Hyun‐Seob Lee,Sang Myun Park
出处
期刊:Progress in Neurobiology [Elsevier]
卷期号:204: 102086-102086 被引量:42
标识
DOI:10.1016/j.pneurobio.2021.102086
摘要

Successful clinical translation of stem cell-based therapy largely relies on the scalable and reproducible preparation of donor cells with potent therapeutic capacities. In this study, midbrain organoids were yielded from human pluripotent stem cells (hPSCs) to prepare cells for Parkinson's disease (PD) therapy. Neural stem/precursor cells (NSCs) isolated from midbrain organoids (Og-NSCs) expanded stably and differentiated into midbrain-type dopamine(mDA) neurons, and an unprecedentedly high proportion expressed midbrain-specific factors, with relatively low cell line and batch-to-batch variations. Single cell transcriptome analysis followed by in vitro assays indicated that the majority of cells in the Og-NSC cultures are ventral midbrain (VM)-patterned with low levels of cellular senescence/aging and mitochondrial stress, compared to those derived from 2D-culture environments. Notably, in contrast to current methods yielding mDA neurons without astrocyte differentiation, mDA neurons that differentiated from Og-NSCs were interspersed with astrocytes as in the physiologic brain environment. Thus, the Og-NSC-derived mDA neurons exhibited improved synaptic maturity, functionality, resistance to toxic insults, and faithful expressions of the midbrain-specific factors, in vitro and in vivo long after transplantation. Consequently, Og-NSC transplantation yielded potent therapeutic outcomes that are reproducible in PD model animals. Collectively, our observations demonstrate that the organoid-based method may satisfy the demands needed in the clinical setting of PD cell therapy.
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