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Human autologous iPSC-derived dopaminergic progenitors restore motor function in Parkinson's disease models

Authors
Song, BinCha, YoungKo, SanghyeokJeon, JehaLee, NayeonSeo, HyemyungPark, Kyung-JoonLee, In-HeeLopes, ClaudiaFeitosa, MelissaLuna, Maria JoseJung, Jin HyukKim, JisunHwang, DabinCohen, Bruce M.Teicher, Martin H.Leblanc, PierreCarter, Bob S.Kordower, Jeffrey H.Bolshakov, Vadim Y.Kong, Sek WonSchweitzer, Jeffrey S.Kim, Kwang-Soo
Issue Date
Feb-2020
Publisher
American Society for Clinical Investigation
Citation
Journal of Clinical Investigation, v.130, no.2, pp.904 - 920
Indexed
SCIE
SCOPUS
Journal Title
Journal of Clinical Investigation
Volume
130
Number
2
Start Page
904
End Page
920
URI
https://scholarworks.bwise.kr/erica/handle/2021.sw.erica/1289
DOI
10.1172/JCI130767
ISSN
0021-9738
Abstract
Parkinson's disease (PD) is a neurodegenerative disorder associated with loss of striatal dopamine, secondary to degeneration of midbrain dopamine (mDA) neurons in the substantia nigra, rendering cell transplantation a promising therapeutic strategy. To establish human induced pluripotent stem cell-based (hiPSC-based) autologous cell therapy, we report a platform of core techniques for the production of mDA progenitors as a safe and effective therapeutic product. First, by combining metabolism-regulating microRNAs with reprogramming factors, we developed a method to more efficiently generate clinical-grade iPSCs, as evidenced by genomic integrity and unbiased pluripotent potential. Second, we established a "spotting"-based in vitro differentiation methodology to generate functional and healthy mDA cells in a scalable manner. Third, we developed a chemical method that safely eliminates undifferentiated cells from the final product. Dopaminergic cells thus express high levels of characteristic mDA markers, produce and secrete dopamine, and exhibit electrophysiological features typical of mDA cells. Transplantation of these cells into rodent models of PD robustly restores motor function and reinnervates host brain, while showing no evidence of tumor formation or redistribution of the implanted cells. We propose that this platform is suitable for the successful implementation of human personalized autologous cell therapy for PD.
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ERICA 과학기술융합대학 (ERICA 의약생명과학과)
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