Differentiation of dopaminergic neurons from human embryonic stem cells : Modulation of differentiation by FGF-20(CELL AND TISSUE ENGINEERING)
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概要
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Derivation of midbrain dopaminergic (DA) neurons from human embryonic stem (hES) cells has been of particular interest because of the clinical potential for DA neuron transplantation in patients with Parkinson's disease (PD). Several protocols for DA neuron differentiation from mouse embryonic stem cells and hES cells have been reported: however, protocols involving hES cells have yet to be improved. Here, we used a slightly modified stromal cell-derived inducing activity method, consisting four different culture stages, to show that KhES-1 cells differentiate into tyrosine hydroxylase (TH)-positive DA neurons. Quantitative real-time PCR analysis showed a marked induction of the DA neuron marker genes NURR1, paired-like homeodomain transcription factor 3 (PITX3), LIM homeobox transcription- factor 1, beta (LMX1B), engrailed-1 (EN1), dopamine transporter (DAT), and aromatic amino acid decarboxylase (AADC) during differentiation. Treatment with fibroblast growth factor (FGF)-20 and FGF-2 at the final differentiation stage induced the increase of DA neuron development-related transcription factors such as NURR1, PITX3, LMX1B, and EN1. FGF-20 and FGF-2 enhanced DA neuron differentiation from hES cell-derived neural progenitor cells directly without any soluble factors from PA6 cells. These results provide valuable information that will assist in efficient DA neuron differentiation from hES cells and for future transplant application.
著者
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Shimada Hideaki
Department of Tissue and Organ Development, Regeneration and Advanced Medical Science, Gifu Universi
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Yoshimura Naoko
Department of Tissue and Organ Development, Regeneration and Advanced Medical Science, Gifu Universi
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Tsuji Akiko
Department of Tissue and Organ Development, Regeneration and Advanced Medical Science, Gifu Universi
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Kunisada Takahiro
Department of Tissue and Organ Development, Regeneration and Advanced Medical Science, Gifu Universi
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Tsuji Akiko
Department Of Tissue And Organ Development Regeneration And Advanced Medical Science Gifu University
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Tsuji Akiko
Department Of Applied Chemistry Faculty Of Engineering Doshisha University
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Yoshimura Naoko
Department Of Tissue And Organ Development Regeneration And Advanced Medical Science Gifu University
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Yoshimura Naoko
Department Of Radiology Kochi Medical School
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Shimada Hideaki
Department Of Tissue And Organ Development Regeneration And Advanced Medical Science Gifu University
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Shimada Hideaki
Department Of Academic Surgery Graduate School Of Medicine Chiba University
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Kunisada Takahiro
Department Of Tissue And Organ Development Regeneration And Advanced Medical Science Gifu University
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Kunisada Takahiro
Department Of Biophysics Faculty Of Science Kyoto University
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Shimada Hideaki
Department Of Academic Surgery (m9) Graduate School Of Medicine Chiba University
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