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在接触促分化因子后,源自人源前脑神经嵴球体的中枢神经系统前体细胞的长期培养和分化。

Long-term culture and differentiation of CNS precursors derived from anterior human neural rosettes following exposure to ventralizing factors.

机构信息

Laboratorio di Tecnologie della Riproduzione, Avantea, Cremona, Italy.

出版信息

Exp Cell Res. 2010 Apr 15;316(7):1148-58. doi: 10.1016/j.yexcr.2010.02.013. Epub 2010 Feb 17.

Abstract

In this study we demonstrated that neural rosettes derived from human ES cells can give rise either to neural crest precursors, following expansion in presence of bFGF and EGF, or to dopaminergic precursors after exposure to ventralizing factors Shh and FGF8. Both regionalised precursors are capable of extensive proliferation and differentiation towards the corresponding terminally differentiated cell types. In particular, peripheral neurons, cartilage, bone, smooth muscle cells and also pigmented cells were obtained from neural crest precursors while tyrosine hydroxylase and Nurr1 positive dopaminergic neurons were derived from FGF8 and Shh primed rosette cells. Gene expression and immunocytochemistry analyses confirmed the expression of dorsal and neural crest genes such as Sox10, Slug, p75, FoxD3, Pax7 in neural precursors from bFGF-EGF exposed rosettes. By contrast, priming of rosettes with FGF8 and Shh induced the expression of dopaminergic markers Engrailed1, Pax2, Pitx3, floor plate marker FoxA2 and radial glia markers Blbp and Glast, the latter in agreement with the origin of dopaminergic precursors from floor plate radial glia. Moreover, in vivo transplant of proliferating Shh/FGF8 primed precursors in parkinsonian rats demonstrated engraftment and terminal dopaminergic differentiation. In conclusion, we demonstrated the derivation of long-term self-renewing precursors of selected regional identity as potential cell reservoirs for cell therapy applications, such as CNS degenerative diseases, or for the development of toxicological tests.

摘要

在这项研究中,我们证明了源自人类胚胎干细胞的神经玫瑰花结可以在 bFGF 和 EGF 的存在下扩张,产生神经嵴前体,或者在暴露于神经诱导因子 Shh 和 FGF8 后产生多巴胺能前体。这两种区域化的前体都能够广泛增殖,并向相应的终末分化细胞类型分化。特别是,从神经嵴前体中获得了外周神经元、软骨、骨、平滑肌细胞,以及色素细胞,而酪氨酸羟化酶和 Nurr1 阳性多巴胺能神经元则来自于 FGF8 和 Shh 预刺激的玫瑰花结细胞。基因表达和免疫细胞化学分析证实了在 bFGF-EGF 暴露的玫瑰花结中,神经前体细胞表达背侧和神经嵴基因,如 Sox10、Slug、p75、FoxD3、Pax7。相比之下,用 FGF8 和 Shh 预刺激玫瑰花结会诱导多巴胺能标志物 Engrailed1、Pax2、Pitx3、基板标志物 FoxA2 和放射状胶质标志物 Blbp 和 Glast 的表达,这与多巴胺能前体细胞起源于基板放射状胶质相一致。此外,在帕金森病大鼠体内移植增殖的 Shh/FGF8 预刺激前体,证明了其植入和终末多巴胺能分化。总之,我们证明了具有特定区域特征的长期自我更新前体的衍生,这些前体可能成为细胞治疗应用的细胞储备库,如中枢神经系统退行性疾病,或用于开发毒理学测试。

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