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源自胚胎干细胞的神经嵴样细胞的多能细胞命运。

Multipotent cell fate of neural crest-like cells derived from embryonic stem cells.

作者信息

Motohashi Tsutomu, Aoki Hitomi, Chiba Kairi, Yoshimura Naoko, Kunisada Takahiro

机构信息

Department of Tissue and Organ Development, Regeneration and Advanced Medical Science, Gifu University Graduate School of Medicine, Gifu, Japan.

出版信息

Stem Cells. 2007 Feb;25(2):402-10. doi: 10.1634/stemcells.2006-0323. Epub 2006 Oct 12.

Abstract

Neural crest cells migrate throughout the embryo and differentiate into diverse derivatives: the peripheral neurons, cranial mesenchymal cells, and melanocytes. Because the neural crest cells have critical roles in organogenesis, detailed elucidation of neural crest cell differentiation is important in developmental biology. We recently reported that melanocytes could be induced from mouse ESCs. Here, we improved the culture system and showed the existence of neural crest-like precursors. The addition of retinoic acid to the culture medium reduced the hematopoiesis and promoted the expression of the neural crest marker genes. The colonies formed contained neural crest cell derivatives: neurons and glial cells, together with melanocytes. This suggested that neural crest-like cells assuming multiple cell fates had been generated in these present cultures. To isolate the neural crest-like cells, we analyzed the expression of c-Kit, a cell-surface protein expressed in the early stage of neural crest cells in vivo. The c-Kit-positive (c-Kit(+)) cells appeared as early as day 9 of the culture period and expressed the transcriptional factors Sox10 and Snail, which are expressed in neural crest cells. When the c-Kit(+) cells were separated from the cultures and recultured, they frequently formed colonies containing neurons, glial cells, and melanocytes. Even a single c-Kit(+) cell formed colonies that contained these three cell types, confirming their multipotential cell fate. The c-Kit(+) cells were also capable of migrating along neural crest migratory pathways in vivo. These results indicate that the c-Kit(+) cells isolated from melanocyte-differentiating cultures of ESCs are closely related to neural crest cells.

摘要

神经嵴细胞迁移至整个胚胎,并分化为多种衍生物:外周神经元、颅间充质细胞和黑素细胞。由于神经嵴细胞在器官发生中起关键作用,详细阐明神经嵴细胞分化在发育生物学中具有重要意义。我们最近报道,小鼠胚胎干细胞可诱导分化为黑素细胞。在此,我们改进了培养系统,并证实了神经嵴样前体细胞的存在。向培养基中添加视黄酸可减少造血作用,并促进神经嵴标记基因的表达。形成的集落包含神经嵴细胞衍生物:神经元、神经胶质细胞以及黑素细胞。这表明在当前培养物中已产生了具有多种细胞命运的神经嵴样细胞。为了分离神经嵴样细胞,我们分析了c-Kit的表达,c-Kit是一种在体内神经嵴细胞早期表达的细胞表面蛋白。c-Kit阳性(c-Kit(+))细胞最早在培养第9天出现,并表达在神经嵴细胞中表达的转录因子Sox10和Snail。当将c-Kit(+)细胞从培养物中分离并重新培养时,它们经常形成包含神经元、神经胶质细胞和黑素细胞的集落。甚至单个c-Kit(+)细胞也形成了包含这三种细胞类型的集落,证实了它们的多能细胞命运。c-Kit(+)细胞在体内也能够沿着神经嵴迁移途径迁移。这些结果表明,从胚胎干细胞黑素细胞分化培养物中分离出的c-Kit(+)细胞与神经嵴细胞密切相关。

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