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人胚胎干细胞中NANOG的过表达可实现无饲养层培养,同时诱导原始外胚层特征。

Overexpression of NANOG in human ES cells enables feeder-free growth while inducing primitive ectoderm features.

作者信息

Darr Henia, Mayshar Yoav, Benvenisty Nissim

机构信息

Department of Genetics, Institute of Life Sciences, The Hebrew University, Jerusalem, Israel.

出版信息

Development. 2006 Mar;133(6):1193-201. doi: 10.1242/dev.02286.

Abstract

Human embryonic stem cells (HESCs) are pluripotent cells derived from the ICM of blastocyst stage embryos. As the factors needed for their growth are largely undefined, they are propagated on feeder cells or with conditioned media from feeder cells. This is in contrast to mouse embryonic stem cells (MESCs) where addition of leukemia inhibitory factor (LIF) replaces the need for a feeder layer. Recently, the transcription factor Nanog was suggested to allow LIF and feeder-free growth of MESCs. Here, we show that NANOG overexpression in HESCs enables their propagation for multiple passages during which the cells remain pluripotent. NANOG overexpressing cells form colonies efficiently even at a very low density, an ability lost upon excision of the transgene. Cells overexpressing NANOG downregulate expression of markers specific to the ICM and acquire expression of a marker specific to the primitive ectoderm (the consecutive pluripotent population in the embryo). Examination of global transcriptional changes upon NANOG overexpression by DNA microarray analysis reveals new markers suggested to discriminate between these populations. These results are significant in the understanding of self-renewal and pluripotency pathways in HESCs, and of their use for modeling early development in humans.

摘要

人胚胎干细胞(HESC)是从囊胚期胚胎的内细胞团(ICM)衍生而来的多能细胞。由于其生长所需的因子很大程度上尚不明确,它们在饲养层细胞上或与饲养层细胞的条件培养基一起培养。这与小鼠胚胎干细胞(MESC)不同,在小鼠胚胎干细胞中,添加白血病抑制因子(LIF)可替代对饲养层的需求。最近,有研究表明转录因子Nanog可使MESC在无LIF和饲养层的条件下生长。在此,我们表明在HESC中过表达NANOG可使其进行多次传代培养,在此过程中细胞保持多能性。即使在非常低的密度下,过表达NANOG的细胞也能高效形成集落,而在切除转基因后这种能力丧失。过表达NANOG的细胞下调ICM特异性标志物的表达,并获得原始外胚层(胚胎中连续的多能细胞群体)特异性标志物的表达。通过DNA微阵列分析检测NANOG过表达后的全局转录变化,揭示了可用于区分这些细胞群体的新标志物。这些结果对于理解HESC中的自我更新和多能性途径以及它们在人类早期发育建模中的应用具有重要意义。

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