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Derivation of human embryonic germ cells: an alternative source of pluripotent stem cells.

机译:人胚胎生殖细胞的衍生:多能干细胞的替代来源。

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Based on evidence suggesting similarities to human embryonic stem cells, human embryonic germ (hEG) cells have been advocated as an alternative pluripotent stem cell resource but have so far received limited attention. To redress this imbalance, human fetal gonads were collected for the isolation and culture of primordial germ cells at 7-9 weeks postconception. We provide evidence for the derivation, culture, and differentiation of hEG cells in vitro. This evidence includes the expression of markers characteristic of pluripotent cells, the retention of normal XX or XY karyotypes, and the demonstration of pluripotency, as suggested by the expression of markers indicative of differentiation along the three germ lineages (ectoderm, mesoderm, and endoderm) and an associated loss of pluripotent markers. In assessing this differentiation, however, we also demonstrate a hitherto unacknowledged overlap in gene expression profiles between undifferentiated and differentiated cell types, highlighting the difficulty in ascribing cell lineage by gene expression analyses. Furthermore, we draw attention to the problems inherent in the management of these cells in prolonged culture, chiefly the difficulty in preventing spontaneous differentiation, which hinders the isolation of pure, undifferentiated clonal lines. While these data advocate the pursuit of pluripotent hEG cell studies with relevance to early human embryonic development, culture limitations carry implications for their potential applicability to ambitious cell replacement therapies.
机译:基于表明与人类胚胎干细胞相似的证据,有人主张将人类胚胎生殖(hEG)细胞作为一种多能干细胞的替代资源,但迄今为止受到的关注有限。为了纠正这种不平衡,在怀孕后7-9周收集了人类胎儿的性腺,以分离和培养原始生殖细胞。我们为体外hEG细胞的衍生,培养和分化提供了证据。该证据包括多能细胞特征性标志物的表达,正常XX或XY核型的保留以及多能性的证明,这表明沿三个胚系(外胚层,中胚层和内胚层)的分化标志物的表达以及相关的多能标记的丧失。然而,在评估这种分化时,我们还证明了未分化和分化细胞类型之间的基因表达谱中迄今尚未确认的重叠,突出了通过基因表达分析确定细胞谱系的难度。此外,我们提请注意长时间培养这些细胞时固有的问题,主要是防止自发分化的困难,这阻碍了纯净,未分化克隆系的分离。尽管这些数据提倡进行与人类早期胚胎发育有关的多能性hEG细胞研究,但培养的局限性对其潜在的雄心勃勃的细胞替代疗法的适用性产生了影响。

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