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Very small embryonic-like stem-cell optimization of isolation protocols: an update of molecular signatures and a review of current in vivo applications

机译:很小的类胚胎干细胞分离方案的优化:分子标记的更新和当前体内应用的综述

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摘要

As the theory of stem cell plasticity was first proposed, we have explored an alternative hypothesis for this phenomenon: namely that adult bone marrow (BM) and umbilical cord blood (UCB) contain more developmentally primitive cells than hematopoietic stem cells (HSCs). In support of this notion, using multiparameter sorting we were able to isolate small Sca1+LinCD45 cells and CD133+LinCD45 cells from murine BM and human UCB, respectively, which were further enriched for the detection of various early developmental markers such as the SSEA antigen on the surface and the Oct4 and Nanog transcription factors in the nucleus. Similar populations of cells have been found in various organs by our team and others, including the heart, brain and gonads. Owing to their primitive cellular features, such as the high nuclear/cytoplasm ratio and the presence of euchromatin, they are called very small embryonic-like stem cells (VSELs). In the appropriate in vivo models, VSELs differentiate into long-term repopulating HSCs, mesenchymal stem cells (MSCs), lung epithelial cells, cardiomyocytes and gametes. In this review, we discuss the most recent data from our laboratory and other groups regarding the optimal isolation procedures and describe the updated molecular characteristics of VSELs.
机译:随着干细胞可塑性理论的首次提出,我们已经探索了针对这种现象的另一种假设:即,成年骨髓(BM)和脐带血(UCB)包含比造血干细胞(HSC)更多的发育原始细胞。为了支持此概念,使用多参数排序,我们能够分离出小的Sca1 + Lin - CD45 -单元格和CD133 + <分别来自鼠BM和人UCB的/ sup> Lin - CD45 -细胞,这些细胞进一步富集用于检测各种早期发育标记,例如SSEA抗原。表面以及细胞核中的Oct4和Nanog转录因子。我们的研究小组和其他机构,包括心脏,大脑和性腺,在各种器官中也发现了类似的细胞群体。由于其原始的细胞特征,例如高的核/细胞质比率和常染色质的存在,它们被称为非常小的胚胎样干细胞(VSEL)。在适当的体内模型中,VSELs分化为长期重生的HSC,间充质干细胞(MSC),肺上皮细胞,心肌细胞和配子。在这篇综述中,我们讨论了来自实验室和其他小组的有关最佳分离程序的最新数据,并描述了VSEL的更新分子特性。

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