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Somatic cell transformation into stem cell-like cells induced by different microenvironments

机译:体细胞转化为不同微环境诱导的干细胞样细胞

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摘要

Development of induced pluripotent stem cell (iPSC) technology introduced a novel way to derive pluripotent stem cells, but the genetic manipulation required to generate iPSCs may lead to uncontrolled tumorigenesis of the established cells and thus limit clinical feasibility of the technology. Numerous attempts have been made to date, and alternative reprogramming of somatic cells to reactivate cellular plasticity after differentiation has been suggested. As a result, it had become clear that cell-to-cell interactions and specific acellular environments can be utilized for somatic cell reprogramming. In our previous studies, embryonic stem cell (ESC)-like cells could be derived from transforming ovarian cells and fetal fibroblasts by cell-to-cell interaction or specific cell-mediated microenvironmental factor(s). This cellular event was induced without undertaking genetic manipulation of progenitor cells. Several differences were found between the cellular properties of niche-induced, ESC-like cells and those of genetically manipulated iPSCs and the referenced ESCs. Thus, we provided evidence that terminally differentiated somatic cells either acquire pluripotency-like activity or possess cellular and genetic plasticity under a specific microenvironment and/or cell-to-cell interaction. In this minireview, we discuss derivation of stem cell-like cells under specific microenvironmental conditions in terms of technical perspectives and limitations.
机译:诱导多能干细胞(iPSC)技术的发展引入了一种衍生多能干细胞的新方法,但生成iPSC所需的基因操作可能导致已建立细胞的不可控制的肿瘤发生,从而限制了该技术的临床可行性。迄今为止,已经进行了许多尝试,并且已经提出了在分化后体细胞的替代性重编程以重新激活细胞可塑性。结果,已经清楚的是,细胞间相互作用和特定的脱细胞环境可以用于体细胞重编程。在我们以前的研究中,胚胎干细胞(ESC)样细胞可通过细胞间相互作用或特定的细胞介导的微环境因子衍生自转化的卵巢细胞和胎儿成纤维细胞。该细胞事件是在不进行祖细胞遗传操作的情况下诱发的。发现在生态位诱导的,类似ESC的细胞与经基因处理的iPSC和参照的ESC的细胞特性之间存在一些差异。因此,我们提供的证据表明,在特定的微环境和/或细胞间相互作用下,终末分化的体细胞要么具有多能性的活性,要么具有细胞和遗传的可塑性。在此小型复习中,我们从技术角度和局限性方面讨论了在特定微环境条件下干细胞样细胞的衍生。

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