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Identification of subpopulations in mesenchymal stem cell-like cultures from human umbilical cord

机译:鉴定人脐带间充质干细胞样培养物中的亚群

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摘要

Background: A variety of cell types can be identified in the adherent fraction of bone marrow mononuclear cells including more primitive and embryonic-like stem cells, mesenchymal stem cells (MSC), lineage-committed progenitors as well as mature cells such as osteoblasts and fibroblasts. Different methods are described for the isolation of single bone marrow stem cell subpopulations - beginning from ordinary size sieving, long term cultivation under specific conditions to FACS-based approaches. Besides bone marrow-derived subpopulations, also other tissues including human umbilical cord (UC) have been recently suggested to provide a potential source for MSC. Although of clinical importance, these UC-derived MSC populations remain to be characterized. It was thus the aim of the present study to identify possible subpopulations in cultures of MSC-like cells obtained from UC. We used counterflow centrifugal elutriation (CCE) as a novel strategy to successfully address this question. Results: UC-derived primary cells were separated by CCE and revealed differentially-sized populations in the fractions. Thus, a subpopulation with an average diameter of about 11 μm and a small flat cell body was compared to a large sized subpopulation of about 19 μm average diameter. Flow cytometric analysis revealed the expression of certain MSC stem cell markers including CD44, CD73, CD90 and CD105, respectively, although these markers were expressed at higher levels in the small-sized population. Moreover, this small-sized subpopulation exhibited a higher proliferative capacity as compared to the total UC-derived primary cultures and the large-sized cells and demonstrated a reduced amount of aging cells. Conclusion: Using the CCE technique, we were the first to demonstrate a subpopulation of small-sized UC-derived primary cells carrying MSC-like characteristics according to the presence of various mesenchymal stem cell markers. This is also supported by the high proliferative capacity of these MSC-like cells as compared to whole primary culture or other UC-derived subpopulations. The accumulation of a self-renewing MSC-like subpopulation by CCE with low expression levels of the aging marker senescence-associated β-galactosidase provides a valuable tool in the regenerative medicine and an alternative to bone-marrow-derived MSC.
机译:背景:可以在骨髓单个核细胞的粘附部分中鉴定出多种细胞类型,包括更多的原始和胚胎样干细胞,间充质干细胞(MSC),沿袭定型祖细胞以及成熟细胞,如成骨细胞和成纤维细胞。 。描述了用于分离单个骨髓干细胞亚群的不同方法-从普通筛分,在特定条件下长期培养到基于FACS的方法开始。除了骨髓来源的亚群外,最近还建议其他组织,包括人脐带(UC),为MSC提供潜在的来源。尽管具有临床重要性,但是这些来自UC的MSC群体仍有待表征。因此,本研究的目的是鉴定从UC获得的MSC样细胞的培养物中可能的亚群。我们使用逆流离心淘析(CCE)作为成功解决此问题的新颖策略。结果:通过CCE分离了UC来源的原代细胞,并在级分中显示了不同大小的种群。因此,将平均直径为约11μm,扁平细胞较小的亚种群与平均直径为约19μm的大型亚种群进行了比较。流式细胞仪分析揭示了某些MSC干细胞标记物的表达,分别包括CD44,CD73,CD90和CD105,尽管这些标记物在小规模人群中以较高的水平表达。此外,与总的UC来源的原代培养物和大细胞相比,这种小亚群显示出更高的增殖能力,并显示出减少的衰老细胞数量。结论:根据各种间充质干细胞标记物的存在,我们首先使用CCE技术来证明具有MSC样特征的小型UC来源的原代细胞亚群。与完整的原代培养或其他UC衍生的亚群相比,这些MSC类细胞的高增殖能力也支持了这一点。 CCE自我更新的MSC样亚群的积累与衰老标志物衰老相关的β-半乳糖苷酶的低表达水平在再生医学中提供了有价值的工具,并且可以替代骨髓来源的MSC。

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