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首页> 外文期刊>Italian Journal of Anatomy and Embryology >Isolation and phenotypical characterization of mesenchymal stem cells from the Wharton’s jelly of preterm human umbilical cord
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Isolation and phenotypical characterization of mesenchymal stem cells from the Wharton’s jelly of preterm human umbilical cord

机译:沃顿早产儿脐带果冻中间充质干细胞的分离和表型表征

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Extraembryonic tissues such as umbilical cord are considered a promising source of stem cells, potentially useful in therapy. Pre-term umbilical cords may be also a useful source of mesenchymal populations, given also that pre-term birth infants may develop diseases during childhood which may be reverted by a cell therapy approach. Pre-term cords can be also made available from therapeutic abortions, providing a further cell source to obtain high numbers of WJ-MSCs. Little is known about the phenotype and differentiative potential of these cells. Preterm UC were obtained following therapeutic abortions after mothers’ informed consent and processed within 12 hours from tissue collection. Characterization of cells was performed at P2 and P5, by both flow cytometry (FC) and ICC, to detect of classical MSC markers, immunomodulatory molecules, tissue-specific markers.The isolation protocol allowed to successfully derive WJ-MSCs which showed the typical morphology, and were routinely passaged up to passage 10. Multi-color flow cytometric analyses showed that isolated cells were positive for classical MSCs markers (CD29, CD44, CD73, CD90, CD105) and. negative (or weakly positive) for typical hematopoietic and endothelial markers (CD45, CD34, CD14, CD68, CD39 and CD31). In addition, we demonstrated the expression of tissue specific markers, both endodermal (CK18, CK19, alpha-fetoprotein and albumin) and neuro-ectodermal (nestin). This may indicate the potential of preterm WJ-MSC to undergo multiple differentiation pathways, as demonstrated for cells isolated from term UC. Preterm WJ-MSCs showed MHC class I expression (but not class II), suggesting hypoimmunogenic properties for these cells. Moreover, B7H3 expression should favor immune tolerance by the host following cellular transplantation. ICC allowed confirming part of the FC data and was used to assess the expression of further antigens. Present data demonstrate that preterm WJ-MSCs can be isolated and expanded, with high reproducibility. these cells do express classical MSC markers and immunomodulatory molecules, independently from the underlying pathology which led to abortion.
机译:胚外组织(如脐带)被认为是有前途的干细胞来源,可能在治疗中有用。考虑到早产婴儿可能会在儿童期发展成疾病,并且可以通过细胞疗法来治愈,因此早产脐带可能也是间充质人群的有用来源。早产脐带也可以从治疗性流产中获得,从而为获得大量WJ-MSC提供了进一步的细胞来源。这些细胞的表型和分化潜能知之甚少。在母亲知情同意后进行治疗性流产后获得早产UC,并在收集组织后的12小时内进行处理。通过流式细胞术(FC)和ICC在P2和P5对细胞进行表征,以检测经典MSC标记,免疫调节分子和组织特异性标记。分离方案可以成功衍生出表现出典型形态的WJ-MSC ,并常规传代至第10代。多色流式细胞术分析表明,分离的细胞对经典MSCs标记(CD29,CD44,CD73,CD90,CD105)呈阳性。对典型的造血和内皮标记(CD45,CD34,CD14,CD68,CD39和CD31)呈阴性(或弱阳性)。此外,我们证明了组织特异性标志物的表达,包括内胚层(CK18,CK19,甲胎蛋白和白蛋白)和神经外胚层(nestin)。这可能表明早产WJ-MSC经历多种分化途径的潜力,如从学期UC分离的细胞所证实的。早产WJ-MSCs显示MHC I类表达(但不显示II类),表明这些细胞的免疫原性较低。此外,B7H3表达应有利于细胞移植后宿主的免疫耐受。 ICC可以确认部分FC数据,并用于评估其他抗原的表达。目前的数据表明,早产WJ-MSC可以被分离和扩增,具有高再现性。这些细胞确实表达经典的MSC标志物和免疫调节分子,而与导致流产的潜在病理学无关。

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