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Isolation, Characterization, and Transduction of Endometrial Decidual Tissue Multipotent Mesenchymal Stromal/Stem Cells from Menstrual Blood

机译:子宫内膜蜕膜组织多能量间充质/干细胞的分离,表征和转导来自月经血

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Mesenchymal stromal/stem cells (MSCs) reveal progenitor cells-like features including proliferation and differentiation capacities. One of the most historically recognized sources of MSC has been the bone marrow, while other sources recently include adipose tissue, teeth, bone, muscle, placenta, liver, pancreas, umbilical cord, and cord blood. Frequently, progenitor isolation requires traumatic procedures that are poorly feasible and associated with patient discomfort. In the attempt to identify a more approachable MSC source, we focused on endometrial decidual tissue (EDT) found within menstrual blood. Based also on recent literature findings, we hypothesized that EDT may contain heterogeneous populations including some having MSC-like features. Thus, we here sought to isolate EDT-MSC processing menstrual samples from multiple donors. Cytofluorimetric analyses revealed that resulting adherent cells were expressing mesenchymal surface markers, including CD56, CD73, CD90, CD105 and CD146, and pluripotency markers such as SSEA-4. Moreover, EDT-MSC showed a robust donogenic potential and could be largely expanded in vitro as fibroblastoid elements. In addition, differentiation assays drove these cells towards osteogenic, adipogenic, and chondrogenic lineages. Finally, for the first time, we were able to gene modify these progenitors by a retroviral vector carrying the green fluorescent protein. From these data, we suggest that EDT-MSC could represent a new promising tool having potential within cell and gene therapy applications.
机译:间充质基质/干细胞(MSCs)揭示了祖细胞样特征,包括增殖和分化能力。最历史最公认的MSC来源是骨髓,而其他来源最近包括脂肪组织,牙齿,骨骼,肌肉,胎盘,肝脏,胰腺,脐带和脐带血。通常,祖子分离需要创伤性程序,其可行并且与患者不适相关。在尝试识别更接近的MSC源,我们专注于月经血液中发现的子宫内膜蜕膜组织(EDT)。在最近的文献发现中,我们假设EDT可能含有异构种群,包括一些具有MSC的特征。因此,我们在这里寻求将EDT-MSC加工来自多个捐赠者的月经样本。细胞杂氟化学分析显示,所得到的粘附细胞表达间充质表面标志物,包括CD56,CD73,CD90,CD105和CD146,以及多能性标记,如SSEA-4。此外,EDT-MSC显示出稳健的膨胀潜力,并且可以在很大程度上在体外扩展,作为纤维细胞元素元素。此外,分化测定将这些细胞推向骨质发生,脂肪组和软骨内谱系。最后,首次,我们能够通过携带绿色荧光蛋白的逆转录病毒载体来改变这些祖细胞。从这些数据来看,我们建议EDT-MSC可以代表具有细胞和基因治疗应用中具有潜力的新有前途的工具。

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