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Nanofibrous substrates support colony formation and maintain stemness of human embryonic stem cells

机译:纳米纤维底物支持集落形成并维持人类胚胎干细胞的干性

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摘要

Inadequate cell numbers in culture is one of the hurdles currently delaying the application of human embryonic stem cells (hESCs) for transplantation therapy. Nanofibrous scaffolds have been effectively used to expand and differentiate non-colony forming multipotent mesenchymal stem cells (MSC) for the repair of tissues or organs. In the present study, we evaluated the influence of nanofibrous scaffolds for hESC proliferation, increase in colony formation, self-renewal properties, undifferentiation and retention of ‘stemness’. Polycaprolactone/collagen (PCL/collagen) and PCL/gelatin nanofibrous scaffolds were fabricated using electrospinning technology. The hESCs were seeded on the nanofibrous scaffolds in the presence or absence of mitomycin-C treated mouse embryonic fibroblasts (MEFs). The hESCs grown on both scaffolds in the presence of the MEFs produced an increase in cell growth of 47.58% (P≤ 0.006) and 40.18% (P≤ 0.005), respectively, over conventional controls of hESCs on MEFs alone. The hESC colonies were also larger in diameter on the scaffolds compared to controls (PCL/collagen, 156.25 ± 7 μM and PCL/gelatin, 135.42 ± 5 μM). Immunohistochemistry of the hESCs grown on the nanofibrous scaffolds with MEFs, demonstrated positive staining for the various stemness-related markers (octamer 4 [OCT-4], tumour rejection antigen-1–60, GCTM-2 and TG-30), and semi-quantitative RT-PCR for the pluripotent stemness genomic markers (NANOG, SOX-2, OCT-4) showed that they were also highly expressed. Continued successful propagation of hESC colonies from nanofibrous scaffolds back to conventional culture on MEFs was also possible. Nanofibrous scaffolds support hESC expansion in an undifferentiated state with retention of stemness characteristics thus having tremendous potential in scaling up cell numbers for transplantation therapy.
机译:培养中细胞数量不足是目前延迟将人类胚胎干细胞(hESC)应用于移植治疗的障碍之一。纳米纤维支架已被有效地用于扩展和分化非集落形成的多能间充质干细胞(MSC),以修复组织或器官。在本研究中,我们评估了纳米纤维支架对hESC增殖,菌落形成增加,自我更新特性,未分化和“干性”保留的影响。聚己内酯/胶原蛋白(PCL /胶原蛋白)和PCL /明胶纳米纤维支架是使用静电纺丝技术制造的。在有丝裂霉素C处理的小鼠胚胎成纤维细胞(MEF)存在或不存在的情况下,将hESC接种在纳米纤维支架上。与仅在MEFs上进行hESC的常规对照相比,在MEFs存在下在两种支架上生长的hESC分别使细胞生长增加了47.58%(P≤0.006)和40.18%(P≤0.005)。与对照相比,支架上的hESC菌落直径也更大(PCL /胶原蛋白为156.25±7μM,PCL /明胶为135.42±5μM)。在具有MEF的纳米纤维支架上生长的hESC的免疫组织化学显示,各种干性相关标记(八聚物4 [OCT-4],肿瘤排斥抗原-1-60,GCTM-2和TG-30)和半多能干基因组标记(NANOG,SOX-2,OCT-4)的定量RT-PCR显示它们也高度表达。还可以将hESC菌落从纳米纤维支架继续成功繁殖回MEF上的常规培养物。纳米纤维支架在未分化状态下支持hESC扩增并保留了茎特征,因此在扩大用于移植治疗的细胞数量方面具有巨大潜力。

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