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首页> 外文期刊>Cytotherapy >Fate of bone marrow mesenchymal stromal cells following autologous transplantation in a rabbit model of osteonecrosis
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Fate of bone marrow mesenchymal stromal cells following autologous transplantation in a rabbit model of osteonecrosis

机译:自体移植在兔骨坏死模型中骨髓间充质基质细胞的命运

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摘要

Background aims. Internalizing quantum dots (i-QDs) are a useful tool for tracking cells in vivo in models of tissue regeneration. We previously synthesized i-QDs by conjugating QDs with a unique internalizing antibody against a heat shock protein 70 family stress chaperone. In the present study, i-QDs were used to label rabbit mesenchymal stromal cells (MSCs) that were then transplanted into rabbits to assess differentiation potential in an osteonecrosis-model. Methods. The i-QDs were taken up by bone marrow-derived MSCs collected from the iliac of 12-week-old Japanese white rabbits that were positive for cluster of differentiation (CD)81 and negative for CD34 and human leukocyte antigen DR. The average rate of i-QD internalization was 93.3%. At 4, 8, 12, and 24 weeks after transplantation, tissue repair was evaluated histologically and by epifluorescence and electron microscopy. Results. The i-QDs were detected at the margins of the drill holes and in the necrotized bone trabecular. There was significant colocalization of the i-QD signal in transplanted cells and markers of osteoblast and mineralization at 4, 8, and 12 weeks post-transplantation, while i-QDs were detected in areas of mineralization at 12 and 24 weeks post-transplantation. Moreover, i-QDs were observed in osteoblasts in regenerated tissue by electron microscopy, demonstrating that the tissue was derived from transplanted cells. Conclusion. These results indicate that transplanted MSCs can differentiate into osteoblasts and induce tissue repair in an osteonecrosis model and can be tracked over the long term by i-QD labeling.
机译:背景目标。内在化量子点(i-QD)是在组织再生模型中追踪体内细胞的有用工具。我们先前通过将QD与抗热激蛋白70家族应激伴侣的独特内在化抗体缀合来合成i-QD。在本研究中,i-QD用于标记兔间充质基质细胞(MSC),然后将其移植到兔中以评估骨坏死模型中的分化潜能。方法。 i-QDs由从12周大的日本白兔的中收集的骨髓来源的MSC吸收,这些MSC的分化簇(CD)81阳性,而CD34和人白细胞抗原DR阴性。 i-QD内部化的平均率为93.3%。移植后第4、8、12和24周,通过组织学,表面荧光和电子显微镜对组织修复进行评估。结果。 i-QD在钻孔边缘和坏死的骨小梁中检测到。在移植后第4、8和12周,i-QD信号在移植细胞中显着共定位,并在成骨和矿化标志物上存在显着共存,而在移植后12和24周的矿化区域中检测到i-QD。此外,通过电子显微镜在再生组织中的成骨细胞中观察到了i-QD,表明该组织来源于移植的细胞。结论。这些结果表明,移植的MSC可以在成骨坏死模型中分化为成骨细胞并诱导组织修复,并且可以通过i-QD标记长期追踪。

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