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首页> 外文期刊>Tissue engineering, Part A >Endothelial progenitor cells and mesenchymal stem cells seeded onto beta-TCP granules enhance early vascularization and bone healing in a critical-sized bone defect in rats.
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Endothelial progenitor cells and mesenchymal stem cells seeded onto beta-TCP granules enhance early vascularization and bone healing in a critical-sized bone defect in rats.

机译:植入β-TCP颗粒的内皮祖细胞和间充质干细胞可增强大鼠的临界大小骨缺损中的早期血管形成和骨愈合。

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摘要

QUESTION/AIM: Lack of vessels indicates an insufficient nutritional supply of a bone graft and may limit the recruitment of bone-forming cells. Our aim was to evaluate the influence of endothelial progenitor cells (EPCs) alone or in combination with mesenchymal stem cells (MSCs) on early vascularization and bone healing in critical-sized defect (CSD) in vivo. METHODS: MSCs from human bone marrow and EPCs from buffy coat were used. A femoral CSD in adult athymic rats was created and stabilized by an external fixateur. The remaining defects were filled with fibronectin-coated beta-tricalcium phosphate (beta-TCP) granules, EPCs seeded on beta-TCP, MSCs seeded on beta-TCP, coculture of EPCs/MSCs seeded on beta-TCP, or autologous bone. Vascularization and bone formation were determined by immunohistology, microCT analysis, and biomechanical testing after 1, 4, and 8 weeks. RESULTS: Early vascularization was significantly improved in EPC/MSC group or EPC group, respectively. At 4 weeks bone formation increased significantly when the CSD was treated with coculture of MSCs/EPCs. Eight weeks after transplantation CSD showed significantly more bony bridgings and significantly increased ultimate load in the EPC/MSC group compared to the other groups. DISCUSSION: This cell approach suggests that there is a synergistic effect and that the initial stage of neovascularization by EPCs is considered to be crucial for complete bone regeneration in the late phase.
机译:问题/目的:血管不足表明骨移植物的营养供应不足,可能会限制成骨细胞的募集。我们的目的是评估单独或与间充质干细胞(MSCs)联合使用的内皮祖细胞(EPC)对体内临界尺寸缺损(CSD)的早期血管形成和骨愈合的影响。方法:使用人骨髓间充质干细胞和血沉棕黄层的内皮祖细胞。成年无胸腺大鼠的股骨CSD由外固定器产生并稳定。剩余的缺陷用纤连蛋白包被的β-磷酸三钙(β-TCP)颗粒填充,EPC植入β-TCP上,MSC植入β-TCP上,EPC / MSC共同培养在β-TCP上,或自体骨。在1、4和8周后通过免疫组织学,microCT分析和生物力学测试确定血管化和骨形成。结果:EPC / MSC组或EPC组的早期血管形成明显改善。在4周时,将MSCs / EPCs共培养处理CSD后,骨形成明显增加。移植后八周,与其他组相比,CPC在EPC / MSC组中显示出明显更多的骨桥并显着增加了最终负荷。讨论:这种细胞方法表明有协同作用,EPC新生血管形成的初始阶段被认为对于晚期骨再生至关重要。

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