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首页> 外文期刊>Biomaterials >The effect of mean pore size on cell attachment, proliferation and migration in collagen-glycosaminoglycan scaffolds for bone tissue engineering.
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The effect of mean pore size on cell attachment, proliferation and migration in collagen-glycosaminoglycan scaffolds for bone tissue engineering.

机译:平均孔径对用于骨组织工程的胶原蛋白-糖胺聚糖支架中细胞附着,增殖和迁移的影响。

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摘要

In the literature there are conflicting reports on the optimal scaffold mean pore size required for successful bone tissue engineering. This study set out to investigate the effect of mean pore size, in a series of collagen-glycosaminoglycan (CG) scaffolds with mean pore sizes ranging from 85 microm to 325 microm, on osteoblast adhesion and early stage proliferation up to 7 days post-seeding. The results show that cell number was highest in scaffolds with the largest pore size of 325 microm. However, an early additional peak in cell number was also seen in scaffolds with a mean pore size of 120 microm at time points up to 48 h post-seeding. This is consistent with previous studies from our laboratory which suggest that scaffold specific surface area plays an important role on initial cell adhesion. This early peak disappears following cell proliferation indicating that while specific surface area may be important for initial cell adhesion, improved cell migration provided by scaffolds with pores above 300 microm overcomes this effect. An added advantage of the larger pores is a reduction in cell aggregations that develop along the edges of the scaffolds. Ultimately scaffolds with a mean pore size of 325 microm were deemed optimal for bone tissue engineering.
机译:在文献中,关于成功进行骨组织工程所需的最佳支架平均孔径的报道相互矛盾。这项研究着手研究平均孔径在一系列平均孔径从85微米至325微米的胶原蛋白-糖胺聚糖(CG)支架中对播种后长达7天的成骨细胞粘附和早期增殖的影响。结果表明,在最大孔径为325微米的支架中,细胞数最高。然而,在播种后长达48小时的时间点,平均孔径为120微米的支架中也发现了细胞数量的早期附加峰。这与我们实验室先前的研究一致,该研究表明支架的比表面积在初始细胞粘附中起着重要作用。细胞增殖后,该早期峰消失,表明虽然比表面积对于初始细胞粘附可能很重要,但孔大于300微米的支架提供的改善的细胞迁移能力克服了这一影响。较大的孔的另一个优点是减少了沿支架边缘发展的细胞聚集。最终,平均孔径为325微米的支架被认为是骨组织工程的最佳选择。

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