小颗粒双相骨替代物支持快速种植床血管化。

M Barbeck, M Dard, M Kokkinopoulou, J Markl, P Booms, R A Sader, C J Kirkpatrick, S Ghanaati
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引用次数: 44

摘要

本研究在大鼠皮下植入模型中研究了两种双相骨替代物(BoneCeramic®400-700 μm和500-1000 μm)颗粒大小对诱导多核巨细胞(MNGCs)和植入床血管形成的影响。通过透射电子显微镜(TEM)研究了两种材料的降解机制和颗粒吞噬作用。两种颗粒类型均诱导主要涉及单个核细胞和少量MNGCs的组织反应。小颗粒组在第30天开始检测到较多的MNGCs,而在第10天仅观察到较高的血管化。透射电镜分析表明,单核细胞和多核细胞都参与了物质的吞噬。此外,结果允许将MNGCs识别为异物巨细胞表型。吞噬颗粒的组织形态学分析显示,两种颗粒类型之间没有差异。结果表明,颗粒大小似乎对早期植入床血管化有影响,也对组织反应后期MNGCs的诱导有影响。此外,研究结果表明,合成骨替代材料可以诱导类似于某些异种材料的组织反应,因此需要阐明其“理想”的物理特性。结果还表明,颗粒大小在研究范围内不改变单核细胞的吞噬作用。最后,研究证实了材料诱导的MNGCs的分化,属于异物巨细胞类型。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Small-sized granules of biphasic bone substitutes support fast implant bed vascularization.

Small-sized granules of biphasic bone substitutes support fast implant bed vascularization.

Small-sized granules of biphasic bone substitutes support fast implant bed vascularization.

Small-sized granules of biphasic bone substitutes support fast implant bed vascularization.

The present study investigated the influence of granule size of 2 biphasic bone substitutes (BoneCeramic® 400-700 μm and 500-1000 μm) on the induction of multinucleated giant cells (MNGCs) and implant bed vascularization in a subcutaneous implantation model in rats. Furthermore, degradation mechanisms and particle phagocytosis of both materials were examined by transmission electron microscopy (TEM). Both granule types induced tissue reactions involving primarily mononuclear cells and only small numbers of MNGCs. Higher numbers of MNGCs were detected in the group with small granules starting on day 30, while higher vascularization was observed only at day 10 in this group. TEM analysis revealed that both mono- and multinucleated cells were involved in the phagocytosis of the materials. Additionally, the results allowed recognition of the MNGCs as the foreign body giant cell phenotype. Histomorphometrical analysis of the size of phagocytosed particles showed no differences between the 2 granule types. The results indicate that granule size seems to have impact on early implant bed vascularization and also on the induction of MNGCs in the late phase of the tissue reaction. Furthermore, the results revealed that a synthetic bone substitute material can induce tissue reactions similar to those of some xenogeneic materials, thus pointing to a need to elucidate their "ideal" physical characteristics. The results also show that granule size in the range studied did not alter phagocytosis by mononuclear cells. Finally, the investigation substantiates the differentiation of material-induced MNGCs, which are of the foreign body giant cell type.

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