Bone inductive potential and dose-dependent response of bovine bone morphogenetic protein combined with type IV collagen carrier.

T J Gao, T S Lindholm, A Marttinen, T Puolakka
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Abstract

Using type IV collagen as carrier, the expression of bovine bone morphogenetic protein (bBMP) activity and the relation of ectopic bone formation to BMP dosage in the reconstitution were investigated in BALB mice. Visible heterotopic bone was induced by GuHCl-extracted bovine BMP at a minimal dose of 0.5 mg within 21 days after the BMP was covalently bound to type IV collagen of weight 5.6 mg. The dose-dependent osteogenetic response of BMP was retained in the BMP/type IV collagen composite. As the BMP dose increased in the reconstitution, the integrated intensity and area of bone and cartilage formation, as quantified by a computerized scanner, were enhanced. Degradation of the collagenous carrier was improved by BMP, and neovascularization of the implant site initiated by type IV collagen was also observed. The covalent binding of BMP to type IV collagen postponed the time-sequence of ectopic bone development induced by BMP alone. The conclusion was that the exaggerated and extended effects of type IV collagen on BMP are mainly due to chemotaxis to progenitor cells, immunogenetically inert, vascular initiation and biodegradability in type IV collagen.

牛骨形态发生蛋白联合IV型胶原载体的骨诱导电位及剂量依赖性反应。
以IV型胶原为载体,研究了BALB小鼠重建过程中牛骨形态发生蛋白(bBMP)活性的表达及异位骨形成与BMP剂量的关系。骨形成蛋白与重5.6 mg的IV型胶原共价结合后21天内,以最小剂量0.5 mg的guhcl提取牛BMP诱导可见异位骨。在BMP/ IV型胶原复合物中,BMP的剂量依赖性成骨反应得以保留。随着重建中BMP剂量的增加,计算机扫描仪量化的骨和软骨形成的综合强度和面积得到增强。BMP促进了胶原载体的降解,IV型胶原也促进了植入部位的新生血管形成。BMP与IV型胶原的共价结合延缓了BMP单独诱导异位骨发育的时间顺序。结果表明,IV型胶原对BMP作用的放大和扩展主要是由于IV型胶原对祖细胞的趋化性、免疫遗传惰性、血管起始性和生物降解性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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