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Enhanced bone formation using hydroxyapatite ceramic coated with fibroblast growth factor-2.

机译:使用涂有成纤维细胞生长因子2的羟基磷灰石陶瓷增强骨骼形成。

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Our objective was to develop a bone substitute coated with fibroblast growth factor-2 (FGF-2) that subsequently releases FGF-2. We investigated the use of our system of bone substitutes to induce bone formation. Hydroxyapatite ceramic buttons (HAP-CBs) were coated with FGF-2 by precipitation in supersaturated calcium phosphate solution. HAP-CBs were coated with high or low doses of FGF-2, denoted as FGF-H and FGF-L. The release of FGF-2 from FGF-H and FGF-L was evaluated using its release profile and bioactivity. The efficacy of the subsequent bone formation was quantified using rats with round-shaped bone defects (5mm in diameter) of the right parietal bone. Group 1 was treated only with HAP-CBs, group 2 with HAP-CBs and drops of FGF-2 solution, group 3 with FGF-L and group 4 with FGF-H. To detect the release of FGF-2 in vivo, the expression of bone morphogenic protein-2 (BMP-2) was measured in the defective bone tissue. FGF-2 was released in vitro from FGF-H and FGF-L, and maintained its bioactivity. Rats treated with FGF-L showed better bone formation than rats from the other groups. BMP-2 expression was detected in the defective bone tissues of group 3 at 14 days, which might indicate in vivo FGF-2 release during this period. A specific FGF-2 concentration may be needed for bone formation, and our system can release FGF-2 at adequate concentrations to induce bone formation.
机译:我们的目标是开发一种涂覆有成纤维细胞生长因子2(FGF-2)并随后释放FGF-2的骨替代物。我们调查了使用我们的骨替代系统来诱导骨形成的过程。通过在过饱和磷酸钙溶液中沉淀,用FGF-2涂覆羟基磷灰石陶瓷纽扣(HAP-CBs)。 HAP-CB涂有高剂量或低剂量的FGF-2,分别表示为FGF-H和FGF-L。使用FGF-2的释放曲线和生物活性评估了FGF-2从FGF-H和FGF-L的释放。使用具有右顶骨的圆形骨缺损(直径5mm)的大鼠来量化随后的骨形成的功效。第1组仅用HAP-CBs治疗,第2组用HAP-CBs和FGF-2滴剂治疗,第3组用FGF-L治疗,第4组用FGF-H治疗。为了检测体内FGF-2的释放,在有缺陷的骨组织中测量了骨形态发生蛋白2(BMP-2)的表达。 FGF-2从FGF-H和FGF-L体外释放,并保持其生物活性。用FGF-L治疗的大鼠显示出比其他组更好的骨形成。在第14天在第3组的缺损骨组织中检测到BMP-2表达,这可能表明在此期间体内FGF-2释放。骨骼形成可能需要特定的FGF-2浓度,并且我们的系统可以释放足够浓度的FGF-2来诱导骨骼形成。

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