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Enhanced bone regeneration in rat calvarial defects implanted with surface-modified and BMP-loaded bioactive glass (13-93) scaffolds

机译:植入表面修饰和BMP的生物活性玻璃(13-93)支架植入后的大鼠颅骨缺损的骨再生增强

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摘要

The repair of large bone defects, such as segmental defects in the long bones of the limbs, is a challenging clinical problem. Our recent work has shown the ability to create porous scaffolds of silicate 13-93 bioactive glass by robocasting which have compressive strengths comparable to human cortical bone. The objective of this study was to evaluate the capacity of those strong porous scaffolds with a grid-like microstructure (porosity = 50%; filament width = 330 μm; pore width = 300 μm) to regenerate bone in a rat calvarial defect model. Six weeks postimplantation, the amount of new bone formed within the implants was evaluated using histomorphometric analysis. The amount of new bone formed in implants composed of the as-fabricated scaffolds was 32% of the available pore space (area). Pretreating the as-fabricated scaffolds in an aqueous phosphate solution for 1, 3, and 6 days, to convert a surface layer to hydroxyapatite prior to implantation, enhanced new bone formation to 46%, 57%, and 45%, respectively. New bone formation in scaffolds pretreated for 1, 3, and 6 days and loaded with bone morphogenetic protein-2 (BMP-2) (1 μg/defect) was 65%, 61%, and 64%, respectively. The results show that converting a surface layer of the glass to hydroxyapatite or loading the surface-treated scaffolds with BMP-2 can significantly improve the capacity of 13-93 bioactive glass scaffolds to regenerate bone in an osseous defect. Based on their mechanical properties evaluated previously and their capacity to regenerate bone found in this study, these 13-93 bioactive glass scaffolds, pretreated or loaded with BMP-2, are promising in structural bone repair.
机译:大骨缺损的修复,例如四肢长骨中的节段性缺损,是一个具有挑战性的临床问题。我们最近的工作表明,可以通过机器人浇铸法制造具有多孔硅酸盐13-93生物活性玻璃支架的能力,其抗压强度可与人的皮质骨相媲美。这项研究的目的是在大鼠颅骨缺损模型中评估那些具有网格状微结构(孔隙率= 50%;细丝宽度= 330μm;孔宽度= 300μm)的坚固多孔支架的再生能力。植入后六周,使用组织形态分析法评估了植入物内形成的新骨量。由制成的脚手架组成的植入物中形成的新骨量为可用孔隙空间(面积)的32%。在植入的磷酸盐水溶液中预处理制成的支架1、3和6天,以在植入前将表面层转化为羟基磷灰石,从而将新骨形成分别提高至46%,57%和45%。预处理1、3和6天并装载骨形态发生蛋白2(BMP-2)(1μg/缺陷)的支架中的新骨形成分别为65%,61%和64%。结果表明,将玻璃的表面层转变为羟基磷灰石或用BMP-2加载经过表面处理的支架可以显着提高13-93种生物活性玻璃支架在骨缺损中再生骨骼的能力。根据先前评估过的机械性能和在本研究中发现的再生骨的能力,这些经过预处理或负载BMP-2的13-93生物活性玻璃支架有望在结构性骨修复中发挥作用。

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