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Preliminary evaluation of a load-bearing BMP-2 carrier for segmental defect regeneration.

机译:对分段缺陷再生的承重BMP-2载体的初步评估。

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Large segmental defects in bones can result from tumor removal, massive trauma, congenital malformation, or non-union fractures. Such defects often are difficult to manage and require multiple-phase surgery to achieve adequate union and function. In this study, we propose a novel design of bone morphogenetic protein 2 (BMP-2) carrier for tissue engineering of segmental defect regeneration. The tube-shaped BMP-2 carrier was fabrication from a poly(propylene fumarate)/tricalcium phosphate (PPF/TCP) composite via casting technique developed in our laboratory. An in vitro evaluation showed that the compressive strength of the carrier decreased about 48% in 12 weeks while maintained a pH in the 6.8-7.4 range. In vivo study was conducted by implanting carriers loaded with 10 microg of BMP-2 in 5 mm rat femur gap model for 15 weeks. X-ray evidence of bridging was first found in the BMP group at 3 weeks. Bridging in all animals (N = 4) in the BMP group was found at 9 weeks. No x-ray evidence of bridging was found in the No BMP group (N = 3). pQCT analysis indicated that the bone mineral density of the callus in the BMP group has reached the level of native femur at 15 weeks after implantation, while the callus in the No BMP group has a bone mineral density at a lower level of 84% to the native femur. Histology analysis shows that a normal fatty bone marrow was restored and mineralized callus formed and bridged the segmental defect.
机译:肿瘤的切除,巨大的创伤,先天性畸形或不愈合的骨折可能导致骨骼中较大的节段性缺损。此类缺陷通常难以管理,需要进行多阶段手术才能实现足够的结合和功能。在这项研究中,我们提出了一种新的骨形态发生蛋白2(BMP-2)载体设计,用于组织工程性节段性缺损的再生。管状BMP-2载体是由富马酸丙二酯/磷酸三钙(PPF / TCP)复合材料通过我们实验室开发的铸造技术制成的。体外评估表明,载体的抗压强度在12周内下降了约48%,而pH值保持在6.8-7.4范围内。通过将载有10微克BMP-2的载体植入5 mm大鼠股骨间隙模型中进行15周的体内研究。 BMP组在3周时首次发现X射线桥接的证据。在第9周发现BMP组中所有动物的桥接(N = 4)。 No BMP组中未发现桥接的X射线证据(N = 3)。 pQCT分析表明,BMP组的愈伤组织的骨矿物质密度在植入后15周达到了天然股骨的水平,而No BMP组的愈伤组织的骨矿物质密度比正常的低84%。股骨。组织学分析表明,正常的脂肪骨髓得以恢复,矿化的愈伤组织形成并弥合了节段性缺损。

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