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Enhanced Bone Regeneration of Cortical Segmental Bone Defects Using Porous Titanium Scaffolds Incorporated with Colloidal Gelatin Gels for Timeand Dose-Controlled Delivery of Dual Growth Factors

机译:使用多孔钛支架与胶体明胶凝胶结合的时间和剂量控制的双重生长因子的多孔钛支架增强皮质节段性骨缺损的骨再生。

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摘要

Porous titanium scaffolds are a promising class of biomaterials for grafting large bone defects, because titanium provides sufficient mechanical support, whereas its porous structure allows bone ingrowth resulting in good osseointegration. To reinforce porous titanium scaffolds with biological cues that enhance and continue bone regeneration, scaffolds can be incorporated with bioactive gels for time- and dose-controlled delivery of multiple growth factors (GFs). In this study, critical femoral bone defects in rats were grafted with porous titanium scaffolds incorporated with nanostructured colloidal gelatin gels. Gels were loaded with bone morphogenetic protein-2 (BMP-2, 3 mg), fibroblast growth factor-2 (FGF-2, 0.6 mg), BMP-2, and FGF-2 (BMP-2/FGF-2, ratio 5:1) or were left unloaded. GF delivery was controlled by fine tuning the crosslinking density of oppositely charged nanospheres. Grafted femurs were evaluated using in vivo and ex vivo micro-CT, histology, and three-point bending tests. All porous titanium scaffolds containing GF-loaded gels accelerated and enhanced bone regeneration: BMP-2 gels gave an early increase (0–4 weeks), and FGF-2 gels gave a late increase (8–12 weeks). Interestingly, stimulatory effects of 0.6 mg FGF-2 were similar to a fivefold higher dose of BMP-2 (3 mg). BMP-2/FGF-2 gels gave more bone outside the porous titanium scaffolds than gels with only BMP-2 or FGF-2, resulted in bridging of most defects and showed superior bone-implant integrity in three-point bending tests. In conclusion, incorporation of nanostructured colloidal gelatin gels capable of time- and dose-controlled delivery of BMP-2 and FGF-2 in porous titanium scaffolds is a promising strategy to enhance and continue bone regeneration of large bone defects.
机译:多孔钛支架是用于移植大骨缺损的有前途的生物材料类别,因为钛提供了足够的机械支撑,而其多孔结构允许骨骼向内生长,从而导致良好的骨整合。为了用增强并继续骨骼再生的生物学线索来增强多孔钛支架,可以将支架与生物活性凝胶结合使用,以时间和剂量控制方式输送多种生长因子(GFs)。在这项研究中,大鼠的关键股骨缺损被植入了结合了纳米结构胶体明胶的多孔钛支架。凝胶中装有骨形态发生蛋白2(BMP-2,3 mg),成纤维细胞生长因子2(FGF-2,0.6 mg),BMP-2和FGF-2(BMP-2 / FGF-2,比例5:1)或被卸载。通过微调带相反电荷的纳米球的交联密度来控制GF的传递。使用体内和体外micro-CT,组织学和三点弯曲试验评估移植的股骨。所有含有GF凝胶的多孔钛支架都可以促进并增强骨骼再生:BMP-2凝胶可以增加早期(0–4周),而FGF-2凝胶可以增加后期(8–12周)。有趣的是,0.6 mg FGF-2的刺激作用类似于高五倍的BMP-2剂量(3 mg)。与仅具有BMP-2或FGF-2的凝胶相比,BMP-2 / FGF-2凝胶在多孔钛支架之外的骨骼更多,导致大多数缺陷的桥接,并在三点弯曲测试中显示出优异的骨植入物完整性。总之,在多孔钛支架中掺入能够按时间和剂量控制的方式将BMP-2和FGF-2递送的纳米结构胶体明胶是增强并继续大骨缺损的骨再生的一种有前途的策略。

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