首页> 外文期刊>Journal of biomedical materials research, Part A >Combination of platelet-rich plasma with polycaprolactone-tricalcium phosphate scaffolds for segmental bone defect repair.
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Combination of platelet-rich plasma with polycaprolactone-tricalcium phosphate scaffolds for segmental bone defect repair.

机译:富血小板血浆与聚己内酯-磷酸三钙支架的组合用于节段性骨缺损修复。

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Porous scaffold biomaterials may offer a clinical alternative to bone grafts; however, scaffolds alone are typically insufficient to heal large bone defects. Numerous studies have demonstrated that osteoinductive growth factor or gene delivery significantly improves bone repair. However, given the important role of vascularization during bone regeneration, it may also be beneficial to incorporate factors that promote vascular ingrowth into constructs. In this study, a strategy combining structural polycaprolactone-20% tricalcium phosphate (PCL-TCP) composite scaffolds with platelet-rich plasma (PRP) was tested. Following bilateral implantation of constructs into 8 mm rat nonunion femoral defects, 3D vascular and bone ingrowth were quantified at 3 and 12 weeks using contrast-enhanced microcomputed tomography (micro-CT) imaging. At week 3, PRP-treated femurs displayed 70.3% higher vascular volume fraction than control femurs. Interestingly, bone volume fraction (BVF) was significantly higher for the empty scaffold group at the early time point. At 12 weeks, BVF measurements between the two groups were statistically equivalent. However, a greater proportion of PRP-treated femurs (83%) achieved bone union as compared to empty scaffold controls (33%). Consistent with this observation, biomechanical evaluation of functional integration also revealed a significantly higher torsional stiffness observed for PRP-treated defects compared to empty scaffolds. Ultimate torque at failure was not improved, however, perhaps due to the slow resorption profile of the scaffold material. Histological evaluation illustrated infiltration of vascularized connective tissue and bone in both groups. Given that bone ingrowth into untreated defects in this model is minimal, PCL-TCP scaffolds were clearly able to promote bone ingrowth but failed to consistently bridge the defect. The addition of PRP to PCL-TCP scaffolds accelerated early vascular ingrowth and improved longer-term functional integration. Taken together, the results of this study suggest that the use of PRP, alone or in combination with other bioactive components, may be an effective approach to augment the ability of porous biomaterial scaffolds to repair orthotopic defects.
机译:多孔支架生物材料可能为骨移植​​提供临床替代方法;然而,仅脚手架通常不足以治愈大的骨缺损。大量研究表明,骨诱导生长因子或基因递送显着改善了骨修复。但是,考虑到血管形成在骨骼再生过程中的重要作用,将促进血管向内生长的因素纳入构建体中也可能是有益的。在这项研究中,策略结合结构聚己内酯20%磷酸三钙(PCL-TCP)复合支架与富血小板血浆(PRP)进行了测试。在将构建体双边植入8 mm大鼠骨不连的股骨缺损后,使用对比增强的微计算机断层扫描(micro-CT)成像在3周和12周对3D血管和骨向内生长进行了定量。在第3周,经PRP处理的股骨比对照股骨显示出高70.3%的血管体积分数。有趣的是,空支架组在早期时间点的骨体积分数(BVF)明显更高。在第12周时,两组之间的BVF测量值在统计上是等效的。然而,与空支架对照(33%)相比,经PRP治疗的股骨(83%)实现骨结合的比例更高。与此观察一致,功能整合的生物力学评估还显示,与空支架相比,PRP治疗的缺损观察到的扭转刚度明显更高。但是,可能由于支架材料的缓慢吸收曲线而没有提高最终破坏时的扭矩。组织学评估显示两组血管化结缔组织和骨均浸润。考虑到在此模型中骨向内生长到未治疗的缺损极少,因此PCL-TCP支架显然能够促进骨向内生长,但未能始终如一地弥合缺损。在PCL-TCP支架中添加PRP可以加速早期血管向内生长,并改善长期功能整合。两者合计,这项研究的结果表明,单独使用PRP或与其他生物活性成分结合使用PRP可能是增强多孔生物材料支架修复原位缺陷能力的有效方法。

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