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具有可控降解性能的透明质酸水凝胶用于定向骨再生。

Hyaluronic acid hydrogels with controlled degradation properties for oriented bone regeneration.

机构信息

Department of Bioengineering, University of Washington, Seattle, WA 98195, USA.

出版信息

Biomaterials. 2010 Sep;31(26):6772-81. doi: 10.1016/j.biomaterials.2010.05.047. Epub 2010 Jun 23.

Abstract

Non-healing fractures can result from trauma, disease, or age-related bone loss. While many treatments focus on restoring bone volume, few try to recapitulate bone organization. However, the native architecture of bone is optimized to provide its necessary mechanical properties. Hyaluronic acid (HA) hydrogel scaffold systems with tunable degradation properties were developed for the controlled delivery of osteoinductive and angiogenic growth factors, thus affecting the quantity and quality of regenerated tissue. HA hydrogels were designed to degrade at fast, intermediate, and slow rates due to hydrolysis and further provided controlled release of cationic proteins due to electrostatic interactions. Scaffolds delivering bone morphogenetic protein-2 (BMP-2) were evaluated in a rat calvarial bone critical size defect model. BMP-2 delivery from the HA hydrogels had a clear osteoinductive effect in vivo and, for all hydrogel types, BMP-2 delivery resulted in significant mineralization compared to control hydrogels. The temporal progression of this effect could be modulated by altering the degradation rate of the scaffold. All three degradation rates tested resulted in similar amounts of mineral formation at the latest (six week) time point examined. Interestingly, however, the fastest and slowest degrading scaffolds seemed to result in more organized bone than the intermediate degrading scaffold, which was designed to degrade in 6-8 weeks to match the healing time. Additionally, healing could be enhanced by co-delivery of vascular endothelial growth factor along with BMP-2.

摘要

非愈合性骨折可由创伤、疾病或与年龄相关的骨质流失引起。虽然许多治疗方法侧重于恢复骨量,但很少有方法尝试再现骨组织。然而,骨骼的固有结构是优化的,以提供其必要的机械性能。具有可调降解特性的透明质酸 (HA) 水凝胶支架系统已被开发用于控制递送电活性和血管生成生长因子,从而影响再生组织的数量和质量。HA 水凝胶由于水解而设计为快速、中等和缓慢降解,并由于静电相互作用进一步提供阳离子蛋白的控制释放。在大鼠颅骨临界尺寸缺损模型中评估了递送骨形态发生蛋白 2 (BMP-2) 的支架。HA 水凝胶中 BMP-2 的递呈在体内具有明显的成骨诱导作用,对于所有水凝胶类型,与对照水凝胶相比,BMP-2 的递呈导致明显的矿化。通过改变支架的降解速率可以调节这种效果的时间进展。在研究的最新(六周)时间点,测试的三种降解速率都导致了相似数量的矿物质形成。然而,有趣的是,最快和最慢降解的支架似乎比设计为在 6-8 周内降解以匹配愈合时间的中等降解支架产生更有组织的骨骼。此外,通过与 BMP-2 共同递送电活性因子可以增强愈合。

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