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首页> 外文期刊>Acta biomaterialia >The influence of collagen and hyaluronan matrices on the delivery and bioactivity of bone morphogenetic protein-2 and ectopic bone formation
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The influence of collagen and hyaluronan matrices on the delivery and bioactivity of bone morphogenetic protein-2 and ectopic bone formation

机译:胶原蛋白和透明质酸基质对骨形态发生蛋白2传递和生物活性以及异位骨形成的影响

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摘要

Bone morphogenetic protein-2 (BMP-2) is known to enhance fracture healing when delivered via a bovine collagen sponge. However, collagen rapidly releases BMP-2 with a high burst phase that is followed by a low sustained phase. As a result, supra-physiological doses of BMP-2 are often required to successfully treat bone defects. High BMP-2 dosing can introduce serious side effects that include edema, bone overgrowth, cyst-like bone formation and significant inflammation. As the release behavior of BMP-2 carriers significantly affects the efficacy of fracture healing, we sought to compare the influence of two BMP-2 delivery matrices with contrasting release profiles on BMP-2 bioactivity and ectopic bone formation. We compared a thiol-modified hyaluronan (Glycosil?) hydrogel that exhibits a low burst followed by a sustained release of BMP-2 to a collagen sponge for the delivery of three different doses of BMP-2, the bioactivities of released BMP-2 and ectopic bone formation. Analysis of bone formation by micro-computed tomography revealed that low burst followed by sustained release of BMP-2 from a hyaluronan hydrogel induced up to 456% more bone compared to a BMP-2 dose-matched collagen sponge that has a high burst and sustained release. This study demonstrates that BMP-2 released with a low burst followed by a sustained release of BMP-2 is more desirable for bone formation. This highlights the therapeutic potential of hydrogels, particularly hyaluronan-based, for the delivery of BMP-2 for the treatment of bone defects and may help abrogate the adverse clinical effects associated with high dose growth factor use.
机译:众所周知,骨形态发生蛋白2(BMP-2)通过牛胶原海绵传递时可增强骨折愈合。然而,胶原蛋白以高爆发期快速释放BMP-2,随后是低持续期。结果,通常需要超生理剂量的BMP-2才能成功治疗骨缺损。高剂量的BMP-2可能引起严重的副作用,包括水肿,骨骼过度生长,囊肿样骨形成和明显的炎症。由于BMP-2载体的释放行为会显着影响骨折愈合的功效,因此我们试图比较两种BMP-2输送基质对BMP-2生物活性和异位骨形成的影响。我们比较了巯基修饰的透明质酸(Glycosil?)水凝胶,该凝胶表现出较低的爆发力,随后将BMP-2持续释放到胶原蛋白海绵中,以递送三种不同剂量的BMP-2,释放的BMP-2和异位骨形成。通过微计算机断层扫描分析的骨形成结果表明,与具有高爆裂和持久性的BMP-2剂量匹配的胶原海绵相比,低爆裂和随后从透明质酸水凝胶中持续释放BMP-2诱导的骨骼最多增加了456%。发布。这项研究表明,对于骨骼形成而言,以低爆发力释放BMP-2然后持续释放BMP-2更为理想。这突出了水凝胶(尤其是透明质酸基水凝胶)在递送BMP-2来治疗骨缺损方面的治疗潜力,并可能有助于消除与使用高剂量生长因子相关的不良临床影响。

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