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仿生超分子纳米纤维在胶原支架内放大低剂量 BMP-2 促进骨再生。

Bone regeneration with low dose BMP-2 amplified by biomimetic supramolecular nanofibers within collagen scaffolds.

机构信息

Department of Materials Science and Engineering, Northwestern University, Evanston, IL 60208, USA.

出版信息

Biomaterials. 2013 Jan;34(2):452-9. doi: 10.1016/j.biomaterials.2012.10.005. Epub 2012 Oct 23.

Abstract

Bone morphogenetic protein-2 (BMP-2) is a potent osteoinductive cytokine that plays a critical role during bone regeneration and repair. In the extracellular environment, sulfated polysaccharides anchored covalently to glycoproteins such as syndecan and also non-covalently to fibronectin fibers have been shown to bind BMP-2 through a heparin-binding domain and regulate its bioactivity. We report here on a synthetic biomimetic strategy that emulates biological BMP-2 signaling through the use of peptide amphiphile nanofibers designed to bind heparin. The supramolecular nanofibers, which integrate the biological role of syndecan and fibronectin, were allowed to form gel networks within the pores of an absorbable collagen scaffold by simply infiltrating dilute solutions of the peptide amphiphile, heparan sulfate, and BMP-2. The hybrid biomaterial enhanced significantly bone regeneration in a rat critical-size femoral defect model using BMP-2 amounts that are one order of magnitude lower than required for healing in this animal model. Using micro-computed tomography, we also showed that the hybrid scaffold was more effective at bridging within the gap relative to a conventional scaffold of the type used clinically based on collagen and BMP-2. Histological evaluation also revealed the presence of more mature bone in the new ossified tissue when the low dose of BMP-2 was delivered using the biomimetic supramolecular system. These results demonstrate how molecularly designed materials that mimic features of the extracellular environment can amplify the regenerative capacity of growth factors.

摘要

骨形态发生蛋白 2(BMP-2)是一种有效的成骨细胞诱导细胞因子,在骨再生和修复过程中起着关键作用。在细胞外环境中,共价锚定在糖蛋白(如连接蛋白)上的硫酸多糖以及非共价结合在纤维连接蛋白纤维上的硫酸多糖已被证明可以通过肝素结合域与 BMP-2 结合并调节其生物活性。我们在这里报告了一种合成仿生策略,该策略通过使用设计用于结合肝素的肽两亲性纳米纤维来模拟生物 BMP-2 信号。超分子纳米纤维整合了连接蛋白和纤维连接蛋白的生物学作用,通过简单地将肽两亲体、硫酸乙酰肝素和 BMP-2 的稀溶液渗透到可吸收胶原支架的孔中,形成凝胶网络。该杂交生物材料在大鼠股骨临界缺损模型中使用 BMP-2 数量显著增强了骨再生,BMP-2 的用量比该动物模型愈合所需的数量低一个数量级。使用微计算机断层扫描,我们还表明,与基于胶原和 BMP-2 的临床中使用的常规支架相比,该杂交支架在间隙内的桥接效果更好。组织学评估还表明,当使用仿生超分子系统以低剂量 BMP-2 给药时,新骨化组织中存在更成熟的骨。这些结果表明,模仿细胞外环境特征的分子设计材料如何增强生长因子的再生能力。

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