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富含自组装肽的静电纺聚己内酯支架促进 h 成骨细胞黏附,并调节分化相关基因表达。

Self-assembling peptide-enriched electrospun polycaprolactone scaffolds promote the h-osteoblast adhesion and modulate differentiation-associated gene expression.

机构信息

Department of Industrial Engineering, University of Padua, Via Marzolo 9, 35131, Padua, Italy.

出版信息

Bone. 2012 Nov;51(5):851-9. doi: 10.1016/j.bone.2012.08.119. Epub 2012 Aug 20.

DOI:10.1016/j.bone.2012.08.119
PMID:22926428
Abstract

Electrospun polycaprolactone (PCL) is able to support the adhesion and growth of h-osteoblasts and to delay their degradation rate to a greater extent with respect to other polyesters. The drawbacks linked to its employment in regenerative medicine arise from its hydrophobic nature and the lack of biochemical signals linked to it. This work reports on the attempt to add five different self-assembling (SA) peptides to PCL solutions before electrospinning. The hybrid scaffolds obtained had regular fibers (SEM analysis) whose diameters were similar to those of the extracellular matrix, more stable hydrophilic (contact angle measurement) surfaces, and an amorphous phase constrained by peptides (DSC analysis). They appeared to have a notable capacity to promote the h-osteoblast adhesion and differentiation process by increasing the gene expression of alkaline phosphatase, bone sialoprotein, and osteopontin. Adding an Arg-Gly-Asp (RGD) motif to a self-assembling sequence was found to enhance cell adhesion, while the same motif condensed with a scrambled sequence did not, indicating that there is a cooperative effect between RGD and 3D architecture created by the self-assembling peptides. The study demonstrates that self-assembling peptide scaffolds are still able to promote beneficial effects on h-osteoblasts even after they have been included in electrospun polycaprolactone. The possibility of linking biochemical messages to self-assembling peptides could lead the way to a 3D decoration of fibrous scaffolds.

摘要

静电纺丝聚己内酯(PCL)能够支持 h-成骨细胞的黏附和生长,并在更大程度上延缓其降解速度,相对于其他聚酯而言。其在再生医学中的应用存在一些缺点,原因在于其疏水性和缺乏与之相关的生化信号。本工作试图在静电纺丝前将五种不同的自组装(SA)肽添加到 PCL 溶液中。所获得的混合支架具有规则的纤维(SEM 分析),其直径与细胞外基质相似,具有更稳定的亲水(接触角测量)表面和受肽约束的非晶相(DSC 分析)。它们似乎通过增加碱性磷酸酶、骨涎蛋白和骨桥蛋白的基因表达,具有显著促进 h-成骨细胞黏附和分化过程的能力。发现添加 Arg-Gly-Asp(RGD)基序到自组装序列中可以增强细胞黏附,而具有乱序序列的相同基序则不能,表明 RGD 与自组装肽创建的 3D 结构之间存在协同效应。该研究表明,即使自组装肽支架已包含在静电纺丝聚己内酯中,它们仍然能够对 h-成骨细胞产生有益的影响。将生化信息与自组装肽结合的可能性可能为纤维支架的 3D 修饰开辟道路。

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