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新型生物材料结合/成骨双功能肽与丝素蛋白膜结合,有效诱导成骨和 。

Novel Biomaterial-Binding/Osteogenic Bi-Functional Peptide Binds to Silk Fibroin Membranes to Effectively Induce Osteogenesis and .

机构信息

Key Laboratory of Silkworm and Bee Resource Utilization and Innovation of Zhejiang Province, Institute of Applied Bioresource Research, College of Animal Science, Zhejiang University, Hangzhou, Zhejiang 310058, P. R. China.

School of Materials Science & Engineering, Zhejiang University, Hangzhou, Zhejiang 310058, P. R. China.

出版信息

ACS Appl Mater Interfaces. 2023 Feb 15;15(6):7673-7685. doi: 10.1021/acsami.2c17554. Epub 2023 Feb 3.

DOI:10.1021/acsami.2c17554
PMID:36735224
Abstract

Peptides can introduce new functions to biomaterials but their immobilization usually relies on inefficient physical adsorption or tedious chemical conjugation. Using the silk fibroin (SF) membrane (SFm) as a model biomaterial, here, we demonstrate a universal strategy for discovering new peptides that can "stick" to a biomaterial to functionalize it. Specifically, two peptide motifs, one screened by phage display biopanning for binding to the biomaterial (i.e., SF) and another derived from an osteogenic growth factor (i.e., bone morphogenetic protein-2), are fused into a new chimeric peptide that can bind to SFm for more efficient osteogenesis. Theoretical simulations and experimental assays confirm that the chimeric peptide binds to SF with high affinity, facilely achieving its immobilization onto SFm. The peptide enables SFm to effectively induce osteogenic differentiation of human mesenchymal stem cells (MSCs) even without other osteogenic inducers and efficiently stimulate bone regeneration in a subcutaneous rat model in 8 weeks, even without MSC seeding, while not causing inflammatory responses. Since biomaterial-binding peptides can be readily screened using phage display and functional peptides can be generated from growth factors, our work suggests a universal strategy for combining them to seek new peptides for binding and functionalizing biomaterials.

摘要

肽可以为生物材料引入新的功能,但它们的固定通常依赖于低效的物理吸附或繁琐的化学偶联。在这里,我们以丝素蛋白(SF)膜(SFm)为模型生物材料,展示了一种发现可以“黏附”生物材料以对其进行功能化的新肽的通用策略。具体来说,通过噬菌体展示生物淘选筛选出两种肽基序,一种与生物材料(即 SF)结合,另一种源自成骨生长因子(即骨形态发生蛋白-2),将它们融合成一种新的嵌合肽,该嵌合肽可以与 SFm 结合,从而更有效地促进成骨。理论模拟和实验检测证实,该嵌合肽与 SF 具有高亲和力,易于将其固定在 SFm 上。该肽使 SFm 能够有效地诱导人间充质干细胞(MSCs)的成骨分化,即使没有其他成骨诱导剂,并且在 8 周内无需 MSC 接种即可有效地刺激皮下大鼠模型中的骨再生,而不会引起炎症反应。由于可以使用噬菌体展示轻松筛选生物材料结合肽,并且可以从生长因子中生成功能性肽,因此我们的工作提出了一种将它们结合起来寻找新的肽来结合和功能化生物材料的通用策略。

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