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将双功能蛋白 tether 到矿化聚合物支架上以调节间充质干细胞行为用于骨再生。 (注:tether 原意为“拴系、系住”,这里不太明确准确含义,可能需结合专业背景进一步理解其确切意思,暂按字面翻译)

Tethering bi-functional protein onto mineralized polymer scaffolds to regulate mesenchymal stem cell behaviors for bone regeneration.

作者信息

Lee Jae Ho, Park Jeong-Hui, Yun Ye-Rang, Jang Jun-Hyeog, Lee Eun-Jung, Chrzanowski Wojciech, Wall Ivan B, Kim Hae-Won

机构信息

Institute of Tissue Regeneration Engineering (ITREN), Dankook University, South Korea.

出版信息

J Mater Chem B. 2013 Jun 7;1(21):2731-2741. doi: 10.1039/c3tb00043e. Epub 2013 Apr 24.

DOI:10.1039/c3tb00043e
PMID:32260979
Abstract

Modifying three-dimensional scaffolds with bioactive extracellular matrix (ECM) molecules enhances their potential use in tissue engineering, by providing natural biochemical/physical cues for cell recognition. Here, we engineered the surface of poly(caprolactone) (PCL) scaffolds, first with bone mineral hydroxyapatite (HA), and then with fibronectin-osteocalcin (FN-OCN) bi-functional protein by means of affinity binding between OCN and HA. While FN is expected to enhance initial adhesion of immature precursor cells, OCN is considered to regulate osteogenic differentiation. Quartz crystal microbalance dissipation analysis revealed FN-OCN protein had a more stable and stronger adherence to the HA-mineralized surface than to the native PCL-surface. Initial adhesion and the spreading of rat mesenchymal stem cells were significantly enhanced on the FN-OCN tethered scaffold. Expression of bone-associated genes (osteopontin, bone sialoprotein II and OCN) was significantly higher on the FN-OCN tethered scaffold. Moreover, those proteins were more abundantly found when cultured on the scaffolds with FN-OCN than those without, as confirmed by immunofluorescence cell labeling and fluorescence activated cell sorting analysis. All taken, the tethering of FN-OCN to a HA-mineralized surface is an effective strategy to provide biopolymer scaffolds improved bi-functional capacity for bone tissue engineering, in terms of initial cell adhesion and osteogenic differentiation.

摘要

用生物活性细胞外基质(ECM)分子修饰三维支架,通过为细胞识别提供天然的生化/物理线索,增强了它们在组织工程中的潜在应用。在此,我们对聚己内酯(PCL)支架表面进行工程化处理,首先用骨矿物质羟基磷灰石(HA)处理,然后通过OCN与HA之间的亲和结合,用纤连蛋白-骨钙素(FN-OCN)双功能蛋白处理。虽然预计FN能增强未成熟前体细胞的初始黏附,但OCN被认为可调节成骨分化。石英晶体微天平耗散分析表明,FN-OCN蛋白与HA矿化表面的黏附比与天然PCL表面的黏附更稳定、更强。在FN-OCN连接的支架上,大鼠间充质干细胞的初始黏附和铺展显著增强。在FN-OCN连接的支架上,骨相关基因(骨桥蛋白、骨唾液酸蛋白II和OCN)的表达显著更高。此外,通过免疫荧光细胞标记和荧光激活细胞分选分析证实,与没有FN-OCN的支架相比,在含有FN-OCN的支架上培养时,这些蛋白质的含量更丰富。综上所述,将FN-OCN连接到HA矿化表面是一种有效的策略,可在初始细胞黏附和成骨分化方面为骨组织工程提供具有改善双功能能力的生物聚合物支架。

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