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具有释放维生素D能力的骨组织工程明胶-羟基磷灰石/氧化石墨烯支架:制备、表征及体外研究

Bone tissue engineering gelatin-hydroxyapatite/graphene oxide scaffolds with the ability to release vitamin D: fabrication, characterization, and in vitro study.

作者信息

Mahdavi Reza, Belgheisi Ghazal, Haghbin-Nazarpak Masoumeh, Omidi Meisam, Khojasteh Arash, Solati-Hashjin Mehran

机构信息

Department of Biomedical Engineering, Amirkabir University of Technology (Tehran Polytechnic), Tehran, Iran.

Department of Biomedical Engineering, Biofabrication Laboratory, Amirkabir University of Technology (Tehran Polytechnic), Tehran, Iran.

出版信息

J Mater Sci Mater Med. 2020 Oct 31;31(11):97. doi: 10.1007/s10856-020-06430-5.

Abstract

Developing smart scaffolds with drug release capability is one of the main approaches to bone tissue engineering. The current study involves the fabrication of novel gelatin (G)-hydroxyapatite (HA)-/vitamin D (VD)-loaded graphene oxide (GO) scaffolds with different concentrations through solvent-casting method. Characterizations confirmed the successful synthesis of HA and GO, and VD was loaded in GO with 36.87 ± 4.87% encapsulation efficiency. Physicochemical characterizations showed that the scaffold containing 1% VD-loaded GO had the best mechanical properties and its porosity percentage and density was in the range of natural spongy bone. All scaffolds were degraded after 1-month, subjecting to phosphate buffer saline. The release profile of VD did not match any mathematical kinetics model, porosities and the degradation rate of the scaffolds were dominant controlling factors of release behavior. Studies on the bioactivity of scaffolds immersed in simulated body fluid indicated that VD and HA could encourage the formation of secondary apatite crystals in vitro. Buccal fat pad-derived stem cells (BFPSCs) were seeded on the scaffolds, MTT assay, alkaline phosphatase activity as an indicator of osteoconductivity, and cell adhesion were conducted in order to evaluate in vitro biological responses. All scaffolds highly supported cell adhesion, MTT assay indicated better cell viability in 0.5% VD-loaded GO containing scaffold, and the scaffold enriched with 2% VD-loaded GO performed the most ALP activity. The results demonstrated the potential of these scaffolds to induce bone regeneration. Developing smart scaffolds with drug release capability is one of the main approaches to bone tissue engineering. The current study involves the fabrication of novel gelatin (G)-hydroxyapatite (HA)-/vitamin D (VD)-loaded graphene oxide (GO) scaffolds with different concentrations through solvent-casting method. Characterizations confirmed the successful synthesis of HA and GO, and VD was loaded in GO with 36.87 ± 4.87% encapsulation efficiency. Physicochemical characterizations showed that the scaffold containing 1% VD-loaded GO had the best mechanical properties and its porosity percentage and density was in the range of natural spongy bone. All scaffolds were degraded after 1-month, subjecting to phosphate buffer saline. The release profile of VD did not match any mathematical kinetics model, porosities and the degradation rate of the scaffolds were dominant controlling factors of release behavior. Studies on the bioactivity of scaffolds immersed in simulated body fluid indicated that VD and HA could encourage the formation of secondary apatite crystals in vitro. Buccal fat pad-derived stem cells (BFPSCs) were seeded on the scaffolds, MTT assay, alkaline phosphatase activity as an indicator of osteoconductivity, and cell adhesion were conducted in order to evaluate in vitro biological responses. All scaffolds highly supported cell adhesion, MTT assay indicated better cell viability in 0.5% VD-loaded GO containing scaffold, and the scaffold enriched with 2% VD-loaded GO performed the most ALP activity. The results demonstrated the potential of these scaffolds to induce bone regeneration.

摘要

开发具有药物释放能力的智能支架是骨组织工程的主要方法之一。当前的研究涉及通过溶剂浇铸法制备不同浓度的新型负载明胶(G)-羟基磷灰石(HA)/维生素D(VD)的氧化石墨烯(GO)支架。表征证实了HA和GO的成功合成,并且VD以36.87±4.87%的包封效率负载在GO中。物理化学表征表明,含有1%负载VD的GO的支架具有最佳的机械性能,其孔隙率百分比和密度在天然松质骨的范围内。所有支架在置于磷酸盐缓冲盐水中1个月后均发生降解。VD的释放曲线不符合任何数学动力学模型,支架的孔隙率和降解速率是释放行为的主要控制因素。对浸泡在模拟体液中的支架的生物活性研究表明,VD和HA可以在体外促进次生磷灰石晶体的形成。将颊脂垫来源的干细胞(BFPSCs)接种在支架上,进行MTT测定、以碱性磷酸酶活性作为骨传导性指标以及细胞黏附实验,以评估体外生物学反应。所有支架都高度支持细胞黏附,MTT测定表明在含有0.5%负载VD的GO的支架中细胞活力更好,并且富含2%负载VD的GO的支架表现出最高的碱性磷酸酶活性。结果证明了这些支架诱导骨再生的潜力。开发具有药物释放能力的智能支架是骨组织工程的主要方法之一。当前的研究涉及通过溶剂浇铸法制备不同浓度的新型负载明胶(G)-羟基磷灰石(HA)/维生素D(VD)的氧化石墨烯(GO)支架。表征证实了HA和GO的成功合成,并且VD以36.87±4.87%的包封效率负载在GO中。物理化学表征表明,含有1%负载VD的GO的支架具有最佳的机械性能,其孔隙率百分比和密度在天然松质骨的范围内。所有支架在置于磷酸盐缓冲盐水中1个月后均发生降解。VD的释放曲线不符合任何数学动力学模型,支架的孔隙率和降解速率是释放行为的主要控制因素。对浸泡在模拟体液中的支架的生物活性研究表明,VD和HA可以在体外促进次生磷灰石晶体的形成。将颊脂垫来源的干细胞(BFPSCs)接种在支架上,进行MTT测定、以碱性磷酸酶活性作为骨传导性指标以及细胞黏附实验,以评估体外生物学反应。所有支架都高度支持细胞黏附,MTT测定表明在含有0.5%负载VD的GO的支架中细胞活力更好,并且富含2%负载VD的GO的支架表现出最高的碱性磷酸酶活性。结果证明了这些支架诱导骨再生的潜力。

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