Department of Pharmaceutical Sciences and Experimental Therapeutics, University of Iowa College of Pharmacy, Iowa City, Iowa, USA.
Department of Pathology, University of Iowa Carver College of Medicine, Iowa City, Iowa, USA.
Tissue Eng Part A. 2021 Aug;27(15-16):1074-1083. doi: 10.1089/ten.TEA.2020.0206. Epub 2020 Nov 26.
Research in bone tissue engineering aims to design materials that are effective at generating bone without causing significant side effects. The osteogenic potential of combining matrices and protein growth factors has been well documented, however, improvements are necessary to achieve optimal therapeutic benefits upon clinical translation. In this article, rat calvarial defects were treated with gene-activated matrices (GAMs). The GAMs used were collagen sponges mineralized with a simulated body fluid (SBF) containing a nonviral gene delivery system. Both and studies were performed to determine the optimal mode of gene delivery. After 6 weeks, the defects were extracted to assess bone formation and tissue quality through histological and microcomputed tomography analyses. The optimal GAM consisted of a collagen sponge with polyethylenimine plasmid DNA (PEI-pDNA) complexes embedded in a calcium phosphate coating produced by SBF, which increased total bone formation by 39% compared with 19% for control samples. A follow-up study was performed to optimize the ratio of growth factors included in the GAM. The optimal ratio for supporting bone formation after 6 weeks of implantation was five parts of pBMP-2 to three parts pFGF-2. These studies demonstrated that collagen matrices biomimetically mineralized and activated with plasmids encoding fibroblast growth factor-2 (FGF-2) and bone morphogenetic protein-2 (BMP-2) can optimally improve bone regeneration outcomes. Impact statement Bone tissue engineering has explored both nonviral gene delivery and the concept of biomimetic mineralization. In this study, we combined these two concepts to further enhance bone regeneration outcomes. We demonstrated that embedding polyethylenimine (PEI)-based gene delivery within a mineral layer formed from simulated body fluid (SBF) immersion can increase bone formation rates. We also demonstrated that the ratio of growth factors utilized for matrix fabrication can impact the amount of bone formed in the defect site. This research highlights a combined approach using SBF and nonviral gene delivery both and and prepares the way for future optimization of synthetic gene activated matrices.
组织工程学旨在设计能够有效生成骨骼而不会引起显著副作用的材料。将基质和蛋白生长因子结合起来的成骨潜力已经得到了很好的证明,然而,为了在临床转化中获得最佳的治疗效果,还需要进行改进。在本文中,使用基因激活基质(GAM)治疗大鼠颅骨缺损。所使用的 GAM 是用含有非病毒基因传递系统的模拟体液(SBF)矿化的胶原海绵。进行了 和 研究以确定最佳的基因传递模式。6 周后,提取缺陷部位,通过组织学和微计算机断层扫描分析评估骨形成和组织质量。最佳的 GAM 由嵌入 SB 矿化的胶原海绵和聚乙烯亚胺质粒 DNA(PEI-pDNA)复合物组成,与对照组相比,总骨形成增加了 39%,为 19%。进行了后续的 研究以优化 GAM 中包含的生长因子的比例。植入 6 周后支持骨形成的最佳比例为五部分 pBMP-2 对三部分 pFGF-2。这些研究表明,用编码成纤维细胞生长因子-2(FGF-2)和骨形态发生蛋白-2(BMP-2)的质粒仿生矿化和激活的胶原基质可以最佳地改善骨再生效果。
影响说明 组织工程学既探索了非病毒基因传递,也探索了仿生矿化的概念。在这项研究中,我们结合了这两个概念,进一步提高了骨再生的效果。我们证明,将基于聚乙烯亚胺(PEI)的基因传递嵌入由模拟体液(SBF)浸泡形成的矿物质层中可以提高成骨率。我们还证明了用于基质制造的生长因子的比例会影响缺陷部位形成的骨量。这项研究强调了使用 SBF 和非病毒基因传递的综合方法 和 ,并为未来优化合成基因激活基质做好了准备。
