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首页> 外文期刊>Tissue engineering, Part A >An Endochondral Ossification-Based Approach to Bone Repair: Chondrogenically Primed Mesenchymal Stem Cell-Laden Scaffolds Support Greater Repair of Critical-Sized Cranial Defects Than Osteogenically Stimulated Constructs In Vivo
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An Endochondral Ossification-Based Approach to Bone Repair: Chondrogenically Primed Mesenchymal Stem Cell-Laden Scaffolds Support Greater Repair of Critical-Sized Cranial Defects Than Osteogenically Stimulated Constructs In Vivo

机译:基于骨修复的内核骨化方法:软弱化学喷射的间充质干细胞 - 升起的支架支持临界大小的颅缺损的修复,而不是体内破坏性刺激的构建体

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摘要

The lack of success associated with the use of bone grafts has motivated the development of tissue engineering approaches for bone defect repair. However, the traditional tissue engineering approach of direct osteogenesis, mimicking the process of intramembranous ossification (IMO), leads to poor vascularization. In this study, we speculate that mimicking an endochondral ossification (ECO) approach may offer a solution by harnessing the potential of hypertrophic chondrocytes to secrete angiogenic signals that support vasculogenesis and enhance bone repair. We hypothesized that stimulation of mesenchymal stem cell (MSC) chondrogenesis and subsequent hypertrophy within collagen-based scaffolds would lead to improved vascularization and bone formation when implanted within a critical-sized bone defect in vivo. To produce ECO-based constructs, two distinct scaffolds, collagen-hyaluronic acid (CHyA) and collagen-hydroxyapatite (CHA), with proven potential for cartilage and bone repair, respectively, were cultured with MSCs initially in the presence of chondrogenic factors and subsequently supplemented with hypertrophic factors. To produce IMO-based constructs, CHA scaffolds were cultured with MSCs in the presence of osteogenic factors. These constructs were subsequently implanted into 7 mm calvarial defects on Fischer male rats for up to 8 weeks in vivo. The results demonstrated that IMO- and ECO-based constructs were capable of supporting enhanced bone repair compared to empty defects. However, it was clear that the scaffolds, which were previously shown to support the greatest cartilage formation in vitro (CHyA), led to the highest new bone formation (p < 0.05) within critical-sized bone defects 8 weeks postimplantation. We speculate this to be associated with the secretion of angiogenic signals as demonstrated by the higher VEGF protein production in the ECO-based constructs before implantation leading to the greater blood vessel ingrowth. This study thus demonstrates the ability of recapitulating a developmental process of bone formation to develop tissue-engineered constructs that manifest appreciable promise for bone defect repair.
机译:与骨移植物相关的成功缺乏成功促使组织工程方法的骨缺损修复方法的发展。然而,传统的组织工程方法的直接骨质发生,模仿胰蛋白尿骨化(IMO)的过程,导致血管化差。在这项研究中,我们推测模仿中的内核骨化(ECO)方法可以通过利用肥大软骨细胞的潜力来分泌支持血管发生的血管生成信号并增强骨修复来提供解决方案。我们假设胶原基支架内的间充质干细胞(MSC)软骨发生的刺激和随后的肥大将导致在体内临界大小的骨缺陷内植入时改善血管化和骨形成。为了产生生态的构建体,分别在软骨因子存在下,分别分别在软骨和骨骼修复中经过验证的潜在的两种不同的支架,胶原透明质酸(Chya)和胶原羟基磷灰石(CHA),其培养有培养的软骨和骨骼修复。补充有肥厚因素。为了产生基于IMO的构建体,在骨质发生因子存在下用MSCs培养CHA支架。随后将这些构建体植入到5周内在Fischer雄性大鼠上植入7mm的颅骨缺陷。结果表明,与空缺陷相比,IMO和生态基构建体能够支持增强的骨骼修复。然而,显而易见的是,前面证明的支架,其在体外(CHYA)中支持最大的软骨形成,导致了最高的新骨形成(P <0.05)在关键尺寸的骨缺损8周后8周后。我们推测这与血管生成信号的分泌相关,如植入植入前的生态蛋白质生产中的更高的VEGF蛋白质产生,导致血管内血管的血管产生。因此,该研究表明,综合骨形成的发育过程的能力,以开发模组工程构造,这些构建体表现出对骨缺损修复的明显应该的通知。

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  • 来源
    《Tissue engineering, Part A》 |2016年第6期|共12页
  • 作者单位

    Royal Coll Surgeons Ireland Dept Anat Tissue Engn Res Grp Dublin 2 Ireland;

    Royal Coll Surgeons Ireland Dept Anat Tissue Engn Res Grp Dublin 2 Ireland;

    Royal Coll Surgeons Ireland Dept Anat Tissue Engn Res Grp Dublin 2 Ireland;

    Royal Coll Surgeons Ireland Dept Anat Tissue Engn Res Grp Dublin 2 Ireland;

    Royal Coll Surgeons Ireland Dept Anat Tissue Engn Res Grp Dublin 2 Ireland;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 人体形态学;
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