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首页> 外文期刊>Tissue engineering, Part A >Acceleration of Vascularized Bone Tissue-Engineered Constructs in a Large Animal Model Combining Intrinsic and Extrinsic Vascularization
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Acceleration of Vascularized Bone Tissue-Engineered Constructs in a Large Animal Model Combining Intrinsic and Extrinsic Vascularization

机译:大型动物模型中的血管化骨组织工程构建体的加速,组合内在血管形成

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摘要

During the last decades, a range of excellent and promising strategies in Bone Tissue Engineering have been developed. However, the remaining major problem is the lack of vascularization. In this study, extrinsic and intrinsic vascularization strategies were combined for acceleration of vascularization. For optimal biomechanical stability of the defect site and simplifying future transition into clinical application, a primary stable and approved nanostructured bone substitute in clinically relevant size was used. An arteriovenous (AV) loop was microsurgically created in sheep and implanted, together with the bone substitute, in either perforated titanium chambers (intrinsic/extrinsic) for different time intervals of up to 18 weeks or isolated Teflon((R)) chambers (intrinsic) for 18 weeks. Over time, magnetic resonance imaging and micro-computed tomography (CT) analyses illustrate the dense vascularization arising from the AV loop. The bone substitute was completely interspersed with newly formed tissue after 12 weeks of intrinsic/extrinsic vascularization and after 18 weeks of intrinsic/extrinsic and intrinsic vascularization. Successful matrix change from an inorganic to an organic scaffold could be demonstrated in vascularized areas with scanning electron microscopy and energy dispersive X-ray spectroscopy. Using the intrinsic vascularization method only, the degradation of the scaffold and osteoclastic activity was significantly lower after 18 weeks, compared with 12 and 18 weeks in the combined intrinsic-extrinsic model. Immunohistochemical staining revealed an increase in bone tissue formation over time, without a difference between intrinsic/extrinsic and intrinsic vascularization after 18 weeks. This study presents the combination of extrinsic and intrinsic vascularization strategies for the generation of an axially vascularized bone substitute in clinically relevant size using a large animal model. The additional extrinsic vascularization promotes tissue ingrowth and remodeling processes of the bone substitute. Extrinsic vessels contribute to faster vascularization and finally anastomose with intrinsic vasculature, allowing microvascular transplantation of the bone substitute after a shorter prevascularization time than using the intrinsic method only. It can be reasonably assumed that the usage of perforated chambers can significantly reduce the time until transplantation of bone constructs. Finally, this study paves the way for further preclinical testing for proof of the concept as a basis for early clinical applicability.
机译:在过去几十年中,已经开发出一系列骨组织工程中的优秀和有希望的策略。但是,剩下的主要问题是缺乏血管化。在本研究中,组合外在和内在血管化策略以加速血管化。为缺陷现场的最佳生物力学稳定性,并将未来的过渡简化到临床应用中,使用临床相关尺寸的初级稳定和批准的纳米结构骨代替。在绵羊中,在绵羊中,在绵羊和骨替代,在穿孔钛室(内在/外在)中,在多达18周或分离的Teflon((r))腔室(内在的)18周。随着时间的推移,磁共振成像和微计算断层扫描(CT)分析说明了AV环中产生的致密血管化。在内在/外在血管形成的12周后,骨代替完全散布在新形成的组织,并在内在/外部和内在血管化18周后。在具有扫描电子显微镜和能量分散X射线光谱的血管化区域中可以证明从无机到有机支架的成功基质改变。仅使用内在血管化方法,18周后支架和骨盘制活性的降解显着降低,而组合的内在外在模型中的12和18周。免疫组织化学染色显示骨组织形成随时间随时间的增加,而没有18周后的内在/外在和内在血管化之间的差异。本研究介绍了使用大型动物模型在临床相关规模中产生轴向血管化骨替代的外在和内在血管形成策略的组合。额外的外在血管化促进骨替代品的组织|生长和重塑过程。外部血管有助于更快的血管化和最终具有内在脉管系统的吻合瘤,使微血管移植骨骼移植在短暂的血管完全性时间之后仅仅使用本征方法。可以合理地假设穿孔室的用法可以显着减少直到骨构造移植的时间。最后,本研究为进一步的临床专用检测铺平了进一步的临床前临床适用性的基础。

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  • 来源
    《Tissue engineering, Part A》 |2015年第10期|共15页
  • 作者单位

    Univ Erlangen Nurnberg Univ Hosp Erlangen Dept Plast &

    Hand Surg D-91054 Erlangen Germany;

    Univ Erlangen Nurnberg Univ Hosp Erlangen Dept Plast &

    Hand Surg D-91054 Erlangen Germany;

    Univ Erlangen Nurnberg Inst Expt &

    Clin Pharmacol &

    Toxicol D-91054 Erlangen Germany;

    Univ Rostock Inst Phys Dept Mat Res &

    Nanostruct D-18055 Rostock Germany;

    Univ Erlangen Nurnberg Univ Hosp Erlangen Dept Plast &

    Hand Surg D-91054 Erlangen Germany;

    Univ Erlangen Nurnberg Univ Hosp Erlangen Dept Plast &

    Hand Surg D-91054 Erlangen Germany;

    Univ Erlangen Nurnberg Univ Hosp Erlangen Dept Plast &

    Hand Surg D-91054 Erlangen Germany;

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

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