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Development of model hydroxyapatite bone scaffolds with multiscale porosity for potential load bearing applications.

机译:具有多孔隙率的模型羟基磷灰石骨支架的开发,可用于潜在的承重应用。

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摘要

Model hydroxyapatite (HA) bone scaffolds consisting of a latticed pattern of rods were fabricated by a solid freeform fabrication (SFF) technique based on the robotic deposition of colloidal pastes. An optimal HA paste formulation for this method was developed. Local porosity, i.e. microporosity (1--30 mum) and sintering porosity (less than 1 mum), were produced by including polymer microsphere porogens in the HA pastes and by controlling the sintering of the scaffolds.; Scaffolds with and without local porosity were evaluated with and without in vitro accelerated degradation. Percent weight loss of the scaffolds and calcium and phosphorus concentrations in solution increased with degradation time. After degradation, compressive strength and modulus decreased significantly for scaffolds with local porosity, but did not change significantly for scaffolds without local porosity. The compressive strength and modulus of scaffolds without local porosity were comparable to human cortical bone and were significantly greater than the scaffolds with local porosity.; Micropores in HA disks caused surface pits that increased the surface roughness as compared to non-microporous HA disks. Mouse mesenchymal stem cells extended their cell processes into these microporous pits on HA disks in vitro. ALP expression was prolonged, cell attachment strength increased, and ECM production appeared greater on microporous HA disks compared to non-microporous HA disks and tissue culture treated polystyrene controls.; Scaffolds with and without microporosity were implanted in goats bones. Microporous scaffolds with rhBMP-2 increased the percent of the scaffold filled with bone tissue compared to microporous scaffolds without rhBMP-2. Lamellar bone inside scaffolds was aligned near the rods junctions whereas lamellar bone was aligned in a more random configuration away from the rod junctions. Microporous scaffolds stained darkly with toluidine blue beneath areas of contact with new bone. This staining might indicate either extracellular matrix (ECM) in the rods or dye bound to the degrading scaffold.; Although the presence of microporous topography alone did not influence bone healing in vivo, micropores were shown to provide tailorability of scaffold mechanical properties, provide a location for the storage and controlled release of a growth factor, and provide a location for bone integration inside the scaffold rods.
机译:由棒的格子图案组成的模型羟基磷灰石(HA)骨支架是通过基于胶体糊剂自动沉积的固体自由形式制造(SFF)技术制造的。为该方法开发了一种最佳的HA糊剂配方。局部孔隙率,即微孔率(1--30μm)和烧结孔隙率(小于1μm),是通过在HA糊剂中加入聚合物微球致孔剂并控制支架的烧结而产生的。在有和没有体外加速降解的情况下,评估具有和没有局部孔隙的支架。支架的重量损失百分比以及溶液中钙和磷的浓度随降解时间的增加而增加。降解后,具有局部孔隙率的脚手架的抗压强度和模量显着降低,而没有局部孔隙率的脚手架的抗压强度和模量没有显着变化。没有局部孔隙的支架的抗压强度和模量与人的皮质骨相当,并且显着大于具有局部孔隙的支架。与非微孔HA磁盘相比,HA磁盘中的微孔会导致表面凹坑,从而增加表面粗糙度。小鼠间充质干细胞在体外将其细胞过程扩展到HA盘上的这些微孔坑中。与非微孔HA盘和组织培养物处理过的聚苯乙烯对照相比,微孔HA盘上的ALP表达延长,细胞附着强度增加并且ECM产量似乎更高。具有和没有微孔的支架被植入山羊骨头中。与没有rhBMP-2的微孔支架相比,具有rhBMP-2的微孔支架增加了填充有骨组织的支架的百分比。支架内的层状骨在杆连接处附近对齐,而层状骨在远离杆连接处排列更随机。微孔支架在与新骨接触的区域下方被甲苯胺蓝深染。这种染色可能表明杆中的细胞外基质(ECM)或与降解支架结合的染料。尽管仅微孔形貌的存在并不影响体内的骨愈合,但已显示微孔可提供支架机械性能的可定制性,为生长因子的储存和控制释放提供位置,并为支架内部的骨整合提供位置棒。

著录项

  • 作者

    Dellinger, Jennifer Gwynne.;

  • 作者单位

    University of Illinois at Urbana-Champaign.;

  • 授予单位 University of Illinois at Urbana-Champaign.;
  • 学科 Engineering Biomedical.; Engineering Materials Science.
  • 学位 Ph.D.
  • 年度 2005
  • 页码 167 p.
  • 总页数 167
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物医学工程;工程材料学;
  • 关键词

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