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在矿化厚的、部分脱矿化胶原支架中自上而下和自下而上方法的差异。

Differences between top-down and bottom-up approaches in mineralizing thick, partially demineralized collagen scaffolds.

机构信息

Department of Stomatology, Tongji Hospital, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, China.

出版信息

Acta Biomater. 2011 Apr;7(4):1742-51. doi: 10.1016/j.actbio.2010.11.028. Epub 2010 Nov 24.

Abstract

Biominerals exhibit complex hierarchical structures derived from bottom-up self-assembly mechanisms. Type I collagen serves as the building block for mineralized tissues such as bone and dentin. In the present study, 250-300 μm thick, partially demineralized collagen scaffolds exhibiting a gradient of demineralization from the base to surface were mineralized using a classical top-down approach and a non-classical bottom-up approach. The top-down approach involved epitaxial growth over seed crystallites. The bottom-up approach utilized biomimetic analogs of matrix proteins to stabilize amorphous calcium phosphate nanoprecursors and template apatite nucleation and growth within the collagen matrix. Micro-computed tomography and transmission electron microscopy were employed to examine mineral uptake and apatite arrangement within the mineralized collagen matrix. The top-down approach could mineralize only the base of the partially demineralized scaffold, where remnant seed crystallites were abundant. Minimal mineralization was observed along the surface of the scaffold; extrafibrillar mineralization was predominantly observed. Conversely, the entire partially demineralized scaffold, including apatite-depleted collagen fibrils, was mineralized by the bottom-up approach, with evidence of both intrafibrillar and extrafibrillar mineralization. Understanding the different mechanisms involved in these two mineralization approaches is pivotal in adopting the optimum strategy for fabricating novel nanostructured materials in bioengineering research.

摘要

生物矿化材料具有复杂的层次结构,这些结构源自自下而上的自组装机制。I 型胶原是骨和牙本质等矿化组织的构建模块。在本研究中,使用经典的自上而下方法和非经典的自下而上方法对具有从基底到表面逐渐脱矿梯度的 250-300μm 厚的部分脱矿胶原支架进行矿化。自上而下的方法涉及在晶种上外延生长。自下而上的方法利用基质蛋白的仿生模拟物来稳定无定形磷酸钙纳米前体,并在胶原基质内模板磷灰石成核和生长。采用微计算机断层扫描和透射电子显微镜来研究矿化胶原基质内的矿化吸收和磷灰石排列。自上而下的方法只能矿化部分脱矿支架的基底,因为那里有丰富的残余晶种。在支架表面观察到的矿化很少;主要观察到纤维外矿化。相反,整个部分脱矿的支架,包括磷灰石耗尽的胶原纤维,都被自下而上的方法矿化了,既有纤维内矿化也有纤维外矿化的证据。了解这两种矿化方法中涉及的不同机制对于在生物工程研究中采用制造新型纳米结构材料的最佳策略至关重要。

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