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用于骨组织工程应用的钴释放 1393 生物活性玻璃衍生支架。

Cobalt-releasing 1393 bioactive glass-derived scaffolds for bone tissue engineering applications.

机构信息

Institute of Biomaterials, Department of Materials Science and Engineering, University of Erlangen-Nuremberg , Cauerstrasse 6, 91058 Erlangen, Germany.

出版信息

ACS Appl Mater Interfaces. 2014 Feb 26;6(4):2865-77. doi: 10.1021/am405354y. Epub 2014 Feb 10.

Abstract

Loading biomaterials with angiogenic therapeutics has emerged as a promising approach for developing superior biomaterials for engineering bone constructs. In this context, cobalt-releasing materials are of interest as Co is a known angiogenic agent. In this study, we report on cobalt-releasing three-dimensional (3D) scaffolds based on a silicate bioactive glass. Novel melt-derived "1393" glass (53 wt % SiO2, 6 wt % Na2O, 12 wt % K2O, 5 wt % MgO, 20 wt % CaO, and 4 wt % P2O5) with CoO substituted for CaO was fabricated and was used to produce a 3D porous scaffold by the foam replica technique. Glass structural and thermal properties as well as scaffold macrostructure, compressive strength, acellular bioactivity, and Co release in simulated body fluid (SBF) were investigated. In particular, detailed insights into the physicochemical reactions occurring at the scaffold-fluid interface were derived from advanced micro-particle-induced X-ray emission/Rutherford backscattering spectrometry analysis. CoO is shown to act in a concentration-dependent manner as both a network former and a network modifier. At a concentration of 5 wt % CoO, the glass transition point (Tg) of the glass was reduced because of the replacement of stronger Si-O bonds with Co-O bonds in the glass network. Compressive strengths of >2 MPa were measured for Co-containing 1393-derived scaffolds, which are comparable to values of human spongy bone. SBF studies showed that all glass scaffolds form a calcium phosphate (CaP) layer, and for 1393-1Co and 1393-5Co, CaP layers with incorporated traces of Co were observed. The highest Co concentrations of ∼12 ppm were released in SBF after reaction for 21 days, which are known to be within therapeutic ranges reported for Co(2+) ions.

摘要

将血管生成治疗剂载入生物材料已成为开发用于工程骨构建的优异生物材料的一种有前途的方法。在这种情况下,释放钴的材料很有意义,因为 Co 是一种已知的血管生成剂。在这项研究中,我们报告了基于硅酸盐生物活性玻璃的释放钴的三维(3D)支架。新型熔融衍生的“1393”玻璃(53wt%SiO2、6wt%Na2O、12wt%K2O、5wt%MgO、20wt%CaO 和 4wt%P2O5)用 CoO 替代 CaO,通过泡沫复制技术制备 3D 多孔支架。研究了玻璃结构和热性能以及支架宏观结构、抗压强度、无细胞生物活性和在模拟体液(SBF)中的 Co 释放。特别是,从先进的微粒子诱导 X 射线发射/卢瑟福背散射光谱分析中得出了关于在支架-流体界面上发生的物理化学反应的详细见解。CoO 表现出浓度依赖性的作用,既是网络形成剂又是网络改性剂。在 5wt%CoO 的浓度下,由于玻璃网络中更强的 Si-O 键被 Co-O 键取代,玻璃的玻璃化转变点(Tg)降低。含有 Co 的 1393 衍生支架的抗压强度>2MPa,与人类松质骨的值相当。SBF 研究表明,所有玻璃支架都形成了一层磷酸钙(CaP),对于 1393-1Co 和 1393-5Co,观察到含有痕量 Co 的 CaP 层。反应 21 天后,在 SBF 中释放出的 Co 浓度最高可达约 12ppm,这在已知的 Co(2+)离子治疗范围内。

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