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首页> 外文期刊>Journal of nanoparticle research: An interdisciplinary forum for nanoscale science and technology >Biomimetic nanoparticles with polynucleotide and PEG mixed-monolayers enhance calcium phosphate mineralization
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Biomimetic nanoparticles with polynucleotide and PEG mixed-monolayers enhance calcium phosphate mineralization

机译:具有多核苷酸和PEG混合单层的仿生纳米颗粒可增强磷酸钙的矿化作用

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Biomineralization of hydroxyapatite (Ca_(10)(PO_4) _6(OH)_2) is of significant importance in biomedical applications such as bone and dental repair, and biomimetic control of mineral formation may lead to more effective restorative procedures. Gold nanoparticles are functional scaffolds on which to assemble multi-component monolayers capable of mimicking protein activity in the templated synthesis of calcium phosphate. The goal of this research was to explore nanoparticle templates with mixed-monolayers of uncharged polar polyethylene glycol (PEG) molecules and highly charged polynucleotide and amino acid molecules in their ability to influence mineralization rates and mineral particle size and morphology. This research demonstrates through time-resolved optical density and dynamic light scattering measurements that the combination of tiopronin, PEG, and DNA presented on a nanoparticle surface decreases nanoparticle aggregation from 59 to 21 nm solvated radius, increases mineralization kinetics from 1.5 × 10~(-3) to 3.1 × 10~(-3) OD/min, and decreases mineral particle size from 685 to 442 nm average radius. FT-IR and TEM data demonstrate that mineralized material, while initially amorphous, transforms to a semi-crystalline material when guided by template interactions. This demonstrates that surface-tailored monolayer protected cluster scaffolds are successful and controllable mineralization templates with further potential for biomedical applications involving calcium phosphate and other biomaterials.
机译:羟基磷灰石(Ca_(10)(PO_4)_6(OH)_2)的生物矿化在生物医学应用(例如骨骼和牙齿修复)中非常重要,仿生控制矿物质形成可能导致更有效的修复程序。金纳米颗粒是功能性支架,在其上组装能够模拟磷酸钙模板化合成中蛋白质活性的多组分单层。这项研究的目的是探索具有不带电荷的极性聚乙二醇(PEG)分子和带高电荷的多核苷酸和氨基酸分子的混合单分子层的纳米颗粒模板,这些模板对矿化速率,矿物质粒径和形态的影响能力。这项研究通过时间分辨的光密度和动态光散射测量表明,硫普罗宁,PEG和DNA组合存在于纳米颗粒表面上,将纳米颗粒的聚集半径从59纳米减小到21纳米,使矿化动力学从1.5×10〜(- 3)到3.1×10〜(-3)OD / min,并将矿物粒径从685平均半径减小到442 nm。 FT-IR和TEM数据表明,矿化的材料最初是无定形的,但在模板相互作用的指导下转变为半结晶的材料。这表明表面定制的单层保护簇支架是成功且可控制的矿化模板,对于涉及磷酸钙和其他生物材料的生物医学应用具有进一步的潜力。

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