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首页> 外文期刊>Angewandte Chemie >Self-Assembled Arrays of Dendrimer-Gold-Nanoparticle Hybrids for Functional Cell Studies
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Self-Assembled Arrays of Dendrimer-Gold-Nanoparticle Hybrids for Functional Cell Studies

机译:自组装的树状聚合物-金纳米颗粒杂种的功能细胞研究阵列。

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摘要

Engineered surfaces with nanoscale features of gold on silicon or glass have recently been used to improve the understanding of adhesion-mediated environmental sensing of cells. Often such surfaces present a cell-binding ligand, such as arginine-glycine-aspartic acid (RGD) peptide motifs, at controlled intramolecular distances on an inert background surface such as polyethylene glycol (PEG). The adhesion mechanism of macromolecular ligands in which direct interaction with cells is nonspecific is not known and the cell response is dictated by the type and the concentration of proteins adsorbed from solution. Dendrimers may increase the availability and multivalency of cell-interacting ligands as a consequence of their branched shape and inherently high concentration of end groups. It is therefore interesting to examine the eventual effect of the macromolecular architecture on the cell viability by the controlled reduction of ligands on a surface. Herein, we demonstrate the fabrication of self-assembled macromolecular hybrid arrays in which the relative position of two anionic macromolecules of different architectures-a carboxy-functionalized dendrimer and a linear polymer-is straightforwardly controlled on a PEG surface. We also show how the interaction of primary human endothelial cells with these surfaces is modulated by the molecular spacing and how protein binding to the macromolecular arrays can be evaluated by using a standard surface plasmon resonance (SPR) technique.
机译:最近,已在硅或玻璃上使用具有金纳米级特征的工程表面来增进对粘附介导的细胞环境感应的理解。这些表面通常在惰性背景表面(例如聚乙二醇(PEG))上以受控的分子内距离呈现出细胞结合配体,例如精氨酸-甘氨酸-天冬氨酸(RGD)肽基序。尚不清楚大分子配体的粘附机制,其中与细胞的直接相互作用是非特异性的,并且细胞反应由溶液中吸附的蛋白质的类型和浓度决定。由于树枝状聚合物的分支形状和端基固有的高浓度,其可以增加与细胞相互作用的配体的利用率和多价。因此,有趣的是通过控制表面配体的还原来检查大分子结构对细胞活力的最终影响。在这里,我们演示了自组装的大分子杂化阵列的制造,其中直接在PEG表面控制不同结构的两个阴离子大分子(羧基官能化的树枝状大分子和线性聚合物)的相对位置。我们还显示了如何通过分子间距调节人类内皮细胞与这些表面的相互作用,以及如何通过使用标准的表面等离子体共振(SPR)技术评估与大分子阵列结合的蛋白质。

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