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首页> 外文期刊>Biomacromolecules >Porous Silicon-Based Cell Microarrays: Optimizing Human Endothelial Cell-Material Surface Interactions and Bioactive Release
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Porous Silicon-Based Cell Microarrays: Optimizing Human Endothelial Cell-Material Surface Interactions and Bioactive Release

机译:多孔硅基细胞微阵列:优化人内皮细胞-材料表面相互作用和生物活性释放。

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Porous silicon (pSi) substrates are a promising platform for cell expansion, since pore size and chemistry can be tuned to control cell behavior. In addition, a variety of bioactives can be loaded into the pores and subsequently released to act on cells adherent to the substrate. Here, we construct a cell microarray on a plasma polymer coated pSi substrate that enables the simultaneous culture of human endothelial cells on printed immobilized protein factors, while a second soluble growth factor is released from the same substrate. This allows three elements of candidate pSi scaffold materials-topography, surface functionalization, and controlled factor release-to be assessed simultaneously in high throughput. We show that protein conjugation within printed microarray spots is more uniform on the pSi substrate than on flat glass or silicon surfaces. Active growth factors are released from the pSi surface over a period of several days. Using an endothelial progenitor cell line, we investigate changes in cell behavior in response to the microenvironment. This platform facilitates the design of advanced functional biomaterials, including scaffolds, and carriers for regenerative medicine and cell therapy.
机译:多孔硅(pSi)衬底是用于细胞扩增的有前途的平台,因为可以调整孔径和化学性质来控制细胞行为。另外,可以将各种生物活性物质加载到孔中,然后释放以作用于粘附在基质上的细胞。在这里,我们在涂有等离子聚合物的pSi底物上构建了一个细胞微阵列,该底物使人内皮细胞能够在印刷的固定蛋白因子上同时培养,而第二种可溶性生长因子则从同一底物上释放出来。这允许在高通量的同时评估候选pSi支架材料的三个要素-形貌,表面功能化和受控因子释放。我们表明,在印制的微阵列点内的蛋白质结合在pSi基板上比在平板玻璃或硅表面上更为均匀。活性生长因子会在几天内从pSi表面释放出来。使用内皮祖细胞系,我们调查响应微环境的细胞行为的变化。该平台促进了先进功能性生物材料的设计,包括支架以及用于再生医学和细胞治疗的载体。

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