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Size-Tunable Nanoneedle Arrays for Influencing Stem Cell Morphology, Gene Expression, and Nuclear Membrane Curvature

机译:用于影响干细胞形态,基因表达和核膜曲率的尺寸可调纳尼柱阵列

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摘要

High-aspect-ratio nanostructures have emerged as versatile platforms for intracellular sensing and biomolecule delivery. Here, we present a microfabrication approach in which a combination of reactive ion etching protocols were used to produce high-aspect-ratio, nondegradable silicon nanoneedle arrays with tip diameters that could be finely tuned between 20 and 700 nm. We used these arrays to guide the long-term culture of human mesenchymal stem cells (hMSCs). Notably, we used changes in the nanoneedle tip diameter to control the morphology, nuclear size, and F-actin alignment of interfaced hMSCs and to regulate the expression of nuclear lamina genes, Yes-associated protein (YAP) target genes, and focal adhesion genes. These topography-driven changes were attributed to signaling by Rho-family GTPase pathways, differences in the effective stiffness of the nanoneedle arrays, and the degree of nuclear membrane impingement, with the latter clearly visualized using focused ion beam scanning electron microscopy (FIB-SEM). Our approach to design high-aspect-ratio nanostructures will be broadly applicable to design biomaterials and biomedical devices used for long-term cell stimulation and monitoring.
机译:高纵横比纳米结构已成为细胞内传感和生物分子递送的通用平台。这里,我们介绍了一种微制造方法,其中使用反应离子蚀刻方案的组合用于产生高纵横比,具有尖端直径的高纵横比,其可以精细地调节20至700nm。我们使用这些阵列引导人间充质干细胞的长期培养(HMSC)。值得注意的是,我们使用纳尼孔尖端的变化来控制界面HMSCs的形态,核大小和F-肌动蛋白对准,并调节核椎板基因的表达,核薄膜基因,是相关蛋白(YAP)靶基因和局灶性粘附基因的表达。这些地形驱动的变化归因于rho-family GTPase途径的信号传导,纳尼罩阵列的有效刚度的差异以及核膜冲击的程度,后者使用聚焦离子束扫描电子显微镜清晰可视化(FIB-SEM )。我们设计高纵横比纳米结构的方法将广义适用于设计生物材料和用于长期细胞刺激和监测的生物医学装置。

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