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Adhesion Assays of Endothelial Cells on Nanopatterned Surfaces within a Microfluidic Channel

机译:微流控通道内纳米图案表面上内皮细胞的粘附测定。

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We present a simple analytical method to measure adhesion of human umbilical vein endothelial cells (HUVECs) and calf pulmonary artery endothelial cells (CPAEs) using nanopatterned, biodegradable poly(lactic-co-glycolic acid) (PLGA) surfaces for potential applications to artificial tissue-engineered blood vessel. Various nanostructured PLGA surfaces (350 nm wide ridges/350 nm grooves, 350 nm ridges/700 nm grooves, 350 nm ridges/1750 nm grooves, 700 nm ridges/350 nm grooves, 1050 nm ridges/350 nm grooves, 1750 nm ridges/350 nm grooves) and flat (unpatterned) surfaces were fabricated on the bottom of polydimethylsiloxane (PDMS) microfluidic channel of 2 mm width and 60 (mu)m height by using thermal imprinting and irreversible channel bonding. To measure adhesion strength of HUVECs and CPAEs, the cells were exposed to a range of shear stress (12, 40, and 80 dyn/cm~(2)) within the channels for 20 min after a preculture for 3 days and the remaining cells were counted under each condition. The highest adhesion strength was found on the surface of 700 nm wide ridges, 350 nm wide grooves for both cell types. The enhanced adhesion on nanopatterned surfaces can be attributed to two aspects: (i) contact guidance along the line direction and (ii) clustered focal adhesions. In particular, the contact guidance induced cell alignment along the line directions, which in turn lowers wall shear stress applied to the cell surface, as supported by a simple hydrodynamic model based on cell morphology.
机译:我们提出了一种简单的分析方法,用于测量人脐静脉内皮细胞(HUVECs)和小腿肺动脉内皮细胞(CPAEs)的粘附力,使用纳米图案化的可生物降解的聚乳酸-乙醇酸(PLGA)表面,可应用于人造组织工程血管。各种纳米结构的PLGA表面(350 nm宽脊/ 350 nm沟槽,350 nm脊/ 700 nm沟槽,350 nm脊/ 1750 nm沟槽,700 nm脊/ 350 nm沟槽,1050 nm脊/ 350 nm沟槽,1750 nm脊/通过使用热压印和不可逆的通道粘接,在宽度为2 mm,高度为60μm的聚二甲基硅氧烷(PDMS)微流体通道的底部制作了350 nm的凹槽和平坦(无图案)的表面。为了测量HUVEC和CPAE的粘附强度,将细胞在预培养3天后暴露于通道内一系列剪切应力(12、40和80 dyn / cm〜(2))下20分钟。在每种情况下都被计数。对于两种电池类型,在700 nm宽的脊和350 nm宽的凹槽表面均发现了最高的粘合强度。纳米图案表面上增强的附着力可归因于两个方面:(i)沿线方向的接触引导和(ii)聚集的局部附着力。特别地,接触引导引起沿线方向的细胞排列,这又降低了施加到细胞表面的壁切应力,这由基于细胞形态的简单流体力学模型所支持。

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