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DNA orientation-specific adhesion and patterning of living mammalian cells on self-assembled DNA monolayers

机译:自组装DNA单层上活哺乳动物细胞的DNA方向特异性粘附和模式

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To better understand cell behaviors on substrates, the precise control of density and orientation of cell-specific ligands remains a great challenge. In this study, we established an easy-to-use approach to manipulate the adhesion and patterning of mammalian cells on gold substrates. We prepared DNA self-assembled monolayers (DNA-SAMs) on gold substrates and found that the sequence-specific orientation of DNA-SAMs played an important role in modulating cell adhesion. We also found that the DNA-SAMs on gold substrates could be used as a potentially universal cell culture substrate, which showed properties similar to cationic polymers (e.g. poly-L lysine, PLL) substrates. Furthermore, we could manipulate cell adhesion by tuning the length of poly adenine (polyA) in the DNA sequence. We also prepared a DNA aptamer-based SAM to regulate cell adhesion by exploiting stimuli-responsive conformational change of the aptamer. By using the well-established DNA spotting technology, we patterned cells on DNA-SAMs to form a spot matrix and four English letters “CELL”. Our findings suggest that DNA-SAMs on gold substrates are potentially useful for making smart surfaces for cell studies, thus introducing a new platform for cell/tissue engineering research.
机译:为了更好地了解底物上的细胞行为,精确控制细胞特异性配体的密度和方向仍然是一个巨大的挑战。在这项研究中,我们建立了一种易于使用的方法来操纵金表面上的哺乳动物细胞的粘附和图案。我们在金底物上制备了DNA自组装单分子层(DNA-SAMs),发现DNA-SAMs的序列特异性方向在调节细胞粘附中起着重要作用。我们还发现,金底物上的DNA-SAMs可用作潜在的通用细胞培养底物,其显示出与阳离子聚合物(例如 poly- L 赖氨酸, PLL)基板。此外,我们可以通过调节DNA序列中聚腺嘌呤(polyA)的长度来操纵细胞粘附。我们还准备了一个基于DNA适体的SAM,通过利用适体的刺激响应构象变化来调节细胞粘附。通过使用成熟的DNA点样技术,我们在DNA-SAMs上对细胞进行了构图,形成了点样矩阵和四个英文字母“ CELL”。我们的发现表明,金底物上的DNA-SAMs可能对制造用于细胞研究的智能表面很有用,从而为细胞/组织工程研究引入了新的平台。

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